CN117567544A - Application of pentacyclic triterpene compounds with alpha, beta-unsaturated ketone structures in preventing and treating neurodegenerative diseases - Google Patents
Application of pentacyclic triterpene compounds with alpha, beta-unsaturated ketone structures in preventing and treating neurodegenerative diseases Download PDFInfo
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- CN117567544A CN117567544A CN202311516483.6A CN202311516483A CN117567544A CN 117567544 A CN117567544 A CN 117567544A CN 202311516483 A CN202311516483 A CN 202311516483A CN 117567544 A CN117567544 A CN 117567544A
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- ODLHGICHYURWBS-LKONHMLTSA-N trappsol cyclo Chemical compound CC(O)COC[C@H]([C@H]([C@@H]([C@H]1O)O)O[C@H]2O[C@@H]([C@@H](O[C@H]3O[C@H](COCC(C)O)[C@H]([C@@H]([C@H]3O)O)O[C@H]3O[C@H](COCC(C)O)[C@H]([C@@H]([C@H]3O)O)O[C@H]3O[C@H](COCC(C)O)[C@H]([C@@H]([C@H]3O)O)O[C@H]3O[C@H](COCC(C)O)[C@H]([C@@H]([C@H]3O)O)O3)[C@H](O)[C@H]2O)COCC(O)C)O[C@@H]1O[C@H]1[C@H](O)[C@@H](O)[C@@H]3O[C@@H]1COCC(C)O ODLHGICHYURWBS-LKONHMLTSA-N 0.000 description 1
- 238000002371 ultraviolet--visible spectrum Methods 0.000 description 1
- OOTXFYSZXCPMPG-BMYLZFHVSA-N ursane Chemical compound C1CCC(C)(C)[C@@H]2CC[C@@]3(C)[C@]4(C)CC[C@@]5(C)CC[C@@H](C)[C@H](C)[C@H]5[C@H]4CC[C@@H]3[C@]21C OOTXFYSZXCPMPG-BMYLZFHVSA-N 0.000 description 1
- 235000010447 xylitol Nutrition 0.000 description 1
- 239000000811 xylitol Substances 0.000 description 1
- 229960002675 xylitol Drugs 0.000 description 1
- HEBKCHPVOIAQTA-SCDXWVJYSA-N xylitol Chemical compound OC[C@H](O)[C@@H](O)[C@H](O)CO HEBKCHPVOIAQTA-SCDXWVJYSA-N 0.000 description 1
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- C07—ORGANIC CHEMISTRY
- C07J—STEROIDS
- C07J63/00—Steroids in which the cyclopenta(a)hydrophenanthrene skeleton has been modified by expansion of only one ring by one or two atoms
- C07J63/008—Expansion of ring D by one atom, e.g. D homo steroids
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- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
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- A61P25/00—Drugs for disorders of the nervous system
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- A61P25/16—Anti-Parkinson drugs
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- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P25/00—Drugs for disorders of the nervous system
- A61P25/28—Drugs for disorders of the nervous system for treating neurodegenerative disorders of the central nervous system, e.g. nootropic agents, cognition enhancers, drugs for treating Alzheimer's disease or other forms of dementia
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Abstract
The invention discloses functions and applications of pentacyclic triterpene compounds in preventing and/or treating neurodegenerative diseases, the compounds are separated and extracted from cynomorium songaricum medicinal materials, and the inventor finds that in the process of evaluating pharmacological activity of the compounds: the compound has remarkable protection effect on nerve cell injury induced by glutamic acid and remarkable protection effect on nerve cell injury induced by oxygen glucose deprivation, so that the compound can be used for treating and preventing neurodegenerative diseases such as stroke, brain injury, amyotrophic lateral sclerosis, huntington disease, parkinson disease and Alzheimer disease, and can be developed into medicines.
Description
Technical Field
The invention relates to the technical field of medicines, and relates to application of pentacyclic triterpene compounds in preparation of medicines for preventing and/or treating neurodegenerative diseases.
Background
Neurodegenerative diseases, characterized by massive loss of specific neurons, are a complex disease with severe disability and mortality in progressive development. Acute neurodegenerative diseases and chronic neurodegenerative diseases are classified, the former mainly including stroke (stroke), brain injury (brain injury); the latter mainly includes Amyotrophic Lateral Sclerosis (ALS), huntington's Disease (HD), parkinson's Disease (PD), alzheimer's Disease (AD), and the like. As the population ages, neurodegenerative diseases have become a serious medical problem in modern society. The neurodegenerative diseases have various pathogenic factors and complex pathogenesis, so that the types of medicines for treating the neurodegenerative diseases are more, and neuroprotective medicines including antioxidant medicines, glutamate receptor antagonists, calcium ion antagonists, anti-inflammatory medicines, anti-apoptosis medicines and the like are important therapeutic measures.
The Chinese medicine believes that the kidney is in the brain and the kidney can prevent and treat central nervous system diseases. A great deal of modern medical research also suggests that kidney tonifying is a very promising approach to treat neurodegenerative diseases.
The herba Cynomorii is dry fleshy stem of Cynomorium songaricum Cynomorium songaricum rupr. Herba Cynomorii has effects of invigorating kidney yang, replenishing essence and blood, loosening bowel to relieve constipation, and can be used for treating kidney yang deficiency, essence and blood deficiency, soreness of waist and knees, sexual impotence, spermatorrhea, and constipation due to intestinal dryness. As a common tonic, cynomorium songaricum is mainly distributed in desert areas such as Xinjiang, qinghai, gansu, ningxia, inner Mongolia, shaanxi and the like, and is known as desert ginseng. The cynomorium songaricum is taken as an important kidney-yang tonifying medicament in traditional Chinese medicines, and has more progress in the aspects of anti-aging, neuroprotection, antioxidation and other pharmacological activities in the cynomorium songaricum extract in recent years, and particularly has researches showing that: ethyl acetate extract (Zheng Lingyan, han Ruilan, 2016) of cynomorium songaricum extract can significantly improve learning and memory retention of D-galactose-aging and scopolamine-aging mice. However, the research on the active ingredients in cynomorium songaricum is very weak, and no report on the neuroprotective active ingredients in cynomorium songaricum exists at present.
