CN109718233A - Bergenin is in preparation for treating the application in pulmonary fibrosis disease drug - Google Patents
Bergenin is in preparation for treating the application in pulmonary fibrosis disease drug Download PDFInfo
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- CN109718233A CN109718233A CN201910150548.7A CN201910150548A CN109718233A CN 109718233 A CN109718233 A CN 109718233A CN 201910150548 A CN201910150548 A CN 201910150548A CN 109718233 A CN109718233 A CN 109718233A
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- pulmonary fibrosis
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Abstract
The present invention provides Bergenin in preparation for treating the application in pulmonary fibrosis disease drug, wherein the structure of Bergenin is shown below,It is experimentally confirmed, Bergenin has good effect to pulmonary fibrosis, has no adverse reaction, and can slow down the mouse pulmonary fibrosis of bleomycin induced, has a good application prospect in treatment, alleviation or in terms of improving pulmonary fibrosis disease.
Description
Technical field
The invention belongs to field of pharmaceutical chemistry technology, more particularly, to a kind of Bergenin in preparation for treating lung fiber
Change the application in disease medicament.
Background technique
Pulmonary fibrosis is the last rank of a variety of interstitial lung diseases (interstitial lung diseases, ILDs)
Section, it is characterized in that pulmonary parenchyma is destroyed and extrtacellular matrix deposition is in interstitial lung and alveolar space.This disease was once considered
It is a kind of chronic inflammation processes, but current evidence shows that fiberization is the alveolar epithelial cells by abnormal activation
(AECs) it drives.These cells generate medium, by reside mesenchymal cell proliferation, the attraction of Circulating fibrocyte and
The formation of stimulation induced fibroblast and myofibroblast stove that epithelial cell changes to mesenchymal cell.Fibroblast
Excessive extracellular matrix, mainly collagen are secreted with myofibroblast stove, lead to the cicatrization of lung structure and is broken
It is bad.Idiopathic pulmonary fibrosis (idiopathic pulmonary fibrosis, IPF) is the most common diffusivity pulmonary fibrosis
Disease, etiology unknown, pathogenesis are unclear so far, lack effective treatment means, median survival interval only 3-5.Traditional view
Think that IPF is to be caused by chronic inflammation, however biopsy does not show obvious inflammation, in disease early stage also few protrusions
Inflammatory signs, and clinically anti-inflammatory treatment produces little effect.The disease is apt to occur in 50~70 years old, especially there is the people of smoking history
Group, male are higher than women.With the pollution of atmosphere, the deterioration of environment, disease incidence has in recent years for epidemiologic data report display
Ascendant trend.The disease incidence of statistics IPF is 6.8-16.3/10 ten thousand at present, and illness rate is 14-42.7/10 ten thousand, in recent years illness people
Group is on the rise.Number of patients whole world conservative estimation 50,000,000, it is contemplated that there is IPF patient 600,000 or so in China.Every year
IPF death is up to 40000.
It in recent years, include glucocorticoid, colchicin, ciclosporin A, half Guang of acetyl for the clinical test drug of IPF
Amino acid, Bosentan, Etanercept, anti-coagulants, Nintedanib, pirfenidone and Imatinib etc., but IPF patient to hormone and
The therapeutic response of various drugs is generally poor, there is no the drug that can definitely improve the final prognosis of patient, American Thoracic doctor at present
Learning to point out in the IPF guide of (ATS), patient IPF must recommend and effectively treat just to be lung transplantation to state of an illness advanced stage unique value,
But since expenses of surgical treatment is expensive, skill level is complicated, donor lung tissue source is in short supply, organ transplantation ethics and medical service law
The presence for the factors such as Laws & Regulations are unsound, limits development of the lung transplantation as IPF patient treatment in China.
There are two the marketed drugs for being directed to the disease at present, is pirfenidone and the Buddhist nun of Boehringer Ingelheim of Roche respectively
Da Nibu, but patient survival cannot be all effectively improved, medical expense is high, and clinical demand is far unmet.Therefore it illustrates
The occurrence and development mechanism of pulmonary fibrosis explores new potential drug target, develops for the curative effect confirmation of pulmonary fibrosis, phase
There is important social effect and medical significance to the drug of safety, reasonable price.
Bergenin (Bengenin) derives from saxifragaceae plant purple bergenia herb herb, Rhizoma Seu Herba Bergeniae, and Myrsinacea is planted
Object ardisia crispa root, stem, leaf.With analgesia, calmness, hypnosis and stable effect.Its analgesic activity is weaker than pethidine, is better than general solution
Hot antalgesic.The apnea inhibiting effect under therapeutic dose, does not also cause gastrointestinal smooth muscle spasmus.To Chronic persistent pain
And internal organ dull pain effect is preferable, it is poor to acute sharp pain (such as postoperative pain, treatment of traumatic pain etc.), advanced cancer pain effect.
While generating analgesic activity, calm and hypnosis can be caused.But it is fine so far, to there is no Bergenin that can slow down idiopathic lung
The relevant report of dimensionization.
