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AU2006336091A1 - Method and markers for the diagnosis of renal diseases - Google Patents

Method and markers for the diagnosis of renal diseases Download PDF

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AU2006336091A1
AU2006336091A1 AU2006336091A AU2006336091A AU2006336091A1 AU 2006336091 A1 AU2006336091 A1 AU 2006336091A1 AU 2006336091 A AU2006336091 A AU 2006336091A AU 2006336091 A AU2006336091 A AU 2006336091A AU 2006336091 A1 AU2006336091 A1 AU 2006336091A1
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nephropathy
neg
diabetes
marker
polypeptide
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Thorsten Kaiser
Harald Mischak
Michael Walden
Stefan Wittke
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Mosaiques Diagnostics and Therapeutics AG
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    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N33/00Investigating or analysing materials by specific methods not covered by groups G01N1/00 - G01N31/00
    • G01N33/48Biological material, e.g. blood, urine; Haemocytometers
    • G01N33/50Chemical analysis of biological material, e.g. blood, urine; Testing involving biospecific ligand binding methods; Immunological testing
    • G01N33/68Chemical analysis of biological material, e.g. blood, urine; Testing involving biospecific ligand binding methods; Immunological testing involving proteins, peptides or amino acids
    • G01N33/6893Chemical analysis of biological material, e.g. blood, urine; Testing involving biospecific ligand binding methods; Immunological testing involving proteins, peptides or amino acids related to diseases not provided for elsewhere

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Description

WO 2007/082586 PCT/EP2006/050327 -1 5 Method and markers for the diagnosis of renal diseases The present invention relates to the diagnosis, particularly differential diagnosis, of renal diseases. 10 The number of patients presenting with renal diseases has been increasing in the recent years. Thus, renal diseases present an increasing problem to the health system. Many renal diseases are irreversible, therefore an early diagnosis and/or a differential diagnosis of renal diseases is important. Early diagnosis and a therapy precisely tailored to each 15 particular disease could reduce the number of patients requiring dialysis and could also reduce the high cardiovascular risk of the patients. Currently, precise diagnosis and/or differential diagnosis relies mostly on kidney biopsies. Although biopsies serve as the current "gold standard" in renal diagnostics, biopsies have 20 the disadvantage of being invasive and therefore being conducted only on selected patients. Urine analysis is a different approach to diagnose renal diseases. However, currently only few parameters of urine are routinely measured, for example creatinin, urea, albumin, blood cells (such as leukocytes and erythrocytes), bacteria, sugar, urobilinogen, bilirubin 25 and pH value. The diagnostic value of these analyses is limited, as they lack sufficient sensitivity and/or selectivity, particularly for differential diagnosis. Several attempts have been made to analyze the proteins contained in urine. 30 V. Thongboonkerd et al. have used two-dimensional polyacrylamide gel electrophoresis (2D-PAGE) in combination with matrix-assisted laser desorption ionization-time-of-flight (MALDI-TOF) mass spectrometry followed by mass fingerprinting to investigate normal human urinary proteins. A total of 67 protein forms of 47 unique proteins was identified (V. Thongboonkerd et al. (2001). Proteomic analysis of normal human urinary proteins WO 2007/082586 PCT/EP2006/050327 -2 isolated by acetone precipitation or ultracentrifuigation. Kidney International, vol. 62, p. 1461-1469). C.S. Spahr et al. have digested the proteins contained in urine samples with trypsin and 5 identified 751 peptides from 124 proteins by means of liquid chromatography-tandem mass spectrometry (C.S. Spahr et al. (2001). Towards defining the urinary proteome using liquid chromatography-tandem mass spectrometry. I. Profiling an unfractionated tryptic digest. Proteomics vol. 1, p. 93-107). 10 These studies relate only to healthy individuals. The studies have not addressed the question whether alterations in presence of urinary polypeptides can be used for diagnosis or differential diagnosis of renal diseases. It has been proposed to use the presence or absence of polypeptides in urine for the 15 diagnosis of membranous glomerulonephritis (MGN) (von Neuhoff et al. (2004). Mass Spectrometry for the Detection of Differentially Expressed Proteins: A Comparison of Surface-Enhanced Laser Desorption/Ionization and Capillary Electrophoresis/Mass Spectrometry. Rapid Communications in Mass Spectrometry, vol. 18: 149-156). However, samples of only 8 patients were used in the study, which was mainly concerned with the 20 comparison of different analysis methods. The actual diagnostic value of the markers has remained unclear. Consequently, there is need for a fast and simple methods and means for diagnosis, particularly differential diagnosis, of renal diseases. 25 Accordingly, the object the present invention is to provide methods and means for the diagnosis of renal diseases, particularly for differential diagnosis of renal diseases. It is an particular object of the present invention to provide methods and means for the diagnosis and/or differential diagnosis of IgA-nephropathy, which is the most common 30 glomerulopathy. According to a first aspect of the present invention, the problem is solved by the use of the presence of at least one polypeptide marker in a urine sample for the diagnosis, preferably the differential diagnosis, of a renal disease, wherein the polypeptide marker is selected 35 from the group of polypeptide markers as shown in table 1 to 22.
WO 2007/082586 PCT/EP2006/050327 -3 In the context of the present invention, it has been found that with the help of the polypeptide markers as shown in table 1 to 22 it is possible to reliably diagnose or differentially diagnose, respectively, different renal diseases. 5 The present invention has numerous advantages compared to the state of the art. First, the presence of the polypeptide markers according to the invention can be determined in urine samples. Therefore, there is no need to take biopsies. Thus, the present invention allows a simplified and fast diagnosis of renal diseases, allowing to screen patients regularly for the presence of renal diseases and to diagnose renal diseases at early stages. Furthermore, the 10 polypeptide markers according to the invention can be used for differential diagnosis between different renal diseases. The high number of markers identified according to the present invention allows to increase both specificity and sensitivity of diagnosis as compared to the use of only a single or a small number of markers. Also, the present invention provides methods which allow to measure said polypeptide markes without the 15 use of specific ligands such as antibodies or aptamers. The polypeptide markers as shown in the tables have been identified by a method named capillary electrophoresis-mass spectrometry (CE-MS), which will be described further below. Furthermore, the method has been described in detail in von Neuhoff et al. (2004) 20 (Mass Spectrometry for the Detection of Differentially Expressed Proteins: A Comparison of Surface-Enhanced Laser Desorption/Ionization and Capillary Electrophoresis/Mass Spectrometry. Rapid Communications in Mass Spectrometry, vol. 18: 149-156). Starting from the parameters defining the polypeptide markers, it is possible by methods known in the art to identify the sequence of the corresponding polypeptides and then to synthesize or 25 produce the corresponding polypeptides, e.g. with the help of protein synthesis or expression of the corresponding gene in appropriate cells. The markers are defined by there mass and their migration time in capillary electrophoresis (CE), particularly mass and their migration time obtained according to Example 1. It is 30 known that CE migration times can vary, typically in the range of 5 min, more typically in the range of 3 minutes. However, the sequence of markers being eluted is typically the same or very similar for each CE system applied. The system can be calibrated by use of polypeptides which are present in almost any urine sample, e.g. by the polypeptides given in tables 23 or 24. Furthermore, the polypeptides given in SEQ ID NO: 1 to SEQ ID NO: 5 35 can serve for calibration.
WO 2007/082586 PCT/EP2006/050327 -4 Variation of the masses between measurements or between different mass spectrometers is relatively small, typically it is in the range of plus or minus 0.05%. In table 1, polypeptide markers are listed which are preferred for the discrimination 5 between healthy individuals and individuals suffering from a renal disease, particularly from a glomerulonephritis or glomerulopathy. In table 2, polypeptide markers are listed, which are preferred for a discrimination between FSGS and the healthy condition. 10 In table 3, polypeptide markers are listed, which can be used for differential diagnosis between FSGS and MCD. In table 4, polypeptide markers are listed, which are preferred for a differential diagnosis of 15 FSGS and MGN. In table 5, polypeptide markers are listed, which are preferred for a differential diagnosis between FSGS on the one hand, and MCD or MGN on the other hand. 20 In table 6, polypeptide markers are listed, which are preferred for diagnosis of MCD as compared to the healthy condition. In table 7, polypeptide markers are listed, which are preferred for differential diagnosis between MCD and MGN. 25 In table 8, polypeptide markers are listed, which are preferred for differential diagnosis between MCD on the one hand, and FSGS or MGN on the other hand. In table 9, polypeptide markers are listed, which are preferred for diagnosis of MGN as 30 compared to the healthy condition. In table 10, polypeptide markers are listed, which are preferred for differential diagnosis between MGN on the one hand, and FSGS or MCD on the other hand. 35 In table 11, polypeptide markers are listed, which are preferred for diagnosis of IgA nephropathy or MGN on the one hand as compared to the healthy condition.
WO 2007/082586 PCT/EP2006/050327 -5 In table 12, polypeptide markers are listed, which are preferred for diagnosis of IgA nephropathy as compared to the healthy condition. In table 13, polypeptide markers are listed, which are preferred for differential diagnosis 5 between IgA-nephropathy and MGN. In table 14, polypeptides are listed with their respective frequency in healthy, FSGS, MCD, and MGN patients. 10 In table 15, polypeptides are listed which have been used for differential diagnosis between healthy individuals and renal patients using support vector machines according to Example 1. In table 16, polypeptides are listed which have been used for differential diagnosis between 15 healthy, FSGS, MCD, and MGN patients using random forest analysis according to Example 1. In table 17, polypeptides are listed which have been used for differential diagnosis between MCD and MGN patients using using support vector machines according to Example 1. 20 In table 18, polypeptides are listed which have been used for differential diagnosis between MCD and FSGS patients using using support vector machines according to Example 1. In table 19, polypeptides are listed which have been used for differential diagnosis between 25 MGN and FSGS patients using using support vector machines according to Example 1. In table 20 and 21, polypeptides are listed which have been identified in von Neuhoff et al. (2004), which has been cited above. 30 In table 22, polypeptides are listed which can be used for diagnosis of diabetes and/or diabetic nephropathy. In table 23, polypeptides are listed, which are preferred as internal standards to standardize the CE-time. 35 WO 2007/082586 PCT/EP2006/050327 -6 In table 24, polypeptides are listed, which are preferred as internal standards to standardize the CE-time if the pressure method (0.3 to 1 psi) according to Example 1 is used. These standards are e.g. preferred as internal standards in diagnosis of IgA-nephropathy. 5 In table 25, clinical data of renal patients are listed whose samples were used for identification of polypeptide markers according to Example 1. Abbreviations: CsA, Cyclosporin A; PS , prednisolone; +, frequent relapse; -, currently no immunosuppression; *, clinically unclear whether MCD or FSGS. 10 The polypeptide markers used according to the present invention can be identified and their presence can be measured in urine samples. Urine samples can be taken as known in the state of the art. Preferably, midstream urine is used in the context of the present invention. 15 The polypeptide markers used according to the present invention can be gene expression products such as proteins, peptides, and fragments or other degradation products of proteins or peptides. They can be modified by posttranslational modifications, e.g. by glycosylation, phoshorylation, alkylation or disulfide bond. It is known that fragments and degradation products can have a different diagnostic value and/or physiological role than 20 the protein or peptide they have been derived from. For example, in different diseases, different proteolytic degradation products or fragments can be found. It is also considered to be within the scope of the present invention if the urine sample is pretreated to chemically modify the polypeptide markers contained in the urine and to measure these chemically modified polypeptide markers. The polypeptide markers according to the 25 present invention have a molecular mass between 400 and 20 000 Da, particularly between 700 and 14000 Da, more particularly between 800 and 11000 Da. Preferred polypeptide markers according to the present invention are listed in tables 1 to 22, particularly in tables 1 to 21, more particularly in tables 1 to 13. 30 Preferred polypeptides for use as internal standards are listed in tables 23 to 24. Preferred are also polypeptide markers which are listed in table I, but not in table 14 and/or 15 andor 16 and/or 17 and/or 18 and/or 19 and/or 20 and/or 21 and/or 22. Preferred are also polypeptide markers which are listed in table 2, but not in table 14 and/or 15 and/or 16 and/or 18. 35 Preferred are also polypeptide markers which are listed in table 3, but not in table 14 and/or 16 and/or 18.
WO 2007/082586 PCT/EP2006/050327 -7 Preferred are also polypeptide markers which are listed in table 4, but not in table 14 and/or 16 and/or 19. Preferred are also polypeptide markers which are listed in table 5, but not in table 14 and/or 16 and/or 18 and/or 19. 5 Preferred are also polypeptide markers which are listed in table 6, but not in table 14 and/or 16. Preferred are also polypeptide markers which are listed in table 7, but not in table 14 and/or 16 and/or 17. Preferred are also polypeptide markers which are listed in table 8, but not in table 14 10 and/or 16. Preferred are also polypeptide markers which are listed in table 9, but not in table 14 and/or 16 and/or 20 and/or 21. Preferred are also polypeptide markers which are listed in table 10, but not in table 14 and/or 16. 15 Preferred are also polypeptide markers which are listed in table 11, but not in table 14 and/or 16. Renal disease according to the present invention relates to any kind of renal disease or kidney dysfunction known to the person skilled in the art, for example IgA-nephropathy, 20 MGN (membranous glomerulonephritis), MCD (minimal-change disease), FSGS (focal segmental glomerulosclerosis), or diabetic nephropathy. Particularly, renal disease relates to a glomerulopathy such as IgA-nephropathy, MGN, MCD, or FSGS. Even more particularly renal disease relates to IgA-nephropathy, MCD, or FSGS. Most particularly, renal disease relates to IgA-nephropathy 25 The glomerulopathies are a subgroup of renal diseases. Glomerulopathies comprise a several diseases of different etiology. Glomerulopathies are characterized by pathomorphological changes in malpighian corpuscles, glomerulus, and Bowman's capsule. As a consequence of these changes, further pathomorphological changes may 30 appear in other parts of the nephron and interstice. IgA-nephropathy is also known as Berger-Nephritis. IgA-nephropathy is the most common glomerulopathy. It may be a specific, kidney-limited, form of purpura Schoenlein-Henoch (also known as anaphylactoid purpura) with increased plasma concentration of IgA. The 35 histopathology includes all forms of glomerular lesions and deposits of IgA in the mesangium. Clinically, IgA nephropathy presents as micro- and macro-hematouria. Therapy may be attempted with ACE inhibitors and omega-3 fatty acids. Progression of WO 2007/082586 PCT/EP2006/050327 -8 the disease occurs over the course of several years and includes transition into progressive renal insufficiency. MGN is characterized by thickening of the basal membrane and granular subepithelial IgG s deposits. MGN becomes frequently manifest in the between the age of 40 and 50. It is frequently caused by medicaments, e.g. gold, D-penicillamine, or ACE inhibitors. Therapy of MGN may be attempted with glucocorticoids or cyclophosphamide. MGN is a nephrotic syndrome, a transition into progressive renal insufficiency may take several years. 10 MCD is also known as lipoid nephrosis. MCD is the most common cause of a nephrotic syndrome in children. The etiology of the disease is unknown. Histologically, no or only very discrete changes can be found. Therapy of MCD may include treatment with glucocorticoids, cyclosporin A, or cyclophosphamide. In children, the disease spontaneously heals in 90% of the cases, in adults in 50% of the cases. A transition into 15 FSGS is possible. FSGS is also known as IgM-nephropathy. FSGS is typically characterized by deposits of IgM and C3 in the mesangium. Clinically, it becomes manifest as a nephrotic syndrome. Therapy of FSGS may include treatment with glucocorticoids, cyclosporin A, or 20 cyclophosphamide. Prognosis is poor and includes transition into progressive renal insufficiency. Diabetic nephropathy is also known as diabetic glomerulosclerosis. Diabetic nephropathy is the most common cause for requirement of dialysis treatment. 25 In summary, it is evident that renal diseases include a variety of diseases which may show quite similar histology. However, etiology, treatment, and prognosis can be quite different for each disease. For example, IgA-nephropathy requires different treatment from any other glomerulopathy described above: In IgA-nephropathy, treatment with ACE inhibitors 30 may be attempted, which would not be recommendable in the case of MGN. Therefore, fast and reliable diagnosis is of great importance for treatment. In the context of the present invention, diagnosing or diagnosis means that, for an individual patient, the probability of having the respective disease is determined. 35 Diagnosis may also include confirming a preliminary diagnosis, particularly a preliminary diagnosis established by a different method.
WO 2007/082586 PCT/EP2006/050327 -9 Furthermore, in a preferred embodiment, diagnosis according to the present invention particularly relates to "differential diagnosis". The term "differential diagnosis" relates to distinguishing between two different diseases, i.e. to determining for an individual patient 5 the probability of having a certain first disease as compared to having a certain second disease. More particularly, differential diagnosis according to the present invention relates to distinguishing between at least two renal diseases chosen from the group consisting of IgA-nephropathy, MGN, MCD, FSGS, and diabetic nephropathy. 10 In another embodiment, the present invention relates to a method for the differential diagnosis of a renal disease, the method comprising: a) measuring the presence or the absence of a polypeptide marker in a urine sample, wherein the polypeptide marker is selected from the group of 15 polypeptide markers shown in table 1 to 22, and b) comparing the probability of the presence of this marker in a disease patient to the probability of the presence of this marker in a control patient, wherein 20 cl) if the probability of the presence of this marker in a disease patient is higher than the probability of the presence of this marker in a control patient, the presence of this marker is indicative for a higher probability of having the disease rather than the control condition, or 25 c2) if the probability of the presence of this marker in a disease patient is lower than the probability of the presence of this marker in a control patient, the absence of the marker is indicative for a higher probability of having the disease rather than the control condition. 30 Preferably, the individual probabilities according to step b) are as indicated in the tables. The term "measuring" according to the present invention relates to determining the presence of a polypeptide or other substance of interest. 35 The decision whether a polypeptide marker is present or absent may depend on definition of a suitable threshold value. The threshold value can either be defined through the sensitivity of the method of measurement, or it can be defined at will. The threshold in the WO 2007/082586 PCT/EP2006/050327 -10 context of the present invention is 25 fmol/pl in a sample which has been injected into a mass spectrometer according to Example 1. However, this threshold may be the same when other methods are used. This threshold coincides with the detection threshold of a typical mass spectrometer. This threshold corresponds approximately to a concentration of 5 the polypeptide marker in the urine sample of 50-5000 pmol/1. If different thresholds are to be used (e.g. when using another detection method), the corresponding probabilities may differ, but can easily be established by the person skilled in the art. The "disease patient" according to the present invention is suffering from a renal disease. 10 Particularly, the disease is at least one from the group consisting of IgA-nephropathy, MGN, MCD, FSGS, and diabetic nephropathy. The "control patient" can either be healthy or suffering from a disease different from the one the disease patient is suffering from, i.e. the control patient can either represent the 15 healthy condition or a disease or group of diseases. Particularly, the represented disease is at least one from the group consisting of IgA-nephropathy, MGN, MCD, FSGS, and diabetic nephropathy. Tables 1 to 14, 16, 20, 21, and 22 list the probability (also designated as "frequency") of a 20 given polypeptide marker being present in a urine sample of a healthy control patient or a control patient suffering from a certain disease. The discrimination factor indicates the difference between the probability of presence in the disease as compared to a given control condition. The discrimination factor can easily be calculated from the respective probabilities. The higher the discrimination factor, the better is the potential of the given 25 marker to distinguish between the disease and the control condition. An absolute value of the discrimination factor of 0.40 or higher is preferred. The person skilled in the art is able to establish similar tables for the polypeptide markers by himself and/or to refine the data contained in the tables, e.g. based on further patient 30 data and/or according to different thresholds for the presence of the polypeptide marker. For diagnosis, the probability of the presence of the polypeptide marker in a disease patient is compared to the probability of the presence of this marker in a control patient, wherein the individual probabilities are as indicated in the tables. If the probability of the presence 35 of this marker in a disease patient is higher than the probability of the presence of this marker in a control patient, then the presence of this marker in the sample is indicative that the patient from whom the sample originates has a higher probability of having the disease WO 2007/082586 PCT/EP2006/050327 -11 rather than the control condition. If the probability of the presence of this marker in a disease patient is lower than the probability of the presence of this marker in a control patient, then the absence of this marker in the sample is indicative that the patient from whom the sample originates has a higher probability of having the disease rather than the 5 control condition. For example, a given marker may have a probability of 73% of being present in a control representing IgA-nephropathy but a probability of 0% of being present in a control representing the healthy condition. If this marker is present in the sample, then the 10 individual is diagnosed as having a 73% probability of suffering from IgA-nephropathy as compared to being healthy. If this marker is not present in the sample, then the individual is diagnosed as having a 73% probability of being healthy instead of suffering from IgA nephropathy. 15 Thus, diagnosis can be established according to statistical methods familiar to the person skilled in the art. The invention can be carried out using only one of the polypeptide markers or using a plurality of the polypeptide markers. Preferably, presence of a plurality of polypeptide 20 markers is measured. Preferably at least 3 of the markers, more preferably at least 10 of the markers, even more preferably at least 20, most preferred at least 50 of the markers according to the present invention are measured. An advantage of the present invention is that it provides a multitude of suitable markers. 25 Measuring a plurality of markes can increase both sensitivity and selectivity of diagnosis. Therefore, also markers which show low discrimination factors between the disease and control can be used for diagnosis if they are combined with other markers. If a plurality of polypeptide markers is used, a "pattern" is be generated which contains the 30 information about the presence for each marker measured. This pattern can then be compared to the pattern of probabilities of presence of the polypeptide markers in a disease or control patient. Each table represents a pattern of probabilities of finding given polypeptide markers in certain disease and control patients. 35 Therefore, in a preferred embodiment, the present invention relates to a method for the differential diagnosis of a renal disease, the method comprising: WO 2007/082586 PCT/EP2006/050327 -12 a) establishing a pattern of presence or absence for a plurality of polypeptide markers in a urine sample, wherein at least one polypeptide marker is selected from the group of polypeptide markers shown in table 1 to 22, and 5 b) comparing the probability of finding this pattern in a disease patient to the probability of finding this pattern in a control patient, wherein cl) if the probability of finding the pattern in a disease patient is higher than the probability of the finding the pattern in a control patient, finding this pattern is 10 indicative for a higher probability of having the disease rather than the control condition, or c2) if the probability of finding the pattern in a disease patient is lower than the probability of the finding the pattern in a control patient, finding this pattern is 15 indicative for a lower probability of having the disease rather than the control condition, or Preferably, the individual probability for the at least one polypeptide marker according to step b) is as indicated in the tables. 20 Comparison of the found pattern with the probability of finding the pattern in a disease or control patient can be performed according to statistical methods known in the art. Preferably, automated methods are employed, e.g. CART-analysis, random forest analysis, and support vector machines (SVM, see e.g. Xiong. M., et al. (2001). Biomarker 25 identification by feature wrappers. Genome Research vol. 11, p. 1878-1887). Comparison can also be performed simultaneously for several different patterns and the probability of finding them. Thus, the measured pattern is typically compared to the probability of finding the pattern in 30 at least two different conditions. An example for diagnosis and differential diagnosis of renal diseases according to this method is shown in Fig. 3. If necessary, the urine samples may be pre-treated before measurement of the polypeptide marker. Particularly, lipids, nucleic acids or polypeptides may be purified from the sample 35 according to methods known in the art, including filtration, centrifugation, or extraction methods such as chloroform/phenol extraction.
WO 2007/082586 PCT/EP2006/050327 - 13 Measuring the presence of a polypeptide marker can be done by any method known in the art. Preferred methods include gas phase ion spectrometry, such as laser desorption/ionization 5 mass spectrometry, surface enhanced laser desorption/ionization time-of flight mass spectrometry (SELDI-TOF MS) and CE-MS. These spectrometry methods allow to measure the polypeptide markers without the need for ligands such as antibodies or aptamers. 10 Urine sample generally are highly complex, i.e. they contain numerous polypeptides. In case of high complexity, a spectrometric analysis becomes difficult. To reduce the complexity of the sample, the polypeptides contained in the sample may be separated by any suitable means, e.g. by electrophoretic separation, affinity-based separation, or separation based on ion exchange chromatography. Particular examples include gel 15 electrophoresis, two-dimensional polyacrylamide gel electrophoresis (2D-PAGE), capillary electrophoresis, metal-affinity chromatography, immobilized metal-affinity chromatography (IMAC), affinity chromatography based on lectins, liquid chromatography, high pressure liquid chromatography (HPLC), and reversed-phase HPLC, cation exchange chromatography, and selectively binding surfaces (such as the surfaces 20 used in SELDI-TOF, see below). 2D-PAGE is commonly used for polypeptide separation and can be combined with mass spectrometry (MS) yielding identification of individual polypeptides. Over 1000 protein spots can be discerned with 2D-PAGE. However, each single spot must be analysed 25 separately by MS/MS for identification. SELDI (surface enhanced laser desorption/ionization) time-of-flight mass spectrometry is currently applied in many fields of biomedical sciences. 30 In the SELDI system, the ProteinChip Arrays are the most important component. They are narrow metal strips carrying 8 or 16 spots in a row on the surface. Samples to be analyzed are directly applied to the spots, either as a standing drop or in volumes up to 500 pl, by using sample holders called "bioprocessors" as supporting units. They are placed onto the arrays during incubation and washing steps and removed again afterwards. The different 35 types of arrays belong to two main series: chromatographic arrays, presenting hydrophobic, hydrophilic, cation-exchanging, anion- exchanging or immobilized metal ion WO 2007/082586 PCT/EP2006/050327 -14 affinity-surfaces, and preactivated arrays with chemical groups to allow the covalent coupling of proteins. Preferably, a chip with cation-exchange surfaces is used. As the ProteinChip Arrays do not only support the sample but specifically interact with the biomolecules, the composition of the analyte depends on the array type used and the 5 washing conditions applied. This explains why the SELDI-process can be defined as a further development of the traditional MALDI (matrix assisted laser desorption / ionization)-technique. In the SELDI-process, only on those polypeptides are measured that actually bind to the chip surface. 10 After binding of sample proteins, the energy absorbing matrix is applied to each spot. The matrix rapidly crystallizes and the analysis can start immediately. The ProteinChip Arrays are placed into the ProteinChip Reader for analysis. The reader is a TOF (time-of-flight) mass spectrometer in which the proteins are desorbed and ionized 15 with the help of a laser beam. As the crystallized proteins are equally distributed on the spot surface, the ionizing laser beam always hits a representative average of the molecules in the analyte, allowing quantitative calculations. After ionization, the proteins are accelerated by an electric field to fly down the flight tube, before reaching the detector. The flight time between the laser striking the array surface and the molecules reaching the 20 detector at the end of the flight tube enables the system to accurately determine the mass of the protein species present in the sample (for more detailed information on the method see the following review: Merchant M and Weinberger SR (2000). Recent advancements in surface-enhanced laser desorption / ionization - time of flight mass spectrometry. Electrophoresis vol. 212, p. 1164-1177). 25 However, the most preferred method is CE-MS, in which capillary electrophoresis (CE) is coupled to mass spectrometry (MS). CE-MS has been described in detail elsewhere (see e.g. German patent application DE 100 21 737, and Kaiser, T., et al., Capillary Electrophoresis coupled mass spectrometry to establish polypeptide patterns in dialysis 30 fluids. J Chromatogr A, vol. 1013, p. 157-171(2003)).
WO 2007/082586 PCT/EP2006/050327 - 15 CE is known to the person skilled in the art. In brief, the sample is loaded onto an electrophoresis capillary and a voltage of up to 50 kV, typically up to 30 kV, is applied. Typical capillaries are fused silica capillaries, i.e. glas capillaries comprising an outer sheath as mechanical support and to improve mechanical flexibility, e.g. a sheath made of 5 thermoplastic material. Typically, the capillary is untreated, i.e. it shows hydroxy-groups on its inside. However, the capillary may also be coated on the inside. E.g., hydrophobic coating can be used to improve discriminatory power. In addition to the voltage, also pressure may be applied, which is typically in the range of 0 to 1 psi. The pressure can also be applied or increased 'during the run. 10 To improve discriminatory power, also a stacking protocol can be applied when loading the sample: Before loading of the sample, a base is loaded, then the sample is loaded, then an acid. The principle is to capture the analyte ions between a base and an acid. If voltage is applied, the positively charges analyte ions move towards the base. There, they get 15 negatively charged and move into the opposite direction towards the acid, where they get positively charged. This stacking repeats itself until acid and base are neutralized. Then, the separation starts from a well concentrated sample. The sample is contained in an appropriate buffer in which polypeptides are soluble, e.g. 20 phosphate buffer. For CE-MS coupling, it is preferred to use volatile solvents and to work under mostly salt-free conditions to avoid contamination of the MS. Examples comprise acetonitrile, isopropanol, methanol, and the like. The solvents can also be combined with water and a weak acid (e.g. 0.1% formic acid), the latter to protonate the analyte. The polypeptides in the sample are separated according to size and charge, which determine the 25 run-time in the capillary. CE is characterized by high separating power and short time of analysis. For subsequent MS analysis, either fractions collected from the CE can be analyzed as separate batches or, preferably, the CE system can be coupled via a suitable interface to the 30 mass spectrometer to allow continous flow analysis. Alternatively, the flow from the CE may be used to generate continuous "separation tracks", which can be analyzed separately.