Based on the earlier-stage study on the chemical components of cynomorium songaricum, the inventor finds that most pentacyclic triterpene components in cynomorium songaricum, including unique malonate triterpenes in cynomorium songaricum such as compound 16 and p-hydroxy cinnamic acid ester triterpenes such as compound 19-23, have remarkable neuroprotective activity, and thus have good application prospects in the aspect of treating neurodegenerative diseases.
Disclosure of Invention
The invention aims to solve the technical problem of providing pentacyclic triterpene compounds, application of pharmaceutical compositions containing the pentacyclic triterpene compounds in preparation of products for preventing and/or treating neurodegenerative diseases, and further provides a preparation method of the pentacyclic triterpene compounds.
In order to solve the technical problems of the invention, the invention adopts the following technical scheme:
the first aspect of the invention provides application of pentacyclic triterpene compounds derived from cynomorium songaricum in preparation of products for preventing and/or treating neurodegenerative diseases, wherein the structures of the compounds are as follows:
in a second aspect, the present invention provides the use of a pharmaceutical composition comprising a pentacyclic triterpene compound according to the first aspect, for the preparation of a product for the prophylaxis and/or treatment of neurodegenerative diseases, which pharmaceutical composition may be prepared according to methods known in the art. Any dosage form suitable for human or animal use may be made by combining the compounds of the invention with one or more pharmaceutically acceptable solid or liquid excipients and/or adjuvants. The compounds of the present invention are typically present in the pharmaceutical compositions thereof in an amount of 0.1 to 95% by weight.
The compounds of the present invention or pharmaceutical compositions containing them may be administered in unit dosage form by the enteral or parenteral route, such as oral, intravenous, intramuscular, subcutaneous, nasal, oral mucosal, ocular, pulmonary and respiratory, cutaneous, vaginal, rectal, etc.
The dosage form may be a liquid, solid or semi-solid dosage form. The liquid dosage forms can be solutions (including true solution and colloid solution), emulsions (including o/w type, w/o type, multiple emulsions and liposomes), suspensions, injections (including water injection, powder injection and infusion), eye drops, nasal drops, lotions, liniments and the like; the solid dosage forms can be tablets (including common tablets, enteric coated tablets, buccal tablets, dispersible tablets, chewable tablets, effervescent tablets, orally disintegrating tablets), capsules (including hard capsules, soft capsules and enteric coated capsules), granules, powder, micropills, dripping pills, suppositories, films, patches, aerosol (powder) and sprays; the semisolid dosage form may be an ointment, gel, paste, or the like.
The compound or the pharmaceutical composition containing the same can be prepared into common preparations, slow-release preparations, controlled-release preparations, targeted preparations and various microparticle administration systems.
For the purpose of tableting the compound of the present invention or a pharmaceutical composition containing the same, various excipients known in the art may be widely used, including diluents, binders, wetting agents, disintegrants, lubricants, glidants. The diluent can be starch, dextrin, sucrose, glucose, lactose, mannitol, sorbitol, xylitol, microcrystalline cellulose, calcium sulfate, calcium hydrogen phosphate, calcium carbonate, etc.; the wetting agent can be water, ethanol, isopropanol, etc.; the binder may be starch slurry, dextrin, syrup, mel, glucose solution, microcrystalline cellulose, acacia slurry, gelatin slurry, sodium carboxymethyl cellulose, methyl cellulose, hydroxypropyl methylcellulose, ethyl cellulose, acrylic resin, carbomer, polyvinylpyrrolidone, polyethylene glycol, etc.; the disintegrating agent can be dry starch, microcrystalline cellulose, low-substituted hydroxypropyl cellulose, cross-linked polyvinylpyrrolidone, cross-linked sodium carboxymethyl cellulose, sodium carboxymethyl starch, sodium bicarbonate and citric acid, polyoxyethylene sorbitol fatty acid ester, sodium dodecyl sulfonate, etc.; the lubricant and glidant may be talc, silicon dioxide, stearate, tartaric acid, liquid paraffin, polyethylene glycol, and the like.
The tablets may be further formulated into coated tablets, such as sugar coated tablets, film coated tablets, enteric coated tablets, or bilayer and multilayer tablets.
For the preparation of the dosage unit into a capsule, the compound of the present invention or a pharmaceutical composition containing the same may be mixed with a diluent, a glidant, and the mixture may be directly placed in a hard capsule or a soft capsule. The compound of the invention or the pharmaceutical composition containing the same can be prepared into particles or pellets by mixing with a diluent, a binder and a disintegrating agent, and then placed into hard capsules or soft capsules. The diluents, binders, wetting agents, disintegrants and glidants used to prepare the compound of the invention or the pharmaceutical composition tablet containing it may also be used to prepare capsules of the compound of the invention or the pharmaceutical composition containing it.
For the preparation of the compound of the present invention or a pharmaceutical composition containing the same into an injection, water, ethanol, isopropanol, propylene glycol or a mixture thereof may be used as a solvent, and a proper amount of a solubilizing agent, a cosolvent, a pH adjustor, an osmotic pressure adjustor, which are commonly used in the art, may be added. The solubilizer or cosolvent can be poloxamer, lecithin, hydroxypropyl-beta-cyclodextrin, etc.; the pH regulator can be phosphate, acetate, hydrochloric acid, sodium hydroxide, etc.; the osmotic pressure regulator can be sodium chloride, mannitol, glucose, phosphate, acetate, etc. For example, mannitol, glucose, etc. can be added as propping agent for preparing lyophilized powder for injection.
For preparing the compound of the present invention or a pharmaceutical composition containing the same into liposomes, phospholipids and cholesterol can be used as carrier materials. The phospholipid may be phosphatidylcholine, dipalmitoyl phosphatidylcholine, distearoyl phosphatidylcholine, dipalmitoyl ethanolamine, dioleoyl phosphatidylcholine, dioleoyl phosphatidylglycerol, phosphatidylethanolamine, sphingomyelin, phosphatidic acid, phosphatidylinositol, phosphatidylserine, phosphatidylglycerol, and octadecylamine.
In addition, colorants, preservatives, fragrances, flavoring agents, or other additives may also be added to the pharmaceutical formulation, if desired. For the purpose of administration, the drug or the pharmaceutical composition of the present invention can be administered by any known administration method to enhance the therapeutic effect.
