CN105012314A - Application of Etonogestrel in the preparation of anti-prostate cancer products - Google Patents
Application of Etonogestrel in the preparation of anti-prostate cancer products Download PDFInfo
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- CN105012314A CN105012314A CN201510385950.5A CN201510385950A CN105012314A CN 105012314 A CN105012314 A CN 105012314A CN 201510385950 A CN201510385950 A CN 201510385950A CN 105012314 A CN105012314 A CN 105012314A
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Abstract
The present invention discloses application of Etonogestrel in the preparation of anti-prostate cancer products. The present invention discloses application of Etonogestrel in the preparation of anti-prostate cancer products. Experiments in the present invention conduct relocation on anti-tumor medicament Etonogestrel approved by FDA and CFDA; according to the different tumor cell lines (tissue types) and mutation sites, drugs with non-anti-tumor indications are screened, and the invention discovers the novel anti-prostate cancer application of Etonogestrel, so as to realize novel application of old medicament.
Description
Technical field
The present invention relates to biological technical field, particularly relate to a kind of Etonogestrel and preparing the application in anti-prostate cancer product.
Background technology
Tumor threatens the most common of human health to be also the most serious a kind of disease, and research and development high efficiency anti-tumor medicine is most important to the life cycle extending patient.In recent years, along with the develop rapidly of cancer genomics and molecular pharmacology, the research and development of new type antineoplastic medicine achieve good achievement, but because new drug development has high input, cycle, the long bottleneck that waits cannot overcome, and the feature such as tumor individual inheritance variation is large, caused many traditional anti-tumor medicine effects not add, new drug is expensive, and side effect is not bright.
The researcheres such as Barabasi AL were published in " Nature Reviews Genetics " opinion in 2011 the article pointed out, the molecular network analysis carried out based on GWAS result of study and mutual work group (interactome) strategy is expected to disclose the new drug target of complex disease and molecular marker, and the understanding that final formation is machine-processed to disease incidence and therapeutic scheme is brand-new.Even more noteworthy, medicine reorientation (drug repositioning) research finds, GWAS studies the tumor susceptibility gene of locking and has protein-protein interaction (protein-protein interaction with it, PPI) gene more easily becomes medicine indirectly target spot, and this finds that there is and helps explain that the mechanism of action of existing medicine and guides the research and development of new drug.2014, show in 101 tumor susceptibility genes of the rheumatoid arthritis that GWAS result of study confluence analysis obtains in the paper that the researcheres such as Okada Y are delivered on " Nature " and have 98 direct or indirect targets being used for treatment medicine for treating rheumatoid arthritis at present, but also studied by medicine reorientation, they have also found that the granted medicine for other indications of dozens of also can be used for treating rheumatoid arthritis.
Summary of the invention
This research is just by integrating the drug data base that in the cancer gene spectrum Cancer Gene Census of cancer group Cosmic version72 data base and protein interaction STRING version 10 data base and DrugBankversion4.2, FDA ratifies, the candidate's reorientation medicine obtained, examination experiment is carried out to tumor cell line, screens the antitumor drug made new advances.The candidate tumor doing tumor cell line screening suppresses medicine to see as follows:
Nicardipine,Promethazine,Estrone,Etonogestrel,Sunlidac,Etonogestrel,Et onogestrel,Levonorgestrel,Mesalazine,Indomethacin,Sulfasalazine,Balsalazid e,Irbesartan,Ibuprofen,Isoprenaline,Pentosan Polysulfate。
An object of the present invention is to provide the novelty teabag of Etonogestrel.
The application of Etonogestrel provided by the invention in preparation treatment carcinoma of prostate product.
Second object of the present invention is to provide the novelty teabag of Etonogestrel.
The invention provides the application of Etonogestrel in preparation suppression prostate gland cancer cell propagation product.
3rd object of the present invention is to provide the novelty teabag of Etonogestrel.
The invention provides the application of Etonogestrel in preparation reduction prostate gland cancer cell IC50 value product.
In above-mentioned application, described prostate gland cancer cell is DU-145.
In above-mentioned application, described product is medicine or test kit.
4th object of the present invention is to provide a kind of product.