WO 2007/082586 PCT/EP2006/050327 -16 In the mass spectrometer, ions generated from the sample are analyzed according to the mass/charge (m/z) quotient. Using mass spectrometry, it is possible to routinely analyze 10 fmol (i.e. 0.1. ng of a 10 kDa polypeptide) with a precision of ± 0.01%. Experimentally, it is possible to analyze even less than 0.1 fmol. 5 Any type of mass spectrometer can be used. In mass spectrometers, an ion-generating device is coupled with an suitable analyzer. For example, the electrospray ionization (ESI) interfaces are most commonly used to produce ions from liquid samples, whereas MALDI is most commonly used to produce ions from individually processed samples. Different 10 kinds of analyzers are available, e.g. ion trap analyzers or time-of-flight (TOF) analyzers. Both ESI and MALDI can be combined with essentially all types of mass spectrometers, although ESI has usually been combined with ion traps, whereas MALDI has usually been combined with TOF. 15 A preferred CE-MS method according to the present invention includes capillary electrophoresis coupled online via ESI to a TOF analyzer. The CE-MS technique permits to measure the presence of several hundred polypeptide markers simultaneously in a short time in a small volume with high sensitivity. Once the 20 presence of the polypeptide markers has been measured, a pattern of the measured polypeptide markers is generated and can be compared to a disease pattern by any of the methods described further above. However, in many cases it will be sufficient for diagnosis to measure only one or a limited number of the markers. 25 The polypeptide sequences can be determined according to methods well-known to the person skilled in the art (see e.g. C.S. Spahr et al. (2001). Towards defining the urinary proteome using liquid chromatography-tandem mass spectrometry. I. Profiling an unfractionated tryptic digest. Proteomics vol. 1, p. 93-107). 30 Depending on the type of polypeptide marker, it is possible to measure its presence or absence by further means. For example, if the polypeptide is biologically active, its presence may be determined by cellular or enzymatic assays.
WO 2007/082586 PCT/EP2006/050327 -17 Presence of a polypeptide can also be determined by use of ligands binding to the polypeptide of interest. Binding according to the present invention includes both covalent and non-covalent binding. 5 A ligand according to the present invention can be any peptide, polypeptide, nucleic acid, or other substance binding to the polypeptide of interest. It is well known that polypeptides, if obtained or purified from the human or animal body, can be modified, e.g. by glycosylation. A suitable ligand according to the present invention may bind the polypeptide also via such sites. 10 Preferred ligands include antibodies, nucleic acids, peptides or polypeptides, and aptamers, e.g. nucleic acid or peptide aptamers. For many polypeptides, suitable ligands are commercially available. Furthermore, methods to generate suitable ligands are well-known in the art. For example, identification and production of suitable antibodies or aptamers is 15 also offered by commercial suppliers. The term "antibody" as used herein includes both polyclonal and monoclonal antibodies, as well as fragments thereof, such as Fv, Fab and F(ab) 2 fragments that are capable of binding antigen or hapten. 20 Preferably, the ligand should bind specifically to the polypeptide to be measured. "Specific binding" according to the present invention means that the ligand should not bind substantially to ("cross-react" with) another polypeptide or substance present in the sample investigated. Preferably, the specifically bound protein or isoform should be bound with at 25 least 3 times higher, more preferably at least 10 times higher and even more preferably at least 50 times higher affinity than any other relevant polypeptide. Non-specific binding may be tolerable, particularly if the investigated peptide or polypeptide can still be distinguished and measured unequivocally, e.g. according to its 30 size on a Western Blot, or by its relatively higher abundance in the sample. A method for measuring the presence of a polypeptide of interest may comprise-the steps of (a) contacting a polypeptide with a specifically binding ligand, (b) (optionally) removing non-bound ligand, (c) measuring the presence or amount of bound ligand.
WO 2007/082586 PCT/EP2006/050327 - 18 Binding of the ligand can be measured by any method known in the art. First, binding of a ligand may be measured directly, e.g. by NMR or surface plasmon resonance. Second, the ligand also serves as a substrate of an enzymatic activity of the peptide or polypeptide of 5 interest, an enzymatic reaction product may be measured (e.g. the presence of a protease can be measured by measuring the amount of cleaved substrate, e.g. by Western Blot). Third, the ligand may be coupled covalently or non-covalently to a label allowing detection and measurement of the ligand. 10 Labeling may be done by direct or indirect methods. Direct labeling involves coupling of the label directly (covalently or non-covalently) to the ligand. Indirect labeling involves binding (covalently or non-covalently) of a secondary ligand to the first ligand. The secondary ligand should specifically bind to the first ligand. Said secondary ligand may be coupled with a suitable label and/or be the target (receptor) of tertiary ligand binding to the 15 secondary ligand. The use of secondary, tertiary or even higher order ligands is often used to increase the signal. Suitable secondary and higher order ligands may include antibodies, secondary antibodies, and the well-known streptavidin-biotin system (Vector Laboratories, Inc.) 20 The ligand or substrate may also be "tagged" with one or more tags as known in the art. Such tags may then be targets for higher order ligands. Suitable tags include biotin, digoxygenin, His-Tag, Glutathion-S-Transferase, FLAG, GFP, myc-tag, influenza A virus haemagglutinin (HIA), maltose binding protein, and the like. In the case of a peptide or polypeptide, the tag is preferably at the N-terminus and/or C-terminus. 25 Suitable labels are any labels detectable by an appropriate detection method. Typical labels include gold particles, latex beads, acridan ester, luminol, ruthenium, enzymatically active labels, radioactive labels, magnetic labels ("e.g. magnetic beads", including paramagnetic and superparamagnetic labels), and fluorescent labels. 30 Enzymatically active labels include e.g. horseradish peroxidase, alkaline phosphatase, beta-Galactosidase, Luciferase, and derivatives thereof. Suitable substrates for detection WO 2007/082586 PCT/EP2006/050327 -19 include di-amino-benzidine (DAB), 3,3'-5,5'-tetramethylbenzidine, NBT-BCIP (4-nitro blue tetrazolium chloride and 5-bromo-4-chloro-3-indolyl-phosphate, available as ready made stock solution from Roche Diagnostics), CDP-StarTM (Amersham Biosciences), ECFTM (Amersham Biosciences). A suitable enzyme-substrate combination may result in a 5 colored reaction product, fluorescence or chemoluminescence, which can be measured according to methods known in the art. Typical fluorescent labels include fluorescent proteins (such as GFP and its derivatives), Cy3, Cy5, Texas Red, Fluorescein, the Alexa dyes (e.g. Alexa 568), and quantum dots. 10 Typical radioactive labels include 35 S, 125I, 32 p 33 p, and the like. Thus, suitable measurement methods according the present invention also include precipitation (particularly immunoprecipitation), electrochemiluminescence (electro 15 generated chemiluminescence), RIA (radioimmunoassay), ELISA (enzyme-linked immunosorbent assay), sandwich enzyme immune tests, electrochemiluminescence sandwich immunoassays (ECLIA), dissociation-enhanced lanthanide fluoro immuno assay (DELFIA), scintillation proximity assay (SPA), turbidimetry, nephelometry, latex enhanced turbidimetry or nephelometry, or solid phase immune tests. Further methods 20 known in the art (such as gel electrophoresis, 2D gel electrophoresis, SDS polyacrylamide gel electrophoresis (SDS-PAGE), Western Blotting), can be used alone or in combination with labeling or other detection methods as described above. The ligand may also be present on an array. Said array contains at least one additional 25 ligand, which may be directed against a peptide, polypeptide or a nucleic acid of interest. Said additional ligand may also be directed against a peptide, polypeptide or a nucleic acid of no particular interest in the context of the present invention. Preferably, ligands for at least five, more preferably at least 10, even more preferably at least 20 polypeptide markers according to the present invention are contained on the array. 30 According to the present invention, the term "array" refers to a solid-phase or gel-like carrier upon which at least two compounds are attached or bound in one-, two- or three- WO 2007/082586 PCT/EP2006/050327 - 20 dimensional arrangement. Such arrays (including "gene chips", "protein chips", antibody arrays and the like) are generally known to the person skilled in the art and typically generated on glass microscope slides, specially coated glass slides such as polycation-, nitrocellulose- or biotin-coated slides, cover slips, and membranes such as, for example, 5 membranes based on nitrocellulose or nylon. The array may include a bound ligand or at least two cells expressing each at least one ligand. 10 It is also contemplated to use "suspension arrays" as arrays according to the present invention (Nolan JP, Sklar LA. (2002). Suspension array technology: evolution of the flat array paradigm. Trends Biotechnol. vol. 20(1), p. 9-12). In such suspension arrays, the carrier, e.g. a microbead or microsphere, is present in suspension. The array consists of different microbeads or microspheres, possibly labeled, carrying different ligands. 15 The invention further relates to a method of producing arrays as defined above, wherein at least one ligand is bound to the carrier material in addition to other ligands. Methods of producing such arrays, for example based on solid-phase chemistry and photo 20 labile protective groups, are generally known (US 5,744,305). Such arrays can also be brought into contact with substances or substance libraries and tested for interaction, for example for binding or change of conformation. Therefore, arrays comprising a polypeptide marker according to the present invention may be used for identifying ligands binding specifically to said peptides or polypeptides. 25 To determine the sequence of a polypeptide, it should be purified to the highest level achievable. However, the polypeptide does not need to be completely isolated. For example, it is enough to have the polypeptide detectable as a coomassie-stained band in a polyacrylamide gel. The corresponding gel piece can then be cut out and used for the next 30 identification steps. After purification of the polypeptide, it can be enzymatically digested with trypsin and the molecular weights of the resulting fragments determined using any suitable method, for example mass spectrometry. Using mass spectrometry, each polypeptide displays a characteristic "fingerprint" of fragments allowing its identification WO 2007/082586 PCT/EP2006/050327 -21 by database searches. In case that the polypeptide to be identified is not present in the database or if the researcher wants to have a closer characterization for any reasons, the polypeptide fragments can also be sequenced according to methods known in the art. 5 CE-MS allows particularly easy determination of the polypeptide sequences. The capillary electrophoresis elution time for each marker is listed in the tables. Thus, it is possible to collect the fraction containing the polypeptide at relatively high purity. If a single fraction contains insufficient material, fractions of more than one experiment may be pooled. 10 Sequences of some of the polypeptide markers are listed as SEQ ID NO: 1 to 5. Their masses as measured by CE-MS and their respective sequences are as follows: SEQ mass sequence description ID NO: [Da] 1 8765,9 FTFHADICTLSEKERQIKKQTALVEL fragment of human albumin, C-terminus VKHKPKATKEQLKAVMDDFAAFV amino acids 531-609. EKCCKADDKETCFAEEGKKLVAAS QAALGL 2 10046,3 TYVPKEFNAETFTFHADICTLSEKER fragment of human albumin, C-terminus, QIKKQTALVELVKHKPKATKEQLKA amino acids 520 to VMDDFAAFVEKCCKADDKETCFAE 609. EGKKLVAASQAALGL 3 950.0 GGRPSRPPQ fragment of Salivary proline-rich protein 4 1292.5 GFRHRHPDEAA fragment of alpha fibrinogen 5 1448.8 GLITLIGINPSLHT fragment of olfactory receptor 8B4 Figure legends: 15 Fig. 1 Depiction of the information from a crude CE-MS analysis (A) as a three dimensional contour plot (left side). Here a contour plot of urine from a healthy volunteer is shown, mass per charge on the Y-axis against the retention time in min (X-axis), signal intensity colour coded. Next, the signal to noise is calculated and 20 the noise removed, thus leaving only actual signals (B). The software calculates the actual mass (C) based on both isotopic distribution and conjugated masses. This WO 2007/082586 PCT/EP2006/050327 - 22 results in a table of up to 1500 polypeptides defined via their mass and retention time. As an example, bottom right shows 17 polypeptides found in the sample. CE t, CE-time (migration time); int., intensity; m.p.c., mass per charge, cal. m., calculated mass. 5 Fig. 2 Contour plots of polypeptides (actual masses) for healthy subjects (NC) and for patients with focal-segmental glomerulosclerosis (FSGS), minimal-change disease (MCD) and membranous glomerulonephritis (MGN) are shown. The upper mass limit for each plot (i.e. the maximum value along the X-axis) is indicated on the top 10 left of each plot. As evident, the contour plots differ significantly between the healthy subjects and the renal disease groups. Fig. 3 Flow sheet for diagnosis and differential diagnosis of renal diseases (example). Samp., sample; MS-dat., MS-data; Disea., disease; Y, yes; N, no; n.d., no disease; 15 d.n., diabetic nephropathy, FSGS, FSGS; MGN, MGN; MCD, MCD; IgA, IgA nephropathy, diff., differential diagnosis The invention is further illustrated by the following examples: 20 Example 1 Participants: 25 After local Ethics Committee approval, informed consent was obtained from all participants. We examined a group of 57 healthy individuals with normal renal function in order to establish normal urinary protein patterns with CE-MS. In addition, we studied 44 patients with biopsy-proven minimal-change disease (n = 16; MCD), membranous glomerulonephritis (n = 18; MGN), and focal-segmental glomerulosclerosis (n = 10; 30 FSGS) (Table 1). CE-MS Analysis: Spot urine samples were collected from all participants in the morning after voiding the 35 first urine. Samples were prepared as described in detail elsewhere (Wittke S, Fliser D, Haubitz M, et al: Determination of peptides and proteins in human urine with CE-MS suitable tool for the establishment of new diagnostic markers. J Chromatogr A 1013:173- WO 2007/082586 PCT/EP2006/050327 - 23 181, 2003). The CE-MS analysis was established as described previously (Kaiser T, Hermann A, Kielstein JT, et al: Capillary Electrophoresis coupled mass spectrometry to establish polypeptide patterns in dialysis fluids. J Chromatogr A 1013: 157-171, 2003), using a Beckman Coulter PAC/E system coupled to a Mariner TOF mass spectrometer 5 (ABI). CE capillaries were from Beckman, ID/OD 75/360 pm and 90 cm in length. The mobile phase used contained 30% methanol and 0.5% formic acid in water. The same liquid was used for the sheath flow, which was applied at 2 pl/min. Sample injection was performed with pressure: 1 psi for 20 sec. Under these conditions about 100 nl of sample could be injected. For sample stacking, the following protocol was applied: injection of IM 10 NH 3 for 7 sec., injection of sample, injection of 2M formic acid for 5 sec. The subsequent CE-MS run was performed at +30 kV with the sequence of the following pressures: 40 min at 0 psi, 2 min at 0.1 psi, 2 min at 0.2 psi, 2 min at 0.3 psi, 2 min at 0.4 psi, 80 min at 0.5 psi. For diagnosis of IgA-nephropathy, the following pressure sequence was used: 40 min at 0.3 psi, 2 min at 0.4 psi, 2 min at 0.6 psi, 2 min at 0.8 psi, 80 min at 1 psi. After each 15 run, the CE capillary was rinsed for 5 min with 0.1 M NaOH, followed by 5 min with water and 5 min with running buffer. Statistical analysis: 20 For discrimination between healthy subjects and different groups of patients with renal diseases we used the method of Random Forests and the corresponding S-Plus program version 6/2002 Breiman L: Random Forests. (http://oz.berkeley.edu/users/breiman/randomforest2001 .pdf). In this procedure, a series of PP subsets of fixed size is selected randomly from all candidate PP. For each subset, a 25 classification tree as described in the Classification and Regression Tree (CART) analysis is generated (Steinberg D, Colla P: CART -- Classification and Regression trees. San Diego, CA, Salford Systems 1997), resulting in a classification rule. The forest prediction is the unweight plurality of class votes of the series of classification rules. Over-fitting is not generated due to large numbers of subset selections. The estimated generalisation error 30 is unbiased due to the method of "out of bag" (oob) estimation: each tree is grown on a bootstrap sample of cases of the learning sample and the validation is estimated on the basis of those cases not selected in the bootstrap sample. Further, discrimination between groups was also performed using support vector machines. 35 This tool has the advantage of discriminating data in high dimensional parameter space. Its fast and stable algorithms showed good performance in the evaluation of clinical markers (Dieterle F, Muller-Hagedorn S, Liebich HM, Gauglitz G: Urinary nucleosides as potential WO 2007/082586 PCT/EP2006/050327 - 24 tumor markers evaluated by learning vector quantization. Artif Intell Med 28:265-279, 2003) and different areas of biological analyses like DNA arrays (Brown MP, Grundy WN, Lin D, et al: Knowledge-based analysis of microarray gene expression data by using support vector machines. Proc Natl Acad Sci USA 97:262-267, 2000). 5 Normal urinary polypeptide pattern analysed with CE-MS: A graphical depiction (contour plot) of a typical sample is presented in Fig. 1 (raw data). In one individual sample, between 900 and 2500 PP with molecular weights from 800 up to 10 30.000 Dalton were detected. Under the conditions used for CE polypeptides with higher molecular weights tend to precipitate. Thus larger proteins in general cannot be detected, although some (e.g. albumin) can be visualised. A list of polypeptides present with high probability that were chosen as internal standards to assure sample comparability is shown in table 23. For analysis of protein-rich samples, such as samples from suspected IgA 15 nephropathy patients, higher pressure was applied and the polypeptides according to table 24 were preferred as internal standards. Repeated analyses of identical samples did not reveal any significant differences under identical conditions of the CE-MS run for an individual sample. 20 The subsequent electronic data manipulation for one example is summarised in Fig. 1. Each run results in the crude spectrum depicted in the upper part of Fig. 1 and is composed of single spectra (blow up Fig. 1) generated every 3 seconds. CE-MS peaks were identified in the first data analysis run (Fig. lA). Next, the charge of each peak was ascertained utilising both isotopic distribution and conjugated peaks (Fig. lB). As a result, conjugated 25 peaks were summarised in one single peak and the real mass was calculated, as shown in Fig. 1 C. Initially, the samples were spiked with external standards of known mass. This allowed subsequent definition of internal standards of PP present with high probability in the urine samples. Thus the CE-time could be normalized to the internal standards. By applying this technique on an average urine sample, roughly 1000 PP can be detected and 30 described/identified by the two parameters mass and CE-migration time. The examination of urine obtained from healthy subjects led to the establishment of peaks defined by actual mass and CE-time of the PP detected, so-called peak lists, and contour plots for each individual. The individual peak lists were deposited in an MS-Access 35 database and the probability of each of the PP to appear in a single sample was calculated. One-hundred seventy-three PP were present in over 90% of the control samples examined. In addition, 156 PP were present in more than 75% of the samples, while additional 361 PP WO 2007/082586 PCT/EP2006/050327 - 25 were found in over 50% of samples from the healthy individuals. These 690 PP were found in more than 50% of all samples obtained from healthy subjects and were used to establish a "normal PP pattern". 5 Urine from patients with renal diseases analysed with CE-MS: Data from the individual runs of 44 patients were sub-grouped in the three disease groups and analysed. The values from these databases, representing typical PP patterns, were subsequently compared. Significant homology of the protein patterns present in urine 10 samples from each patient group was found within the groups. Typical examples of urinary PP patterns from patients with MCD, FSGS, and MGN are shown in Fig. 2. Each disease presents a typical protein contour plot, revealing more than 500 PP. Subsequently, the data from the three groups were compared with those obtained in healthy subjects. Table 16 shows 124 PP found in the urine of more than 95% of healthy subjects and reveals the 15 differences to patients with MCD, FSGS, and MGN. Statistical analysis for discrimination of healthy individuals and patients with renal disease using CE-MS data was applied. A list of 800 PP, present with more than 50% probability in either disease group was chosen for Random Forest analysis. The correct classification 20 rate for the discrimination between healthy subjects and renal patients was 96.5 %, as shown in the following list: Class Healthy Renal Classification subjects patients error (n=57) (n=44) 0/ classified as healthy 56 2 3.5 classified as patients 42 2.3 After cross-validation a sensitivity of 81.3% and a specificity of 94.3% could be obtained. 25 Discrimination of the disease groups was achieved in the learning sample. However, most likely due to the small number of FSGS patients, these could not be discriminated from MCD when applying cross-validation. Hence, FSGS and MCD were combined into one group. For the discrimination between healthy subjects, MCD/FSGS and MGN, four PP were selected by CART from the list to build a classification tree with five terminal nodes 30 (table 15).The correct classification rate in the learning sample is 94.1%. After cross- WO 2007/082586 PCT/EP2006/050327 - 26 validation it reduces to 84.3% (93.8% for healthy controls, 71.4% for MCD/FSGS and 92.9% for MGN). Alternatively, statistical analysis was performed using support vector machines on the 5 same data; table 16 shows PP that were employed in this analysis. Using these PP, the correct classification was 98.0% after complete cross-validation. Table 17 depicts PP that were used to discriminate between MCD and MGN. Here the correct classification was 94.1 % after complete cross-validation. Further, it was possible to separate patients with MCD and FSGS and patients with MGN and FSGS with (cross-validated) classification 10 rates of 92.3 % and 89.3%, respectively (tables 18 and 19). These results can be valued as a first approach using support vector machines to classify a limited number of patients. With increasing patients data the classification will further improve and become more stable. The results also indicate that for stable classification the number of applicable variables (polypeptides) depends on the number of cases (patients), hence an increase in 15 patients will allow to use even more PP for classification.