The amount of the compound of the present invention or a pharmaceutical composition containing the same to be administered may vary widely depending on the nature and severity of the disease to be prevented or treated, the individual condition of the patient or animal, the route of administration and the dosage form, etc. Generally, suitable dosages of the compounds of the present invention are in the range of 0.001 to 150mg/kg body weight, preferably 0.1 to 100mg/kg body weight, more preferably 1 to 60 mg/kg body weight, and most preferably 2 to 30mg/kg body weight per day. The above-mentioned dosages may be administered in one dosage unit or in several dosage units, depending on the clinical experience of the physician and the dosage regimen involved in the application of other therapeutic means.
The compounds or pharmaceutical compositions of the present invention may be administered alone or in combination with other therapeutic or symptomatic agents. When the compound of the present invention has a synergistic effect with other therapeutic agents, its dosage should be adjusted according to the actual circumstances.
Such neurodegenerative diseases include, but are not limited to, stroke, brain injury, amyotrophic lateral sclerosis, huntington's disease, parkinson's disease, and alzheimer's disease.
The products of the first and second aspects of the invention include, but are not limited to, pharmaceutical products.
In a third aspect, the present invention provides a method for preparing pentacyclic triterpene compounds according to the first and second aspects, comprising the steps of: extracting herba Cynomorii with 95% ethanol under reflux, concentrating, extracting with organic solvent, subjecting to silica gel column chromatography, reversed phase silica gel column chromatography and preparative HPLC to obtain the above compound, and analyzing and identifying its structure by various spectroscopy methods to obtain pentacyclic triterpene compounds mainly including ursane type and oleanane type.
Wherein said organic solvent extraction is a method well known in the art. Suspending the extract in water, and extracting with ethyl acetate, chloroform, dichloromethane, petroleum ether, and chloroform-methanol (1:1); the number of extraction is 1-3, preferably 3.
Wherein the macroporous adsorption resin is nonpolar, weak polar, medium polar, polar and strong polar macroporous adsorption resin well known in the art; preferably, non-polar, weakly polar and moderately polar macroporous adsorption resins are used.
Wherein the macroporous adsorption resin is styrene type, styrene divinylbenzene type, crosslinked polystyrene type, styrene nitrile type, methylstyrene type, methacrylate type, methacrylic acid type, acrylic acid type, acrylamide type, vinylpyrrolidone type, sulfoxide type, phenol-formaldehyde type or nitrogen oxide type which are known in the art according to the structure; preferably, a styrene type, acrylate type or methacrylate type macroporous adsorbent resin is used.
Specific types of macroporous adsorbent resins include, but are not limited to, D101, DA201, D301, D3520, D4006, D4020, H103, H107, H30, H60, AB-8, X-5, NKA, diaion HP-20, sepabeads SP-700, HP2MGL, HPD100, HPD722, HPD-600, HPD-826, ADS-17, amberlite XAD-4, XAD-1600, etc.
The macroporous adsorption resin eluting solvent adopts 50 to 95 percent ethanol, and the volume of the macroporous adsorption resin eluting solvent is 2 to 4 columns; preferably, the elution is performed using 70-95% ethanol.
Wherein the silica gel column chromatography is a method well known in the art. Evaporating the extract to dryness, dissolving in chloroform or methanol, adding appropriate amount of silica gel, stirring, drying, loading onto silica gel column, and gradient eluting with chloroform-methanol, chloroform-acetone, petroleum ether-acetone, dichloromethane-methanol, dichloromethane-acetone, etc.; preferably, chloroform-methanol is used, with dichloromethane-methanol as the eluting solvent.
The gel column chromatography can be performed by using Sephadex LH-20, HW-40, and other types of gel, and methanol, chloroform-methanol (2:1), and petroleum ether-chloroform-methanol (5:5:1) as eluting solvents.
Wherein the reverse phase silica gel column chromatography is usually reverse phase C 18 、C 8 The filler takes methanol-water or acetonitrile-water as a mobile phase; preferably, C is used 18 Is a filler, and methanol-water is a mobile phase.
Wherein said preparative HPLC is usually selected from reversed phase C 18 、C 8 And the filler takes methanol-water or acetonitrile-water as a mobile phase, and 0.1 to 1 percent of formic acid, acetic acid, trifluoroacetic acid and the like can be added into the mobile phase according to the requirement.
The beneficial technical effects are as follows:
1, the invention provides a new application of pentacyclic triterpene compounds in preventing or treating neurodegenerative diseases.
2, experiments prove that the compound has the following two obvious pharmacological activities: firstly, the compounds can protect nerve cell injury induced by glutamic acid; second, the compounds can obviously protect nerve cell damage induced by oxygen glucose deprivation.
And 3, the preparation method of the compound is mature, and is simple and easy to obtain.
Detailed Description
The following examples and pharmacological activity experiments are provided to further illustrate the present invention, but are not meant to limit the invention in any way. The experimental methods, in which specific conditions are not noted in the following examples, were selected according to conventional methods and conditions, or according to the commercial specifications.
In the following examples, the full or corresponding chinese names of the partial substances are as follows:
UV-visible spectrum
IR-Infrared Spectroscopy
FT-IR Fourier transform Infrared Spectroscopy
ODS carbon-eighteen bonded silica gel
ESIHRMS electrospray high resolution Mass Spectrometry
ESIMS electrospray Mass Spectrometry
1 H-NMR hydrogen Spectroscopy
13 C-NMR Nuclear magnetic resonance carbon Spectroscopy
The room temperature described in the examples below is generally 15 to 25℃as is conventional in the art.
EXAMPLE 1 preparation method of pentacyclic triterpene Compounds
60kg of dry cynomorium songaricum is crushed and then extracted by an extraction tank, 95% ethanol is refluxed and extracted for 3 times each for 2 hours, the supernatant is collected after filtration, and the ethanol is recovered under reduced pressure to obtain 8.4kg of crude extract. Dispersing herba Cynomorii extract with water, extracting with chloroform, and recovering solvent from chloroform part to obtain extract 1.5kg. Mixing chloroform part with silica gel 1:1, loading onto silica gel chromatographic column, gradient eluting with chloroform-methanol (1:0→1:1), detecting triterpene component by TLC, and collecting triterpene enriched part. After recovering the solvent, the solvent was purified repeatedly by silica gel column chromatography, ODS reverse phase silica gel column chromatography, sephadex LH-20 gel column chromatography and preparative HPLC to give compounds 1 (11.5 mg), 2 (1.95 mg), 3 (7.3 mg), 4 (3.42 mg), 5 (7 mg), 6 (2.6 mg), 7 (5.1 mg), 8 (5 g), 9 (1.2 mg), 10 (2.5 mg), 11 (5.51 mg), 12 (4.1 mg), 13 (3.3 mg), 14 (3.0 mg), 15 (2.9 mg), 16 (13.8 mg), 18 (4 mg), 19 (14.1 mg), 20 (3.41 mg), 21 (3.06 mg), 22 (30.8 mg), 23 (8.1 mg), and the structure was identified as a pentacyclic triterpene compound by analysis by various spectroscopic means.