Summary of the invention
In view of this, the present invention is directed to propose a kind of substance suitable for treating specific pulmonary fibrosis disease drug.
In order to achieve the above objectives, the technical scheme of the present invention is realized as follows:
Bergenin is in preparation for treating the application in pulmonary fibrosis disease drug, wherein the knot of the Bergenin
Shown in structure such as following formula (I):
Preferably, the pulmonary fibrosis disease is idiopathic pulmonary fibrosis disease.
Preferably, the dosage of the Bergenin is 10mg/kg~400mg/kg.
Preferably, form of administration is tablet, capsule, pill, suppository, aerosol, oral liquid, granule, dissipates
Agent, injection, syrup, vina, tincture, distillate medicinal water or film.
The present invention also provides a kind of drugs for treating pulmonary fibrosis disease, including Bergenin and Bergenin are in medicine
Acceptable auxiliary material on, and pharmaceutically one of acceptable salt, ester, hydrate and two or more.
Preferably, the pulmonary fibrosis disease is idiopathic pulmonary fibrosis disease.
Preferably, pharmaceutically acceptable salt includes organic salt and inorganic salts.
Preferably, the organic salt includes mesylate, formates, acetate, trifluoroacetate, maleate, winestone
Hydrochlorate, succinate, fumarate, citrate, benzene sulfonate, toluenesulfonate, naphthalene sulfonate, lactate and benzene first
One or more of hydrochlorate;The inorganic salts include one of hydrochloride, hydrobromate, sulfate and phosphate or
It is two or more.
Preferably, the drug is one of oral, injection, implantation, external application, spraying or Sucked medicine form.
Compared with the existing technology, Bergenin of the present invention is in preparation for treating in pulmonary fibrosis disease drug
Using having the advantage that
It is of the invention studies have shown that Bergenin has good effect to pulmonary fibrosis, have no adverse reaction, Bo Lai can be slowed down
The mouse pulmonary fibrosis of mycin induction has a good application prospect in treatment, alleviation or in terms of improving pulmonary fibrosis disease.
Detailed description of the invention
Fig. 1 is the changes of weight curve of each group mouse.
Fig. 2 is the collagen content of each group mouse lung.
Fig. 3 is each group mouse pulmonary fibrosis area;
Fig. 4 is each group mouse pulmonary fibrosis ratio column diagram.
Specific embodiment
In addition to being defined, technical term used in following embodiment has universal with those skilled in the art of the invention
The identical meanings of understanding.Test reagent used in following embodiment is unless otherwise specified conventional biochemical reagent;It is described
Experimental method is unless otherwise specified conventional method.
Below with reference to embodiment, the present invention will be described in detail.
The present invention provides a kind of Bergenins to prepare the application in the drug for treating pulmonary fibrosis disease,
In, shown in the structure of Bergenin such as following formula (I):
Embodiment 1
Influence of the Bergenin to the mouse idiopathic pulmonary fibrosis of bleomycin induced
The preparation of pulmonary fibrosis animal model: C57BL/6J is taken, mass fraction is by (week old 8-10 weeks) wild-type mice
10% chloraldurate gives mouse peritoneal injecting anesthetic with 0.5mL/100g (weight), and it is mould that intratracheal invasive injection 2U/Kg wins Lay
Element.
It is grouped situation: the physiological saline (mass fraction 0.9%Nacl) of normal group (sodium chloride group) injection same volume;
Model group is handled the 7th to 14 day according to the above modeling and in bleomycin, gives mouse coordinative solvent carboxymethyl by stomach-filling daily
Sodium cellulosate;Mouse 100mg/kg gives by stomach-filling daily when bleomycin is handled the 7th to 14 day in Bergenin treatment group
Bergenin, using coordinative solvent sodium carboxymethylcellulose as control.Each group Lung collagen and fibrosis are detected at the 14th day
Severity.The every day entry mouse weight of each group draws changes of weight curve.
Table 1 is the changes of weight table of each group mouse
Lung collagen detection (i.e. hydroxyproline content measurement): injecting the 14th day execution mouse in bleomycin, separates
Mouse right lung, is put into 5mL amperes of bottles, and 120 DEG C of baking oven drying are added the hydrochloric acid that 3ml concentration is 12mol/L, hydrolyze 6 at 120 DEG C
Hour, pH to 6.5-8.0 is adjusted with the NaOH that concentration is 10 mol/L after hydrolysis, is filtered using the filter that aperture is 5 μm residual
Slag obtains filtrate, and it is 10 mL that PBS (phosphate buffer solution) adjustment total volume is added in filtrate, obtains sample A;Take 50 μ L samples
350 μ L deionized waters are added in A, and toluene-sodium-sulfonchloramide (Chloramine T) solution that 200 mL concentration are 1.41% is added, incubation at room temperature
20 minutes, the perchloric acid solution that 200 μ L concentration are 18.9% is added, and (perchloric acid was incubated at room temperature 5 minutes, is added
200 μ L concentration are paradime thylaminobenzaldehyde (P-DMAB) solution that concentration is 20%, and 65 DEG C are incubated for 20 minutes, obtain sample
B;It takes 200 μ L sample B to measure light absorption value of the sample B at 570nm wavelength into 96 orifice plates, utilizes L- hydroxyproline standard product
(Sigma) concentration and absorbance is transverse and longitudinal coordinate, draws standard curve, and the corresponding regression equation of establishing criteria curve calculates
The concentration of institute's sample hydroxyproline.
