CN103110652A - Application of chebulagic acid in preparation of medicament for treating diseases resulted from human enterovirus type 71 infection - Google Patents

Application of chebulagic acid in preparation of medicament for treating diseases resulted from human enterovirus type 71 infection Download PDF

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CN103110652A
CN103110652A CN2013100555496A CN201310055549A CN103110652A CN 103110652 A CN103110652 A CN 103110652A CN 2013100555496 A CN2013100555496 A CN 2013100555496A CN 201310055549 A CN201310055549 A CN 201310055549A CN 103110652 A CN103110652 A CN 103110652A
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chebulagic acid
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human enterovirus
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viral
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CN103110652B (en
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张连峰
杨亚军
刘江宁
修晶辉
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Institute of Laboratory Animal Science of CAMS
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Abstract

The invention discloses an application of chebulagic acid in the preparation of a medicament for treating diseases resulted from a human enterovirus type 71 infection. Preferably, the diseases resulted from the human enterovirus type 71 infection comprise foot and mouth disease, herpangina, viral meningitis, viral encephalitis, flaccid paralysis, pulmonary edema or viral myocarditis. In-vivo and in-vitro experiments show that chebulagic acid can inhibit replication and lesions of the human enterovirus type 71 in cells, has a good therapeutic effect for the diseases resulted from the human enterovirus type 71 infection, and has a clinical application prospect.