The spectrum information and nuclear magnetic signals of the above compounds are as follows:
compound 1: a white powder of the pigment is mixed with the pigment,+33.1(c 0.07,CH 3 CN).UV(CH 3 CN)λ max nm(logε):191(3.95),228(3.86).CD(c 0.07,CH 3 CN)Δε 209 -3.72,Δε 235 9.88,Δε 343 -1.95.IRν max 3453,2951,1699,1662cm -1 .(-)-ESIHRMS m/z 467.3159[M-H] - (calcd 467.3167for C 30 H 43 O 4 -). 1 H-NMR 13 The C-NMR data are shown in Table 1 and Table 2.
Compound 2: a white powder of the pigment is mixed with the pigment,-183.7(c 0.02,CH 3 CN).CD(c 0.02,CH 3 CN)Δε 215 -2.00.IRν max 3276,2959,1693cm -1 .(-)-ESIHRMS m/z 455.3506[M-H] - (calcd 455.3531for C 30 H 47 O 3 -). 1 H-NMR 13 The C-NMR data are shown in Table 1 and Table 2.
Compound 3: a white powder of the pigment is mixed with the pigment,+28.5(c 0.1,CH 3 CN).CD(c 0.1,CH 3 CN)Δε 222 -1.39.IRν max 2925,1735,1690cm -1 .(-)-ESIHRMS m/z 555.3682[M-H] - (calcd 555.3691for C 34 H 51 O 6 -). 1 H-NMR(500MHz,CDCl 3 )δ3.75(3H,s,H-4'),3.38(2H,s,H-2'). 13 C-NMR(125MHz,CDCl 3 ) Delta 167.2 (C-3 '), 166.3 (C-1'), 52.5 (C-4 '), 41.8 (C-2'). Other 1 H-NMR 13 The C-NMR data are shown in Table 1 and Table 2.
Compound 4: a white powder of the pigment is mixed with the pigment,+27.8(c 0.07,CH 3 CN).CD(c 0.07,CH 3 CN)Δε 221 -1.22.IRν max 3230,2924,1757,1730,1692cm -1 .(-)-ESIHRMS m/z 556.3699[M-H] - (calcd 555.3691for C 34 H 51 O 6 -). 1 H-NMR(500MHz,CDCl 3 )δ3.68(3H,s,H-4'),3.31(2H,s,H-2'). 13 C-NMR(125MHz,CDCl 3 ) Delta 166.2 (C-3 '), 165.2 (C-1'), 51.4 (C-4 '), 40.6 (C-2'). Others 1 H-NMR 13 The C-NMR data are shown in Table 1 and Table 2.
TABLE 1 Compounds 1 to 4 1 H-NMR data (δin ppm)
# Coupling constant reading from HMQC spectra
Is measured at a 500MHz in CDCl 3 or b 600 MHz in Pyridine-d5.
Tables 21 to 4 13 C-NMR data (δin ppm)
Is measured at a 125 MHz in CDCl 3 or b 150 MHz in Pyridine-d5.
Compound 5: white powder, (-) -ESIMS m/z 467[ M-H] - . 1 H-NMR(500MHz,CDCl 3 )δ7.02(1H,d,J=10.1Hz,H-1),5.81(1H,d,J=10.1Hz,H-2),5.42(1H,t,J=3.7Hz,H-12),4.20(1H,dd,J=11.5,5.1Hz,H-15),2.82(1H,dd,J=13.7,4.0Hz,H-18),1.17(3H,s,H-27),1.16(3H,s,H-23),1.14(3H,s,H-26),1.07(3H,s,H-24),0.94(3H,s,H-25),0.92(3H,s,H-30),0.90(3H,s,H-29); 13 C-NMR(125MHz,CDCl 3 )δ205.3(C-3),183.0(C-28),158.8(C-1),144.7(C-13),125.4(C-2),124.0(C-12),68.2(C-15),53.2(C-5),47.8(C-14),46.0(C-17),45.1(C-19),44.6(C-4),41.9(C-18),41.8(C-9),41.5(C-8),39.6(C-10),35.9(C-7),33.6(C-16),33.2(C-21),33.1(C-29),32.2(C-22),30.8(C-20),27.9(C-23),23.7(C-11),23.6(C-30),21.7(C-24),20.0(C-27),19.2(C-6),18.8(C-25),18.2(C-26).
Compound 6, white powder, (-) -ESIMS m/z 513[ M-H ]] - . 1 H-NMR(500MHz,CDCl 3 )δ5.27(1H,t,J=3.7Hz,H-12),4.65(1H,d,J=3.3Hz,H-3),4.12(1H,dd,J=6.6,3.3Hz,H-2),2.19(1H,d,J=11.4Hz,H-18),2.15(3H,s,H-2'),1.30(3H,s,H-25),1.08(3H,s,H-23),1.07(3H,s,H-27),0.95(3H,d,J=6.4Hz,H-30),0.88(3H,s,H-24),0.86(3H,d,J=6.4Hz,H-29),0.81(3H,s,H-26); 13 C-NMR(125MHz,CDCl 3 )δ181.7(C-28),170.5(C-1'),138.0(C-13),125.8(C-12),80.8(C-3),69.4(C-2),55.4(C-5),52.6(C-18),48.0(C-9),47.9(C-17),43.6(C-1),42.1(C-14),39.6(C-8),39.0(C-20),39.0(C-19),38.8(C-22),37.5(C-4),36.7(C-10),36.7(C-7),30.6(C-21),29.3(C-24),27.9(C-15),24.1(C-16),23.6(C-11),23.4(C-6),21.2(C-30),21.2(C-2'),18.1(C-27),18.0(C-23),17.1(C-29),17.0(C-26),16.5(C-25).