WO 2007/082586 PCT/EP2006/050327 27 Table 1: 5 molecular migration discrimination frequency weight time [min] factor frequency [%] [Da] glomerulo- healthy nephritis 830,5 25,3 0,42 55 12 836,5 35 0,64 80 16 862,4 48,7 0,45 57 12 866,4 37,9 0,62 77 16 870,4 33,9 0,45 52 7 874,5 29,7 0,46 75 29 876,4 48,9 -0,41 57 98 882,6 36,5 -0,4 55 95 903,4 46,8 -0,42 14 55 909,4 40,3 0,67 70 3 - 925,4 50,7 0,63 77 14 926,5 36,1 -0,44 32 76 943,5 30 0,52 80 28 946,5 46,8 -0,44 41 84 950,5 36 0,61 66 5 952,5 32 0,52 64 12 956,4 49,5 -0,54 7 60 978,5 35 0,53 55 2 980,6 34,6 -0,45 43 88 982,5 31,9 0,53 64 10 983,5 35,1 0,41 55 14 988,6 49,9 -0,48 9 57 990,6 32 0,42 61 19 991,4 37,7 0,41 55 14 994,5 33,3 0,51 75 24 995,6 36,4 0,46 68 22 1000,5 34 -0,58 36 95 1006,4 35,7 -0,48 _30 78 1008,5 34,4 -0,5 43 93 1010,6 30,6 -0,58 25 83 1013,4 39,3 -0,43 9 52 1015,6 38,2 0,47 52 5 1028,6 37,8 -0,55 43 98 1033,6 39,1 0,62 70 9 1038,6 34,4 0,43 57 14 1046,6 38,6 -0,76 20 97 1047,6 30,4 -0,44 41 84 1073,6 34,7 0,59 75 16 1075,6 29 -0,43 20 64 1102,6 32,9 0,4 52 12 1108,6 29,8 0,47 86 40 WO 2007/082586 PCT/EP2006/050327 28 1110,4 46,9 -0,5 20 71 1121,6 42,3 -0,46 16 62 1122,5 50,2 -0,41 25 66 1135,6 42,7 -0,61 5 66 1138,6 39,3 0,55 73 17 1139,6 32,2 0,52 59 7 1141,6 38 -0,6 7 67 1157,6 28,5 0,5 80 29 1159,6 39 -0,65 16 81 1163,7 38,1 0,47 50 3 1171,6 32,8 0,64 66 2 1182,6 47,2 -0,45 20 66 1191,6 50,5 -0,41 50 91 1191,8 18,3 0,56 66 10 1198,8 29,2 0,44 75 31 1203,7 24,7 -0,52 5 57 1209,6 50,5 -0,42 48 90 1211,6 31,3 0,5 66 16 1212,7 30,6 0,57 66 9 1219,6 37,3 0,57 77 21 1220,6 30,2 0,42 75 33 1223,5 51,6 -0,6 30 90 1224,7 33,6 -0,41 59 100 1225,7 41,3 0,45 50 5 1235,6 41,4 -0,41 59 100 1237,7 41,6 -0,49 18 67 1246,7 30,5 -0,47 18 66 1256,6 53,4 0,41 55 14 1264,7 26,7 0,44 52 9 1268,6 53,7 -0,47 5 52 1269,7 39,8 0,45 64 19 1270,5 52,5 -0,51 5 55 1279,7 38,3 0,48 64 16 1280,6 51,9 -0,53 9 62 1286 30,7 0,41 84 43 1292,5 53 -0,59 27 86 1297,6 38,7 0,45 86 41 1302,7 31,8 0,54 86 33 1303,6 40,7 -0,44 11 55 1311,8 31,5 0,58 77 19 1319,9 34,8 0,4 59 19 1324,2 40,5 0,5 59 9 1325,5 35,2 0,54 80 26 1333,8 38,8 0,65 82 17 1335,7 39,2 0,57 80 22 1338,7 29,6 0,46 57 10 1338,7 47,2 0,8 82 2 1350,7 50,3 -0,48 2 50 1353,7 39,3 -0,44 45 90 1354,8 45,6 0,55 93 38 1371,7 39,9 0,6 64 3 1371,8 19,3 0,63 89 26 1389,8 19,5 0,5 84 34 1390,7 41,1 0,45 64 19 WO 2007/082586 PCT/EP2006/050327 29 1398,9 30,5 0,59 73 14 1401,8 46,2 -0,53 9 62 1405,9 17,3 0,49 59 10 1408,9 26,8 0,42 52 10 1414,6 38,1 0,62 86 24 1415,7 33,3 0,45 50 5 1419,8 39,7 0,48 77 29 1424,9 35,4 -0,46 25 71 1442,8 33,3 0,63 84 21 1444,6 37,8 0,53 82 29 1448,8 30,3 0,42 75 33 1465,9 28,8 0,59 66 7 1472,1 31,2 0,57 70 14 1474,9 16,9 0,65 77 12 1482 30,4 0,57 84 28 1484 30,4 0,58 89 31 1486,5 30,6 0,45 66 21 1498,7 34,9 0,52 66 14 1499,9 30,6 0,56 91 34 1502,8 28,8 0,44 75 31 1502,9 16,8 0,66 68 2 1508,9 16,8 0,48 57 9 1511,7 38,4 0,55 80 24 1518 26,8 0,45 93 48 1520,7 27,9 0,45 64 19 1527,9 34,7 0,43 73 29 1529,7 54,1 -0,48 36 84 1535 28,3 0,61 73 12 1537,9 31,5 0,43 70 28 1540,7 29,8 0,5 66 16 1542,5 27,2 0,4 52 12 1548,3 31,1 0,46 89 43 1556,8 33,7 0,59 89 29 1567 31,9 0,45 86 41 1567,6 53,9 -0,53 2 55 1568,6 34,3 0,41 70 29 1573,8 40,4 0,44 89 45 1574,8 33,9 0,41 61 21 1582,9 27,8 0,51 61 10 1588,4 47,9 -0,61 11 72 1596,9 34 0,64 86 22 1604,3 21,6 0,5 64 14 1604,7 38,1 0,42 73 31 1605,7 53,3 -0,4 34 74 1611,7 53,2 -0,48 36 84 1612,8 36,8 0,58 91 33 1622 19,2 0,51 91 40 1633,8 24,6 0,42 75 33 1644 18,8 0,46 55 9 1652,3 28,6 0,44 84 40 1669,9 33,4 0,54 75 21 1676 25,3 0,52 64 12 1681,6 40 0,51 82 31 1686,8 38,2 0,67 91 24 WO 2007/082586 PCT/EP2006/050327 30 1690,8 25,5 0,44 75 31 1692,5 44,2 -0,41 39 79 1699,1 41,9 0,62 86 24 1711 43,3 -0,45 20 66 1718,5 22,6 0,57 66 9 1726 36,3 0,62 70 9 1729,2 26 0,57 70 14 1732 51,6 -0,41 36 78 1739,8 35,7 0,45 86 41 1746,2 46,2 -0,59 25 84 1747,7 50,8 -0,52 5 57 1752,9 39,9 0,46 68 22 1763 24,4 0,57 80 22 1770,4 45,4 0,4 89 48 1777,6 28,6 0,53 70 17 1793,6 28,3 0,49 55 5 1804,7 34 0,45 100 55 1808,1 45,6 0,49 55 5 1810,1 31,8 0,45 64 19 1811,3 31,3 0,55 93 38 1813,4 54,7 -0,47 7 53 1815,2 27,7 0,5 66 16 1819,9 24,1 0,5 64 14 1820,1 31,8 0,48 91 43 1821,2 18,2 0,52 57 5 1822,9 40,7 -0,6 23 83 1824,3 37 -0,52 27 79 1826,1 21,8 0,45 59 14 1831,9 41,5 0,5 59 9 1847,8 57 -0,66 27 93 1851,2 31,6 0,48 86 38 1853 31,2 0,59 82 22 1853,6 46,7 0,47 50 3 1854,2 28,8 0,45 52 7 1856,8 56,3 -0,51 18 69 1857,1 39 0,46 75 29 1864,6 28,6 0,65 82 17 1867 31,8 0,6 91 31 1883 29,1 -0,49 32 81 1885,7 57,5 -0,4 55 95 1889,2 30,1 0,41 55 14 1889,8 46,4 -0,58 39 97 1891,6 32,3 0,55 77 22 1894,9 22 0,67 86 19 1896,8 53,3 -0,44 11 55 1898,7 26,51 0,45 59 14 1904 27,5 0,48 50 2 1913,4 30,1 0,44 55 10 1916,8 44,7 -0,52 14 66 1920,7 30,6 0,46 91 45 1933,9 32,8 -0,55 36 91 1934,2 16,1 0,71 73 2 1936,5 46,6 -0,42 25 67 1936,7 32,8 0,5 80 29 WO 2007/082586 PCT/EP2006/050327 31 1944,2 47 -0,68 18 86 1951,1 53 -0,48 16 64 1966,3 25,1 0,71 82 10 1973,7 57,1 -0,5 9 59 1977,4 42,9 -0,47 41 88 1982,9 32,2 0,58 82 24 . .1989,3 43,7 0,69 84 16 1990,8 . . 47,3 -0,71 11 83 2011,5 42 0,41 70 29 2022,6 34,6 0,46 68 22 2025 24,2 0,41 50 9 2028,4 29,9 0,55 80 24 2030,4 31,7 -0,49 32 81 2030,8 46,5 -0,61 25 86 2033,5 27,5 0,46 55 9 2042 26,4 0,47 95 48 2042,5 40,7 0,5 70 21 2045,9 25,3 0,43 84 41 2047 45,4 -0,46 52 98 2050,8 38,2 0,47 82 34 2065,3 20,9 0,49 52 3 2092 26,7 0,52 66 14 2092,5 41,3 0,59 75 16 2099,2 36,9 0,58 84 26 2103,6 26,7 0,46 89 43 2105,4 32,5 0,52 66 14 2109,3 27,9 0,47 68 21 2117,1 57,1 -0,57 20 78 2127,2 39,6 0,46 75 29 2129,5 35,1 -0,58 39 97 2140,1 26,8 0,52 64 12 2144,3 22 0,47 75 28 2146,3 25,8 0,74 77 3 2147,2 38,4 0,43 64 21 2152,7 29,5 0,51 70 19 2157,2 24,4 0,41 50 9 2174,4 24,6 0,46 68 22 2178,5 21,4 0,48 57 9 2182,5 27,6 0,55 80 24 2207,2 41,9 0,41 61 21 2210,7 25,7 0,64 86 22 2217,7 41,9 0,5 84 34 2221,1 40,7 -0,5 14 64 2223,5 22,6 0,6 68 9 2228,1 25,9 0,51 91 40 2233 31,1 -0,4 55 95 2241,1 22,7 0,49 80 31 2290,7 36,2 0,47 52 5 2291,1 21,9 0,45 50 5 2308,9 26,2 0,41 61 21 2312,5 22,9 0,45 57 12 2322,5 47,1 0,47 52 5 2356,3 24 0,41 57 16 2364,4 38,9I 0,49 73 24 WO 2007/082586 PCT/EP2006/050327 32 2370,7 27,3 0,4 52 12 2391,2 24,3 0,58 70 12 2406,4 31,8 0,43 84 41 .2409,1 41,9 0,43 84 41 2421 28,7 0,41 70 29 2423,1 27,4 0,41 68 28 2426,5 38,5 0,58 89 31 2427,4 24 0,53 84 31 2432,2 38,3 0,66 80 14 2464 47,2 .- 0,55 7 62 2465 22,8 0,7 75 5 2473,4 41,9 0,44 52 9 2490,7 26,7 0,43 70 28 2493,6 24,6 0,63 77 14 2522,9 24,4 0,47 68 21 2529,2 41,4 -0,47 14 60 2535 37,7 0,42 82 40 2540,5 25,5 0,65 75 10 2548,2 35,1 -0,46 36 83 2566,4 22,2 0,5 57 7 2568,9 26,9 0,41 70 29 2573,7 16,3 0,57 66 9 2584 43,8 -0,56 41 97 2593,4 25 0,41 57 16 2614,1 22,5 0,42 59 17 2619,7 22,9 0,47 50 3 2621,4 25,8 0,56 68 12 2644,1 32,5 -0,48 45 93 2660,8 27,1 0,4 59 19 2665,3 39,4 0,46 57 10 2677,6 23,6 0,58 68 10 2698,4 32,1 -0,47 32 79 2713,2 41,3 -0,51 11 62 2719,9 20,2 0,49 55 5 2752,8 25,3 0,56 82 26 2780,4 28,3 0,52 66 14 2790,3 26,8 0,46 61 16 2793,7 36,3 0,64 80 16 2809,1 37,2 -0,48 30 78 2812,5 32,8 0,46 61 16 2830,9 33,2 0,49 68 19 2937,1 26,6 0,46 55 9 2973,7 34,9 -0,58 30 88 2978 26,3 -0,49 34 83 2990,4 33,6 -0,47 20 67 3007,5 30,5 -0,45 23 67 3017,7 46,8 -0,42 18 60 3057,1 56,4 -0,41 43 84 3058,8 35,5 -0,41 45 86 3121,4 42,5 -0,43 57 100 3137 37 -0,42 41 83 3139,4 43,7 -0,53 25 78 3152,6 38,2 -0,45 55 100 3177,4 22,3 -0,45 27 72 WO 2007/082586 PCT/EP2006/050327 33 3187,7 48,6 -0,4 41 81 3209,2 34,3 -0,47 50 97 3219,5 20,2 0,48 61 14 3255,8 42,9 -0,48 36 84 3262 31,5 -0,52 34 86 3281 36,8 I-0,66 32 98 3282 49,4 -0,4 55 95 3290,9 36,9 .- 0,57 36 93 3295,8 38,4 -0,55 43 98 3303,2 38,6 -0,57 27 84 3308,6 21,3 0,53 57 3 3309,7 43,6 -0,41 32 72 3319,3 46,2 -0,45 50 95 3333,4 23,3 -0,56 32 88 3334,6 41,7 -0,54 32 86 3337,4 36,2 -0,45 43 88 3343,8 43,8 -0,46 45 91 3405,7 37,8 -0,6 39 98 3422,5 38,7 -0,58 32 90 3436 26,4 -0,5 20 71 3479,3 48,5 -0,5 50 100 3503,3 23,2 -0,43 16 59 3530,9 36,8 -0,54 27 81 3583,3 25,2 -0,67 23 90 3589,5 39,1 -0,65 25 90 3617,4 44,8 -0,4 18 59 3631,2 33,1 -0,55 16 71 3634,9 42,6 -0,41 39 79 3682,4 42,8 -0,47 27 74 3686,1 32,6 -0,71 11 83 3697,4 38,8 -0,42 11 53 3701,8 43,4 -0,63 9 72 3707 31,9 -0,69 7 76 3719,6 44,7 -0,42 41 83 3723,3 32,5 -0,65 32 97 3735,8 43,9 -0,5 30 79 3760,8 25,9 -0,51 18 69 3802,7 46,2 -0,43 14 57 3816,7 32,2 -0,52 14 66 3852,2 36,9 -0,45 36 81 3871,7 42,9 -0,41 23 64 3946,9 33,1 -0,54 39 93 3969,6 31,3 -0,52 34 86 3987 30,5 -0,42 55 97 4026,2 30,5 -0,42 11 53 4044,7 31,2 -0,57 30 86 4055,2 24,1 0,41 57 16 4154,2 23,7 0,63 77 14 4170,6 46,1 -0,45 7 52 4183,7 26,6 0,42 52 10 4241,2 24,4 0,75 89 14 4283,1 24,3 0,55 64 9 4290,8 41,1 -0,45 43 88 4654,8 38,8 -0,4 11 52 WO 2007/082586 PCT/EP2006/050327 34 4713,7 26,9 0,63 68 5 4748,5 25,4 -0,56 39 95 4772,1 28,9 -0,43 9 52 4801,2 37,5 -0,49 39 88 4827,1 27,3 0,51 52 2 4863,7 39,2 -0,53 18 71 5213,8 36,8 -0,43 7 50 5229,1 39,9 -0,43 9 52 5575,8 35,7 -0,48 14 62 6171,5 39,6 -0,5 43 93 6212,4 30,6 -0,5 9 59 6400,9 23,4 0,51 52 2 7409,9 26,2 0,49 61 12 7556,6 26,2 0,59 75 16 7572,8 25,7 0,42 55 12 8054,8 16,7 0,63 82 19 8341,2 16,6 0,59 66 7 8653,1 17,2 0,4 52 12 8765,9 17,6 0,56 89 33 9060,7 23 0,46 57 10 9076 23 0,58 68 10 9182 17,1 0,55 64 9 9223,1 22,8 0,64 70 7 9335,5 17,5 0,47 50 3 9868,8 29,5 -0,57 20 78 9933,5 18,4 0,47 50 3 10046,3 18,1 0,7 89 19 10390,1 20,2 0,58 70 12 10518,8 20,9 0,56 75 19 Table 2 molecular migration discrimination frequency [%] weight [Dal time [mini factor FSGS healthy 803,4 35,2 0,44 60 16 807,3 35,4 0,41 50 9 809,3 252 0,5 50 0 817,2 25.6 0,47 50 3 830,5 25,3 0,68 80 12 836,5 35 0,54 70 16 866,4 37,9 0,64 80 16 870,4 33,9 0,43 50 7 874A 49,7 0,57 60 3 907,4 27,5 0,57 60 3 909,4 40,3 0,57 60 3 915,4 35 0,48 50 2 925,4 50,7 0,56 70 14 926,5 36,1 -0,46 30 76 939,6 33,1 0,61 70 9 943,5 30 0,42 70 28 946,5 46,8 -0,54 30 84 950,5 36 0,75 80 5 952,5 32 0,58 70 12 WO 2007/082586 PCT/EP2006/050327 35 953,6 34,5 -0,52 20 72 956,4 49,5 -0,5 10 60 958,5 32,5 0,48 70 22 9745 27,6 0,41 60 19 978,5 35 0,48 50 2 980,6 34,6 -0,58 30 88 981,6 37,4 -0,47 50 97 982,5 31,9 0,7 80 10 988,6 49,9 -0,47 10 57 990,6 32 0.41 60 19 994,5 33,3 0,46 70 24 995,6 36,4 0,48 70 22 1000.5 34 -0.55 40 95 1002,6 38,5 0,53 60 7 1005,5 35 0,54 70 16 10064 35,7 -0,58 20 78 1008,5 34,4 -0,63 30 93 1010,6 30,6 -0,53 30 83 1010,6 50,8 -0,64 0 64 1013,4 39,3 -0,52 0 52 1015,6 38,2 0,55 60 5 1021.5 32,1 0,45 50 5 1028,6 37,8 -0,58 40 98 1033,6 39,1 0,71 80 9 1041,5 51,6 -0,4 20 60 1046,6 38,6 -0,77 20 97 1049,5 39,9 0,45 50 5 1055,6 36,4 0,51 60 9 1071,5 38,7 0,48 50 2 1073,6 34,7 0,64 80 16 1075,6 29 -0,44 20 64 1090,5 36,2 0,42 70 28 1106,6 19,6 0,41 50 9 110 29,8 0,4 80 40 1110,4 46,9 -0,41 30 71 1121,6 42,3 -0,62 0 62 1126,5 42,7 0,51 60 9 1135,6 42,7 -0,66 0 66 1138,6 39,3 0,63 80 17 1139,6 32,2 0,53 60 7 11416_ 38 -0,57 10 67 1157,6 28.5 0,51 80 29 1157,6 169 0,5 50 0 1159,6 39 -0,61 20 81 1164,6 38,7 0,46 60 14 1171,6 32,8 0,48 50 2 1182,6 47,2 -0,66 0 66 1186,6 32 0,47 80 33 11916 50,5 -0,71 20 91 1191,8 18,3 0,5 60 10 1192,6 40,9 0,46 70 24 1203,7 24,7 -0,47 10 57 1209,6 50,5 -0,5 40 90 1211,6 31,3 0,64 80 16 WO 2007/082586 PCT/EP2006/050327 36 1212.7 30,6 0,61 70 9 1219,6 37,3 0,59 80 21 1220,6 30,2 0,57 90 33 1224,7 33,6 -0,5 50 100 1225,7 41,3 0,55 60 5 1235,6 41,4 -0,4 60 100 1236,7 34,8 0,44 70 26 237. 41,6 -0,47 20 67 1246,7 30,5 -0,46 20 66 1258,7 20,9 0,5 60 10 1263,7 38,6 0,65 70 5 1268,6 53,7 -0,52 0 52 269,7 39,8 0,51 70 19 1270,5 52,5 -0,55 0 55 1270,6 25,7 0,55 60 5 1274,6 38 0,56 70 14 12797 38,3 0,44 60 16 1280,6 51,9 -0,52 10 62 1288,6 46,1 -0,44 40 84 1292,5 53 -0,66 20 86 1294,6 54,4 0,56 70 14 13027 31.8 0,57 90 33 1303,6 40,7 -0,45 10 55 1304,8 24,6 0,5 50 0 1305,9 33,4 0,6 70 10 1308,6 53,6 -0,54 30 84 1309,8 38,9 0,41 50 9 1310,7 . 52,5 0,5 50 0 1311,8 31,5 0,51 70 19 1325,5 35,2 0,44 70 26 1333,8 38,8 0,63 80 17 1335,7 39,2 0,68 90 22 1338,7 47,2 0,78 80 2 1338,7 29,6 0,7 80 10 1350,7 50,3 -0,5 0 50 1353,7 39,3 -0,5 40 90 1354,8 45,6 0,52 90 38 1367,7 26,2 0,41 50 9 1371,7 39,9 0,6 70 3 1371,8 19,3 0,64 90 26 1377,7 25,4 0,67 70 3 1383,7 52,7 -0,53 0 53 1386 24,4 0,41 50 9 1389,8 19,5 0,56 90 34 1390,7 41,1 0,71 90 19 1394,3 48,1 0,48 60 12 1398,9 30,5 0,56 70 14 1401,8 46,2 -0,62 0 62 1403,8 34,4 0,57 60 3 1405,9 17,3 0,6 70 10 1408,9 26,8 0,5 60 10 14112 45,4 0,41 70 29 1414,6 38,1 0,76 100 24 1414,7 26,6 0,48 50 2 WO 2007/082586 PCT/EP2006/050327 37 1419,8 39,7 0.41 70 29 1424,9 35,4 -0,61 10 71 1426,8 38,7 0,41 50 9 1434,8 41,2 0,48 50 2 1442,8 33,3 0,69 90 21 1444,6 37,8 0,61 90 29 1465,9 28,8 0,53 60 7 1472,1 31,2 0,46 60 14 1474,9 16,9 0,58 70 12 1482 30,4 0,42 70 28 1484 30,4 0,49 80 31 1487,7 41,4 -0,41 50 91 1490,9 53,4 -0,41 30 71 1493,7 33,7 0,41 70 29 1498,7 34,9 0,46 60 14 1499,9 30,6 0,56 90 34 1501,1 29,5 0,45 50 5 1502,9 16,8 0,68 70 2 1508,9 .16,8 0,51 60 9 1511,7 38,4 0,56 80 24 1517,6 54,8 0,48 60 12 1518 26,8 0,52 100 48 1518,9 42,5 0,48 60 12 1520,7 27,9 0,41 60 19 1527,9 34,7 0,41 70 29 1529,7 54,1 -0,44 40 84 1535 28,3 0,68 80 12 1536,6 35 0,46 60 14 1537,9 31,5 0,52 80 28 1540,7 29,8 0,44 60 16 1547 38,3 0,5 90 40 1548,3 31,1 0,47 90 43 1553,2 54,4 0,48 60 12 1556,8 33,7 0,51 80 29 1567 31,9 0,49 90 41 1567,6 53,9 -0,55 0 55 1588,4 47,9. -0,62 10 72 1589,7 54,3 -0,44 40 84 1591,6 32,6 0,53 60 7 1596.9 34 0,58 80 22 1598,7 28,5 0,48 60 12 1604,3 21,6 0,56 70 14 1604,7 38,1 0,49 80 31 1605,7 53,3 -0,44 30 74 1607,7 41 0,48 60 12 1611,7 53,2 -0,54 30 84 1612,8 36,8 0,47 80 33 1619,7 53,9 -0,52 10 62 1622 19,2 0,6 100 40 1644 18,8 0,41 50 9 1669,9 33,4 0,59 80 21 1671,3 25,4 0,42 80 38 1681,6 40 0,59 90 31 1686,8 38,2 0,66 90 24 WO 2007/082586 PCT/EP2006/050327 38 1692,5 44,2 -0,59 20 79 1695,1 23,6 0,48 60 12 1699,1 41,9 0,46 70 24 1711 43,3 -0,46 20 66 1713,4 24,6 0,41 60 19 1718,5 22,6 0,41 so50 9 1723,3 26,5 0,43 60 17 1726 36,3 0,61 70 9 1729,1 37,7 0,41 50 9 1729,2 26 0,66 80 14 1732 51,6 -0,48 30 78 1739,8 35,7 0,49 90 41 1746,2 46,2 -0,54 30 84 1747,7 50,8 -0,47 10 57 1751,4 40,8 0,42 80 38 1752,9 39,9 0,48 70 22 1763 24,4 0,68 90 22 1770,4 45,4 0,52 100 48 1772,6 28,5 0,44 60 16 1776,1 43,6 -0,43 40 83 1777,6 28,6 0,73 90 17 1783,4 29,2 0,51 70 19 1784,9 31,4 0,47 50 3 1786,9 35,9 0,53 70 17 1788,6 31 0,49 90 41 1792,4 42,3 0,59 80 21 1794,9 40,4 0,4 80 40 1804,7 34 0,45 100 55 1808,1 45,6 0,55 60 5 1810,1 31,8 0,41 60 19 1811,3 31,3 0,52 90 38 1813,4 54,7 -0,43 10 53 1815,1 39,3 0,41 60 19 1815,2 27,7 0,44 60 16 1820,1 31,8 0,57 100 43 1821,2 18,2 0,45 50 5 1821,5 42,1 0,46 70 24 1822,9 40,7 -0.73 10 83 1824,3 37 -0,59 20 79 1831,7 25,2 0,43 50 7 1831,9 41,5 0,61 70 9 1844,2 34,6 0,62 90 28 1847,8 57 -0,73 20 93 1849,6 37,2 -0,41 40 81 1851,2 31,6 0,52 90 38 1853 31,2 0,58 80 22 1853,4 18,3 0,5 50 0 1853,6 46,7 0,57 60 3 1854,2 28,8 0,43 50 7 1856,8 56,3 -0,59 10 69 1857,1 39 0,51 80 29 1864,6 28,6 0,43 60 17 1867 31,8 0,49 80 31 1870,5 16,1 0,45 50 5 WO 2007/082586 PCT/EP2006/050327 39 1871,7 43,2 0,65 70 5 1881,4 34,3 0,47 80 33 1889,2 30,1 0,56 70 14 1889,8 46,4 -0,67 30 97 1891,6 32,3 0,58 80 22 1894,9 22 0,71 90 19 1894,9 56 -0,46 20 66 1898,7 26,5 0,46 60 14 1900,7 30,4 -0,63 20 83 1902,8 33,1 0,53 70 17 1904 27,5 0,48 50 2 1904,3 43,2 0,41 50 9 1916,8 44,7 -0,46 20 66 1920,5 46,1 0,44 60 16 19207 30,6 0,45 90 45 1925,3 52,5 0,57 90 33 1928,4 33,2 0,48 70 22 1933,9 32,8 -0,41 50 91 1934,2 16,1 0,78 80 2 1936,5 46,6 -0,47 20 67 1936,7 32,8 0,51 80 29 1944,2 47 -0,66 20 86 1950,9 34,5 0,59 90 31 1951,1 53 -0,54 10 64 1966,3 25,1 0,6 70 10 1973,7 57,1 -0,49 10 59 1977,4 42,9 -0,48 40 88 1982,9 32,2 0,46 70 24 1989,3 43,7 0,54 70 16 1990,8 47,3 -0,83 0 83 9994 35,6 0.4 80 40 2005,3 39,6 0,49 80 31 2013,8 45,3 -0,47 20 67 2022,6 34,6 0,48 70 22 2028,4 29,9 0,66 90 24 2030,8 46,5 -0,56 30 86 2033,5 27,5 0,51 60 9 2042 26,4 0,52 100 48 2042,5 40,7 0,49 70 21 2047 45,4 -0,48 50 98 2048,2 33,1 -0,6 40 100 2057,2 36,3 0,43 100 57 2063 24,3 0,6 60 0 2065,3 20,9 0,57 60 3 2077.3 35,8 -0,42 10 52 2092,5 41,3 - 0,44 60 16 2099,2 36,9 0,54 80 26 2105,4 32,5 0,56 70 14 2114,9 42 0,48 70 22 2117,1 57,1 -0,68 10 78 2121 26,9 0,61 80 19 2127,2 39,6 0,61 90 29 2140,1 26,8 0,48 60 12 2144,3 22 0,42 70 28 WO 2007/082586 PCT/EP2006/050327 40 2146,3 25,8 0,57 60 3 2147,2 38,4 0,69 90 21 2152,7 29,5 0,51 70 19 2163,4 27,6 0,6 70 10 2174,4 24,6 _0,58 80 22 2178,5 21,4 0,41 50 9 2178,7 47,5 -0,4 20 60 2182,5 27,6 0,46 70 24 2200,3 47 0,5 50 0 2210,7 25,7 0,58 80 22 2212,9 46,3 -0,44 40 84 2221,1 40,7 -0,44 20 64 2223,5 22,6 0,41 50 9 2228,1 25,9 0,5 90 40 2233 31,1 -0,65 30 95 2257,2 46,6 -0,4 60 100 2258,9 33,6 0,62 100 38 2290,7 36,2 0,45 50 5 2291,1 21,9 0,45 50 5 2322,5 47,1 0,55 60 5 2334,2 41,2 - 0,45 50 5 2338,2 40,4 0,53 60 7 2367,7 43,2 -0.43 40 83 2375,2 36,5 0,42 80 38 2391,2 24,3 0,48 60 12 2409,1 41,9 0,49 90 41 2423,1 27,4 0,42 70 28 2426,5 38,5 0,49 80 31 2427,4 24 0,59 90 31 2429,9 39,3 -0,46 30 76 2432,2 38,3 0,76 90 14 2435 21,6 0,48 50 2 2438,3 526 0,46 60 14 2443,4 31,9 -0,44 40 84 2464 47,2 -0,52 10 62 2465 22,8 0,65 70 5 2473,4 41,9 0,51 60 9 2490,5 43 0,43 60 17 2490,7 26,7 0,42 70 28 2493,6 24,6 0,66 80 14 2529,2 41,4 -0,5 10 60 2536,6 24,8 0,51 60 9 2540,5 25,5 0,5 60 10 2542,6 42,1 0,41 50 9 2568,9 26,9 0,41 70 29 2570,5 57,1 -0,58 20 78 2573,7 16,3 0,51 60 9 2584 43,8 -0,67 30 97 2591,5 37,7 -0,4 10 50 2592,5 56,6 -0,42 20 62 2593,4 25 0,44 60 16 2608,6 37,6 0,43 90 47 2614,1 225 0,53 70 17 2619,7 22,9 0,47 50 3 WO 2007/082586 PCT/EP2006/050327 41 2621,4 25,8 0,48 60 12 2627,4 44,8 -0,41 50 91 2630,6 41,7 0,41 60 19 2646,7 21.9 0,53 60 7 26608 27,1 0,51 70 19 2677,6 23,6 0,5 60 10 2679,5 35 -0,5 50 100 2687,4 41,9 -0,4 60 100 2690,3 24,8 0,45 50 5 2713,2 41,3 -0,52 10 62 2720,6 39,5 0,47 50 3 2752,8 25,3 0,44 70 26 2767,4 31,4 -0,55 40 95 2780,4 28,3 0,46 60 14 2793,7 36,3 0,64 80 16 28254 36.5 -0,48 50 98 2830,9 _ 33,2 0,51 70 19 2841 37,1 -0,42 30 72 2854,4 43,8 -0.47 50 97 2883,6 28,9 0,63 80 17 2892,2 32,1 0,51 80 29 28985 42,3 -0,44 40 84 2902,9 42,1 -0,48 60 12 2911,7 36,8 -0,54 30 84 2918 42.2 -0,54 20 74 2937,1 26,6 0,51 60 9 2945,1 22,6 0,41 50 9 2973,7 34,9 -0,58 30 88 2978 26,3 -0,53 30 83 2986,9 47,3 -0,41 40 81 2990,4 33,6 -0,57 10 67 3012,1 39,4 -0,4 60 100 3017,7 46,8 -0,5 10 60 3022,8 33,8 -0,57 40 97 3038,1 __ 33,7 -0,51 30 81 3047,7 35,9 -0,49 30 79 3057.1 56,4 -0,54 30 84 3058,8 _ 35,5 -0,46 40 86 3080,2 31,7 -0,4 20 60 3098,8 42,6 -0,4 60 100 3108,8 44,7 -0,45 50 95 3121 .4 425 -0,5 50 100 3137 37 -0,53 30 83 3139,4 43,7 -0,58 20 78 3152,6 38,2 -0,4 60 100 3158 8 43,3 -0,51 40 91 3166,2 41,2 -0,43 50 93 3177,4 22,3 -0,52 20 72 3187,7 48,6 -0,41 40 81 3209,2 34,3 -0,67 30 97 3255,8 42,9 -0,64 20 84 3262 31,5 -0,46 40 86 3281 36,8 -0,78 20 98 3290,9 36,9 -0,53 40 93 WO 2007/082586 PCT/EP2006/050327 42 3293,2 54,2 -0,47 50 97 3295,8 38,4 -0,48 50 98 3303,2 38,6 -0,54 30 84 3308,6 21,3 0,57 60 3 3315,1 54,1 -0,61 10 71 3319,3 46,2 -0,45 50 95 3322,8 27,3 -0,48 30 78 3333,4 23,3 -0,68 20 88 3334,6 41,7 -0,56 30 86 3337,4 36,2 -0,58 30 88 3343,8 43,8 -0,61 30 91 3360,1 44,3 -0,4 60 100 3376.2 45,2 -0,47 50 97 3402,4 33,8 -0,48 50 98 3405,7 37,8 -0,58 40 98 3421,8 21,1 0,47 50 3 3422,5 38,7 -0,6 30 90 3436 26,4 -0,61 10 71 3503,3 23,2 .