The collagen content table of 2 each group mouse lung of table
Fibrosis area quantitative statistics are carried out to lung tissue section: mouse lung is fixed by paraformaldehyde, is routinely dehydrated,
After paraffin embedding, slice, H&E (haematoxylin Yihong) dyeing, the processing of neutral gum mounting, dyed using microscope acquisition HE is just set
Image data, every slice randomly select ten visuals field, using 6.0 software of Image-Pro Plus to pulmonary fibrosis area into
Row statistics.
Table 3 is each group mouse pulmonary fibrosis ratio table
Experimental result is as shown in Figures 1 to 4, and as shown in Figure 1, mouse weight keeps flat after Bergenin treatment group self administration of medication
Surely, show that Bergenin can improve animal health condition;By Fig. 2 it is found that compared with the mouse of model group, Bergenin is controlled
Hydroxyproline content is substantially reduced in the lung tissue for the treatment of group group mouse, shows that Bergenin can reduce what bleomycin was induced
Collagen content inhibits the synthesis of collagen in the lung tissue of bleomycin induced, and p < 0.05, i.e., statistically have conspicuousness
Difference;And as can be seen from figs. 3 and 4 H&E dyeing observation and statistical analysis show the mouse pulmonary fibrosis of Bergenin treatment group
Degree is significantly lower than model group mouse, shows that Bergenin can effectively slow down the mouse pulmonary fibrosis of bleomycin induced.
To sum up, Bergenin has good effect to pulmonary fibrosis, has no adverse reaction, and can slow down the small of bleomycin induced
Mouse pulmonary fibrosis has a good application prospect in treatment, alleviation or in terms of improving pulmonary fibrosis disease.
The above is only a specific embodiment of the invention, are not intended to limit the invention, all in spirit and original of the invention
Within then, any modification, equivalent replacement, improvement and so on be should all be included in the protection scope of the present invention.
Claims (9)
1. Bergenin is in preparation for treating the application in pulmonary fibrosis disease drug, wherein the structure of the Bergenin
As shown in following formula (I):
2. application according to claim 1, it is characterised in that: the pulmonary fibrosis disease is idiopathic pulmonary fibrosis disease
Disease.
3. application according to claim 1, it is characterised in that: the dosage of the Bergenin is 10mg/kg~400mg/
kg。
4. the form of administration of application according to claim 1 is tablet, capsule, pill, suppository, aerosol, oral solution
Body preparation, granule, powder, injection, syrup, vina, tincture, distillate medicinal water or film.
5. a kind of drug for treating pulmonary fibrosis disease, which is characterized in that pharmaceutically including Bergenin and Bergenin
Acceptable auxiliary material, and pharmaceutically one of acceptable salt, ester, hydrate and two or more.
6. drug according to claim 5, it is characterised in that: the pulmonary fibrosis disease is idiopathic pulmonary fibrosis disease
Disease.
7. drug according to claim 5, it is characterised in that: pharmaceutically acceptable salt includes organic salt and inorganic salts.
8. drug according to claim 7, it is characterised in that: the organic salt includes mesylate, formates, acetic acid
Salt, trifluoroacetate, maleate, tartrate, succinate, fumarate, citrate, benzene sulfonate, to methylbenzene
One or more of sulfonate, naphthalene sulfonate, lactate and benzoate;The inorganic salts include hydrochloride, hydrogen bromine
One or more of hydrochlorate, sulfate and phosphate.
9. drug according to claim 4 be oral, injection, implantation, external application, be sprayed or Sucked medicine form in one
Kind.
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| CN201910150548.7A CN109718233A (en) | 2019-02-28 | 2019-02-28 | Bergenin is in preparation for treating the application in pulmonary fibrosis disease drug |
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| CN201910150548.7A CN109718233A (en) | 2019-02-28 | 2019-02-28 | Bergenin is in preparation for treating the application in pulmonary fibrosis disease drug |
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Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
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| CN110403949A (en) * | 2019-08-21 | 2019-11-05 | 天津龙尔达科技发展有限公司 | Application of salidroside in preparation of medicine for treating pulmonary fibrosis diseases |
| CN110522835A (en) * | 2019-07-19 | 2019-12-03 | 江西中医药大学 | Pharmaceutical composition and the preparation method and application thereof with lung mescenchymal stem cell directed differentiation effect in regulation pulmonary fibrosis microenvironment |
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Cited By (2)
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| CN110522835A (en) * | 2019-07-19 | 2019-12-03 | 江西中医药大学 | Pharmaceutical composition and the preparation method and application thereof with lung mescenchymal stem cell directed differentiation effect in regulation pulmonary fibrosis microenvironment |
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Application publication date: 20190507 |