Compound 7: white powder, (+) -ESIMS m/z 465[ M+Na ]]+. 1 H-NMR(500MHz,CDCl 3 )δ5.14(1H,t,J=3.5Hz,H-12),3.53(1H,d,J=10.8Hz,H-27),3.22(1H,dd,J=11.0,4.6Hz,H-3),3.20(1H,d,J=10.8Hz,H-27),1.10(3H,s,H-28),1.00(3H,s,H-23),0.99(3H,s,H-24),0.95(3H,s,H-26),0.94(3H,d,J=6.3Hz,H-29),0.81(3H,d,J=5.8Hz,H-30),0.79(3H,s,H-25); 13 C-NMR(150MHz,CDCl 3 )δ138.7(C-13),125.0(C-12),79.0(C-3),69.9(C-27),55.2(C-5),54.0(C-18),47.7(C-9),42.1(C-14),40.0(C-8),39.4(C-19),39.4(C-20),38.8(C-1),38.8(C-17),38.1(C-4),36.9(C-10),35.2(C-22),32.8(C-7),30.6(C-21),28.1(C-12),27.3(C-2),26.0(C-16),23.4(C-11),23.3(C-12),23.3(C-28),21.3(C-29),18.3(C-6),17.4(C-30),16.8(C-24),15.7(C-26),15.6(C-25).
Compound 8: white powder, (-) -ESIMS m/z 455[ M-H] - . 1 H-NMR(500MHz,Pyridine-d 5 )δ5.51(1H,t,J=3.3Hz,H-12),3.47(1H,dd,J=11.2,4.5Hz,H-3),2.65(1H,d,J=11.3Hz,H-18),1.26(3H,s,H-23),1.25(3H,s,H-27),1.07(3H,s,H-26),1.04(3H,s,H-24),1.02(3H,d,J=6.2Hz,H-29),0.97(3H,d,J=5.9Hz,H-30),0.91(3H,s,H-25); 13 C-NMR(125MHz,Pyridine-d 5 )δ179.62(C-28),138.98(C-13),125.4(C-12),77.9(C-3),55.5(C-5),53.3(C-18),49.4(C-17),47.8(C-9),42.2(C-14),39.7(C-8),39.2(C-19),39.1(C-20),39.1(C-1),38.8(C-4),37.2(C-22),37.0(C-10),33.3(C-7),30.8(C-21),28.5(C-23),28.4(C-15),27.8(C-2),24.6(C-16),23.6(C-27),23.4(C-11),21.1(C-30),18.5(C-6),17.2(C-29),17.2(C-26),16.3(C-24),15.4(C-25).
Compound 9: white powder, (-) -ESIMS m/z 453[ M-H] - . 1 H-NMR(600MHz,Pyridine-d 5 )δ6.70(1H,dd,J=10.5,2.8Hz,H-11),5.81(1H,d,J=10.5Hz,H-12),3.51(1H,dd,J=11.2,4.6Hz,H-3),1.27(3H,s,H-23),1.12(3H,s,H-26),1.12(3H,s,H-25),1.05(3H,s,H-27),1.00(3H,s,H-29),0.95(3H,s,H-24),0.93(3H,s,H-30); 13 C-NMR(150MHz,Pyridine-d 5 )δ178.92(C-28),136.58(C-13),133.8(C-18,overlapped with solvent)127.0(C-12),126.0(C-11),78.1(C-3),55.3(C-5),54.9(C-9),48.7(C-17),42.5(C-14),41.1(C-8),41.0(C-19),39.6(C-4),38.5(C-1),37.5(C-21),37.1(C-10),36.3(C-22),33.3(C-15),32.1(C-7),32.8(C-20),32.4(C-29),28.5(C-23),28.1(C-2),25.7(C-16),24.4(C-30),20.1(C-27),18.8(C-6),18.4(C-25),17.1(C-26),16.1(C-24).
Compound 10: white powder, (-) -ESIMS m/z 453[ M-H] - . 1 H-NMR(500MHz,CDCl 3 )δ5.28(1H,t,J=3.3Hz,H-12),3.22(1H,dd,J=11.3,4.3Hz,H-3),2.82(1H,dd,J=13.7,4.0Hz,H-18),1.13(3H,s,H-27),0.99(3H,s,H-23),0.93(3H,s,H-26),0.91(3H,s,H-24),0.90(3H,s,H-30),0.77(3H,s,H-29),0.75(3H,s,H-25); 13 C-NMR(125MHz,CDCl 3 )δ182.8(C-28),143.6(C-13),122.6(C-12),79.0(C-3),55.2(C-5),47.6(C-9),46.5(C-17),45.9(C-19),41.6(C-14),41.0(C-18),39.3(C-8),38.7(C-4),38.4(C-1),37.1(C-10),33.8(C-21),33.0(C-7),32.6(C-29),32.4(C-22),30.7(C-20),28.1(C-23),27.7(C-15),27.2(C-2),25.9(C-27),23.6(C-11),23.4(C-16),23.0(C-30),18.3(C-6),17.1(C-26),15.5(C-24),15.3(C-25).
Compound 11: white powder, (-) -ESIMS m/z 453[ M-H] - . 1 H-NMR(500MHz,Pyridine-d 5 )δ5.49(1H,brs,H-21),3.50(1H,t,J=8.0Hz,H-3),1.75(3H,s,H-30),1.26(3H,s,H-24),1.14(3H,d,J=6.0Hz,H-29),1.09(3H,s,H-26),1.06(3H,s,H-27),1.05(3H,s,H-23),0.89(3H,s,H-25); 13 C-NMR(150MHz,Pyridine-d 5 )δ178.5(C-28),143.5(C-20),118.3(C-21),78.5(C-3),56.3(C-5),51.42(C-9),50.0(C-18),49.7(C-17),42.7(C-14),41.6(C-8),39.9(C-13),39.8(C-1),39.7(C-4),38.8(C-22),38.2(C-19),37.8(C-10),35.1(C-7),34.0(C-12),30.0(C-16),29.0(C-24),28.7(C-15),28.3(C-2),24.1(C-29),22.6(C-30),22.3(C-11),19.1(C-6),17.0(C-25),16.8(C-23),16.7(C-26),15.4(C-27).