- 0,49 10 59 3530,9 36,8 -0,51 30 81 3547,3 38,5 -0,4 10 50 3583,3 25,2 -0,9 0 90 3589,5 39,1 -0,8 10 90 3631,2 33,1 -0,51 20 71 3634,9 42,6 -0,49 30 79 3682,4 42,8 -0,44 30 74 3686,1 32,6 -0,73 10 83 3697,4 38,8 -0,43 10 53 S3701,8 43,4 -0,62 10 72 3707 31,9 -0,76 0 76 37196 44,7 -0,43 40 83 3723,3 32,5 -0,77 20 97 3760,8 25,9 -0,49 20 69 3802,7 46,2 -0,47 10 57 3816,7 32,2 -0,56 10 66 3852,2 36,9 -0,41 40 81 3871,7 42,9 -0,54 10 64 3946,9 33,1 -0,63 30 93 3955,9 23,6 0,41 50 9 3969,6 31.3 -0,46 40 86 3987 30,5 -0,47 50 97 4026,2 30,5 -0,53 0 53 4044,7 31,2 -0,56_ 30 86 4055,2 24,1 0,54 70 16 4154,2 23,7 0,66 80 14 4170,6 46,1 -0,42 10 52 4241,2 24,4 0,66 80 14 4283,1 24,3 0,41 50 9 4306,5 41,4 -0,4 20 60 4335,8 27,1 0,43 50 7 4527,7 26 0,48 50 2 4594,6 20,6 0,45 50 5 4654,8 38,8 -0,42 10 52 4713,7 26,9 0,65 70 5 WO 2007/082586 PCT/EP2006/050327 43 4748,5 25,4 -0,45 50 95 4772,1 28,9 -0,42 10 52 4863,7 39,2 -0,51 20 71 5213,8 36,8 -0,4 10 50 5229,1 39,9 -0,52 0 52 5428.4 33,5 -0,44 30 74 5575,8 35,7 -0,52 10 62 5845,8 21,8 0,5 50 0 6171,5 39,6 -0,63 30 93 6212,.4 30,6 -0,49 10 59 6238,6 30,9 -0,56 20 76 7556,6 26,2 0,44 60 16 7885,4 209 0,45 50 5 8054,8 16,7 0,61 80 19 8341,2 16,6 0,53 60 7 8765,9 17,6 0,47 80 33 9076 23 0,5 60 10 9223,1 22,8 0,53 60 7 S9465,1 23.3 0,5 50 0 9868,8 29,5 -0,68 10 78 9933,5 18,4 0,47 50 3 10046,3 18.1 0,61 80 19 10518,8 20.9 0,51 70 19 Table 3: molecular migration discrimination frequency frequency FSGS MCD 830,5 25,3 0,49 80 31 865,4 35,5 0,43 80 38 907,4 27,5 0,41 60 19 1005,5 35 0,45 70 25 1008,5 34,4 -0,45 30 75 1015,6 38,2 0,47 60 13 1026,5 33,2 -0,4 10 50 1041,5 51,6 -0,42 20 63 1055,6 36,4 0,41 60 19 1085,6 50,8 -0,42 20 63 1088,6 37,4 0,49 80 31 1107,5 40,2 -0,45 30 75 1128,5 44,3 0,41 60 19 1138,6 22,9 -0,4 10 50 1160,6 48,8 -0,44 50 94 1191,6 50,5 -0,49 20 69 1199,6 31 . -0,63 0 63 1207,7 36,6 0,41 60 19 1208,6 38,6 0,41 60 19 1211,6 31,3 0,43 80 38 1224,7 33,6 -0,44 50 94 1270,6 25,7 0,41 60 19 1274,6, 50,7 -0,44 50 94 WO 2007/082586 PCT/EP2006/050327 44 1282,7 38,4 0,43 80 38 1294,6 54,4 0,45 70 25 1304,8 24,6 0,44 50 6 1305,9 33,4 0,51 70 19 1308,6 53,6 -0,45 30 75 1377,7 25,4 0,45 70 25 1390,7 41,1 0,4 90 50 1404,9 29,4 0,43 80 38 1493,7 33,7 0,51 70 19 1518,9 42,5 0,41 60 19 1581 37,8 -0,44 50 94 1594,8 54,8 -0,4 60 100 1607,7 41 0,41 60 19 1650,7 25,4 -0,46 10 56 1695,7 54,7 -0,4 10 50 1766,6 44,9 -0,41 40 81 1826,9 50,8 -0,59 10 69 1880,3 57,4 -0,42 20 63 1887,8 33,8 0,4 90 50 1900,7 30,4 -0,61 20 81 1925,3 52,5 0,59 90 31 1950,9 34,5 0,59 90 31 1992,9 48,5 0,44 50 6 2005,3 39,6 0,43 80 38 2011,5 42 -0,64 30 94 2048,2 33,1 -0,41 40 81 2063 24,3 0,41 60 19 2077,3 35,8 -0,59 10 69 2121 26,9 0,43 80 38 2163,4 27,6 0,51 70 19 2174,4 24,6 0,43 80 38 2258,9 33,6 0,75 100 25 2412,3 42,7 -0,42 20 63 2453,2 49,7 -0,42 20 63 2487,9 38 0,41 60 19 2570,5 57,1 -0,42 20 63 2679,5 35 -0,44 50 94 2690,3 24,8 0,5 50 0 2819,4 32,2 0,44 50 6 2864,7 29,1 -0,49 20 69 2883,6 28,9 0,55 80 25 2889,2 20,2 0,41 60 19 2918 42,2 -0,68 20 88 2986,9 47,3 -0,41 40 81 3209,2 34,3 -0,51 30 81 3255,8 42,9 -0,42 20 63 3315,1 54,1 -0,4 10 50 3402,4 33,8 -0,44 50 94 3583,3 25,2 -0,5 0 50 4335,8 27,1 0,44 50 6 9182 17,1 -0,42 20 63 WO 2007/082586 PCT/EP2006/050327 45 Table 4: molecular migration discrimination frequency [%] weight [Da] time [min] factor FSGS MGN 819,5 35,7 -0,47 20 67 909,4 40,3 -0,4 60 100 939,6 33,1 0,59 70 11 978,5 23,9 -0,4 10 50 1017,4 36,6 -0,43 40 83 1081,7 29,6 0,49 60 11 1201,5 51,6 0,43 60 17 1282,7 38,4 0,47 80 33 1284,8 55,1 -0,4 10 50 1305,9 33,4 0,42 70 28 1338,7 29,6 0,41 80 39 1341,8 33,1 -0,43 40 83 1359,5 47,4 0,53 70 17 1394,3 48,1 0,43 60 17 1403,8 34,4 0,43 60 17 1423,6 22,3 -0,47 20 67 1490,7 33,7 -0,47 20 67 1493,5 57 -0,46 10 56 1497,9 26,7 -0,48 30 78 1504,4 30,5 -0,42 30 72 1517,6 54,8 0,43 60 17 1526,4 39,4 -0,42 30 72 1529,5 32,4 0,43 60 17 1576,4 42,5 0,48 70 22 1591,7 51,2 0,44 100 56 1595,4 31 -0,48 30 78 1692,4 30,4 -0,41 20 61 1734,6 27,2 -0,48 30 78 1768,9 44,7 0,63 80 17 1790,8 38,8 0,4 90 50 1802,5 25,6 -0,42 30 72 1844,2 34,6 0,4 90 50 1883 29,1 0,44 50 6 1885,7 57,5 0,42 70 28 1900,7 30,4 -0,47 20 67 1920,5 46,1 0,49 60 11 1925,3 52,5 0,57 90 33 1933,9 32,8 0,44 50 6 1971,5 18,9 -0,47 20 67 1986,6 35,8 -0,42 30 72 2011,5 42 -0,42 30 72 2015,1 49,6 -0,42 30 72 2079,7 21,8 -0,51 10 61 2121 26,9 0,47 80 33 2129,5 35,1 0,43 60 17 2146,3 25,8 -0,4 60 100 2274 37 -0,4 10 50 2292,4 35,3 -0,48 30 78 WO 2007/082586 PCT/EP2006/050327 46 2312,5 22,9 -0,63 20 83 2338,2 40,4 0,43 60 17 2338,6 26 -0,49 40 89 2356,3 24 -0,43 40 83 2421 28,7 -0,44 50 94 2449,3 28,3 -0,53 30 83 2451,7 35,5 -0,43 40 83 2453,6 32 -0,53 30 83 2469,3 32,5 -0,51 10 61 2471,7 23,8 -0,42 30 72 2525,5 35,6 0,68 90 22 2566,4 22,2 -0,42 30 72 2591,5 37,7 -0,4 10 50 2607 47,6 0,48 70 22 2639,6 45,2 -0,46 10 56 2665,3 39,4 -0,49 40 89 2712,9 22,6 -0,42 30 72 2758,5 40,9 0,42 70 28 2912,9 57,5 -0,4 10 50 3041,2 45 0,41 80 39 3107,2 26,4 -0,4 10 50 3182,9 34,3 0,44 50 6 3313,8 31,6 -0,48 30 78 3479,3 48,5 0,53 70 17 4827,1 27,3 -0,43 40 83 5829,7 20,8 -0,41 20 61 8216,9 16,8 -0,4 10 50 8371,2 15,8 -0,41 20 61 8466,3 18 -0,51 10 61 8518,7 15,7 -0,48 30 78 8578,4 17 -0,47 20 67 9182 17,1 -0,69 20 89 Table 5 molecular migration discrimination frequency [% weight [Da] time [minm] factor FSGS MVCD + MGN 939,6 33,1 0,49 70 21 1282,7 38,4 0,45 80 35 1305,9 33,4 0,46 70 24 1359,5 47,4 0,44 70 26 1493,7 33,7 0,41 70 29 1650,7 25,4 -0,4 10 50 1734,6 27,2 -0,41 30 71 1900,7 30,4 -0,54 20 74 1925,3 52,5 0,58 90 32 2011,5 42 -0,52 30 82 2121 26,9 0,45 80 35 2258,9 33,6 0,41 100 59 WO 2007/082586 PCT/EP2006/050327 47 2312,5 22,9 -0,48 20 68 2449,3 28,3 -0,41 30 71 2525,5 35,6 0,49 90 41 2607 47,6 0,41 70 29 2690,3 24,8 0,41 50 9 2918 42,2 -0,51 20 71 9182 17,1 -0,56 20 76 Table 6: molecular Migration time discrimination frequency [%] weight [Da] [min] factor MCD control 836,5 35 0,59 75 16 862,4 48,7 0,44 56 12 866,4 37,9 0,41 56 16 866,5 23,1 0,55 56 2 870,4 33,9 0,43 50 7 876,4 48,9 -0,61 38 98 881,5 25,7 0,46 75 29 882,6 36,5 -0,64 31 95 888,6 29,9 -0,47 6 53 903,4 46,8 -0,49 6 55 914,5 34,3 0,47 50 3 925,4 50,7 0,61 75 14 943,5 30 0,47 75 28 950,5 36 0,51 56 5 956,4 49,5 -0,48 13 60 958,5 32,5 0,46 69 22 974,5 37,9 0,41 50 9 988,5 33,9 0,43 50 7 990,6 32 0,44 63 19 991,4 37,7 0,42 56 14 1000,5 34 -0,51 44 95 1006,4 35,7 -0,4 38 78 1010,6 50,8 -0,45 19 64 1010,6 30,6 -0,52 31 83 1033,6 39,1 0,41 50 9 1034,5 31,4 0,47 50 3 1046,6 38,6 -0,59 38 97 1047,6 30,4 -0,47 38 84 1085,6 50,8 0,49 63 14 1102,6 32,9 0,44 56 12 1104,6 43,3 -0,45 6 52 1108,6 29,8 0,42 81 40 1110,4 46,9 -0,46 25 71 1122,5 50,2 -0,41 25 66 1135,6 42,7 -0,53 13 66 1138,6 39,3 0,7 88 17 1138,6 22,9 0,48 50 2 1139,6 32,2 0,49 56 7 1141,6 38 -0,61 6 67 1159,6 39 -0,56 25 81 1171,6 32,8 0,8 81 2 1182,6 47,2 -0,41 25 66 1191,8 18,3 0,46 56 10 WO 2007/082586 PCT/EP2006/050327 48 1199,6 31 0,61 63 2 1203,7 24,7 -0,51 6 57 1219,6 37,3 0,48 69 21 1223,5 51,6 -0,65 25 90 1233,7 49,6 0,45 50 5 1237,7 41,6 -0,42 25 67 1246,7 30,5 -0,41 25 66 1256,6 53,4 0,49 63 14 1264,7 26,7 0,66 75 9 1268,6 53,7 -0,45 6 52 1269,7 39,8 0,44 63 19 1270,5 52,5 -0,49 6 55 1274,6 50,7 0,49 94 45 1280,6 51,9 -0,5 13 62 1292,5 53 -0,49 38 86 1296,6 53,8 0,53 56 3 1302,7 31,8 0,55 88 33 1310,7 36,8 0,41 56 16 1311,8 31,5 0,44 63 19 1324,2 40,5 0,6 69 9 1324,5 54,3 0,45 63 17 1325,5 35,2 0,55 81 26 1333,8 38,8 0,52 69 17 1338,7 47,2 0,86 88 2 1338,7 29,6 0,52 63 10 1350,7 50,3 -0,44 6 50 1354,8 45,6 0,62 100 38 1365 22,3 0,49 63 14 1371,8 19,3 0,49 75 26 1389,8 19,5 0,41 75 34 1401,8 46,2 -0,5 13 62 1414,6 38,1 0,57 81 24 1415,7 33,3 0,51 56 5 1424,9 35,4 -0,52 19 71 1442,8 33,3 0,61 81 21 1444,6 37,8 0,46 75 29 1448,8 30,3 0,42 75 33 1472,1 31,2 0,42 56 14 1474,9 16,9 0,63 75 12 1482 30,4 0,47 75 28 1484 30,4 0,5 81 31 1486,5 30,6 0,61 81 21 1499,9 30,6 0,53 88 34 1502,8 28,8 0,5 81 31 1502,9 16,8 0,55 56 2 1508,9 16,8 0,54 63 9 1511,7 38,4 0,7 94 24 1535 28,3 0,57 69 12 1548,3 31,1 0,44 88 43 1556,8 33,7 0,52 81 29 1561,9 28,1 0,46 88 41 1567,6 53,9 -0,55 0 55 1573,8 40,4 0,43 88 45 1574,3 53,4 -0,41 13 53 1588,4 47,9 -0,6 13 72 1591,6 32,6 0,49 56 7 1596,9 34 0,53 75 22 1604,3 21,6 0,55 69 14 1611,7 53,2 -0,41 44 84 WO 2007/082586 PCT/EP2006/050327 49 1612,8 36,8 0,55 88 33 1622 19,2 0,42 81 40 1629,6 49,6 0,47 50 3 1635,2 27,8 0,41 75 34 1644 18,8 0,41 50 9 1658,4 39 0,44 88 43 1669,9 33,4 0,48 69 21 1671,3 42,6 0,42 56 14 1676 25,3 0,44 56 12 1681,6 40 0,56 88 31 1686,8 38,2 0,63 88 24 1692,4 30,4 0,41 56 16 1699,1 41,9 0,63 88 24 1718,5 22,6 0,48 56 9 1746,2 46,2 -0,53 31 84 1747,7 50,8 -0,51 6 57 1751,4 40,8 0,43 81 38 1752,9 39,9 0,46 69 22 1766,6 44,9 0,52 81 29 1776,1 43,6 -0,45 38 83 1777,6 28,6 0,58 75 17 1804,7 34 0,45 100 55 1811,3 31,3 0,5 88 38 1813,4 54,7 -0,53 0 53 1815,2 27,7 0,41 56 16 1820,1 31,8 0,44 88 43 1821,2 18,2 0,45 50 5 1822,9 40,7 -0,52 31 83 1824,3 37 -0,42 38 79 1831,9 41,5 0,54 63 9 1847,8 57 -0,62 31 93 1851,2 31,6 0,43 81 38 1853 31,2 0,4 63 22 1854,9 53,6 -0,44 6 50 1856,8 56,3 -0,44 25 69 1864,6 28,6 0,64 81 17 1867 31,8 0,56 88 31 1889,8 46,4 -0,53 44 97 1894,9 22 0,56 75 19 1896,8 53,3 -0,43 13 55 1909,7 47,9 0,49 63 14 1913,4 30,1 0,46 56 10 1916,8 44,7 -0,59 6 66 1934,2 16,1 0,48 50 2 1944,2 47 -0,61 25 86 1951,1 53 -0,45 19 64 1955,3 48,4 0,44 63 19 1966,3 25,1 0,65 75 10 1973,7 57,1 -0,46 13 59 1982,9 32,2 0,57 81 24 1989,3 43,7 0,66 81 16 1990,8 47,3 -0,7 13 83 2011,5 42 0,64 94 29 2017,6 33,2 0,45 81 36 2030,4 31,7 -0,44 38 81 2030,8 46,5 -0,61 25 86 2047 45,4 -0,42 56 98 2050,8 38,2 0,47 81 34 2092,5 41,3 0,66 81 16 WO 2007/082586 PCT/EP2006/050327 50 2098,3 52 0,5 69 19 2099,2 36,9 0,49 75 26 2103,6 26,7 0,44 88 43 2106,1 46,1 0,41 56 16 2117,1 57,1 -0,4 38 78 2129,5 35,1 -0,47 50 97 2130,3 18,4 0,42 56 14 2139,3 36,9 0,41 56 16 2146,3 25,8 0,59 63 3 2151,6 42,6 0,44 56 12 2157,2 24,4 0,54 63 9 2182,5 27,6 0,51 75 24 2189,1 40,9 -0,48 19 67 2207,2 41,9 0,48 69 21 2210,7 25,7 0,59 81 22 2217,7 41,9 0,53 88 34 2223,5 22,6 0,54 63 9 2228,1 25,9 0,48 88 40 2238,4 46,3 -0,41 44 84 2281,7 45,6 -0,5 31 81 2426,5 38,5 0,56 88 31 2432,2 38,3 0,55 69 14 2464 47,2 -0,5 13 62 2465 22,8 0,51 56 5 2522,9 24,4 0,42 63 21 2529,2 41,4 -0,42 19 60 2535 37,7 0,42 81 40 2540,5 25,5 0,58 69 10 2548,2 35,1 -0,45 38 83 2566,4 22,2 0,49 56 7 2593,4 25 0,41 56 16 2621,4 25,8 0,5 63 12 2644,1 32,5 -0,43 50 93 2698,4 32,1 -0,48 31 79 2713,2 41,3 -0,43 19 62 2752,8 25,3 0,49 75 26 2790,3 26,8 0,41 56 16 2793,7 36,3 0,66 81 16 2809,1 37,2 -0,46 31 78 2921,4 30,4 0,43 69 26 2933,8 39,4 -0,47 6 53 2973,7 34,9 -0,5 38 88 3007,5 30,5 -0,48 19 67 3017,7 46,8 -0,42 19 60 3139,4 43,7 -0,4 38 78 3179,2 44,3 0,41 75 34 3262 31,5 -0,49 38 86 3281 36,8 -0,48 50 98 3282 49,4 -0,45 50 95 3290,9 36,9 -0,56 38 93 3295,8 38,4 -0,48 50 98 3333,4 23,3 -0,5 38 88 3334,6 41,7 -0,42 44 86 3343,8 43,8 -0,41 50 91 3433,3 44,5 -0,42 56 98 3530,9 36,8 -0,5 31 81 3589,5 39,1 -0,58 31 90 3631,2 33,1 -0,52 19 71 3686,1 32,6 -0,7 13 83 WO 2007/082586 PCT/EP2006/050327 51 3697,4 38,8 -0,41 13 53 3701,8 43,4 -0,54 19 72 3707 31,9 -0,63 13 76 3723,3 32,5 -0,47 50 97 3760,8 25,9 -0,5 19 69 3816,7 32,2 -0,47 19 66 4154,2 23,7 0,42 56 14 4170,6 46,1 -0,45 6 52 4241,2 24,4 0,67 81 14 4283,1 24,3 0,54 63 9 4707,5 20,5 0,42 56 14 4713,7 26,9 0,45 50 5 4748,5 25,4 -0,57 38 95 4772,1 28,9 -0,45 6 52 5213,8 36,8 -0,44 6 50 7409,9 26,2 0,44 56 12 7556,6 26,2 0,53 69 16 8054,8 16,7 0,5 69 19 8765,9 17,6 0,48 81 33 9076 23 0,58 69 10 9182 17,1 0,54 63 9 9223,1 22,8 0,56 63 7 9868,8 29,5 -0,53 25 78 10046,3 18,1 0,62 81 19 10390,1 20,2 0,5 63 12 10518,8 20,9 0,62 81 19 Table 7: molecular migration time discrimination frequency [%] weight [Da] [min] factor MCD MGN 814,5 28,8 -0,46 38 83 819,5 35,7 -0,48 19 67 856,5 28,9 0,42 75 33 863,4 28,8 -0,54 13 67 864,5 37,3 -0,48 19 67 879,6 26,9 0,72 94 22 882,6 36,5 -0,41 31 72 909,4 40,3 -0,56 44 100 928,4 49,4 0,53 81 28 934,5 33,9 -0,41 31 72 935,6 36,6 0,46 63 17 946,5 46,8 0,47 69 22 952,5 32 -0,46 38 83 1005,5 35 -0,42 25 67 1008,5 34,4 0,53 75 22 1015,6 38,2 -0,71 13 83 1017,4 36,6 -0,52 31 83 1022,5 39,1 -0,52 31 83 1028,6 37,8 0,47 69 22 1073,6 34,7 -0,56 44 100 1085,6 50,8 0,51 63 11 1108,5 50,1 0,45 56 11 1113,6 33,7 -0,48 19 67 1138,6 22,9 0,44 50 6 1147,6 49,7 0,46 63 17 1152,5 40,7 -0,65 19 83 1208,6 38,6 -0,42 19 61 WO 2007/082586 PCT/EP2006/050327 52 1211,6 31,3 -0,46 38 83 1213,6 50 -0,43 13 56 1224,7 33,6 0,8 94 33 1225,7 41,3 -0,42 25 67 1270,6 25,7 -0,48 19 67 1277,6 50 0,46 63 17 1279,7 38,3 -0,63 31 94 1283,9 28,9 -0,48 19 67 1301,7 34 -0,43 13 56 1319,9 34,8 -0,46 38 83 1329,8 37,5 -0,47 25 72 1337,6 52 0,47 69 22 1341,8 33,1 -0,58 25 83 1350,8 26,8 -0,42 19 61 1365 22,3 0,4 63 22 1381,1 32,3 -0,63 31 94 1398,9 30,5 -0,44 50 94 1404,9 29,4 -0,63 38 100 1423,6 22,3 -0,48 19 67 1426,8 38,7 -0,42 25 67 1433 33,7 -0,53 19 72 1465,9 28,8 -0,45 44 89 1482,8 36,3 -0,46 38 83 1487,7 41,4 0,54 88 33 1490,7 33,7 -0,48 19 67 1512,8 35,9 0,41 69 28 1527,9 34,7 -0,44 50 94 1543,8 34,9 -0,52 31 83 1558,1 23,4 -0,42 19 61 1560,5 39,5 -0,46 38 83 1569,8 48,3 0,5 50 0 1574,8 33,9 -0,58 31 89 1593,8 36,7 0,41 69 28 1595,4 31 -0,4 38 78 1602,8 58,1 0,51 63 11 1605,9 23,7 -0,65 13 78 1607,7 41 -0,42 19 61 1612,8 26,3 -0,43 13 56 1623,3 41,4 -0,47 31 78 1671,3 42,6 0,45 56 11 1726 36,3 -0,51 44 94 1729,2 26 -0,45 44 89 1744,1 34,3 -0,63 38 100 1768,9 44,7 0,52 69 17 1774,6 36,5 -0,47 31 78 1786,9 35,9 -0,41 31 72 1799 28,8 -0,47 25 72 1802,5 25,6 -0,53 19 72 1826,9 50,8 0,52 69 17 1839,1 35,5 -0,44 50 94 1857,1 39 -0,44 50 94 1859,4 22,8 -0,42 25 67 1863,8 57,5 0,42 81 39 1876,2 40,1 -0,51 38 89 1878,7 49,9 0,47 75 28 1880,3 57,4 0,51 63 11 1883 29,1 0,44 50 6 1885,7 57,5 0,47 75 28 1887,8 33,8 -0,5 50 100 WO 2007/082586 PCT/EP2006/050327 53 1898,7 26,5 -0,52 31 83 1924,2 32,9 -0,64 25 89 1933,9 32,8 0,57 63 6 1936,7 32,8 -0,44 56 100 1949,1 38,5 0,43 88 44 1950,9 34,5 -0,58 31 89 1971,5 18,9 -0,48 19 67 1977,4 42,9 0,4 63 22 1988,9 28,8 -0,4 38 78 2005,3 39,6 -0,46 38 83 2011,3 29 -0,43 13 56 2033,5 27,5 -0,53 25 78 2035,6 30,9 -0,54 13 67 2065,3 20,9 -0,47 25 72 2077,3 35,8 0,41 69 28 2109,3 27,9 -0,51 44 94 2140,1 26,8 -0,51 38 89 2152,7 29,5 -0,51 44 94 2160,4 27,9 -0,49 6 56 2163,4 27,6 -0,48 19 67 2167,3 27,8 -0,41 31 72 2174,4 24,6 -0,51 38 89 2178,5 21,4 -0,4 38 78 2189,1 40,9 -0,48 19 67 2258,9 33,6 -0,64 25 89 2274 37 -0,44 6 50 2288,8 41,4 -0,65 13 78 2291,1 21,9 -0,47 25 72 2292,4 35,3 -0,4 38 78 2308,9 26,2 -0,46 38 83 2332,4 35,4 -0,54 13 67 2341,2 26,3 -0,49 6 56 2356,3 24 -0,46 38 83 2367,7 43,2 0,58 75 17 2380 39,6 -0,51 44 94 2391,2 24,3 -0,44 50 94 2423,1 27,4 -0,45 44 89 2434,4 34,7 -0,44 6 50 2446,2 24,7 -0,42 19 61 2451,7 35,5 -0,46 38 83 2453,6 32 -0,52 31 83 2453,8 20,4 -0,49 6 56 2455,6 27,7 -0,41 31 72 2461,1 40,5 -0,47 25 72 2469,3 32,5 -0,42 19 61 2471,7 23,8 -0,41 31 72 2475,5 22,3 -0,42 19 61 2480,2 47,2 0,4 63 22 2483,8 19,6 -0,47 25 72 2493,6 24,6 -0,5 50 100 2500,3 30,4 0,53 75 22 2518,7 38,9 -0,46 38 83 2521,3 48,3 -0,49 13 61 2525,5 35,6 0,4 63 22 2527,3 40,8 -0,53 19 72 2553,7 24,7 __-0,42 19 61 2573,7 16,3 -0,45 44 89 2579,5 15,2 -0,48 19 67 2608,6 57,7 0,45 56 11 WO 2007/082586 PCT/EP2006/050327 54 2614,1 22,5 -0,47 31 78 2619,6 38,3 -0,42 19 61 2642,4 40,9 0,46 63 17 2660,8 27,1 -0,47 31 78 2665,3 39,4 -0,58 31 89 2666 23 -0,43 13 56 2677,6 23,6 -0,51 44 94 2701 34,8 0,4 63 22 2784,3 45,2 -0,59 19 78 2825,4 36,5 0,49 88 39 2830,9 33,2 -0,57 38 94 2864,7 29,1 0,52 69 17 2889,2 20,2 -0,42 19 61 2902,9 42,1 -0,42 25 67 2912,9 57,5 -0,44 6 50 2921,4 30,4 0,52 69 17 2940,5 40,4 -0,4 38 78 3041,2 45 0,42 81 39 3044,8 48,6 0,4 63 22 3082,3 43,1 0,42 75 33 3169 37,5 0,42 75 33 3205,8 28,3 0,53 75 22 3209,2 34,3 0,48 81 33 3255,8 42,9 0,4 63 22 3256,3 23,1 -0,48 19 67 3303,2 38,6 0,44 50 6 3308,6 21,3 -0,47 31 78 3313,8 31,6 -0,53 25 78 3325,5 43,5 0,44 50 6 3336,8-- 53,8 0,51 56 6 3405,7 37,8 0,46 63 17 3422,5 38,7 0,45 56 11 3479,3 48,5 0,58 75 17 3578,2 32,5 -0,53 19 72 3881,9 26,2 -0,42 19 61 3969,6 31,3 . 