Product provided by the invention, its active component is Etonogestrel; Described product has following at least one function:
1) carcinoma of prostate is treated;
2) prostate gland cancer cell propagation is suppressed;
3) prostate gland cancer cell IC50 value is reduced.
In the said goods, described prostate gland cancer cell is DU-145.
In the said goods, described product is medicine or test kit.
Experiment of the present invention proves, the present invention is to FDA, the granted medicine Etonogestrel of CFDA carries out tumour medicine reorientation, the cell line (organization type) different according to tumor and mutational site are not that anti-tumor drug screens to indication, find this novelty teabag of Etonogestrel anti-prostate cancer, realize old medicine and newly use.
Accompanying drawing explanation
Fig. 1 is 96 well culture plate medicine sieve medicine template distributions.
Fig. 2 is that Etonogestrel is responsive to carcinoma of prostate; EC50=11.6796; IC50=16.0136; R
2=0.9788.
Detailed description of the invention
The experimental technique used in following embodiment if no special instructions, is conventional method.
Material used in following embodiment, reagent etc., if no special instructions, all can obtain from commercial channels.
In following embodiment, medicine to be measured is Etonogestrel, and its chemical structural formula is:
it is drug bank product, and catalog number is DB00294.
The source of the prostate gland cancer cell DU-145 below in embodiment, people Lung Squamous Carcinoma Cells NCI-H1703 and human lung carcinoma cell NCI-H2122 is as follows:
DU-145 ATCC HTB-81
NCI-H1703 ATCC CRL-5889
NCI-H2122 ATCC CRL-5985
Main instrument below in embodiment and consumptive material
DMSO(from Sigma,Cat.No.D4540)
The 96-well white saturating Tissue Culture Plate in the end (from Corning, Cat.No.3610)
CellTiter Glo test kit (from Promega, Cat.No.G7573)
Doxorubicin positive drug (from MCE, Cat.No.HY-15142)
Fetal Bovine Serum(from Gibco,Cat#10099141)
100mm culture dish (from Corning, Cat#430167)
RPMI-1640medium(from Gibco,Cat#A1049101)
DMEM medium(from Gibco,Cat#11995081)
DMEM/F12medium(from Gibco,Cat#11330057)
EMEM medium(from Gibco,Cat#10370021)
Mutidrop 384 cell liquor separator (Thermo, Cat#5840150)
The multi-functional plate reading machine of EnSpire (Perkin Elmer, Cat#2300-001M)
Embodiment 1, CELLTITER-GLO detect Etonogestrel anti-prostate cancer
One, the preparation of orifice plate to be measured
1, plating cells
A) complete medium needed for each cell is prepared.
B) before experiment starts, confirm the medicine sieve cell name be marked on 100mm culture dish, culture medium and generation time, the information such as generation, guarantee that experiment is errorless.
C) attached cell operation refer step d) to i), suspension cell operation refer step j) to l).
D) vacuum pump is utilized to draw cell culture medium during sterile working.
E) with the aseptic PBS solution rinse cell surface layer of 2ml, then vacuum pump sucking-off PBS waste liquid is used.
F) 1ml 0.25% (w/v) Trypsin-0.038% (w/v) EDTA solution digestion cell is added gently to culture dish, mix gently several under, solution covers cell surface layer, under inverted microscope, observation of cell digestion situation, stops trypsinization effect when cell will come off.
G) in culture dish, add the preheated complete medium of 5ml 37 DEG C, blow and beat cell gently with pipet, make it split away off bottom culture dish.
H) this cell suspension is transferred in 15ml or 50ml sterile centrifugation tube, the centrifugal 5min of 1000rpm.
I) vacuum pump sterile working sucking-off supernatant culture medium is utilized.Add the complete medium re-suspended cell precipitation that 5ml 37 DEG C is preheated, blow and beat mixing gently.
J) blow and beat cell gently with pipet, make it split away off completely bottom culture dish.
K) this cell suspension is transferred in 15ml or 50ml sterile centrifugation tube, the centrifugal 5min of 1000rpm.
L) vacuum pump sterile working sucking-off supernatant culture medium is utilized.Add the complete medium re-suspended cell precipitation that 5ml 37 DEG C is preheated, blow and beat mixing gently.