Compound 12: white powder, (-) -ESIMS m/z 455.5[ M-H] - . 1 H-NMR(500MHz,Pyridine-d 5 )δ3.51(1H,dd,J=10.2,5.8Hz,H-3),1.28(s,3H,H-23),1.28(s,3H,H-27),1.19(s,3H,H-26),1.05(s,3H,H-24),0.98(s,3H,H-25),0.93(s,3H,H-29),0.88(s,3H,H-30); 13 C-NMR(150MHz,Pyridine-d 5 )δ179.4(C-28),138.3(C-13),129.7(C-18),78.5(C-3),56.3(C-5),51.6(C-9),50.0(C-17),45.2(C-14),42.2(C-8),42.0(C-19),39.9(C-4),39.7(C-1),38.1(C-21),37.8(C-10),36.9(C-12),35.9(C-7),34.1(C-16),33.3(C-20),32.7(C-30),29.2(C-11),28.7(C-23),28.2(C-15),26.00(C-2),24.8(C-29),22.5(C-22),21.7(C-27),19.2(C-6),18.6(C-26),17.1(C-24),16.9(C-25).
Compound 13: white powder, (-) -ESIMS m/z 507[ M+Cl ]] - . 1 H-NMR(500MHz,CDCl 3 )δ5.36(1H,t,J=3.2Hz,H-12),3.22(1H,dd,J=11.2,4.4Hz,H-3),2.60(1H,s,H-18),1.26(3H,s,H-27),1.21(3H,s,H-29),0.99(3H,s,H-23),0.95(3H,d,J=6.7Hz,H-30),0.91(3H,s,H-25),0.79(3H,s,H-24),0.69(3H,s,H-26).; 13 C-NMR(125MHz,CDCl 3 )δ178.5(C-28),138.2(C-13),129.4(C-12),79.2(C-3),73.3(C-19),55.3(C-5),53.4(C-18),51.7(C-17),48.0(C-9),47.4(C-20),41.3(C-14),40.1(C-8),38.9(C-4),38.6(C-1),37.6(C-22),37.1(C-10),32.9(C-7),28.4(C-15),28.3(C-23),27.6(C-2),27.4(C-21),26.2(C-29),25.7(C-16),24.7(C-27),23.8(C-11),18.6(C-6),16.8(C-26),16.3(C-24),15.7(C-30),15.4(C-25).
Compound 14: white powder, (+) -ESIMS m/z 429[ M+H ]]+. 1 H-NMR(600MHz,CDCl 3 )δ5.31(1H,t,J=3.7Hz,H-12),3.22(1H,dd,J=11.5,4.4Hz,H-3),2.23(1H,dd,J=13.3,3.7Hz,H-18),1.14(3H,s,H-27),1.00(3H,s,H-23),0.96(3H,s,H-28),0.95(3H,s,H-26),0.93(3H,s,H-29),0.90(3H,s,H-24),0.79(3H,s,H-25); 13 C-NMR(150MHz,CDCl 3 )δ143.2(C-13),124.4(C-12),79.0(C-3),72.2(C-17),55.2(C-5),48.8(C-18),48.3(C-19),47.6(C-9),41.5(C-14),39.6(C-8),38.8(C-1),38.5(C-4),37.1(C-10),36.8(C-22),36.5(C-21),32.8(C-28),32.8(C-7),31.0(C-20),28.1(C-23),27.3(C-16),27.2(C-15),25.5(C-27),25.5(C-29),24.0(C-11),23.6(C-2),18.4(C-6),17.1(C-26),15.6(C-24),15.3(C-25).
Compound 15: white powder, (+) -ESIMS m/z 443[ M+H ]]+. 1 H-NMR(500MHz,Pyridine-d 5 )δ5.25(2H,t,J=3.3Hz,H-12),3.95(1H,d,J=10.5Hz,H-28),3.51(1H,d,J=10.5Hz,H-28),3.49(1H,dd,J=10.8,5.4Hz,H-3),1.28(3H,s,H-27),1.25(3H,s,H-25),1.08(3H,s,H-23),1.05(3H,s,H-26),0.99(3H,m,H-30),0.97(3H,s,H-29),0.96(3H,s,H-24); 13 C-NMR(150MHz,Pyridine-d 5 )δ140.0(C-13),125.4(C-12),78.5(C-3),69.5(C-18),56.1(C-5),55.0(C-18),48.5(C-9),42.8(C-14),40.7(C-8),40.3(C-20),40.2(C-19),39.8(C-1),39.6(C-4),39.1(C-10),37.5(C-17),36.6(C-7),33.7(C-21),31.6(C-15),29.2(C-22),28.6(C-2),27.0(C-23),24.2(C-11),24.1(C-16),24.0(C-27),22.0(C-30),19.2(C-6),18.2(C-29),17.4(C-26),17.0(C-25),16.3(C-24).
Compound 16: colorless needle crystals (methanol) (-) -ESIMS m/z 541[ M-H ]] - . 1 H-NMR(500MHz,Pyridine-d 5 )δ5.48(1H,t,J=3.4Hz,H-12),4.85(1H,dd,J=11.6,4.3Hz,H-3),3.82(2H,s,H-2'),2.64(1H,d,J=11.3Hz,H-18),1.23(3H,s,H-27),1.06(3H,s,H-25),1.02(3H,s,H-23),1.02(3H,d,J=6.2Hz,H-30),0.97(3H,d,J=6.2Hz,H-29),0.93(3H,s,H-26),0.82(3H,s,H-24); 13 C-NMR(125MHz,Pyridine-d 5 )δ179.9(C-28),170.3(C-3'),167.9(C-1'),139.3(C-13),125.4(C-12),81.6(C-3),55.6(C-5),53.6(C-18),48.1(C-17),47.8(C-9),42.5(C-14),39.9(C-2'),39.9(C-8),39.5(C-19),39.4(C-20),38.3(C-1),38.1(C-4),37.5(C-22),37.0(C-10),33.4(C-7),31.1(C-21),28.7(C-23),28.7(C-15),28.2(C-2),24.9(C-16),23.9(C-27),23.6(C-11),21.4(C-30),18.5(C-6),17.5(C-29),17.4(C-26),17.0(C-24),15.5(C-25).