0,45 56 11 4183,7 26,6 -0,47 31 78 4290,8 41,1 0,4 63 22 4527,7 26 -0,53 19 72 4565,8 25,1 -0,44 6 50 4719,5 39,3 -0,44 6 50 4827,1 27,3 -0,58 25 83 5112,9 33,1 -0,5 0 50 5829,7 20,8 -0,49 13 61 6106,5 27 -0,56 0 56 7885,4 20,9 -0,49 13 61 8341,2 16,6 -0,57 38 94 8371,2 15,8 -0,49 13 61 8466,3 18 -0,42 19 61 8518,7 15,7 -0,53 25 78 _8578,4 17 -0,48 19 67 9335,5 17,5 -0,41 31 72 9465,1 23,3 -0,49 13 61 9944,2 16,7 -0,48 19 67 10949,7 26,3 -0,56 0 56 WO 2007/082586 PCT/EP2006/050327 55 Table 8: molecular migration time discrimination frec uency [%] weight [Da] [min] factor MCD FSGS + MGN 863,4 28,8 -0,45 13 57 879,6 26,9 0,58 94 36 909,4 40,3 -0,42 44 86 928,4 49,4 0,46 81 36 935,6 36,6 0,41 63 21 946,5 46,8 0,44 69 25 952,5 32 -0,41 38 79 1005,5 35 -0,43 25 68 1008,5 34,4 0,5 75 25 1015,6 38,2 -0,63 13 75 1022,5 39,1 -0,44 31 75 1028,6 37,8 0,4 69 29 1073,6 34,7 -0,49 44 93 1085,6 50,8 0,48 63 14 1138,6 22,9 0,43 50 7 1147,6 49,7 0,41 63 21 1152,5 40,7 -0,53 19 71 1199,6 31 0,41 63 21 1208,6 38,6 -0,42 19 61 1211,6 31,3 -0,45 38 82 1224,7 33,6 0,54 94 39 1270,6 25,7 -0,46 19 64 1279,7 38,3 -0,51 31 82 1341,8 33,1 -0,43 25 68 1381,1 32,3 -0,54 31 86 1404,9 29,4 -0,55 38 93 1433 33,7 -0,46 19 64 1487,7 41,4 0,48 88 39 1543,8 34,9 -0,44 31 75 1560,5 39,5 -0,41 38 79 1569,8 48,3 0,43 50 7 1574,8 33,9 -0,47 31 79 1602,8 58,1 0,41 63 21 1605,9 23,7 -0,52 13 64 1607,7 41 -0,42 19 61 1623,3 41,4 -0,44 31 75 1726 36,3 -0,42 44 86 1729,2 26 -0,42 44 86 1744,1 34,3 -0,52 38 89 1786,9 35,9 -0,4 31 71 1826,9 50,8 0,54 69 14 1876,2 40,1 -0,41 38 79 1880,3 57,4 0,48 63 14 1887,8 33,8 -0,46 50 96 1898,7 26,5 -0,44 31 75 1924,2 32,9 -0,54 25 79 1933,9 32,8 0,41 63 21 1950,9 34,5 -0,58 31 89 2005,3 39,6 -0,45 38 82 2033,5 27,5 -0,46 25 71 2035,6 30,9 -0,48 13 61 2065,3 20,9 -0,43 25 68 2077,3 35,8 0,47 69 21 2140,1 26,8 -0,41 38 79 2152,7 29,5 -0,42 44 86 2163,4 27,6 -0,49 19 68 WO 2007/082586 PCT/EP2006/050327 56 2174,4 24,6 -0,48 38 86 2189,1 40,9 -0,42 19 61 2258,9 33,6 -0,68 25 93 2288,8 41,4 -0,55 13 68 2332,4 35,4 -0,45 13 57 2367,7 43,2 0,5 75 25 2493,6 24,6 -0,43 50 93 2500,3 30,4 0,43 75 32 2527,3 40,8 -0,42 19 61 2614,1 22,5 -0,44 31 75 2660,8 27,1 -0,44 31 75 2665,3 39,4 -0,4 31 71 2784,3 45,2 -0,46 19 64 2825,4 36,5 0,45 88 43 2830,9 33,2 -0,48 38 86 2864,7 29,1 0,51 69 18 2883,6 28,9 -0,43 25 68 2889,2 20,2 -0,42 19 61 2918 42,2 0,45 88 43 2921,4 30,4 0,47 69 21 3205,8 28,3 0,43 75 32 3209,2 34,3 0,49 81 32 3255,8 42,9 0,41 63 21 3308,6 21,3 -0,4 31 71 3402,4 33,8 0,4 94 54 3578,2 32,5 -0,46 19 64 3583,3 25,2 0,43 50 7 4527,7 26 -0,46 19 64 4827,1 27,3 -0,43 25 68 7885,4 20,9 -0,45 13 57 8341,2 16,6 -0,45 38 82 9465,1 23,3 -0,45 13 57 Table 9: molecular weight Migration time discrimination frequency [% IDal [minl factor MGN control 803,4 35,2 0,4 56 16 814,5 28,8 0,59 83 24 815,5 30,9 -0,45 17 62 819,5 35,7 0,63 .67 3 830,5 25,3 0,49 61 12 836,5 35 0,73 89 16 844,5 309 0,61 61 0 847,5 359 0,44 61 17 862,4 48,7 0,55 67 12 863,4 28,8 0,67 67 0 864,5 37,3 0,65 67 2 866,4 37,9 0,79 94 16 870,4 33,9 0,49 56 7 873,5 38,3 0,45 50 5 874,4 49,7 0,58 61 3 874,5 29,7 0,6 89 29 WO 2007/082586 PCT/EP2006/050327 57 879,6 26,9 -0,74 22 97 881,525,7 0,48 78 29 903,4 46,8 -0,44 11 55 907,4 27,5 0,47 50 3 909 40,3 0,97 100 3 925,4 .. 50,7 .0,7 83 14 926,5 36,1 -0,48 28 76 928,4 49,4 -0,57 28 84 929,5 39,9 -0,46 33 79 934,5 33,9 0,52 72 21 9375 41,7 0,48 100 52 943,5 30 0,61 89 28 946,5 46,8 -0,62 22 84 950,5 36 0,61 67 5 952,5 32 0,71 83 12 956,4 49,5 -0,6 0 60 968,6 30,5 0,43 56 12 978,5 35 0,7 72 2 978,5 23,9 0,48 50 2 980,6 34,6 -0,43 44 88 981,6 37,4 -0,41 56 97 982,5 31,9 0,56 67 10 983,5 35,1 0,58 72 14 986,5 30,3 0,54 61 7 987,4 45,1 0,54 56 2 988,5 33,9 0,49 56 7 988,6 49,9 -0,57 0 57 990,6 32 0,42 61 19 991,4 37,7 0,47 61 14 994,5 33,3 0,7 94 24 995,6 36,4 0,61 83 22 998,5 35,8 0,42 56 14 1000,5 . 34 -0,67 28 95 1005,5 35 0,51 67 16 1006,4 35,7 -0,5 28 78 1008,5 34,4 . -0,71 22 93 1010,6 50,8 -0,58 6 64 10130,6 3 6 -0,66 17 83 10134 39,3 -0,52 0 52 1015,6 38,2 0,78 83 5 1017,4 36,6 0,63 83 21 1022,5 39,1 0,61 83 22 1028,6 37,8 -0,76 22 98 1033,6 39,1 0,75 83 9 1038,6 34,4 0,58 72 14 10466 38,6 -0,91 6 97 1047,6 30,4 -0,46 39 84 1049,5 39,9 ..... 0,56 61 5 1051,5 36,2 -0,47 17 64 S1055,6 36,4 0,41 50 9 1058,6 21,5 0,56 56 0 1060,6 - 32.. 0,55 94 40 WO 2007/082586 PCT/EP2006/050327 58 1071,5 38,7 0,54 56 2 1073,6 34,7 0,84 100 16 1075,6 29 -0,47 17 64 1081,7 29,6 -0,41 11 52 1090,5 36,2 0,56 83 28 1106,5 37,2 0,44 89 45 11 08,6 29,8 055 94 40 1109,6 34,9 -0,54 11 66 1110, 46,9 -0,6 11 71 1113,6 33,7 0,55 67 12 1114,5 37,4 -0,48 6 53 11216 42,3 -0,51 11 62 1122,5 50,2 -0,43 22 66 1131,7 34,9 0,41 67 26 1132,6 36,7 -0,45 44 90 1134,7 16,9 0,48 50 2 1135,6 42,7 -0,66 0 66 1136,6 31,6 0,43 56 12 1139,6 32,2 0,54 61 7 1141,6 38 -0,62 6 67 1150,6 35,8 0,46 94 48 1152,5 40,7 0,7 83 14 1157.6 28,5 0,6 89 29 1159,6 39 -0,75 6 81 1163,7 38,1 0,58 61 3 1171,6 32,8 0,59 61 2 1181,6 37,8 0,48 89 41 1186,6 32 0,51 83 33 1191,6 50,5 -0,41 50 91 1191,8 18,3 0,67 78 10 1198,8 29,2 0,63 94 31 1199,3 49,9 -0,46 6 52 1203,7 24.7 -0, 57 0 57 1211,6 31,3 0,68 83 16 1212,7 30,6 0,75 83 9 1219,6 37,3 0,63 83 21 1220,6 30,2 0,51 83 33 1223,5 51,6 -0,67 22 90 1224,7 33,6 -0,67 33 100 1225,7 41,3 0,61 67 5 1226,7 41,6 0,47 50 3 1235,6 41,4 -0,5 50 100 1236,7 34,8 0,41 67 26 1237,7 41,6 -0,56 11 67 1246,7 30,5 -0,54 11 66 1254,8 52,4 -0,44 33 78 1264,6 45,9 0,52 61 9 1268,6 53,7 -0,46 6 52 1269.7 39,8 0,42 61 19 1270,5 52,5 -0,5 6 55 1270,6 25,7 0,61 67 5 1273,8 24,8 0,54 6 7 WO 2007/082586 PCT/EP2006/050327 59 1274,6 38 0,42 56 14 1277,6 50 -0,45 17 62 1279,7 38,3 0,79 94 16 1280,6 51,9 -0,57 6 62 1283,9 28,9 0,61 67 5 1286 30,7 0,57 100 43 1292,5 53 -0,64 22 86 1297,6 38,7 0,53 94 41 1302,7 31,8 0,51 83 33 1303,6 40,7 -0,55 0 55 1308,6 53,6 -0,4 44 84 1311,8 31,5 0,75 94 19 1319,9 34,8 0,64 83 19 1321,9 41,1 -0,5 50 100 1324,2 40,5 0,52 61 9 1325,5 35,2 0,57 83 26 1331,7 35,4 -0,48 11 59 1333,8 38,8 0,77 94 17 1335.4 53,4 -0,52 0 52 1335,7 39,2 0,72 94 22 1338,7 47,2 0,76 78 2 1341,8 33,1 0,68 83 16 1350,7 50,3 -0,5 0 50 1350,8 26,8 0,46 61 16 1353,7 39,3 -0,51 39 90 1354,8 45,6 0,51 89 38 1355,7 36,3 0,4 56 16 1367,7 26,2 0,41 50 9 1370,8 33 0,41 50 9 13__71,7 39,9 0,74 78 3 1371,8 19,3 0,74 100 26 1374,8 42,1 0,43 56 12 1377,7 25,4 0,52 56 3 1378,5 45,4 -0,41 56 97 1381,1 32,3 0,58 94 36 1386 24,4 0,47 56 9 1389,8 19,5 0,54 89 34 1390,7 41,1 0,42 61 19 1395,5 25,4 0,43 50 7 1397,8 36,1 0,45 56 10 1398,9 30,5 0,81 94 14 1401,8 46,2 -0,51 11 62 1404,9 29,4 0,53 100 47 1405,9 17,3 0,62 72 10 1408,9 268_ 0,56 67 10 1414,6 38,1 0,59 83 24 1415,7 33,3 0,45 50 5 1419,8 39,7 0,6 89 29 1423,6 22,3 0,61 67 5 1424,9 18,5 0,55 67 12 14268 38,7 0,58 67 9 1433 33,7 0,46 72 2G WO 2007/082586 PCT/EP2006/050327 60 1439,6 25,4 0,41 50 9 1439,7 38,1 0,41 89 48 1442,8 33,3 0,63 83 21 1444,6 37,8 0,54 83 29 14488 30,3 0,45 78 33 1453,1 27,1 0,51 61 10 1462,7 53,6 -0,48 50 98 1465,9 28,8 0,82 89 7 1472,1 31,2 0,75 89 14 1473,6 30,3 0,41 67 26 1474,9 16,9 0,71 83 12 1482 -30,4 0,72 100 28 1482,8 36,3 0,47 83 36 1484 30,4 0,69 100 31 1487,7 41,4 -0,58 33 91 1493,5 57 0,56 56 0 1497,9 26,7 0,57 78 21 1498,7 34,9 0,7 83 14 1499,9 30,6 0,6 94 34 1501,1 29,5 0,5 56 5 1502,8 28,8 0,41 72 31 1502,9 16,8 0,76 78 2 1504,4 30,5 0,41 72 31 1508,9 16,8 0,41 50 9 1510,1 39,5 0,48 89 41 1511,7 38,4 0,43 67 24 1518 26,8 0,46 94 48 1520,7 27,9 0,64 83 19 1522,5 26,4 0,42 61 19 1527,9 34,7 0,65 94 29 1529,7 54,1 -0,62 22 84 1535 28,3 0,6 72 12 1537,9 31,5 0,56 83 28 1539,4 28,7 0,49 89 40 1540,7 29,8 0,68 83 16 1542,5 27,2 0,49 61 12 1543,8 34,9 0,54 83 29 1548,3 31,1 0,46 89 43 1552,3 35,5 0,41 100 59 1556,8 33,7 0,71 100 29 1558,1 23,4 0,52 61 9 1567 31,9 0,59 100 41 1567,6 53,9 -0,5 6 55 1568,6 34,3 0,54 83 29 1573,8 40,4 0,5 94 45 1574,3 53,4 -0,42 11 53 1574,8 33,9 0,68 89 21 1576,4 42,5 -0,62 22 84 1578 52,5 -0,48 50 98 1582,9 27,8 0,67 78 10 1588,4 47,9 -0,61 11 72 1589,7 54,3 -0,46 WO 2007/082586 PCT/EP2006/050327 61 1595,4 31 0,61 78 17 1596,9 34 0,78 100 22 1604,3 21,6 0,42 56 14 1604,7 38,1 0,41 72 31 1605,7 53,3 -0,46 28 74 1605,9 23,7 0,74 78 3 1607,7 41 0,49 61 12 1611,7 53,2 -0,51 33 84 1612,8 36,8 0,67 100 33 1612,8 26,3 052 56 3 1613,9 36,3 -0,46 39 84 1617,9 44,8 -0,4 44 84 1619,7 53,9 -0,45 17 62 1622 19,2 0,55 94 40 1629,5 32 0,42 61 19 1633,8 24,6 0,62 94 33 1635,2 27,8 0,43 78 34 1644 18,8 0,52 61 9 1652,3 286 0,6 100 40 1665 27,5 0,45 50 5 1666,3 23,3 0,48 89 41 1669,9 33,4 0,57 78 21 1676 253 0,66 78 12 1681,6 40 0,41 72 31 1686,8 38,2 0,7 94 24 1690,8 25,5 0,63 94 31 1692,4 30,4 0,46 61 16 1695,1 23,6 0,43 56 12 1699,1 41,9 0,7 94 24 1702,9 24,5 0,42 56 14 1706,8 21,5 0,51 67 16 1711 43,3 -0,54 11 66 1713,4 24,6 0,42 61 19 1718,5 22,6 0,75 83 9 1723,3 26,5 0,49 67 17 1726 36,3 0,86 94 9 1729,2 26 0,75 89 14 1732 51,6 -0,44 33 78 1734,6 27,2 0,47 78 31 1739,8 35,7 0,48 89 41 1744,1 34,3 0,67 100 33 1746,2 46,2 -0,68 17 84 1747,7 50,8 -0,57 0 57 1752,9 39,9 0,44 67 22 1763 24,4 0,72 94 22 1768,9 44,7 -0,63 17 79 1770,4 45,4 0,46 94 48 1772,6 28,5 0,4 56 16 1774,6 36,5 0,61 78 17 1782,1 33 0,43 94 52 1786,9 35,9 0,55 72 17 1788,6 31 0,42 83 41 WO 2007/082586 PCT/EP2006/050327 62 1791 25 0,58 67 9 1792 25,1 0,4 56 16 1793,6 28,3 0,67 72 5 1802,5 25,6 0,53 72 19 1804,7 34 0,45 100 55 1808,1 45,6 0,56 61 5 1810,1 31,8 0,64 83 19 1811,3 31,3 0,62 100 38 1813,4 54,7 -0,42 11 53 1815,2 27,7 0,62 78 16 1819,9 24,1 0,7 83 14 1820,1 31,8 0,46 89 43 1821,2 18,2 0,61 67 5 1822,9 40,7 -0,61 22 83 1824,3 37 -0,57 22 79 1826,1 21,8 0,64 78 14 1831,9 41,5 0,41 50 9 1833,5 20,4 0,48 50 2 1837,6 38,2 0,41 72 31 1839,1 35,5 0,58 94 36 1847,8 57 -0,65 28 93 1849,6 37,2 -0,48 33 81 1851,2 31,6 0,51 89 38 1853 31,2 0,78 100 22 1853,6 46,7 0,47 50 3 1854,2 28,8 0,54 61 7 1856,8 56,3 -0,52 17 69 1857,1 39 0,65 94 29 1859,4 22,8 0,63 67 3 1860,3 25,9 0,4 56 16 1863,8 57,5 -0,54 39 93 1864,6 28,6 0,77 94 17 1867 31,8 0,69 100 31 1870,4 30,4 0,46 94 48 1870,5 16,1 0,45 50 5 1876,2 40,1 0,65 89 24 1878,7 49,9 -0,52 28 79 1878,9 30,2 0,41 72 31 1880,3 57,4 -0,44 11 55 1883 29,1 -0,75 6 81 1885,7 57,5 -0,67 28 95 1887,8 33,8 0,48 100 52 1889,8 46,4 -0,58 39 97 1891,6 32,3 0,72 94 22 1894,9 22 0,75. 94 19 1894,9 56 -0,43 22 66 1896,8 53,3 -0,5 6 55 1898,7 26,5 0,7 83 14 1904 27,5 0.59 61 2 1913,4 30,1 0,51 61 10 1913,9 53,9 -0,4 39 79 1916, 44,7-0,49 17 6 WO 2007/082586 PCT/EP2006/050327 63 1920,7 _30, 0,55 100 45 1924,2 32,9 0,51 89 38 1931,4 266 0,43 56 12 1933,9 32,8 -0,86 6 91 1934,2 16,1 0,87 89 2 1936,5 46,6 -0,45 22 67 1936,7 32,8 0,71 100 29 1944,1 32,2 0,47 83 36 1944,2 47 -0,75 11 86 1949,1 38,5 -0,42 44 86 1950,9 34,5 0,58 89 31 1951,1 53 -0,47 17 64 1966,3 25,1 0,84 94 10 1971,3 35,1 0,48 89 41 1971,5 18,9 0,61 67 5 1973,7 57,1 -0.53 6 59 1977 25,5 0,46 94 48 1977,4 42,9 -0,66 22 88 1982,9 32,2 0,65 89 24 1986,6 35,8 0,46 72 26 1988,9 28,8 0,61 78 17 1989,3 43,7 0,79 94 16 1990,8 47,3 -0,66 17 83 2005,3 39,6 0,52 83 31 2011,3 29 0,47 56 9 2011,5 42 0,43 72 29 2013,8 45,3 -0,51 17 67 2022,6 34,6 0,55 78 22 2025 24,2 0,58 67 9 2028,4 29,9 0,7 94 24 32030,4 31,7 -0,64 17 81 2030,8 46,5 -0,64 22 86 _ 2032,1 30,6 0,42 56 14 2033,5 27,5 0,69 78 9 2035,6 30,9 0,41 67 26 2042 26,4 0,52 100 48 2042,5 40,7 0,63 83 21 2045,9 25,3 0,53 94 41 2047 45,4 -0,48 50 98 2050,8 38,2 0,54 89 34 2052,5 _ 38,7 0,41 67 26 2057,2 36,3 0,43 100 57 2065,3 20,9 0,69 72 3 2079,7 21,8 0,54 61 7 2092 26,7 0,75 89 14 2092,5 41,3 0,62 78 16 2093,1 25,3 0,47 56 9 2095,3 33,7 0,46 89 43 2099,2 36,9 0,69 94 26 2103,6 26,7 0,51 94 43 2105,4 32,5 0,64 78 14 2109,
I
, 0,74 94 WO 2007/082586 PCT/EP2006/050327 64 2116,3 20,3 0,51 67 16 2117,1 57,1 -0,66 11 78 2121,1 43,1 0,4 61 21 2127,2 39,6 0,48 78 29 2129,5 35,1 -0,8 17 97 2140,1 26,8 0,77 89 12 2144,3 22 0.67 94 28 2146,3 25,8 0,97 100 3 2152,7 29,5 0,75 94 19 2157,2 24,4 0,41 50 9 2163,4 27,6 0,56 67 10 2167,3 27,8 0,45 72 28 2172,5 36,7 0,46 94 48 2174,4 24,6 0,66 89 22 2178,5 21,4 0,69 78 9 2182,5 27,6 0,65 89 24 2197,9 29 0,48 67 19 2200,2 33,6 0,47 78 31 2205,6 23 0,42 56 14 2207,2 41,9 0,46 67 21 2210,7 25,7 0,72 94 22 2212,9 46,3 -0,46 39 84 2217,7 41,9 0,6 94 34 2221,1 40,7 -0,64 0 64 2223,5 22,6 0,75 83 9 2228,1 25,9 0,55 94 40 2230,1 22,8 0,52 56 3 2241 41,1 0,47 78 31 2241,1 22,7 0,63 94 31 22,7 94 31 2246,6 39,1 0,41 94 53 2253,1 22,4 0,54 56 2 2258,9 33,6 0,51 89 38 2264,4 34.8 -0,44 17 60 2266 18,5 0,5 50 0 2273,5 22,4 0,42 56 14 2279,1 47,2 -0,5 44 95 2279,5 34, 8 . 0,46 94 48 2288,8 _41,4 0,45 78 33 2288,9 27 0,48 67 19 2290,7 36,2 0,61 67 5 2291,1 21,9 0,67 72 5 2302,9 36,7 0,52 100 48 2308,9 26,2 0,63 83 21 2312,5 22,9 0,71 83 12 2322,5 47,1 0,61 67 5 2325,5 19,5 0,5 50 0 2334,2 41,2 0,45 50 5 2352,4 24,7 0,42 61 19 2356,3 24 0,68 83 16 2364,4 38,9 0,65 89 24 23677 43,2 -0,66 17 83 2370,7 27,3 049 WO 2007/082586 PCT/EP2006/050327 65 2380 39,6 0,62 94 33 2383,9 21,1 0,52 56 3 2389,2 34,4 0 ,41 89 48 2391,2 24,3 0,82 94 12 2396,5 34,6 0,49 61 12 2406,4 31,8 0,59 100 41 2409,1 41,9 0,48 89 41 2414,5 40,8 0,4 61 21 2421 28,7 0,65 94 29 2423,1 27,4 0,61 89 28 2426,5 38,5 0,63 94 31 2427,4 24 0,63 94 31 2429,9 39,3 -0,48 28 76 2432,2 38,3 0,7 83 14 2435 21,6 0,54 56 2 2443,4 31,9 -0,46 39 84 2446,2 24,7 0,44 61 17 2449,3 28,3 0,45 83 38 2451,7 35,5 0,44 83 40 2453,6 32 0,7 83 14 2453,8 20,4 0,56 56 0 2455,6 27,7 0,5 72 22 2461,1 40,5 0,58 72 14 2464 -... 