M) count cell suspension with cell counter, adjustment cell suspension carries out plating cells experiment to proper density fishplate bar.
DU-145 cell is carried out according to the method described above, obtains DU-14596 porocyte culture plate.
DU-145 cell, complete medium is RPMI-1640, is life product, and A1049101, fishplate bar density (cells/well) is 4000.
2, medicine Etonogestrel to be measured prepares and dosing (200X final concentration):
1) medicine Etonogestrel motherboard preparation to be measured
A) with DMSO, medicine Etonogestrel to be measured is diluted to 20mM stand-by.
Getting the 20mM medicine 79 to be measured μ L configured in a) step adds in dilution plate the first row first hole, add the DMSO solvent of 54 μ L subsequently to the first row second hole in the 9th hole, 25 μ L solution are got in the second hole from the first hole, from the second hole, 25 μ L solution are got in the 3rd hole after mixing, the like to the 9th hole, ensure medicine successively carry out 3.16 times of multiple proportions gradient dilutions.
2) positive drug Doxorubicin (MCE, Cat.No.HY-15142) motherboard preparation
A) with DMSO, positive drug Doxorubicin is diluted to 6mM stand-by.
B) 6mM positive drug Doxorubicin solution is added in dilution plate, this medicine to be measured of DMSO solution 1:3.16 times of multiple proportions gradient dilution.
3, the preparation of medicine working plate and dosing
A) medicine to be measured and positive drug application of sample template are illustrated in fig. 1 shown below, and wherein, S1208: positive drug Doxorubicin, DMSO: Positive control wells, Cpd 1,2,3: medicine to be measured, DMSO final concentration is 0.5% (DMSO is compatible).
B) in working plate, add the specific complete medium of 95 μ l cell, corresponding 9 holes of each medicine, with multiple tracks volley of rifle fire difference transferase 45 μ l a series of (9 holes) solution (10X final concentration) that doubling dilution is good successively from medicine to be measured and positive drug doxorubicin motherboard, obtain the cell culture medium containing variable concentrations medicine.
C) from incubator, take out step 1 prepare DU-14596 porocyte culture plate, by Fig. 1 dosing template arrangement mode (Fig. 1) respectively to adding the above-mentioned cell culture medium (10X final concentration) containing variable concentrations medicine b) prepared of 10 μ l in DU-14596 porocyte culture plate, put into CO
2incubator 37 DEG C cultivates 72h, obtains the 96 hole medicine sieve plates of DU-145.
Not add the hole in contrast of any medicine.
Final concentration in 96 orifice plates of above-mentioned medicine to be measured, positive drug Doxorubicin and control wells and dosing situation as follows:
The final concentration (μM) of medicine to be measured in the 2-10 hole of Fig. 1 is followed successively by: 100,31.64557,10.01442,3.16912,1.002886,0.317369,0.100433,0.031783,0.010058;
The final concentration (μM) of positive drug Doxorubicin in the 2-10 hole of Fig. 1 is followed successively by: 30,9.493671,3.004326,0.950736,0.300866,0.095211,0.03013,0.009535,0.003017;
In addition, in 96 orifice plates S1208 hole (E1-H1 and A12-D12): 10 μ l final concentrations, 100 μMs of Doxorubicin solution (solvent is the complete medium solution comprising 0.5%DMSO), DMSO hole (A1-D1, E12-H12 and A11-H11): 10 μ l comprise the complete medium solution of 0.5%DMSO.
Two, CELLTITER-GLO fluorecyte activity monitor system detects
1, CellTiter-Glo preparation of reagents
A) before using, CellTiter-Glo reagent Buffer is melted, equilibrate to room temperature and use.
B) before using, CellTiter-Glo reagent agar substrate is melted, equilibrate to room temperature and use.
C) get the CellTiter-Glo Buffer that 100ml balances to join in bottled CellTiter-Glo reagent agar substrate, make its abundant resuspended formation enzyme/substrate mixture, namely so-called CellTiter-Glo detectable.