Compound 18: white powder, (-) -ESIMS m/z 507[ M+Cl ]] - . 1 H-NMR(500MHz,Pyridine-d 5 )δ5.49(1H,t,J=3.5,H-12),4.12(1H,td,J=10.5,4.3Hz,H-2),3.42(1H,d,J=10.5Hz,H-3),2.65(1H,d,J=11.3Hz,H-18),1.30(3H,s,H-27),1.23(3H,s,H-25),1.10(3H,s,H-23),1.07(3H,s,H-26),1.00(3H,s,H-24),1.00(3H,d,J=5.9Hz,H-30),0.97(3H,d,J=6.2Hz,H-29); 13 C-NMR(150MHz,Pyridine-d 5 )δ180.3(C-28),139.7(C-13),125.9(C-12),84.2(C-3),69.0(C-2),56.3(C-5),53.9(C-18),48.5(C-17),48.4(C-1),48.4(C-9),42.9(C-14),40.4(C-8),40.2(C-4),39.8(C-19),39.8(C-20),38.8(C-10),37.8(C-22),33.9(C-7),31.4(C-21),29.8(C-23),29.0(C-15),25.3(C-16),24.3(C-11),24.1(C-27),21.8(C-30),19.2(C-6),18.1(C-29),17.9(C-26),17.9(C-24),17.4(C-25).
Compound 19: white powder, (-) -ESIMS m/z 617[ M-H] - . 1 H-NMR(500MHz,Pyridine-d 5 )δ8.01(1H,d,J=15.9Hz,H-7'),7.57(2H,d,J=8.5Hz,H-2',6'),7.16(2H,d,J=8.5Hz,H-3',5'),6.62(1H,d,J=15.9Hz,H-8'),5.64(1H,td,J=10.9,4.4Hz,H-2),5.48(1H,t,J=3.3Hz,H-12),2.66(1H,d,J=11.2Hz,H-18),1.32(3H,s,H-27),1.26(3H,s,H-23),1.13(3H,s,H-24),1.09(3H,s,H-26),1.04(3H,s,H-25),1.03(3H,d,J=6.3Hz,H-29),0.97(3H,d,J=6.2Hz,H-30). 13 C-NMR(125MHz,Pyridine-d 5 )δ180.1(C-28),167.5(C-9'),161.4(C-4'),144.71(C-7'),139.4(C-13),130.6(C-2',6'),126.2(C-1'),125.4(C-12),116.9(C-3',5'),116.00(C-7'),79.9(C-3),73.4(C-2),55.6(C-5),53.6(C-18),48.1(C-17),48.0(C-9),44.9(C-1),42.6(C-14),40.5(C-8),40.0(C-19),39.5(C-4),39.4(C-20),38.6(C-10),37.5(C-22),33.5(C-7),31.2(C-21),29.3(C-15),28.7(C-23),25.0(C-16),23.9(C-27),23.7(C-11),21.5(C-30),18.8(C-6),17.7(C-24),17.5(C-25),17.4(C-26),16.8(C-29).
Compound 20: white powder, (-) -ESIMS m/z 617[ M-H] - . 1 H-NMR(500MHz,Pyridine-d 5 )δ7.99(1H,d,J=15.9Hz,H=7'),7.55(2H,d,J=8.6Hz,H-2',6'),7.17(2H,d,J=8.6Hz,H-3',5'),6.58(1H,d,J=15.9Hz,H-8'),5.67(1H,td,J=10.5,4.5Hz,H-2),5.53(1H,t,J=3.8Hz,H-12),3.66(1H,d,J=10.5Hz,H-3),3.34(1H,dd,J=14.0,4.5Hz,H-18),1.34(3H,s,H-27),1.33(3H,s,H-25),1.15(3H,s,H-23),1.11(3H,s,H-30),1.03(3H,s,H-29),1.01(3H,s,H-24),0.96(3H,s,H-26); 13 C-NMR(150MHz,Pyridine-d 5 )δ180.0(C-28),167.2(C-9'),161.1(C-4'),144.7(C-7'),144.4(C-13),130.3(C-2',6'),125.9(C-1'),122.1(C-12),116.6(C-3',5'),115.8(C-8'),79.6(C-3),73.1(C-2),55.4(C-5),47.8(C-9),46.2(C-17,19),44.4(C-1),42.0(C-8),41.7(C-18),40.2(C-4),39.6(C-14),38.4(C-10),34.0(C-21),33.0(C-7),33.3(C-22),32.9(C-29),30.7(C-20),29.0(C-23),28.1(C-15),26.0(C-27),23.7(C-11),23.5(C-16,30),18.6(C-6),17.4(C-26),17.2(C-24),16.4(C-25).
Compound 21: white powder, (-) -ESIMS m/z 617[ M-H] - .1H-NMR(500MHz,Pyridine-d 5 )δ8.02(1H,d,J=15.9Hz,H-7'),7.57(2H,overlapped with solvent),7.18(2H,d,J=8.6Hz,H-3',5'),6.71(1H,d,J=15.9Hz,H-8'),5.48(1H,t,J=3.2Hz,H-12),5.27(1H,d,J=10.5Hz,H-3),4.31(1H,td,J=10.5,4.4Hz,H-2),3.32(1H,dd,J=13.5,3.4Hz,H-18),1.28(3H,s,H-27),1.07(3H,s,H-25),1.05(3H,s,H-26),1.02(3H,s,H-30),1.02(3H,s,H-29),1.01(3H,s,H-23),0.97(3H,s,H-24);13C-NMR(150MHz,Pyridine-d 5 )δ180.3(C-28),168.0(C-9'),161.4(C-4'),145.0(C-6'),145.0(C-13),130.6(C-2',6'),126.3(C-1'),122.3(C-12),116.8(C-3',5'),116.1(C-8'),85.1(C-3),66.4(C-2),55.5(C-5),48.4(C-9),48.1(C-19),46.7(C-1),46.5(C-17),42.2(C-14),42.0(C-18),39.9(C-8),39.8(C-4),38.4(C-10),34.3(C-21),33.3(C-7),33.2(C-29),33.0(C-22),31.0(C-20),29.0(C-23),28.3(C-15),26.2(C-27),23.9(C-16),23.8(C-11),23.7(C-30),18.7(C-6),18.3(C-26),17.4(C-24),16.8(C-25).