47,2 -0,62 0 62 2465 22,8 0,89 94 5 2469,3 32,5 0,49 61 12 2471,7 23,8 0,53 72 19 2473,4 41,9 0,52 61 9 2475.5 22,3 0,49 61 12 2480,2 47,2 -0,5 22 72 2483,8 19,6 0,55 72 17 2485,9 47,5 0,41 72 31 2490,7 26,7 0,56 83 28 2493,4 46 -0,48 33 81 2493,6 24,6 0,8 100 14 2500,3 30,4 -0,57 22 79 2502,9 33 0,46 61 16 2507,3 17,2 0,48 50 2 2518,7 38,9 0,59 83 24 2521.3 48,3 0,56 61 5 2522,9 24,4 0,63 83 21 2525,5 35,6 -0,64 22 86 2527,3 40,8 0,6 72 12 2529,2 41,4 -0,49 11 60 2535 37,7 0,55 94 40 2536,6 24,8 0,47 56 9 2540,5 25,5 0,79 89 10 2548,2 35,1 -0,55 28 83 2553,7 24,7 .0,44 61 17 2561,3 21,6 0,48 50 2 2566,4 22,2 0,65 72 7 - 258,9 26,9 0,48 78 WO 2007/082586 PCT/EP2006/050327 66 2570,5 57,1 -0,44 33 78 2573,7 16,3 0,8 89 9 2576,2 25,4 0,46 67 21 2579,5 15,2 ._0,63 67 3 2584 43,8 -0,69 28 97 2592,5 56,6 -0,45 17 62 2593,4 25 0,4 56 16 2601,6 23,2 0,45 56 10 2607 47,6 -0,52 22 74 2608,6 37,6 0,42 89 47 2614,1 22,5 0,61 78 17 2619,6 38,3 0,4 61 21 2619,7 22,9 0,63 67 3 2621,4 25,8 0,66 78 12 2627,4 44,8 -0,41 50 91 2630,6 41,7 0,53 72 19 2639,6 45,2 0,5 56 5 2642,4 40,9 -0,61 17 78 2644,1 32,5 -0,6 33 93 2646,7 21,9 0,43 50 7 2654,3 37,2 -0,54 11 66 2658,5 24,7 -0,42 44 86 2660,8 27,1 0,59 78 19 2665,3 39,4 0,79 89 10 2666 23 0,45 56 10 2677,6 23,6 0,84 94 10 2687,9 282 0,5 56 5 2697,3 42,4 -0,48 6 53 2698,4 32,1 -0,52 28 79 2706,7 18,5 0,48 50 2 2707,2 34,1 0,45 72 28 2712,9 22,6 0,52 72 21 S2713,2 41,3 -0,57 6 62 2719,9 20,2 0,67 72 5 2733,4 34,6 -0,42 44 86 2752,8 25,3 0,69 .94 26 2758,5 40,9 -0,43 28 71 2775,5 26,3 0,43 50 7 2780,4 28,3 0,7 83 14 2784,3 45,2 0,61 78 17 2790,3 26,8 0,62 78 16 2793,7 36,3 0,62 78 16 2809,1 . .37,2 -0,61 17 78 2812,5 32,8 0,62 78 16 2823,3 39,9 -0,43 44 88 2825,4 36,5 -0,59 39 98 2830,9 33,2 0,75 94 19 2834,1 38,2 -0,45 28 72 2841,6 37,1 -0,45 28 72 2848,8 36,3 -0,5 44 95 2854,4 43,8 -041 56 97 2875,1 5, 0, 50 0 WO 2007/082586 PCT/EP2006/050327 67 2883,6 28,9 0,44 61 17 2898,5 42,3 -0,4 44 84 2902,9 42,1 0,55 67 12 2908,2 49,2 -0,42 22 64 2912,9 57,5 0,5 50 0 2937,1 26,6 0,52 61 9 2945,1 22,6 0,52 61 9 2972,2 _ _25,6 0,48 67 19 2973,7 34,9 -0,66 22 88 2978 26,3 -0,66 17 83 2978,3 41,7 -0,52 28 79 2990,4 33,6 -0,51 17 67 3007,5 30,5 -0,45 22 67 3041,2 45 -0,61 39 100 .53044,8 4,6 - 52 22 74 3057,1 56,4 -0,51 33 84 3058,8 35,5 -0,42 44 86 3061,9 30,4 0,54 89 34 3077 28,4 -0,55 28 83 3082,3 43,1 -0,46 33 79 3098,8 42,6 -0,44 56 100 3114,9 44,5 -0,53 33 86 3121,4 42,5 -0,56 44 100 3133,8 43,9 -0.45 17 62 3139,4 43,7 -0,61 17 78 S 3149,7 41,6 -0,48 50 98 3152,6 38,2 -0,61 39 100 3169 37,5 -0,41 33 74 3177,4 22,3 -0,5 22 72 3187,7 48,6 -0,53 28 81 3190,9 28,8 -0,42 22 64 3193,1 35,5 -0,46 6 52 3205,8 28,3 -0,64 22 86 3209,2 34,3 -0,63 33 97 3219,5 20,2 0,7 83 14 3232,5 35,7 -0,46 11 57 3255,8 42,9 -0,62 22 84 3256,3 231 0,65 67 2 3258,6 36,3 -0,52 17 69 3260,9 57,3 -0,48 6 53 3262 31,5 -0,58 28 86 3281 36,8 -0,76 22 98 3290,9 36,9 -0,6 33 93 3293,2 54,2 -0,47 50 97 3295,8 38,4 -0,65 33 98 3300,3 44,5 0,41 50 9 3303,2 38,6 -0,79 6 84 3308,6 21,3 0,74 78 3 3309,7 43,6 -0,56 17 72 3319,3 46,2 -0,56 39 95 3320 26,7 0,42 56 14 ,4 "3 - -1,55 3 -- WO 2007/082586 PCT/EP2006/050327 68 3334,6 41,7 -0,64 22 86 3336,8 53,8 -0,58 6 64 3337,4 36,2 -0,49 39 88 3343,8 43,8 -041 50 91 3372 32,5 0,51 83 33 3381,9 43,9 -0,42 11 53 3398,9 44,5 -0,41 50 91 3402,4 33,8 -0,43 56 98 34057 37,8 -0,82 17 98 422,5 38,7 -0,79 11 90 3433,3 44,5 -0,43 56 98 3436 26,4 -0,54 17 71 3442,8 42,5 -0,44 56 100 3451,5 32,6 -0,43 22 66 3479,3 48,5 -0,83 17 100 3503,3 23,2 -0,48 11 59 3530,9 36,8 -0,59 22 81 3552 38,8 -0,48 6 53 3578,2 32,5 0,58 72 14 3583,3 25,2 -0,79 11 90 3589,5 39,1 -0,62 28 90 3617.4 44,8 -0,53 6 59 3631,2 33,1 -0,6 11 71 36349 42,6 -0,52 28 79 3669,7 36,7 -0,47 17 64 36824 42,8 -0,57 17 74 3686,1 32,6 -0,72 11 83 3697,4 38,8 -0,42 11 53 3701,8 434 -0,72_ 0 72 3707 31,9 -0,7 6 76 3719,6 447 -0,55 28 83 3723,3 32,5 -0,74 22 97 3735,8 43,9 -0,68 11 79 37397 47,7 -0,44 33 78 760,8 25,9 -0,52 17 69 3802,7 46,2 -0,51 6 57 816,7 32,2 -0,54 11 66 3852,2 36,9 -0,59 22 81 3871,7 42,9 -0,42 22 64 3881,9 26,2 0,51 61 10 3946,9 33,1 -0,65 28 93 3955,9 23,6 0,41 50 9 3969 6 31,3 -0,75 11 86 3987 30,5 -0, 52 44 97 4006,7 45,9 -0,43 22 66 4026,2 30,5 -0,48 6 53 4044,7 31,2 -0,75 11 86 4055,2 24,1 0.46 61 16 4102,1 41,9 -0,5 0 50 4154,2 23,7 0,81 94 14 4170,6 46,1 -0,46 6 52 204186,G 0,07 "78 10 WO 2007/082586 PCT/EP2006/050327 69 4241,2 244 0,86 100 14 4283,1 24,3 0,64 72 9 4290,8 41,1 -0,66 22 88 4364,4 23,9 -0,42 11 53 4369,9 27,1 0,53 94 41 4527,7 26 0,7 72 2 4565,8 25,1 041 50 9 46264 27,2 0,61 67 5 4654,8 38,8 -0,41 11 52 4713,7 26,9 0,78 83 5 4719,5 39,3 0,5 50 0 4748,5 25,4 -0,61 33 95 4772,1 28,9 -0,41 11 52 4801,2 37,5 -0,71 17 88 4827,1 27,3 0,82 83 2 4863,7 39,2 -0,65 6 71 5112,9 33,1 0,5 50 0 5213,8 36,8 -0,44 6 50 5229,1 39,9 -0,41 11 52 5575,8 35,7 -0,57 6 62 5829,7 20,8 0,59 61 2 5845,8 21,8 0,5 50 0 6106,5 27 0,56 56 0 6171,5 39,6 -0,54 39 93 6212,4 30,6 -059 0 59 6238,6 30,9 -0,43 33 76 6400,9 23,4 0,7 72 2 7190,3 _ 26,5 0,43 50 7 7284,9 40,7 0,5 50 0 7409,9 26,2 0,6 72 12 7556,6 26,2 0,73 89 16 7572,8 25,7 0,55 67 12 7885,4 20,9 0,56 61 5 8054,8 16,7 0,75 94 19 8216,9 16,8 0,45 50 5 8341,2 16,6 0,88 94 7 8371,2 15,8 0,61 61 0 8466,3 18 0,56 61 5 8518,7 15,7 0,76 78 2 8578,4 17 0,61 67 5 8653,1 17,2 0,55 67 12 8765,9 17,6 . 0,67 100 33 8803,1 16,2 0,47 50 3 8928,6 17 0,49 56 7 9060,7 23 0,62 72 10 9076 23 0,62 72 10 9182 17,1 0,8 89 9 9208 22,9 0,61 67 5 9223,1 22,8 0,76 83 7 9335,5 17,5 0,69 72 3 9465,1 23,3 0,61 61 0 9480, 23,6 0,56 5 WO 2007/082586 PCT/EP2006/050327 70 9621,9 19,2 _058 67 9 9868,8 29,5 _ .- 0,55 22 78 9933,5 18,4 0,52 56 3 9944,2 16,7 0,63 67 3 10046,3 18,1 0,81 100 19 10390,1 20,2 0,77 89 12 10518,8 20,9 0,53 72 19 10949,7 26,3 0,5 56 5 Table 10: molecular migration discrimination frequency weight [Da] time [min] factor [%] MGN FSGS + MCD 814,5 28,8 0,41 83 42 819,5 35,7 0,47 67 19 863,4 28,8 0,44 67 23 864,5 37,3 0,44 67 23 879,6 26,9 -0,59 22 81 909,4 40,3 0,5 100 50 928,4 49,4 -0,41 28 69 1015,6 38,2 0,53 83 31 1017,4 36,6 0,49 83 35 1022,5 39,1 0,41 83 42 1073,6 34,7 0,42 100 58 1152,5 40,7 0,53 83 31 1224,7 33,6 -0,44 33 77 1279,7 38,3 0,52 94 42 1283,9 28,9 0,44 67 23 1301,7 34 0,4 56 15 1319,9 34,8 0,41 83 42 1329,8 37,5 0,41 72 31 1341,8 33,1 0,53 83 31 1381,1 32,3 0,48 94 46 1404,9 29,4 0,46 100 54 1423,6 22,3 0,47 67 19 1433 33,7 0,41 72 31 1490,7 33,7 0,47 67 19 1543,8 34,9 0,41 83 42 1574,8 33,9 0,47 89 42 1595,4 31 0,43 78 35 1602,8 .58,1 -0,43 11 54 1605,9 23,7 0,55 78 23 1612,8 26,3 0,4 56 15 1726 36,3 0,41 94 54 1744,1 34,3 0,5 100 50 1768,9 44,7 -0,56 17 73 1774,6 36,5 0,43 78 35 1799 28,8 0,41 72 31 1802,5 25,6 0,49 72 23 1839,1 35,5 0,41 94 54 1876,2 40,1 0,43. 89 46 1883 29,1 -0,44 6 50 1885,7 57,5 -0,45 28 73 1898,7 26,5 0,41 83 42 1924,2 32,9 0,5 89 38 WO 2007/082586 PCT/EP2006/050327 71 1933,9 32,8 -0,52 6 58 1971,5 18,9 0,47 67 19 2011,3 29 0,4 56 15 2079,7 21,8 0,42 61 19 2109,3 27,9 0,44 94 50 2140,1 26,8 0,43 89 46 2152,7 29,5 0,41 94 54 2160,4 27,9 0,4 56 15 2274 37 0,42 50 8 2288,8 41,4 0,51 78 27 2292,4 35,3 0,43 78 35 2312,5 22,9 0,45 83 38 2332,4 35,4 0,44 67 23 2338,6 26 0,43 89 46 2341,2 26,3 0,44 56 12 2356,3 24 0,45 83 38 2367,7 43,2 -0,45 17 62 2380 39,6 0,44 94 50 2391,2 24,3 0,41 94 54 2421 28,7 0,41 94 54 2451,7 35,5 0,45 83 38 2453,6 32 0,53 83 31 2453,8 20,4 0,44 56 12 2461,1 40,5 0,41 72 31 2469,3 32,5 0,46 61 15 2471,7 23,8 0,41 72 31 2500,3 30,4 -0,43 22 65 2521,3 48,3 0,42 61 19 2525,5 35,6 -0,51 22 73 2527,3 40,8 0,45 72 27 2639,6 45,2 0,4 56 15 2642,4 40,9 -0,41 17 58 2665,3 39,4 0,54 89 35 2677,6 23,6 0,44 94 50 2784,3 45,2 0,51 78 27 2830,9 33,2 0,44 94 50 2912,9 57,5 0,42 50 8 3041,2 45 -0,42 39 81 3205,8 28,3 -0,43 22 65 3256,3 23,1 0,44 67 23 3313,8 31,6 0,51 78 27 3336,8 53,8 -0,44 6 50 3479,3 48,5 -0,56 17 73 3578,2 32,5 0,41 72 31 4183,7 26,6 0,43 78 35 4527,7 26 0,41 72 31 4827,1 27,3 0,53 83 31 5112,9 33,1 0,42 50 8 5829,7 20,8 0,46 61 15 6106,5 27 0,48 56 8 8341,2 16,6 0,48 94 46 8371,2 15,8 0,46 61 15 8466,3 18 0,46 61 15 8518,7 15,7 0,51 78 27 8578,4 17 0,47 67 19 9182 17,1 0,43 89 46 9944,2 16,7 0,44 67 23 10949,7 26,3 0,48 56 8 WO 2007/082586 PCT/EP2006/050327 72 Table 11: molecular migration discrimination frequency r[%] weight [Da] time [min] factor IgA + control MGN 800,5 22,5 -0,41 14 55 866,5 22 0,52 52 0 874,7 19,2 0,45 52 7 S879,5 15,6 -0,84 9 93 937,5 23 0,43 57 14 981,6 21,3 -0,42 34 76 995,5 21,4 0,5 54 3 1010,6 16,3 -0,57 5 62 1028,6 21,2 -0,56 13 69 1046,5 21,5 -0,74 9 83 1060,7 17,4 0,47 61 14 1134,6 20,4 -0,59 41 100 1169,5 45,7 -0,52 4 55 1194,7 22,9 -0,68 32 100 1219,7 23,7 0,43 61 17 1224,7 18,1 -0,58 11 69 1235,3 23,2 -0,59 27 86 1250,6 23 -0,52 48 100 1265,6 23 -0,77 23 100 1285,8 18 0,54 57 3 1297,6 22,1 0,61 75 14 1321,7 23,6 -0,46 20 66 1333,7 22,8 0,54 54 0 1335,5 21,1 0,45 63 17 1368,8 17 0,65 75 10 1386,9 17,2 0,75 79 3 1404,8 16 0,61 75 14 1424,4 32,1 -0,57 43 100 1438,5 23,6 -0,43 54 97 1448,6 17,5 0,57 64 7 1460,9 19,5 0,54 54 0 1482 17,7 0,65 71 7 1493,8 20 0,48 52 3 1499,9 17,6 0,77 88 10 1539,7 34,1 -0,72 25 97 1567 19,2 0,59 63 3 1579,5 22,9 -0,56 30 86 1585 18,1 0,77 91 14 1621,8 13,4 0,47 75 28 1644,4 20,8 0,63 63 0 1651,9 17,2 0,64 68 3 1698,1 18,4 0,72 96 24 1760 17,7 0,5 57 7 1805,1 19,8 0,5 50 0 1811,2 17,9 0,83 96 14 1819,7 20,4 0,52 59 7 1829,1 18 0,5 98 48 1851,1 17,8 0,77 84 7 1863,8 37 -0,52 38 90 1867,2 18,6 0,82 86 3 1872,9 18,6 0,65 71 7 1878,5 17,3 0,52 59 7 WO 2007/082586 PCT/EP2006/050327 73 1880,1 37,5 -0,48 7 55 1895,1 16,2 0,63 77 14 1924,5 20,4 0,52 52 0 1943 19,5 0,79 86 7 1955 19,9 0,41 52 10 1977 12,7 -0,57 5 62 2039,1 18,6 -0,49 27 76 2042,1 17,7 0,68 75 7 2048 19,9 -0,54 46 100 2057,3 19,1 0,71 71 0 2133,3 21,5 0,5 64 14 2147 19,5 0,54 68 14 2174,9 27,8 -0,81 9 90 2233,1 18,1 -0,48 11 59 2246,2 22,1 0,68 68 0 2249,1 18,7 -0,42 23 66 2258,6 18,9 0,5 50 0 2279,5 22,5 0,5 54 3 2377,4 18,4 -0,67 13 79 2389,2 18,6 0,59 66 7 2405,6 17,8 0,59 59 0 2427,1 16,4 0,84 95 10 2502,2 19,2 0,5 61 10 2518,7 18,8 0,61 64 3 2540,4 16 0,68 75 7 2562,9 19,1 -0,52 38 90 2566,7 13,9 0,66 70 3 2608,3 21,8 0,54 75 21 2621,5 16,5 0,68 71 3 2649,6 28,9 -0,5 13 62 2695,4 19,7 -0,54 43 97 2742,3 23,7 -0,61 36 97 2752,4 15,5 0,83 93 10 2755,3 23,6 0,68 71 3 2790,6 16,4 0,64 64 0 2799,7 20,4 -0,45 48 93 2825 20,8 -0,63 38 100 2838,7 20,3 -0,57 36 93 2914,8 17 0,43 50 7 2936,8 16 0,7 70 0 3011,5 24,5 -0,68 32 100 3013,3 16,8 -0,42 20 62 3040,9 25,5 -0,72 25 97 3098,3 24,8 -0,51 11 62 3205,9 15,7 -0,53 9 62 3209,4 19 -0,67 16 83 3265,5 24 -0,66 23 90 3281,1 27,3 -0,56 38 93 3287,4 25,2 -0,54 39 93 3303,5 28,7 -0,49 23 72 3333,2 14,1 -0,64 5 69 3359,6 26,2 -0,72 4 76 3375,6 25,3 -0,5 9 59 3385,7 21,2 -0,61 32 93 3402,3 17,8 -0,56 13 69 3405,3 21,6 -0,75 18 93 3416,7 26,4 -0,46 9 55 3432,5 25,6 -0,69 7 76 3441,6 25,4 -0,45 55 100 WO 2007/082586 PCT/EP2006/050327 74 3457,8 25,4 -0,45 55 100 3502,8 14,8 -0,48 7 55 3582,9 14,2 -0,72 7 79 3969,1 18,1 -0,43 13 55 3987,1 17,3 -0,63 27 90 4044,5 18 -0,44 14 59 4054,8 15,5 0,45 59 14 4098,2 20,5 -0,56 23 79 4153,7 14,7 0,58 71 14 4240,6 14,8 0,63 84 21 4290,3 23,4 -0,65 7 72 4306,5 23,5 -0,57 2 59 4369,2 15,5 0,44 75 31 4626 15,7 0,52 55 3 4712,9 15,8 0,72 79 7 4748 14,7 -0,67 20 86 6171,4 23 -0,7 16 86 6186,7 23,3 -0,67 20 86 8764,7 12,8 0,468 88 41 9868,4 17,2 -0,63 9 72 10044,3 13,1 0,65 89 24 10516,9 13,9 0,45 52 7 12719 22,6 -0,44 25 69 Table 12: molecular migration time discrimination frequency 1%] weight [Da] [min] factor IgA control 800,5 22,5 -0,44 12 55 852,6 19,7 0,51 51 0 862,4 27,2 0,56 56 0 866,5 22 0,58 58 0 879,5 15,6 -0,91 2 93 937,5 23 0,49 63 14 981,6 21,3 -0,48 28 76 995,5 21,4 0,55 58 3 1008,5 20 -0,44 12 55 1010,6 16,3 -0,6 2 62 1028,6 21,2 -0,57 12 69 1033,7 21,6 0,53 53 0 1046,5 21,5 -0,8 2 83 1134,6 20,4 -0,63 37 100 1144,7 25,8 0,48 51 3 1169,5 45,7 -0,51 5 55 1181,6 23,7 0,48 65 17 1194,7 22,9 -0,65 35 100 1219,7 23,7 0,55 72 17 1224,7 18,1 -0,64 5 69 1235,3 23,2 -0,61 26 86 1250,6 23 -0,49 51 100 1265,6 23 -0,79 21 100 1297,6 22,1 0,63 77 14 1321,7 23,6 -0,52 14 66 1333,7 22,8 0,63 63 0 1335,5 21,1 0,55 72 17 1368,8 17 0,64 74 10 1386,9 17,2 0,71 74 3 WO 2007/082586 PCT/EP2006/050327 75 1404,8 16 0,58 72 14 1424,4 32,1 -0,49 51 100 1448,6 17,5 0,54 60 7 1482 17,7 0,61 67 7 1493,8 20 0,55 58 3 1499,9 17,6 0,76 86 10 1539,7 34,1 -0,66 30 97 1567 19,2 0,5 53 3 1573,8 27,8 0,49 77 28 1579,5 22,9 -0,65 21 86 1585 18,1 0,79 93 14 1621,8 13,4 0,47 74 28 1644,4 20,8 0,63 63 0 1651,9 17,2 0,62 65 3 1689,7 32,2 0,47 53 7 1698,1 18,4 0,74 98 24 1811,2 17,9 0,84 98 14 1819,7 20,4 0,47 53 7 1829,1 18 0,49 98 48 1851,1 17,8 0,74 81 7 1863,8 37 -0,43 47 90 1867,2 18,6 0,8 84 3 1872,9 18,6 0,63 70 7 1878,5 17,3 0,49 56 7 1880,1 37,5 -0,48 7 55 1895,1 16,2 0,58 72 14 1924,5 20,4 0,51 51 0 1943 19,5 0,79 86 7 1955 19,9 0,43 53 10 1977 12,7 -0,57 5 62 2039,1 18,6 -0,53 23 76 2042,1 17,7 0,7 77 7 2048 19,9 -0,6 40 100 2057,3 19,1 0,67 67 0 2133,3 21,5 0,56 70 14 2147 19,5 0,44 58 14 2174,9 27,8 -0,8 9 90 2233,1 18,1 -0,52 7 59 2246,2 22,1 0,79 79 0 2249,1 18,7 -0,49 16 66 2279,5 22,5 0,5 53 3 2377,4 18,4 -0,79 0 79 2389,2 18,6 0,63 70 7 2405,6 17,8 0,58 58 0 2427,1 16,4 0,83 93 10 2483,4 21,6 -0,47 12 59 2502,2 19,2 0,57 67 10 2518,7 18,8 0,52 56 3 2540,4 16 0,68 74 7 2562,9 19,1 -0,52 37 90 2566,7 13,9 0,71 74 3 2608,3 21,8 0,65 86 21 2621,5 16,5 0,69 72 3 2649,6 28,9 -0,5 12 62 2695,4 19,7 -0,59 37 97 2742,3 23,7 -0,62 35 97 2752,4 15,5 0,85 95 10 2755,3 23,6 0,8 84 3 2761,3 17,7 -0,4 12 52 2790,6 16,4 0,6 60 0 2799,7 20,4 -0,42 51 93 WO 2007/082586 PCT/EP2006/050327 76 2825 20,8 -0,67 33 100 2838,7 20,3 -0,58 35 93 2936,8 16 0,67 67 0 3011,5 24,5 -0,63 37 100 3013,3 16,8 -0,48 14 62 3040,9 25,5 -0,69 28 97 3098,3 24,8 -0,57 5 62 3205,9 15,7 -0,57 5 62 3209,4 19 -0,73 9 83 3265,5 24 -0,69 21 90 3281,1 27,3 -0,56 37 93 3287,4 25,2 -0,47 47 93 3303,5 28,7 -0,49 23 72 3333,2 14,1 -0,67 2 69 3359,6 26,2 -0,71 5 76 3375,6 25,3 -0,54 5 59 3385,7 21,2 -0,56 37 93 3402,3 17,8 -0,57 12 69 3405,3 21,6 -0,79 14 93 3416,7 26,4 -0,44 12 55 3432,5 25,6 -0,67 9 76 3502,8 14,8 -0,53 2 55 3582,9 14,2 -0,72 7 79 3841,4 14,9 -0,44 42 86 3969,1 18,1 -0,41 14 55 3987,1 17,3 -0,62 28 90 4044,5 18 -0,42 16 59 4098,2 20,5 -0,51 28 79 4153,7 14,7 0,51 65 14 4240,6 14,8 0,61 81 21 4290,3 23,4 -0,63 9 72 4306,5 23,5 -0,56 2 59 4712,9 15,8 0,68 74 7 4748 14,7 -0,68 19 86 6171,4 23 -0,68 19 86 6186,7 23,3 -0,65 21 86 8764,7 12,8 0,45 86 41 9868,4 17,2 -0,63 9 72 10044,3 13,1 0,64 88 24 Table 13: molecular migration time discrimination frequency [%] weight [Da] (min] factor IgA MGN 816,7 16 -0,47 7 54 852,6. 19,7 0,51 51 0 862,4 27,2 0,56 56 0 874,7 19,2 -0,43 42 85 943,6 17,5 -0,59 26 85 977,6 18 -0,5 12 62 994,5 18,3 -0,52 2 54 1004,6 22,4 -0,49 5 54 1040,4 19,5 -0,59 2 62 1060,7 17,4 -0,41 51 92 1099,8 17,5 -0,57 28 85 1108,6 17,3 -0,5 42 92 1143,6 30,2 0,45 60 15 WO 2007/082586 PCT/EP2006/050327 77 1157,5 31,6 0,47 63 15 1179,6 31,6 0,49 72 23 1186,7 19,7 -0,49 5 54 1195,6 31,4 0,64 79 15 1198,8 17,7 -0,49 28 77 1203,7 19,3 0,45 60 15 1217,6 30,1 0,78 93 15 1219,7 23,7 0,49 72 23 1239,6 30,6 0,75 91 15 1252,7 20,5 -0,81 12 92 1255,6 29,4 0,49 72 23 1261,5 30,1 0,51 74 23 1268,4 23 -0,51 26 77 1270,7 16,6 -0,47 7 54 1285,8 18 -0,46 47 92 1287,6 18,8 -0,55 14 69 1311,8 17,9 -0,46 23 69 1335,5 21,1 0,41 72 31 1340,6 16,7 -0,52 9 62 1343,1 18,5 -0,48 21 69 1350,8 19 -0,48 14 62 1365,7 21,2 -0,62 7 69 1377,8 17,1 -- 0,47 7 54 1381 19,8 -0,62 7 69 1402,4 18,7 -0,52 2 54 1405,8 31,3 0,54 70 15 1424,8 14,7 -0,5 12 62 1446,7 32,7 0,44 67 23 1455,8 20,7 -0,7 7 77 1464,1 21,3 -0,55 7 62 1465,7 19,4 -0,67 2 69 1470,8 17,3 -0,47 7 54 1472 21,3 -0,53 16 69 1484,5 17,5 -0,73 12 85 1486,4 19,5 -0,58 12 69 1514,6 19,4 -0,49 5 54 1519,1 13,4 -0,5 12 62 1523,7 33 0,65 95 31 1539,6 21,8 -0,62 30 92 1545,8 33,5 0,61 84 23 1556,7 19,6 -0,85 0 85 1561,8 33,3 0,55 93 38 1561,9 19,8 -0,57 5 62 1573,8 27,8 0,61 77 15 1579,5 22,9 -0,41 21 62 1596,9 18,3 -0,6 9 69 1603 19,1 -0,55 7 62 1611,6 32,9 0,51 51 0 1627,6 19,6 -0,52 2 54 1637,8 19,3 -0,6 9 69 1651,8 34 0,59 74 15 1707,6 19,7 -0,42 12 54 1726 20,1 -0,6 9 69 1775,9 20,8 -0,42 12 54 1782,3 18,9 -0,42 35 77 1787,7 19,3 -0,48 14 62 1791,3 19,3 -0,56 21 77 1793,1 23 -0,61 16 77 1799,3 18,7 -0,54 0 54 1845,3 20,1 -0,68 9 77 1876,8 19,2 -0,52 33 85 WO 2007/082586 PCT/EP2006/050327 78 1887,6 21,5 -0,45 9 54 1891,2 18,7 -0,59 2 62 1936,5 21,6 -0,46 23 69 1968,5 27,3 -0,5 12 62 1971,3 22,2 -0,5 12 62 1988,9 18,9 -0,42 12 54 2014,9 18,1 -0,69 23 92 2025,9 21,7 -0,49 5 54 2063,8 17,7 -0,49 51 100 2085,9 21 -0,45 9 54 2113 18,6 -0,42 12 54 2129,1 16,6 -0,57 5 62 2135,3 18,1 -0,68 9 77 2147 19,5 -0,42 58 100 2154,1 21,2 -0,44 33 77 2159 23,1 -0,47 37 85 S2166,6 20,1 -0,48 14 62 2171,7 21,1 -0,41 21 62 2178,4 14,9 -0,52 9 62 2183,5 16,3 -0,47 7 54 2229,5 20,2 -0,7 7 77 _2246,2 22,1 0,48 79 31 2290,5 20,1 -0,41 21 62 2292,2 20,6 -0,47 7 54 S2309,7 16 -0,52 2 54 2325,2 18,2 -0,53 16 69 2361,6 17,3 -0,49 5 54 2377,4 18,4 -0,54 0 54 2407,5 19,3 -0,45 9 54 2421,1 16,1 -0,62 0 62 2464,4 .19,8 -0,69 23 92 2466,6 17 -0,48 21 69 2475,8 18,8 -0,64 21 85 2483,4 21,6 -0,73 12 85 2493,3 14,9 -0,57 28 85 2522,4 16,3 .- 0,41 28 69 2547,1 17,9 -0,55 14 69 2553,7 17,7 -0,72 5 77 2573,5 20,3 -0,45 16 62 2586,7 185 -0,59 2 62 2599,2 21 -0,68 9 77 2608,3 21,8 0,48 86 38 2669,1 18,4 -0,52 2 54 2676 20,6 -0,55 14 69 2681,5 20,1 -0,42 12 54 2684,2 19,4 -0,55 7 62 2687,5 19,2 -0,59 2 62 S2755,3 23,6 0,53 84 31 2807,6 17,3 -0,47 7 54 2810,5 18,1 -0,5 12 62 2831,2 19 -0,43 19 62 2847,7 16,5 -0,5 35 85 2914,8 17 -0,45 40 85 S2959,7 16,6 -0,47 7 54 3030 16,7 -0,44 26 69 3062,1 17,9 -0,54 23 77 3441,6 25,4 0,62 70 8 3478,6 27,6 0,78 86 8 3495,5 25,8 0,71 79 8 3841,4 14,9 -0,43 42 85 4183,6 16,3 -0,45 9 _54 WO 2007/082586 PCT/EP2006/050327 79 4479,4 14,8 -0,45 9 54 4483,2 16,2 -0,47 7 54 4527,6 16,3 -0,5 12 62 4566,6 16,6 -0,52 2 54 4594,4 14,2 -0,45 9 54 8053,8 12,9 -0,44 26 69 WO 2007/082586 PCT/EP2006/050327 80 Table 14: 5 mass CEt frequency [%] mass CEt frequency [%] [Da] [min] control FSGS MCD MGN [Da [rmin] control FSGS MCD MGN 3012,09 39,45 100 60 94 72 1028,57 37,79 98 40 69 22 1539,67 50,20 100 90 100 89 876,41 48,89 98 70 38 67 2249,19 33,82 100 80 100 83 2205,03 36,94 98 70 88 83 3152,55 38,22 100 60 69 39 3402,40 33,83 98 50 94 56 3360,09 44,33 100 60 81 72 2377,60 32,06 98 80 94 83 3001,97 48,35 100 100 100 89 2175,03 44,27 98 80 100 100 2257,19 46,60 100 60 81 67 2385,45 45,47 98 80 81 94 2563,42 32,22 100 90 75 72 2046,99 45,39 98 50 56 50 2158,98 46,70 100 90 88 89 2409,90 32,54 98 100 94 94 3287,97 43,92 100 90 100 89 3433,28 44,46 98 70 56 56 3385,76 36,60 100 100 81 72 1545,75 54,72 98 90 100 89 3271,80 44,05 100 80 94 61 2736,31 32,30 97 00 94 89 2007,69 33,06 100 90 88 89 3723,33 32,48 97 20 50 22 1194,61 39,46 100 70 88 83 1737,76 41,29 97 90 88 89 1265,62 40,37 100 70 94 72 1378,54 45,45 97 60 81 56 1435,69 39,91 100 90 94 89 2854,41 43,80 97 50 75 56 1261,53 49,63 100 80 88 61 2068,54 41,06 97 80 81 61 1438,56 37,63 100 100 100 100 2663,36 36,38 97 80 88 83 1446,50 52,53 100 80 94 67 2085,50 39,21 97 100 94 94 3265,77 42,28 100 80 75 78 2682,49 35,03 97 90 75 89 3121,36 42,46 100 50 75 44 1046,57 38,63 97 20 38 6 1911,14 37,40 100 90 100 94 2994,61 40,63 97 90 88 72 1321,91 41,10 100 70 69 50 2583,98 43,75 97 30 62 28 2695,49 35,27 100 70 88 78 2129,48 35,14 97 60 50, 17. 