D) mix vortex gently, and be repeatedly inverted the uniform solution of acquisition.In general, in 1 minute, CellTiter-Glo substrate reagent will fully dissolve, subpackage, keeps in Dark Place for subsequent use at-20 DEG C, avoids multigelation.
2, detect
A), before detecting, the 96 hole medicine sieve plates of above-mentioned one 3 DU-145 obtained are balanced 20-30 minute at room temperature.
B) cellular morphology and the death condition of every block culture plate observed by inverted microscope, mark abnormal conditions and repetition measurement once.
C) in all medicine sieve apertures, the CellTiter-Glo reagent of above-mentioned 1 preparation of 100 μ l is added, mixing.
D) on 96 hole microwell plate agitators, fully shake mixing 2 minutes, make the complete cracking of cell.
E) lucifuge room temperature is placed after 15 minutes and is carried out luminescence signal detection, ensures the stability of signal.
F) use during the multi-functional plate reading machine 570nm of EnSpire and read luminescence signal.
G) analyzing and processing data.
The 96 hole medicine sieve plate results of DU-145 as shown in Figure 2.
Calculate IC50 value, result is as shown in table 1.
Adopting uses the same method detects the IC50 value that Etonogestrel makes employment Lung Squamous Carcinoma Cells NCI-H1703 and human lung carcinoma cell NCI-H2122, and result is as table 1.
Can find out, Etonogestrel has Specific Inhibitory Effect to prostate gland cancer cell propagation, can be used as the medicine for the treatment of carcinoma of prostate.
Table 1 is the IC50 value of different cell under Etonogestrel drug effect
| Cell | IC50 value |
| DU-145 | 16.0136 |
| NCI-H1703 | 100 |
| NCI-H2122 | 100 |
Claims (7)
- The application of 1.Etonogestrel in preparation treatment carcinoma of prostate product.
- 2.Etonogestrel suppresses the application in prostate gland cancer cell propagation product in preparation.
- 3. application according to claim 1 and 2, is characterized in that: described prostate gland cancer cell is DU-145.
- 4., according to described application arbitrary in claim 1-3, it is characterized in that: described product is medicine or test kit.
- 5. a product, its active component is Etonogestrel; Described product has following 1) and/or 2) function:1) carcinoma of prostate is treated;2) prostate gland cancer cell propagation is suppressed.
- 6. product according to claim 5, is characterized in that: described prostate gland cancer cell is DU-145.
- 7. the product according to claim 5 or 6, is characterized in that: described product is medicine or test kit.
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| CN201510385950.5A CN105012314B (en) | 2015-06-30 | 2015-06-30 | Applications of the Etonogestrel in anti-prostate cancer product is prepared |
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| CN201510385950.5A CN105012314B (en) | 2015-06-30 | 2015-06-30 | Applications of the Etonogestrel in anti-prostate cancer product is prepared |
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Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN105816467A (en) * | 2016-03-18 | 2016-08-03 | 上海交通大学 | Application of Etonogestrel in preparation of products for preventing B-cell lymphoma |
Citations (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN1349416A (en) * | 1999-05-04 | 2002-05-15 | 美国家庭用品有限公司 | Contraceptive compositions contaiing indoline derivatives and progestational agents |
-
2015
- 2015-06-30 CN CN201510385950.5A patent/CN105012314B/en active Active
Patent Citations (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN1349416A (en) * | 1999-05-04 | 2002-05-15 | 美国家庭用品有限公司 | Contraceptive compositions contaiing indoline derivatives and progestational agents |
Non-Patent Citations (1)
| Title |
|---|
| 陆连英等: "雌激素受体和孕激素受体在前列腺癌中的表达", 《南通医学院学报》 * |
Cited By (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN105816467A (en) * | 2016-03-18 | 2016-08-03 | 上海交通大学 | Application of Etonogestrel in preparation of products for preventing B-cell lymphoma |
| WO2017156967A1 (en) * | 2016-03-18 | 2017-09-21 | 上海交通大学 | Use of etonogestrel in preparation of anti-b cell lymphoma products |
| CN105816467B (en) * | 2016-03-18 | 2019-01-22 | 上海交通大学 | Etonogestrel is preparing the application in anti-B cell lymphoma product |
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| CN105012314B (en) | 2017-12-08 |
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