Compound 22: white powder, (-) -ESIMS m/z 617[ M-H] - .1H-NMR(600MHz,pyridine-d 5 )δ8.02(1H,d,J=15.9Hz,H-7'),7.57(2H,overlapped with solvent),7.16(2H,d,J=8.6Hz,H-3',5'),6.69(1H,d,J=15.9Hz,H-2'),5.48(1H,t,J=3.4Hz,H-12),5.28(1H,d,J=10.5Hz,H-3),4.31(1H,td,J=10.5,4.5Hz,H-2),2.65(1H,d,J=11.3Hz,H-18),1.24(3H,s,H-27),1.08(3H,s,H-23),1.06(3H,s,H-24),1.05(3H,s,H-26),1.01(3H,s,H-25),1.00(3H,d,J=6.3Hz,H-29),0.97(3H,d,J=6.3Hz,H-30);13C-NMR(150MHz,Pyridine-d 5 )δ179.9(C-28),167.9(C-9'),161.3(C-4'),144.8(C-7'),139.4(C-13),130.6(C-2',6'),126.3(C-1'),125.4(C-12),116.8(C-3',5'),116.1(C-8'),85.1(C-3),66.4(C-2),55.6(C-5),53.5(C-18),48.6(C-9),48.1(C-17),48.0(C-1),42.6(C-14),40.0(C-8),39.8(C-4),39.5(C-19),39.4(C-20),38.3(C-10),37.5(C-22),33.4(C-7),31.1(C-21),29.1(C-23),28.7(C-15),24.9(C-16),24.0(C-27),23.7(C-11),21.4(C-30),18.7(C-6),18.3(C-24),17.5(C-26),17.4(C-29),16.9(C-25).
Compound 23: white powder, (-) -ESIMS m/z 617[ M-H] - .1H-NMR(500MHz,Pyridine-d 5 )δ8.16(1H,d,J=8.6Hz,H-3',5'),7.16(1H,d,J=8.6Hz,H-2',6'),6.94(1H,d,J=12.9Hz,H-3”),6.10(1H,d,J=12.9Hz,H-2”),5.47(1H,t,J=3.2Hz,H-12),5.22(1H,d,J=9.8Hz,H-3),4.27(1H,m,H-2),2.65(1H,d,J=11.2Hz,H-18),1.20(3H,s,H-27),1.06(3H,s,H-23),1.04(3H,s,H-24),0.99(3H,s,H-29),0.99(3H,s,H-26),0.98(3H,s,H-25),0.97(3H,s,H-30).13C-NMR(150MHz,Pyridine-d 5 )δ167.7(C-1'),161.0(C-7'),144.1(C-3'),139.9(C-13),134.3(C-5',9'),127.2(C-4'),125.9(C-12),117.6(C-2'),116.4(C-6',8'),85.5(C-3),66.8(C-2),56.1(C-5),54.1(C-18),49.2(C-9),48.6(C-17),48.5(C-1),43.1(C-14),40.53(C-4),40.2(C-8),40.0(C-19),38.8(C-20),38.0(C-10),33.8(C-7),31.6(C-22),30.5(C-21),29.6(C-23),29.2(C-15),25.4(C-16),24.5(C-11),24.2(C-27),21.9(C-30),19.2(C-6),18.7(C-24),18.1(C-29),18.0(C-26),17.4(C-25).
Neuroprotective activity test of pentacyclic triterpene compounds
Experimental example 1 glutamic acid-induced SK-N-SH neuroblastoma cell injury model
The experimental method comprises the following steps: SK-N-SH cells were routinely cultured and then incubated with SK-N-SH cells for 4 hours, respectively, using the positive tool drug donepezil (3. Mu. Mol/L)/screening compound (10. Mu. Mol/L). Then, the SK-N-SH cells are damaged by glutamic acid, a glutamic acid damage model is established, and after the damage is carried out for 4 hours, the survival rate of the cells is detected by an MTT method.
Experimental results: as can be seen from table 3: of the compounds isolated from cynomorium songaricum, 12 pentacyclic triterpenes have remarkable neuroprotective activity on glutamate-induced neuronal damage
Experimental example 2 sodium dithionite induced SK-N-SH neuroblastoma cell oxygen glucose deprivation model
The experimental method comprises the following steps: SK-N-SH cells were routinely cultured and then incubated with the SK-N-SH cells for 4 hours using the positive tool drug donepezil (3. Mu. Mol/L)/PHPB (10. Mu. Mol/L)/screen-feeding compound (10. Mu. Mol/L), respectively. And then, damaging SK-N-SH cells by using sodium dithionite, establishing an oxygen sugar deprivation model, and detecting the cell survival rate by an MTT method after 24 hours of damage.
Experimental results: as can be seen from table 3: of the compounds isolated from cynomorium songaricum, 12 pentacyclic triterpenes have significant protective activity against oxygen glucose deprived injured nerve cells.
TABLE 3 neuroprotective Activity of cynomorium songaricum isolated compounds (10. Mu. Mol/ml)
**P<0.01vs Control;#P<0.05vs Model,##P<0.01vs Model,###P<0.001vs Model
Reference is made to:
zheng Lingyan, han Ruilan, 2016. Active site of Cynomorium Intelligence development and mechanism research. Vol. Shuoshi. University of inner Mongolian medical science, huand Haote, p.47.
Claims (8)
1. Pentacyclic triterpene compounds and pharmaceutically acceptable salts thereof are shown below,
2. the application of pentacyclic triterpene compounds and pharmaceutically acceptable salts thereof in preparing medicines for preventing and/or treating neurodegenerative diseases,
3. the use of pentacyclic triterpene compounds according to claim 1, and pharmaceutically acceptable salts thereof, for the preparation of a medicament for the prophylaxis and/or treatment of neurodegenerative diseases.
4. A pharmaceutical composition comprising an effective amount of the pentacyclic triterpene compound according to claim 1, a pharmaceutically acceptable salt thereof, and a pharmaceutically acceptable carrier.
5. Use of a pharmaceutical composition comprising an effective amount of a pentacyclic triterpene compound according to claim 2 and a pharmaceutically acceptable carrier for the manufacture of a medicament for the prophylaxis and/or treatment of neurodegenerative diseases.
6. Use according to claim 5, characterized in that: the dosage form of the pharmaceutical composition is selected from tablets, capsules, pills, granules, oral liquid, injection and suspension.
7. Use according to claim 2 or 3, said neurodegenerative diseases comprising stroke, brain injury, amyotrophic lateral sclerosis, huntington's disease, parkinson's disease or alzheimer's disease.
8. A process for preparing the pentacyclic triterpene compounds according to claim 1 and claim 2, comprising the steps of: reflux extracting herba Cynomorii with 95% ethanol, concentrating, extracting with organic solvent, macroporous adsorbent resin, silica gel column chromatography, reversed phase silica gel column chromatography, and preparative HPLC to obtain target compound.
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