1235,59 41,42 100 60 69 50 981,56 37,39 97 50 81 56 2799,94 37,08 100 80 88 83 879,55 26,95 97 60 94 22 2169,75 39,56 100 100 100 94 2394,29 36,32 97 100 100 94 1224,74 33,57 100 50 94 33 3986,98 30,46 97 50 69 44 1451,67 41,11 100 100 100 83 2483,58 38,74 97 90 81 78 3479,32 48,53 100 70 75 17 1523,73 54,29 97 90 100 89 2649,94 45,91 100 90 75 78 1889,76 46,38 97 30 44 39 2687,36 41,87 100 60 75 61 1507,64 54,43 97 90 100 89 3458,52 44,64 100 90 94 72 3209,22 34,27 97 30 81 33 3442,84 42,54 100 80 94 56 3022,82 33,82 97 40 62 61 2048,19 33,07 100 40 81 61 1765,17 35,50 97 90 88 94 2679,46 34,99 100 50 94 67 1367,67 53,27 97 90 94 94 2227,34 38,28 100 70 62 83 2726,38 40,38 97 100 88 100 1239,52 50,23 100 100 100 78 1179,57 52,17 97 80 100 83 3098,80 42,63 100 60 81 56 1651,86 55,15 97 90 100 78 WO 2007/082586 PCT/EP2006/050327 81 2839,07 35,41 100 80 88 83 3376,24 45,17 97 50 88 67 3417,12 45,12 100 70 81 61 3293,15 54,21 97 50 75 50 3426,20 42,48 100 70 88 72 1579,50 39,43 97 100 94 94 3041,16 45,04 100 80 81 39 3474,27 43,37 95 70 75 67 1508,70 41,26 98 90 94 61 2848,83 36,33 95 70 75 44 1462,67 53,58 98 70 88 50 3319,28 46,22 95 50 62 39 3280,96 36,76 98 20 50 22 1000,52 33,96 95 40 44 28 1077,33 29,62 98 100 100 100 3281,97 49,44 95 60 50 56 2742,25 42,25 98 90 75 89 1885,74 57,47 95 70 75 28 3092,71 43,86 98 90 81 78 3556,92 34,85 95 100 75 78 196,*66 45,45 98 80 100 89 1609,17 42,60 95 100 94 89 6187,55 39,78 98 60 94 67 2767,41 31,39 95 40 69 56 2825,42 36,54 98 50 88 39 3108,81 44,70 95 50 75 56 1255,55 49,81 98 100 100 78 2233,00 31,06 95 30 69 56 2717,56 34,43 98 60 69 61 882,55 36,55 95 60 31 72 3149,67 41,62 98 70 88 50 1680,16 37,32 95 100 94 100 1195,53 51,76 98 70 94 83 1673,80 54,59 95 80 94 61 3496,02 43,85 98 90 94 61 2336,78 42,47 95 70 94 89 1561,69 54,17 98 90 100 83 1217,64 48,54 95 100 94 83 1250,63 41,97 98 70 100 89 1489,49 42,21 95 90 94 72 3295,77 38,36 98 50 50 33 2442,06 46,85 95 70 81 67 3405,68 37,84 98 40 62 17 2279,06 47,16 95 70 69 44 1578,01 52,53 98 70 75 50 4748,51 25,38 95 50 38 33 1134,58 37,11 98 90 94 94 1766,84 35,15 95 100 100 100 Table 15: Frequency Frequency Frequency Frequency Mass CE-time Healthy FSGS MCD MGN [Da] [min] [%] [%] 1%] . __ 1435,69 32,7 94 86 100 7 1282,39 29,3 69 29 29 0 3531,01 26,9 69 0 0 0 5801,94 13,3 69 0 7 7 5 Table 16: healthy vs. renal patients mass [Da] CE time [min] 909,4 40,3 1159,6 39,0 1338,7 47,2 1686,8 38,2 1847,8 .. 57,0 1966,3 25,1 1990,8 47,3 WO 2007/082586 PCT/EP2006/050327 82 2146,3 25,8 2432,2 38,3 2465,0 22,8 3707,0 31,9 Table 17: MGN vs. MCD Mass CE t 879,6 26,9 1279,7 38,3 1341,8 33,1 1404,9 29,4 1569,8 48,3 1574,8 33,9 1605,9 23,7 2527,3 40,8 5112,9 33,1 5 Table 18: MCD vs. FSGS Mass CE t 1199,6 31,0 1826,9 50,8 2077,3 35,8 2258,9 33,6 2918,0 42,2 Table 19: MGN vs. FSGS Mass CE t 2312,5 22,9 2453,6 32,0 2639,6 45,2 9182,0 17,1 10 Table 20: mass CE time mass CE time [Da) min] %healthy % MGN [Da] [min_ %healthy % MGN 4098,2 40,1 100 0 1933,02 41,5 100 12 3685,9 35,9 100 0 1889,82 49,3 100 12 3531,3 42,9 100 0 1636,69 46,8 100 12 3359,7 48,4 100 0 1579,76 47,3 100 12 3287,4 47,4 100 0 1438,66 45,4 100 12 WO 2007/082586 PCT/EP2006/050327 83 3265,3 51,6 100 0 1321,59 45,8 100 12 3098,5 46,9 100 0 1255,53 53 100 12 3041,3 46,5 100 0 1200,53 53,4 100 12 3011,3 46,5 100 0 2427,43 27 12 100 2742,2 45,8 100 0 1829,09 33,8 12 100 2563,2 34,5 100 0 4627,01 28,7 0 88 2483,5 44,5 100 0 2621,42 29 0 88 2385,2 50,4 100 0 1942,57 34,8 0 88 1893,1 42,5 100 0 1867,06 33,8 0 88 1639,9 47,5 100 0 1759,92 32,5 0 88 1609,7 47,3 100 0 1460,83 39,8 0 88 1580,9 41,3 100 0 3013,36 36,6 88 12 1508,7 46,6 100 0 2838,9 39,8 88 12 1489,6 46,2 100 0 2710,31 52,8 88 12 1424,7 56 100 0 2395,04 40,4 88 12 1407,6 54,6 100 0 1876,91 37,2 88 12 1160,6 52,7 100 0 1863,86 59,2 88 12 981,53 41 100 0 1651,81 56,5 88 12 980,54 38 100 0 1561,56 56,1 88 12 876,4 52,2 100 0 1523,72 56,1 88 12 2752,9 29,3 0 100 1473,66 46,4 88 12 6171,1 43,4 88 0 1261,49 53,2 88 12 3851,9 41,2 88 0 1195,5 54 88 12 3706,8 35,2 88 0 10047 22,3 12 88 3634,2 43,6 88 0 4713,94 28,8 12 88 3631,3 36,3 88 0 4241,41 26,7 12 88 3478,9 47,9 88 0 1811,13 34,6 12 88 3376,3 48,5 88 0 1753,98 32,7 12 88 3338,2 38,6 88 0 1698,06 34,1 12 88 3292,7 56,7 88 0 1584,91 32,7 12 88 3280,6 42,2 88 0 4353,62 33,6 75 0 3271,5 47,3 88 0 4102,45 45,2 75 0 3248,5 47,2 88 0 4044,58 34,1 75 0 2849,2 39,4 88 0 3987,48 34,8 75 0 2736,4 39,3 88 0 3947,22 36 75 0 2682,1 37,3 88 0 3589,65 41,3 75 0 2642,6 44,7 88 0 3433,12 48,6 75 0 2584,3 51,9 88 0 3416,92 48,6 75 0 2257,1 50,3 88 0 3295,53 42 75 0 2204,9 44 88 0 3261,55 35,6 75 0 2196,9 49,9 88 0 3258,52 37,8 75 0 2039,2 35,8 88 0 3193,48 37,3 75 0 1680,8 47 88 0 3152,6 40,3 75 0 1635,8 56,8 88 0 3092,08 47,6 75 0 1539,7 46,3 88 0 2863,25 40,6 75 0 1423,7 54,4 88 0 2854,55 52,4 75 0 1422,5 55 88 0 2698,37 37,2 75 0 1353,7 43,2 88 0 2548,42 37,7 75 0 1046,6 42,6 88 0 2464,07 50,8 75 0 WO 2007/082586 PCT/EP2006/050327 84 3969,5 34,4 100 12 2406,98 50,6 75 0 3496,1 47,1 100 12 2279 50,2 75 0 3442,2 47,9 100 12 2233,02 35,7 75 0 3405,4 42,4 100 12 2226,97 43 75 0 3385,6 41,5 100 12 2019,97 41,1 75 0 3281,7 53 100 12 1991,95 36,2 75 0 3209,4 37,1 100 12 1849,85 41,1 75 0 2799,9 42,4 100 12 1768,95 48,7 75 0 2378 38,8 100 12 1755,02 48,2 75 0 2170 42,6 100 12 1737,78 48,2 75 0 2008 37 100 12 1462,63 56,1 75 0 1949 41,5 100 12 1446,6 56 75 0 1425,78 41,6 75 0 Table 21: mass CE time [Da] [min] %healthy % MGN 1405,6 55,7 75 0 1389,6 55,3 75 0 1322,6 45,4 75 0 1262,6 56,4 75 0 1246,6 55,6 75 0 1224,8 35,4 75 0 1141,7 41,6 75 0 1028,6 41,9 75 0 946,43 50,5 75 0 3723,1 35,5 100 25 3458,2 48,2 100 25 3001,8 51,8 100 25 2825,3 40,8 100 25 2695,3 39,1 100 25 2679,2 39,2 100 25 2410 39,6 100 25 2394 39,3 100 25 2048 35,9 100 25 1911,1 41,6 100 25 1545,7 57,3 100 25 1507,7 57,3 100 25 1467,8 41 100 25 1451,7 46,4 100 25 1435,7 46,3 100 25 1265,6 44,6 100 25 1250,6 45,7 100 25 1239,4 53,7 100 25 1235,6 44 100 25 1217,6 53,3 100 25 1194,6 44,1 100 25 WO 2007/082586 PCT/EP2006/050327 85 1179,5 55 100 25 1716 32,1 25 100 4827,2 29,3 0 75 2937,4 29,6 0 75 2057,4 37 0 75 1851,1 33,8 0 75 1680,1 33,6 0 75 1517,9 30,2 0 75 1483,9 32,5 0 75 1481,9 33,8 0 75 1404,8 29 0 75 1398,8 34,1 0 75 1367,6 56,1 88 25 1157,6 54,9 88 25 3474,3 47,9 75 12 3402,5 37 75 12 2761,4 34,7 75 12 2644,1 33,5 75 12 2587,2 34,9 75 12 2579,7 50,5 75 12 2579,7 41,4 75 12 2175 50 75 12 2069,1 49,5 75 12 2047 49,5 75 12 1170,6 46 75 12 1386,8 32,3 25 88 8766,7 21,6 12 75 4154,4 26,4 12 75 3842,8 25,7 12 75 1873 33,9 12 75 1566,9 33,2 12 75 1499,9 33,7 12 75 1368,8 31,6 12 75 1285,7 31,1 12 75 1108,6 32,2 12 75 1099,6 31,2 12 75 1060,6 31,6 12 75 Table 22: healthy, disease, time [ min ] mass [Da] frequency frequency type 22,9 ± 3,05 834,5 0,10 3% 54% Diabetes pos. 22,9 ± 3,03 869,4 0,17 14% 63% Diabetes pos. 24,2 + 1,89 874,5 ± 0,09 28% 66% Diabetes pos. 22,2 ± 2,19 907,5 0,13 0% 41% Diabetes pos. 29,0 ± 2,35 910,5 . 0,09 15% 47% Diabetes pos.
WO 2007/082586 PCT/EP2006/050327 86 22,9 + 3,18 947,6 ± 0,22 17% 51% Diabetes pos. 26,8 ± 2,98 950,5 ± 0,12 0% 24% Diabetes pos. 23,2 ± 4,87 995,6 ± 0,14 23% 50% Diabetes pos. 27,4 ± 3,59 1082,6 ± 0,16 .. 0% 44% Diabetes pos. 32,3 ± 1,99 1096,5 ± 0,14 10% 51% Diabetes pos. 26,8 ± 3,85 1176,6 ± 0,13 21% 59% Diabetes pos. 22,3 ± 3,45 1222,8 ± 0,22 17% 56% Diabetes pos. 30,6 ± 3,31 1236,6 ± 0,11 24% 59% Diabetes pos. 52,6 ± 4,80 1285,0 ± 0,09 14% 54% Diabetes pos. 28,8 ± 3,98 1332,7 + 0,20 23% 55% Diabetes pos. 49,8 ± 4,72 1332,8 ± 0,16 8% 38% Diabetes pos. 26,7 ± 2,79 1355,8 ± 0,15 17% 56% Diabetes pos. 24,6 ± 2,84 1386,8 ± 0,14 53% 77% Diabetes pos. 26,8 ± 3,26 1403,7 ± 0,21 8% 46% Diabetes pos. 17,8 ± 4,12 1405,9 ± 0,15 14% 56% Diabetes pos. 31,5 ± 3,71 1442,7 ± 0,27 15% 55% Diabetes pos. 32,1 ± 3,38 1449,8 ± 0,14 41% 85% Diabetes pos. 31,3 ± 5,27 1592,4 ± 0,38 3% 46% Diabetespos. 43,4 ± 4,41 1783,4 ± 0,30 33% 63% Diabetes pos. 29,4 ± 3,08 1789,2 ± 0,39 28% 75% Diabetes pos. 38,4 ± 1,09 1818,9 ± 0,21 28% 67% Diabetes pos. 37,7 ± 1,04 1821,4 ± 0,39 14% 56% Diabetes pos. 24,4 ± 2,55 1829,2 ± 0,23 45% 81% Diabetes pos. 51,1 ± 4,11 1854,7 ± 0,41 14% 54% Diabetes pos. 37,6 ± 3,30 1856,8 ± 0,48 33% 56% Diabetes pos. 24,7 ± 2,63 1872,9 ± 0,35 43% 72% Diabetes pos. 28,3 ± 3,47 1949,5 ± 0,32 17% 73% Diabetes pos. 31,6 ± 2,90 1955,1 ± 0,32 55% 79% Diabetes pos. 31,3 ± 3,00 1971,0 ± 0,45 20% 54% Diabetes pos. 37,8 ± 2,40 2032,0 ± 0,30 25% 60% Diabetes pos. 30,9 ± 4,69 2061,4 ± 0,58 10% 38% Diabetes pos. 33,8 ± 3,76 2092,2 ± 0,46 18% 45% Diabetes pos. 27,7 ± 4,43 2185,6 ± 0,46 10% 36% Diabetes pos. 32,9 ± 1,48 2189,4 ± 0,34 14% 54% Diabetes pos. 39,6 ± 5,31 2229,4 ± 0,48 5% 39% Diabetes pos. 24,5 ± 5,14 2229,9 ± 0,33 25% 63% Diabetes pos. 28,3 ± 3,30 2502,9 ± 0,56 20% 48% Diabetes pos. 24,9 ± 4,84 2621,6 ± 0,97 20% 45% Diabetes s. 37,5 ± 4,52 2669,8 ± 0,39 23% 67% Diabetes pos. 20,8 ± 4,47 2752,2 ± 0,76 35% 64% Diabetes pos. 24,9 ± 4,31 2795,7 ± 0,96 13% 40% Diabetes pos. 48,2 ± 3,61 3246,1 ± 0,43 0% 30% Diabetes pos. 20,9 ± 3,33 3844,0 ± 0,52 3% 54%o Diabetes pos. 21,9 ± 2,62 4961,5 ± 0,89 10% 40% Diabetes pos. 18,6 ± 2,91 5497,0 ± 0,66 18% 42% Diabetes pos. 20,4 ± 2,20 808,4 + 0,10 58% 9% Diabetes neg. 45,3 ± 2,03 897,5 ± 0,09 48% 7% Diabetes neg. 31,4 ± 1,08 929,5 ± 0,11 98% 46% Diabetes neg. 41,2± 1,41 946,4±0,10 85% 36% Diabetes neg.
WO 2007/082586 PCT/EP2006/050327 87 28,0 ± 1,04 980,5 ± 0,07 85% 31% Diabetes neg. 26,7 ± 2,26 1000,5 + 0,09 83% 41% Diabetes neg. 27,8 ± 1,51 1008,5 ± 0,10 95% 41% Diabetes neg. 29,3 ± 2,55 1012,5 ± 0,10 63% 17% Diabetes neg. 43,6 ± 2,03 1047,5 ± 0,11 90% 26% Diabetes neg. 25,0 + 3,91 1052,6 ± 0,08 45% 4% Diabetes neg. 37,4 ± 5,63 1066,5 ± 0,14 58% 13% Diabetes neg. 22,8 ± 1,78 1075,5 ± 0,13 68% 26% Diabetes neg. 28,9 ± 3,89 1088,6 ± 0,15 65% 21% Diabetes neg. 44,4 ± 2,06 1106,5 ± 0,11 80% 18% Diabetes neg. 34,1 ± 1,80 1107,5 ± 0,10 88% 35% Diabetes neg. 42,8 ± 3,26 1120,5 ± 0,06 60% 14% Diabetes neg. 29,1 ± 2,26 1134,6 ± 0,10 95% 49% Diabetes neg. 28,2 ± 3,00 1137,7 ± 0,11 70% 24% Diabetes neg. 45,5 ± 2,34 1139,5 ± 0,20 83% 22% Diabetes neg. 32,9 ± 1,25 1159,6 ± 0,11 80% 27% Diabetes neg. 23,3 ± 4,17 1180,5 ± 0,16 50% 9% Diabetes neg. 43,8 ± 2,08 1200,6 ± 0,11 95% 50% Diabetes neg. 27,2 ± 3,22 1204,6 ± 0,17 60% 17% Diabetes neg. 44,9 ± 2,53 1209,5 ± 0,09 83% 17% Diabetes neg. 47,8 ± 2,73 1224,6 ± 0,12 75% 19% Diabetes neg. 25,6 ± 2,43 1246,7 ± 0,15 73% 30% Diabetes neg. 47,9 ± 2,66 1268,6 ± 0,09 68% 25% Diabetes neg. 43,9 ± 1,80 1277,5 ± 0,10 70% 28% Diabetes neg. 46,0 ± 2,69 1278,5 ± 0,09 58% 10% Diabetes neg. 33,1 ± 1,82 1282,6 ± 0,13 62% 7% Diabetes neg. 29,3 ± 3,88 1331,7 ± 0,18 65% 12% Diabetes neg. 45,9 + 4,78 1405,5 ± 0,33 93% 45% Diabetes neg. 44,4 ± 3,90 1423,6 ± 0,16 60% 20% Diabetes neg. 19,2 ± 3,40 1484,8 ± 0,19 68% 13% Diabetes neg. 36,9 ± 2,02 1609,6 ± 0,13 85% 13% Diabetes neg. 38,9 ± 3,78 1639,7 ± 0,27 63% 19% Diabetes neg. 33,2 ± 3,34 1662,9 ± 0,21 62% 5% Diabetes neg. 35,8 + 2,19 1664,6 ± 0,29 66% 10% Diabetes neg. 36,2 ± 4,78 1666,6 ± 0,34 75% 29% Diabetes neg. 35,9 + 2,98 1678,1 ± 0,44 60% 18% Diabetes neg. 37,3 ± 2,99 1716,8 ± 0,23 73% 19% Diabetes neg. 46,5 ± 4,38 1717,5 ± 0,37 79% 15% Diabetes neg. 37,9 ± 4,18 1746,0 ± 0,33 83% 34% Diabetes neg. 25,1 + 2,25 1817,6 ± 0,27 65% 8% Diabetes neg. 34,2 ± 3,95 1823,4 ± 0,47 73% 30% Diabetes neg. 29,1 ± 3,59 1849,8 ± 0,30 100% 56% Diabetes neg. 49,3 + 4,49 1914,1 ± 0,36 88% 38% Diabetes neg. 44,2 ± 4,23 1916,7 ± 0,33 69% 10% Diabetes neg. 39,8 + 2,19 2030,8 ± 0,35 93% 38% Diabetes neg. 31,9 + 1,61 2118,9 ± 0,21 73% 14% Diabetes neg. 41,2 ± 2,45 2179,3 ± 0,42 58% 17% Diabetes neg. 20,1 + 2,78 2219,0 ± 0,26 53% 13% Diabetes neg. 25,8 ± 2,70 2256,9 ± 0,47 85% 26% Diabetes neg.
WO 2007/082586 PCT/EP2006/050327 88 45,1 ± 5,23 2273,4 ± 0,42 79% 22% Diabetes neg. 40,7 ± 1,90 2279,0 ± 0,33 90% 20% Diabetes neg. 26,8 ± 3,73 2320,2 ± 0,55 78% 34% Diabetes neg. 23,6 ± 3,10 2332,2 ± 0,35 53% 11% Diabetes neg. 44,5 ± 3,08 2345,6 ± 0,46 75% 34% Diabetes neg. 25,7 ± 5,16 2384,5 ± 0,63 65% 21% Diabetes neg. 38,5 ± 3,62 2423,9 ± 0,41 88% 29% Diabetes neg. 34,2 ± 2,92 2429,9 ± 0,51 65% 18% Diabetes neg. 23,3 ± 2,54 2443,3 ± 0,46 66% 5% Diabetes neg. 41,7 ± 3,72 2548,1 ± 0,57 69% 15% Diabetes neg. 27,3 ± 4,77 2548,3 ± 0,66 83% 35% Diabetes neg. 43,6 ± 2,08 2548,3 ± 0,23 95% 41% Diabetes neg. 24,0 ± 3,11 2581,5 ± 0,47 60% 13% Diabetes neg. 24,0 ± 2,70 2587,4 + 0,40 80% 26% Diabetes neg. 41,7 ± 3,06 2606,8 ± 0,55 78% 35% Diabetes neg. 31,3 ± 4,92 2636,4 ± 0,48 72% 12% Diabetes neg. 25,5 ± 3,62 2644,2 ± 0,41 88% 33% Diabetes neg. 29,2 ± 1,07 2654,0 ± 0,37 66% 0% Diabetes neg. 29,8 ± 3,50 2698,2 ± 0,63 90% 29% Diabetes neg. 43,0 ± 2,26 2710,5 ± 0,37 79% 5% Diabetes neg. 25,1 ± 1,64 2761,3 ± 0,35 88% 44% Diabetes neg. 31,3 ± 2,79 2808,5 ± 0,56 79% 22% Diabetes neg. 42,0 ± 3,22 2876,5 ± 0,48 62% 7% Diabetes neg. 33,7 ± 3,34 2898,7 ± 0,50 85% 43% Diabetes neg. 42,2 ± 2,68 2908,1 ± 0,53 72% 17% Diabetes neg. 35,4 ± 2,63 2917,6 ± 0,58 72% 12% Diabetes neg. 35,4 ± 0,77 2978,1 ± 0,49 85% 35% Diabetes neg. 36,1 ± 1,42 2994,6 ± 0,80 83% 24% Diabetes neg. 43,5 ± 2,99 3023,4 ± 0,65 93% 34% Diabetes neg. 44,4 ± 3,35 3045,2 ± 0,61 69% 12% Diabetes neg. 22,9 ± 3,47 3076,4 + 0,96 66% 7% Diabetes neg. 35,7 ± 1,99 3082,3 ± 0,43 73% 22% Diabetes neg., 33,6 ± 3,53 3136,8 ± 0,61 95% 47% Diabetes neg. 21,7 ± 3,14 3154,8 ± 0,44 55% 10% Diabetes neg. 26,5 ± 1,92 3193,7 ± 0,53 78% 32% Diabetes neg. 24,4 ± 3,02 3206,3 ± 0,72 66% 7% Diabetes neg. 28,2 ± 2,80 3250,9 ± 0,71 63% 18% Diabetes neg. 48,2 ± 3,46 3293,2 ± 0,74 93% 39% Diabetes neg. 31,4 ± 1,60 3295,7 ± 0,33 95% 40% Diabetes neg. 27,2 ± 3,58 3338,4 ± 0,79 80% 34% Diabetes neg. 37,3 ± 2,11 3381,6 ± 0,63 78% 26% Diabetes neg. 27,6 + 2,49 3452,1 ± 0,49 58% 15% Diabetes neg. 37,3 ± 1,50 3463,0 ± 0,83 72% 15% Diabetes neg. 19,6 ± 2,89 3583,4 ± 0,75 79% 20% Diabetes neg. 34,0 ± 2,55 3634,4 ± 0,74 86% 29% Diabetes neg. 37,7 ± 2,61 3681,8 ± 1,38 55% 14% Diabetes neg. 25,5 ± 2,25 3686,2 ± 0,60 86% 20% Diabetes neg. 36,0 ± 3,89 3735,7 ± 0,57 70% 28% Diabetes neg. 30,3 ± 1,58 3852,3 ± 0,56 83% 41% Diabetes neg.
WO 2007/082586 PCT/EP2006/050327 89 29,6 ± 1,46 4098,4 ± 0,59 93% 20% Diabetes neg. 28,8 ± 1,18 5428,8 ± 0,67 70% 19% Diabetes neg. 33,1 ± 0,69 6187,5 ± 1,13 83% 10% Diabetes neg. 26,0 ± 4,82 6212,0 ± 1,41 75% 26% Diabetes neg. 23,3 ± 2,19 9868,8 4 1,33 66% 0% Diabetes neg. 21,7 ± 5,12 830,5 ± 0,11 4% 40% Nephropathy pos. 32,4 ± 1,83 866,4 ± 0,11 0% 40% Nephropathy pos. 30,6 ± 3,07 909,5 ± 0,13 11% 40% Nephropathy pos. 32,8 ± 3,14 937,5 ± 0,11 14% 73% Nephropathy pos. 24,9 ± 2,97 952,5 ± 0,16 11% 40% Nephropathy pos. 32,1 ± 2,44 1033,5 ± 0,11 5% 40% Nephropathy pos. 24,4 ± 2,87 1060,6 ± 0,16 17% 68% Nephropathy pos. 27,5 ± 2,86 1131,6 ± 0,16 20% 68% Nephropathy pos. 33,4 ± 3,48 1181,6 ± 0,15 22% 73% Nephropathy pos. 33,0 ± 2,52 1203,6 ± 0,14 9% 50% Nephropathy pos. 26,5 ± 3,68 1211,6 ± 0,14 14% 40% Nephropathy pos. 33,1 ± 0,91 1219,6 ± 0,15 18% 40% Nephropathy pos. 32,8 ± 3,30 1225,6 ± 0,13 12% 40% Nephropathy pos. 30,7 ± 3,18 1297,7 ± 0,20 31% 82% Nephropathy pos. 34,1 ± 2,05 1333,7 ± 0,23 9% 40% Nephropathy pos. 44,7 ± 4,06 1337,5 ± 0,20 19% 59% Nephropathy pos. 27,9 ± 4,19 1398,8 ± 0,36 29% 77% Nephropathy pos. 21,3 ± 5,08 1423,7 ± 0,49 6% 50% Nephropathy pos. 28,1 ± 4,95 1439,8 ± 0,19 19% 68% Nephropathy pos. 24,5 ± 2,42 1466,0 ± 0,27 9% 77% Nephropathy pos. 27,5 ± 4,93 1482,0 ± 0,42 33% 40% Nephropathy pos. 29,8 ± 4,43 1482,9 ± 0,28 18% 40% Nephropathy pos. 24,3 ± 2,65 1483,7 ± 0,28 26% 91% Nephropathy pos. 24,6 ± 1,98 1500,0 ± 0,20 38% 86% Nephropathy pos. 24,6 ± 2,90 1553,1 ± 0,28 14% 64% Nephropathy pos. 29,0 ± 4,83 1556,7 ± 0,45 26% 73% Nephropathy pos. 24,2 ± 2,48 1567,0 ± 0,22 26% 86% Nephropathy pos. 28,8 ± 4,53 1596,9 ± 0,31 21% 86% Nephropathy pos. 24,5 ± 2,43 1652,8 ± 0,25 14% 59% Nephropathy pos. 26,3 ± 2,63 1669,8 ± 0,37 20% 64% Nephropathy pos. 33,1 ± 3,22 1729,2 ± 0,36 6% 45% Nephropathy pos. 30,5 ± 4,11 1744,4 ± 0,46 16% 59% Nephropathy pos. 25,1 ± 3,42 1754,4 ± 0,41 53% 95% Nephropathy pos. 24,2 ± 1,56 1776,0 ± 0,27 9% 50% Nephropathy pos. 18,5 ± 3,55 1791,0 ± 0,38 7% 40% Nephropathy pos. 32,2 ± 5,38 1792,9 ± 0,31 28% 40% Nephropathy pos. 9,7 ± 2,54 1799,8 ± 0,29 0% 40% Nephropathy pos. 25,3 ± 2,89 1810,9 ± 0,38 43% 91% Nephropathy pos. 24,6 ± 2,34 1851,1 ± 0,21 43% 95% Nephropathy pos. 27,2 + 4,46 1867,3 ± 0,42 38% 91% Nephropathy pos. 25,0 + 3,97 1966,0 ± 0,53 16% 40% Nephropathy pos. 28,7 + 3,08 1982,8 ± 0,57 11% 40% Nephropathy pos. 29,5 + 5,53 1986,3 ± 0,36 15% 64% Nephropathy pos. 23,3 + 4,46 2045,9 ± 0,32 32% 40% Nephropathy pos.
WO 2007/082586 PCT/EP2006/050327 90 33,7 ± 3,16 2115,1 ± 0,53 30% 40% Nephropathy pos. 20,5 ± 2,78 2177,1 ± 0,37 9% 40% Nephropathy pos. 18,1 ± 4,24 2241,6 ± 0,41 9% 59% Nephropathy pos. 21,2 ± 2,49 2250,7 ± 0,38 23% 64% Nephropathy pos. 27,5 ± 2,53 2258,7 ± 0,49 9% 59% Nephropathy pos. 20,0 ± 3,30 2356,4 ± 0,41 13% 59% Nephropathy pos. 28,1 ± 3,95 2391,4 ± 0,42 13% 64% Nephropathy pos. 25,7 ± 4,85 2406,1 ± 0,57 20% 77% Nephropathy pos. 22,8 ± 4,28 2423,2 ± 0,53 14% 64% Nephropathy pos. 21,9 ± 4,45 2427,3 + 0,40 31% 91% Nephropathy pos. 19,2 ± 4,24 2465,1 ± 0,62 9% 77% Nephropathy pos. 25,4 ± 5,25 2493,0 ± 0,38 9% 50% Nephropathy pos. 19,5 ± 4,66 2494,0 ± 0,66 12% 77% Nephropathy pos. 23,7 ± 4,27 2494,9 ± 0,49 7% 40% Nephropathy pos. 24,4 ± 5,51 2522,0 + 0,67 17% 82% Nephropathy pos. 20,1 ± 3,61 2540,5 ± 0,54 14% 68% Nephropathy pos. 22,3 ± 4,72 2593,5 ± 0,30 7% 55% Nephropathy pos. 20,0 ± 4,87 2613,9 ± 0,83 14% 55% Nephropathy pos. 35,1 ± 1,62 2726,5 ± 0,67 61% 20% Nephropathy pos. 25,0 ± 4,39 2775,1 ± 0,56 12% 40% Nephropathy pos. 21,8 ± 3,78 2790,7 ± 0,55 19% 86% Nephropathy pos. 25,9 ± 3,30 2892,2 ± 0,50 9% 50% Nephropathy pos. 16,8 ± 2,72 2919,0 ± 0,26 2% 50% Nephropathy pos. 21,9 ± 3,23 2937,0 ± 0,49 13% 86% Nephropathy pos. 20,0 ± 4,81 2958,8 ± 0,80 5% 59% Nephropathy pos. 34,4 ± 2,72 2962,0 ± 0,54 12% 20% Nephropathy pos. 28,9 ± 3,56 3059,7 ± 0,78 30% 40% Nephropathy pos. 28,3 ± 5,96 3088,0 ± 0,79 7% 20% Nephropathy pos. 26,1 ± 2,72 3369,2 ± 0,73 21% 40% Nephropathy pos. 26,0 ± 2,89 3483,4 ± 0,95 30% 40% Nephropathy pos. 24,5 ± 3,92 4183,3 ± 1,44 4% 40% Nephropathy pos. 21,0 + 5,35 4241,0 ± 0,62 29% 73% Nephropathy pos. 23,4 + 4,09 4370,2 ± 1,01 11% 40% Nephropathy pos. 22,8 ± 2,94 4527,6 ± 0,67 1% 45% Nephropathy pos. 21,7 ± 3,00 4713,6 ± 0,44 7% 64% Nephropathy pos. 24,6 + 3,73 7556,6 ± 1,55 2% 40% Nephropathy pos. 16,7 ± 5,54 8055,1 ± 2,10 12% 40% Nephropathy pos. 13,2 ± 5,19 8765,8 ± 0,96 37% 82% Nephropathy pos. 15,3 ± 4,97 9181,0 ± 1,28 10% 64% Nephropathy pos. 14,0 ± 4,20 10046,1 ± 0,96 21% 77% Nephropathy pos. 18,7 ± 5,50 10208,0 ± 1,24 2% 40% Nephropathy pos. 17,4 ± 4,02 10518,2 ± 1,10 23% 64% Nephropathy pos. 35,3 ± 5,04 924,5 ± 0,12 50% 0% Nephropathy neg. 43,1 ± 2,61 928,4 ± 0,08 65% 14% Nephropathy neg. 45,7 ± 2,25 955,5 ± 0,14 60% 5% Nephropathy neg. 23,8 ± 2,94 1010,6 ± 0,09 67% 5% Nephropathy neg. 31,2 ± 1,53 1028,5 ± 0,09 84% 32% Nephropathy neg. 45,9 ± 2,27 1041,4 ± 0,10 57% 0% Nephropathy neg. 31,5 ± 1,98 1046,5 + 0,09 87% 32% Nephropathy neg.
WO 2007/082586 PCT/EP2006/050327 91 43,4 ± 2,24 1047,5 ± 0,12 68% 0% Nephropathy neg. 18,1 ± 4,34 1050,7 ± 0,12 60% 0% Nephropathy neg. 32,9 + 3,03 1084,4 ± 0,11 69% 18% Nephropathy neg. 46,7 ± 2,63 1125,5 ± 0,12 63% 9% Nephropathy neg. 46,3 ± 2,70 1157,5 ± 0,10 83% 32% Nephropathy neg. 43,7 + 1,70 1160,5 ± 0,07 72% 18% Nephropathy neg. 44,5 + 3,67 1179,5 ± 0,09 97% 36% Nephropathy neg. 45,0 ± 2,24 1191,6 ± 0,09 60% 9% Nephropathy neg. 46,2 ± 2,59 1195,5 ± 0,10 98% 32% Nephropathy neg. 44,2 ± 1,83 1200,6 ± 0,13 86% 0% Nephropathy neg. 45,9 ± 2,04 1223,5 ± 0,10 80% 9% Nephropathy neg. 44,5 ± 2,15 1239,6 ± 0,08 89% 0% Nephropathy neg. 47,8 ± 3,08 1246,6 ± 0,11 60% 5% Nephropathy neg. 46,8 ± 2,20 1254,7 ± 0,19 56% 5% Nephropathy neg. 43,2 ± 2,90 1261,5 ± 0,16 91% 36% Nephropathy neg. 48,6 ± 2,90 1262,5 ± 0,09 65% 0% Nephropathy neg. 43,9 ± 2,16 1277,6 ± 0,11 67% 0% Nephropathy neg. 36,7 ± 3,04 1288,7 ± 0,18 72% 23% Nephropathy neg. 47,2 ± 3,17 1292,5 ± 0,14 67% 18% Nephropathy neg. 47,8 ± 2,58 1308,5 ± 0,09 66% 0% Nephropathy neg. 48,2 ± 2,67 1321,6 ± 0,11 53% 0% Nephropathy neg. 34,8 ± 1,81 1321,7 ± 0,23 98% 41% Nephropathy neg. 46,0 ± 4,93 1351,7 ± 0,15 63% 9% Nephropathy neg. 47,7 ± 2,99 1367,6 ± 0,14 97% 23% Nephropathy neg. 37,8 + 2,93 1378,6 ± 0,16 87% 36% Nephropathy neg. 47,5 ± 2,59 1389,7 ± 0,15 86% 18% Nephropathy neg. 46,5 ± 2,28 1407,8 ± 0,20 79% 9% Nephropathy neg. 44,6 ± 4,84 1422,1 ± 0,33 70% 0% Nephropathy neg. 45,4 + 3,62 1423,8 ± 0,19 75% 0% Nephropathy neg. 48,0 ± 2,97 1424,7 ± 0,16 95% 18% Nephropathy neg. 47,6 ± 3,40 1446,7 ± 0,16 92% 23% Nephropathy neg. 46,5 + 2,95 1450,4 ± 0,25 62% 9% Nephropathy neg. 48,0 ± 2,95 1462,6 ± 0,17 97% 9% Nephropathy neg. 35,7 ± 1,90 1487,7 ± 0,15 70% 18% Nephropathy neg. 47,8 ± 2,35 1490,6 ± 0,12 72% 9% Nephropathy neg. 49,2 ± 2,77 1491,7 ± 0,12 81% 14% Nephropathy neg. 49,0 ± 3,14 1507,8 ± 0,17 99% 32% Nephropathy neg. 49,2 ± 2,86 1523,7 ± 0,11 97% 18% Nephropathy neg. 48,6 ± 2,70 1529,7 ± 0,19 83% 9% Nephropathy neg. 49,2 + 3,26 1539,7 ± 0,19 98% 23% Nephropathy neg. 49,0 ± 3,19 1545,7 ± 0,13 99% 23% Nephropathy neg. 49,8 ± 2,76 1561,6 ± 0,19 90% 18% Nephropathy neg. 48,4 + 3,12 1567,7 ± 0,20 65% 9% Nephropathy neg. 48,1 ± 2,66 1573,7 ± 0,27 63% 5% Nephropathy neg. 48,5 ± 4,03 1577,8 ± 0,35 94% 9% Nephropathy neg. 50,6 ± 3,40 1587,1 ± 0,34 65% 0% Nephropathy neg. 48,6 ± 2,68 1589,7 ± 0,14 86% 18% Nephropathy neg. 45,9 ± 3,83 1591,7 ± 0,30 79% 18% Nephropathy neg. 49,3 ± 3,22 1594,8 ± 0,14 88% 14% Nephropathy neg.
WO 2007/082586 PCT/EP2006/050327 92 48,8 ± 2,78 1605,7 ± 0,13 73% 18% Nephropathy neg. 48,5 ± 2,81 1611,7 ± 0,14 73% 5% Nephropathy neg. 46,3 ± 5,12 1636,4 ± 0,39 79% 23% Nephropathy neg. 49,5 + 3,37 1651,8 ± 0,19 99% 23% Nephropathy neg. 45,2 + 5,96 1657,7 ± 0,23 60% 5% Nephropathy neg. 49,5 ± 3,33 1673,8 ± 0,14 95% 23% Nephropathy neg. 49,6 ± 3,05 1689,8 ± 0,18 86% 0% Nephropathy neg. 26,9 + 3,18 1706,8 ± 0,30 78% 27% Nephropathy neg. 49,4 ± 2,84 1734,4 ± 0,40 65% 5% Nephropathy neg. 49,2 ± 3,17 1739,7 ± 0,22 59% 5% Nephropathy neg. 45,1 ± 4,21 1748,0 ± 0,28 55% 5% Nephropathy neg. 44,2 + 4,71 1813,6 ± 0,38 58% 5% Nephropathy neg. 39,1 ± 3,48 1817,0 ± 0,29 85% 18% Nephropathy neg. 51,7 ± 3,48 1841,0 ± 0,23 59% 9% Nephropathy neg. 50,4 ± 4,56 1848,2 ± 0,43 58% 0% Nephropathy neg. 51,5 ± 2,94 1856,8 ± 0,24 59% 5% Nephropathy neg. 52,7 ± 4,24 1863,8 ± 0,31 88% 14% Nephropathy neg. 52,7 ± 3,92 1885,8 ± 0,20 70% 5% Nephropathy neg. 47,7 ± 4,69 1902,1 ± 0,33 75% 0% Nephropathy neg. 50,6 ± 3,95 1924,0 ± 0,48 68% 0% Nephropathy neg. 26,6 ± 1,76 2048,5 ± 0,44 86% 20% Nephropathy neg. 25,8 ± 1,39 2085,9 ± 0,24 83% 32% Nephropathy neg. 39,9 ± 1,45 2087,8 ± 0,34 72% 23% Nephropathy neg. 52,8 ± 4,09 2117,1 ± 0,17 78% 9% Nephropathy neg. 28,3 ± 3,90 2129,7 ± 0,42 63% 0% Nephropathy neg. 40,4 ± 1,53 2158,9 ± 0,26 86% 32% Nephropathy neg. 39,7 ± 1,71 2174,9 ± 0,36 97% 45% Nephropathy neg. 32,6 ± 1,79 2227,1 ± 0,41 81% 23% Nephropathy neg. 29,3 ± 3,50 2249,0 ± 0,41 92% 41% Nephropathy neg. 40,6 + 1,25 2257,1 ± 0,35 94% 45% Nephropathy neg. 46,2 ± 5,11 2273,5 ± 0,38 71% 18% Nephropathy neg. 40,8 + 2,66 2296,0 ± 0,40 63% 20% Nephropathy neg. 40,9 ± 3,32 2327,6 ± 0,52 85% 36% Nephropathy neg. 41,8 ± 2,45 2343,3 ± 0,43 77% 27% Nephropathy neg. 40,8 ± 1,31 2385,3 ± 0,32 95% 45% Nephropathy neg. 40,9 ± 2,68 2471,5 ± 0,52 69% 14% Nephropathy neg. 41,5 ± 2,64 2493,5 ± 0,48 74% 18% Nephropathy neg. 52,9 ± 3,98 2570,4 ± 0,27 71% 5% Nephropathy neg. 34,1 ± 0,72 2642,8 ± 0,40 86% 36% Nephropathy neg. 36,1 ± 2,56 2687,1 ± 0,49 84% 23% Nephropathy neg. 42,8 ± 2,33 2710,6 ± 0,46 88% 18% Nephropathy neg. 50,6 ± 4,73 2748,6 ± 0,36 64% 0% Nephropathy neg. 37,8 ± 1,92 2986,6 ± 0,55 74% 23% Nephropathy neg. 23,3 ± 2,07 3007,4 ± 0,50 65% 9% Nephropathy neg. 25,9 + 2,35 3038,3 ± 0,70 46% 0% Nephropathy neg. 46,0 ± 2,91 3045,4 ± 0,36 59% 5% Nephropathy neg. 53,3 + 4,05 3057,2 ± 0,64 76% 9% Nephropathy neg. 38,9 ± 2,57 3109,0 ± 0,57 88% 14% Nephropathy neg. 41,9 + 3,55 3187,6 ± 0,47 71% 14% Nephropathy neg.
WO 2007/082586 PCT/EP2006/050327 93 26,6 ± 1,15 3193,6 ± 0,41 61% 0% Nephropathy neg. 48,3 ± 3,69 3223,8 + 0,41 88% 18% Nephropathy neg. 31,7 ± 3,65 3265,1 ± 0,64 93% 41% Nephropathy neg. 29,5 ± 1,76 3291,0 ± 0,52 81% 23% Nephropathy neg. 49,2 ± 3,70 3293,1 ± 0,43 91% 14% Nephropathy neg. 49,9 ± 3,57 3315,0 ± 0,45 67% 5% Nephropathy neg. 43,3 ± 2,04 3319,9 ± 0,66 86% 23% Nephropathy neg. 49,1 ± 3,35 3336,7 ± 0,38 63% 9% Nephropathy neg. 38,5 ± 2,05 3359,9 ± 0,42 98% 41% Nephropathy neg. 38,5 ± 1,92 3360,1 ± 0,65 98% 20% Nephropathy neg. 38,5 ± 2,03 3417,1 ± 0,48 95% 45% Nephropathy neg. 38,5 ± 1,09 3433,3 ± 0,43 92% 41% Nephropathy neg. 51,6 ± 3,50 3478,9 ± 0,48 74% 5% Nephropathy neg. 31,7 ± 2,29 3589,7 ± 0,48 73% 18% Nephropathy neg. 33,2 ± 3,71 3633,4 ± 0,95 80% 18% Nephropathy neg. 36,0 ± 3,18 3636,6 ± 0,73 58% 0% Nephropathy neg. 37,9 ± 2,69 3719,5 ± 0,61 67% 9% Nephropathy neg. 42,0 ± 3,21 3739,7 ± 0,99 73% 14% Nephropathy neg. 25,8 ± 1,20 3947,3 ± 0,67 92% 32% Nephropathy neg. 39,4 ± 1,13 4006,6 ± 0,49 62% 5% Nephropathy neg. 26,0 ± 3,97 4044,9 ± 0,56 78% 14% Nephropathy neg. 30,5 ± 2,17 4070,4 ± 0,48 57% 5% Nephropathy neg. 29,5 ± 0,93 4098,6 ± 0,52 86% 32% Nephropathy neg. 34,3 ± 2,08 4102,5 ± 0,50 77% 14% Nephropathy neg. 34,7 ± 0,63 4290,7 ± 0,52 76% 18% Nephropathy neg. 23,5 ± 1,61 4405,8 ± 0,54 51% 0% Nephropathy neg. 30,4 ± 1,31 4801,5 ± 1,06 65% 0% Nephropathy neg. 32,4 ± 1,31 4863,8 ± 0,64 67% 5% Nephropathy neg. 29,5 ± 2,25 5214,0 ± 1,29 51% 0% Nephropathy neg. 33,0 ± 0,99 6172,0 ± 1,57 65% 0% Nephropathy neg. 33,2 ± 0,75 6187,8 ± 0,75 95% 45% Nephropathy neg. 23,8 ± 1,86 9869,7 ± 1,06 69% 14% Nephropathy neg. Table 23: migration time [min] dt [min] mass [Da) 15,490396 0,158804 8054,473633 15,803237 0,155143 8765,233398 16,034266 0,174906 1621,9104 16,185061 0,147871 9180,99707 16,645294 0,198704 10045,20703 17,663696 0,165531 10388,81348 17,980883 0,178564 10518,18457 19,917442 0,234131 9220,939453 20,34516 0,170572 1877,789429 20,479975 0,221246 3842,693604 20,519386 0,265078 4747,932617 21,465685 0,217493 4154,003906 21,480436 0,362197 2427,251709 21,804012 0,271715 4240,856445 WO 2007/082586 PCT/EP2006/050327 94 22,221563 0,191069 4282,796387 22,777784 0,245503 3840,540527 24,304148 0,319715 7556,177734 24,579231 0,291986 879,519653 24,813087 0,224198 1867,731689 25,283239 0,22054 2266,040771 26,177101 0,289898 2172,188721 26,773794 0,352887 2914,05542 26,81407 0,297343 962,591919 28,254925 0,581783 4353,585938 28,825331 0,258778 1250,62439 29,308136 0,852391 1060,239014 29,822325 0,595913 1682,720947 30,75272 0,175961 943,492859 30,762201 0,263861 1108,647949 30,926645 0,138075 1368,781738 31,305229 0,301605 3987,548828 31,433071 0,515308 1099,419434 32,165497 0,198377 3122,730713 32,222111 0,226858 1829,089966 33,427856 0,151562 2767,015625 34,053886 0,252424 1302,691772 34,15913 0,233032 3722,875977 34,557327 0,186137 2039,143433 34,681156 0,20976 3685,918213 35,30254 0,207782 2389,097168 35,502213 0,388916 3209,800293 36,314056 0,183495 980,526123 36,404907 0,145751 1008,513733 36,424831 0,150486 1000,48761 36,720509 0,128397 2717,472656 36,777012 0,164648 2663,246826 37,557594 0,165628 3556,580566 37,572525 0,185484 1743,890381 37,680653 0,160958 1134,580566 37,700241 0,171622 4097,981934 38,050472 0,156383 3152,361572 38,155159 0,217341 2825,309082 38,17057 0,432096 882,532654 38,281631 0,20781 996,190369 38,57658 0,370648 1425,324829 38,687305 0,15052 3385,513916 38,830559 0,056085 1352,824097 38,921108 0,150325 5000,982422 39,241917 0,178206 3775,720459 39,433277 0,235333 3405,60791 39,484215 0,140887 1046,52771 39,513248 0,093703 2154,053955 39,936756 0,195951 6171,129395 40,533363 0,158628 1194,581543 40,537457 0,221485 2205,064941 40,607231 0,426674 1235,384888 WO 2007/082586 PCT/EP2006/050327 95 40,686531 0,122381 1265,634888 40,83009 0,191972 2642,264893 41,506096 0,161887 4159,304199 41,604115 0,217324 1250,585449 41,818069 0,163642 2742,253418 42,079609 0,266392 1463,643311 42,105633 0,172054 1489,658936 42,131275 0,184863 1473,643555 42,144161 0,162716 1451,710938 42,573879 0,234118 3098,450928 42,636433 0,041732 1487,660034 42,811199 0,246696 1579,670776 42,940624 0,1884 3121,243164 43,093792 0,106392 3271,523438 43,115334 0,607341 1834,878052 43,46143 0,193155 3442,135498 43,494144 0,20218 3495,841797 43,549488 0,217899 3473,905029 43,740391 0,12795 3108,919434 44,191006 0,18629 3359,583496 44,230297 0,233319 3416,526611 44,934914 0,127421 1991,917114 45,538418 0,214716 2197,337158 45,675098 0,12333 1889,864502 46,313114 0,259721 2385,597168 47,216648 0,168651 2649,602539 47,279705 0,127824 2343,072998 47,526871 0,19233 2584,635986 48,441795 0,239347 1160,526001 48,804813 0,251244 1261,53125 49,519478 0,243133 1274,625244 51,416531 0,33207 1195,518677 51,492035 0,213235 1211,559204 51,657627 0,822884 1223,348633 53,168346 0,293424 1351,643433 53,240913 0,216809 1367,655151 53,259499 0,15916 1770,30481 54,59832 0,234281 1507,742432 55,038143 0,329349 1594,211426 57,475471 0,325805 1840,810547 58,191887 0,129 2021,900879 58,898354 0,484288 2608,239746 60,082333 0,507699 1863,939453 Table 24: migration time [min] dt [min] mass (Dal 12,295616 0,092835 8053,516 12,331619 0,12201 1621,946 12,508785 0,139706 8765,729 12,696615 0,122507 9181,114 WO 2007/082586 PCT/EP2006/050327 96 12,906662 0,115952 10046,58 13,103853 0,041984 2427,001 14,332394 0,144029 4153,814 14,426023 0,131007 4240,702 14,496774 0,385605 3841,615 14,585806 0,105399 4282,281 15,094264 0,132582 879,5324 15,123884 0,069059 1868,033 15,236325 0,136994 7555,679 15,641728 0,159929 962,6218 16,194395 0,167525 1060,664 16,280394 0,28676 4353,476 16,363562 0,082856 1682,889 16,427116 0,09725 1743,982 16,50071 0,133981 1108,646 16,904119 0,128321 1829,115 17,017418 0,23895 3987,366 17,409172 0,158398 2767,263 17,716999 0,1571 1302,722 17,891594 0,202698 3722,962 18,049681 0,191037 2039,257 18,140236 0,176836 3686,508 18,528196 0,076336 3209,884 19,106394 0,148381 1008,572 19,118612 0,156251 1000,564 19,173443 0,122128 980,5635 19,335644 0,098819 2663,262 19,367334 0,112794 2718,314 20,023649 0,199337 3556,408 20,041323 0,195353 1134,629 20,063593 0,224531 4098,26 20,300522 0,113124 3152,333 20,347666 0,200969 882,5596 20,470793 0,208903 2825,334 20,889994 0,26629 3385,819 20,93943 0,057322 1425,772 21,519066 0,226397 5000,98 21,655712 0,298068 3775,697 21,755213 0,316991 1046,586 21,850452 0,518151 3405,871 22,747589 0,302407 1235,601 22,763943 0,277557 1194,603 22,997269 0,34528 1265,661 23,013165 0,225846 2642,188 23,017294 0,551478 6171,03 23,838888 0,406385 1250,653 24,025209 0,261109 2742,267 24,137253 0,135523 1463,693 24,14039 0,158709 1473,664 WO 2007/082586 PCT/EP2006/050327 97 24,220345 0,206216 1489,686 24,355286 0,409203 1451,684 24,686199 0,240303 3098,376 24,915867 0,332783 1579,718 25,093962 0,214003 3121,259 25,181305 0,33936 3272,276 25,634459 0,407648 3441,958 25,648405 0,344555 3495,801 25,928818 0,283113 3108,66 26,411203 0,355909 3359,75 26,493782 0,341234 3416,324 27,775286 0,346393 2196,686 28,415859 0,219954 2385,565 29,471397 0,2699 2649,791 29,74654 0,131224 2584,214 30,499264 0,32736 1160,556 30,832899 0,269278 1261,477 32,240211 0,415696 1195,543 32,240601 0,406316 1223,53 32,29216 0,268596 1212,024 33,24297 0,403599 1367,633 34,039223 0,467469 1507,75 34,274136 0,432896 1594,746 35,978645 0,326975 1841,202 37,237282 0,110906 2608,186 37,342949 0,6411 1863,833 Table 25: Sex Age Diagnosis S-creatinine Proteinuria Immunosuppression M 63 FSGS 95 0.02 PS M 18 FSGS 99 0.05 CsA M 63 FSGS 93 0.05 PS F 49 FSGS 80 0.05 CsA+PS F 23 FSGS 69 0.54 CsA F 26 FSGS 16 0,7 CsA F 56 FSGS 80 0.8 M 62 FSGS 150 1,9 M 26 FSGS 144 4,9 F 26 FSGS 150 11.0 CsA+PS M 69 MGN 128 0.02 CsA M 62 MGN 91 0.17 M 23 MGN 150 0.3 M 37 MGN 73 0.33 M 43 MGN 82 0.7 PS M 48 MGN 100 1.0 CsA+PS F 68 MGN 150 1.0 F 21 MGN 80 1.0 CsA+PS M 44 MGN 118 1.0 CsA M 45 MGN 93 1.3 WO 2007/082586 PCT/EP2006/050327 98 M 48 MGN 133 2.4 M 37 MGN 93 2.6 M 78 MGN 99 3.3 M 47 MGN 93 3.5 PS F 34 MGN 80 3.5 CsA+PS M 66 MGN 132 3.6 M 38 MGN 100 4.0 CsA+PS M 43 MGN 85 5,1 F 43 MCD 114 0.01 CsA M 45 MCD + 93 0.01 F 52 MCD + 118 0.01 M 52 MCD 93 0.01 F 44 MCD + 80 0.02 CsA M 39 MCD* 93 0.02 M 51 MCD 93 0.05 M 18 MCD .77 0.05 CsA+PS F 70 MCD * 95 0.08 M 69 MCD 93 0,08 F 29 MCD + 160 0.1 M 62 MCD + 93 0.1 M 21 MCD 57 0.12 F 43 MCD 114 0,01 CSA F 25 MCD 80 1,2 M 52 MCD 93 0.4 PS F 80 MCD * 145 7.9

Claims (18)

1. Use of the presence of at least one polypeptide marker in a urine sample for the diagnosis of a renal disease, wherein the polypeptide marker is selected from the group of polypeptide markers as shown in tables 1 to 22.
2. The use according to claim 1, wherein the renal disease is chosen from the group consisting of IgA-nephropathy, MGN, MCD, FSGS, and diabetic nephropathy.
3. The use according to claim 1, wherein the renal disease is IgA-nephropathy.
4. The use according to claim 1, wherein diagnosis relates to differential diagnosis between at least two diseases chosen from the group consisting of IgA-nephropathy, MGN, MCD, FSGS, and dia betic nephropathy.
5. The use according to claim 1, wherein the polypeptide marker is selected from the group of poly peptide markers as shown in tables 1 to 13.
6. The use according to claim 3, wherein the polypeptide marker is selected from the group of poly peptide markers as shown in tables 11 to 13.
7. A method for the diagnosis of a renal disease, the method comprising: a) measuring the presence or the absence of a polypeptide marker in a urine sample, wherein the polypeptide marker is selected from the group of polypeptide markers shown in tables 1 to 22, and b) comparing the probability of the presence of this marker in a disease patient to the prob ability of the presence of this marker in a control patient, wherein cl) if the probability of the presence of this marker in a disease patient is higher than the probability of the presence of this marker in a control patient, the presence of this marker is indicative for a higher probability of having the disease rather than the con trol condition, or c2) if the probability of the presence of this marker in a disease patient is lower than the probability of the presence of this marker in a control patient, the absence of the marker is indicative for a higher probability of having the disease rather than the con- WO 2007/082586 PCT/EP2006/050327 100 trol condition.
8. The method according to claim 7, wherein the individual probabilities in step b) are as indicated in the tables.
9. The method according to claim 7, wherein the control represents the healthy condition.
10. The method according to claim 7, wherein the control represents a renal disease, particularly chosen from the group consisting of IgA-nephropathy, MGN, MCD, FSGS, and diabetic neph ropathy.
11. The method according to claim 7, wherein the polypeptide marker is selected from the group of polypeptide markers shown in tables 11 to 13.
12. The method according to claim 7, wherein the method comprises detecting a plurality of the polypeptide markers, preferably at least 3, more preferably at least 10, most preferably at least 50 of the polypeptide markers.
13. The method according to claim 7, wherein ELISA, quantitative Western Blot, radio-immuno assay, surface plasmon resonance, array, gel electrophoresis, capillary electrophoresis, gas phase ion spectrometry, or mass spectrometry is used for detecting the presence of the marker or mark ers.
14. The method according to claim 7, wherein the polypeptide markers in the sample are separated by capillary electrophoresis before measurement.
15. The method according to claim 14, wherein mass spectrometry is used for detecting the presence of the marker or markers.
16. Use of capillary electrophoresis-mass spectrometry for the diagnosis, particularly differential diagnosis, of a renal disease in vitro.
17. The use according to claim 16, wherein the renal disease is selected from the group consisting of IgA-nephropathy, MGN, MCD, FSGS, and diabetic nephropathy.
18. Use of capillary electrophoresis-mass spectrometry for the differential diagnosis between at least two renal diseases selected from the group consisting of IgA-nephropathy, MGN, MCD, FSGS, and diabetic nephropathy.
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