Description

The application of Chebulagic acid in preparation treatment human enterovirus 71 infects diseases induced medicine
Technical field
The present invention relates to field of medicaments, the particularly application of Chebulagic acid in preparation treatment human enterovirus 71 infects diseases induced medicine.
Background technology
Chebulagic acid (Chebulagic acid) mainly is present in the fruit of Combretum Racemosum plant Fructus Chebulae, belongs to hydrolyzable tannin on structure, and molecular formula is C 41H 30O 27, its structural formula is suc as formula shown in I:
Figure BDA00002847437900011
Formula I
Chebulagic acid has multiple biological activity, comprises antiinflammatory, antioxidation, antibiotic and antitumor etc.In addition, Chebulagic acid also suppresses copying of a small amount of virus, such as herpes simplex virus (HSV), viruses of human hepatitis C (HCV) and human immunodeficiency virus (HIV).
Human enterovirus 71 is the member of Picornaviridae enterovirus genus, belong to human intestine's virus A, be called for short EV71, often cause the diseases such as hand-foot-mouth disease, herpangina, viral meningitis, viral encephalitis, slowness paralysis, pulmonary edema, viral myocarditis, be referred to as enterovirns type 71 and infect.The multiple infant of being born in below 6 years old of this class disease, the minority state of an illness is comparatively serious, even can cause death.This disease all can occur throughout the year, is common in 4-9 month.
EV71 viral infection infant is generally 38 ℃ of left and right mainly with the heating onset, heating simultaneously, in the oral cavity, brothers, buttocks erythra occurs, or ulcer in the oral cavity, enanthema occur.Part patient has cough to wait the performance of flu sample in early days.Severe complication can appear in the minority infant.This class patient continues high heat mostly, PD is rapid, how occurring central nervous system, respiratory system, blood circulation severe complication in 3-5 days after morbidity, and can cause death, the cause of death is mainly cerebral edema, cerebral hernia, central breathing, circulatory failure.EV71 virus is repeatedly outburst worldwide, via gastrointestinal tract or respiratory infectious, according to the data of Ministry of Public Health, from 2008 in October, 2012, interior ground hand foot and mouth disease incidence rate was always high, suffered from the patient and surpassed 5,000,000 people, death toll surpasses 2000, and epidemic situation is still severe.
At present, infection does not still have generally acknowledged specific medicament or vaccine for EV71.
Summary of the invention
The technical problem to be solved in the present invention is for providing the application of Chebulagic acid in the medicine of the disease that the infection of preparation treatment human enterovirus 71 causes.
As preferably, described Chebulagic acid is Chebulagic acid monomer and/or chebule hydrochlorate.
Human enterovirus 71 is called for short EV71, and is spherical in shape for the member of Picornaviridae enterovirus genus, and icosahedron is three-dimensional symmetrical, without peplos and synapse, and diameter 24-30 nanometer, nucleic acid is the sub-thread positive chain RNA.Polypeptide VP1, VP2, VP3, the VP4 of EV71 type viral gene group coding consist of protomer, and the latter is assembled into the subunit with pentamer spline structure again, and 60 subunits interconnect by domain separately, the final shell that forms virus.Three polypeptide of VP1, VP2 and VP3 are exposed to the surface of virus coat, closely are connected with virus core and VP4 is embedded in the inboard of virus coat.EV71 virus can be via gastrointestinal tract or respiratory tract infection.
Described human enterovirus 71 infects the disease that causes and refers to that the enterovirns type 71 infection causes infectious disease, comprises the various diseases such as hand-foot-mouth disease, herpangina, viral meningitis, viral encephalitis, slowness paralysis, pulmonary edema and viral myocarditis.
the present invention utilizes the EV71 that laboratory is set up to infect people's rhabdomyoma cell model and mouse model, Chebulagic acid inhibition human enterovirus 71 is copied and treat the diseases induced effect of human enterovirus 71 infection to be studied, result shows: the EV71 viral infection is after 72 hours, without a large amount of pathological changes of medication therapy groups visible cell, and have no obvious pathological changes through the cell of 25 μ g/ml Chebulagic acid treatments, the Chebulagic acid concentration of effectively protecting 50% people's rhabdomyoma cell to avoid the EV71 infection is 12.5 μ g/ml, and when drug level during more than or equal to 25 μ g/ml, can suppress people's rhabdomyoma cytopathy that virus causes fully.
EV71 infecting mouse scale-model investigation result shows: the Chebulagic acid that gives 1mg/kg body weight dosage every day, continued medication 5 days, the symptom of infecting mouse weakens, the mortality rate of mice is down to 60%, and the model group mouse death rate is 100%, illustrate that Chebulagic acid has therapeutical effect to infecting due to EV71, has potential applicability in clinical practice.
Description of drawings
Fig. 1 behaves, and rhabdomyoma cell infection EV71 virus gave Chebulagic acid after 2 hours or isopyknic normal saline is processed, and processed the cell AO/EB coloration result of rear 0 hour, 48 hours, 72 hours;
Fig. 2 is the survival rate curve of various dose Chebulagic acid treatment EV71 infecting mouse;
Fig. 3 is that Chebulagic acid is respectively organized the impact of virus load on the EV71 virus infected mice.
The specific embodiment
The invention discloses the application of a kind of Chebulagic acid in preparation treatment human enterovirus 71 infects diseases induced medicine, those skilled in the art can use for reference this paper content, suitably improve technological parameter and realize.Special needs to be pointed out is, all similarly replace and change apparent to those skilled in the art, and they all are deemed to be included in the present invention.Application of the present invention is described by preferred embodiment, and the related personnel obviously can change methods and applications as herein described within not breaking away from content of the present invention, spirit and scope or suitably change and combination, realizes and use the technology of the present invention.
In order to make those skilled in the art understand better technical scheme of the present invention, the present invention is described in further detail below in conjunction with specific embodiment.
Embodiment 1 Chebulagic acid suppresses EV71 virus copying in cell
Infect in people's rhabdomyoma cell model at EV71, will newly cultivate people's rhabdomyoma cell and be seeded in 96 orifice plates, every porocyte quantity is 2 * 10 4Individual.Cultivate after 24 hours the beginning virus inoculation in 37 ℃ of incubators.
The EV71 that uses be the CONTINENTAL AREA OF CHINA epidemic isolates, strain name FY0805 separates from the Fuyang, it number is HQ882182 that gene order is stored in NCBI.The dosage of virus inoculation cell is 100TCID 50, volume is 98 microlitres, continues to cultivate in 37 ℃ of incubators.
The Chebulagic acid physiological saline solution, and in as a child administration of virus infected cell 2, injection volume is 2 microlitres, the cell of administration does not give 2 microlitre normal saline.Observe 72 hours inner cell pathological changes, the half effective inhibition concentration that calculates medicine is 12.5 μ g/ml.
People's rhabdomyoma cell infection EV71 virus is after 2 hours, giving final concentration is the Chebulagic acid treatment of 25 μ g/ml, respectively at carrying out AO/EB dyeing after administration in 0 hour, 48 hours, 72 hours, with isopyknic physiologic saline for substitute Chebulagic acid as negative control, observe the pathological changes situation of Chebulagic acid treatment group cell and normal saline group cell, its result as shown in Figure 1; Fig. 1 result shows: a large amount of pathological changes of normal saline group cell visible cell, and have no obvious cytopathy through the cells of 25 μ g/ml Chebulagic acid treatments, illustrate: Chebulagic acid can suppress EV71 virus copying in cell.
The therapeutical effect of embodiment 2 Chebulagic acids to the EV71 virus infected mice
The purpose of this experiment be the checking Chebulagic acid in Mice Body to the therapeutic effect of EV71 viral infection, model used is the model of CONTINENTAL AREA OF CHINA EV71 virus strain infection 10 age in days ICR mices.Strain is the adapted strain of clinical separation strain FY0805 in Mice Body, and strain is called MP10, and the storage of gene order in NCBI number is HQ712020.With 1 * 10 7TCID 50The MP10 virus of dosage after lumbar injection infects 10 age in days ICR mices, can cause mice to show in 4 days after acroparalysis and the symptom that loses weight, and all dead in infecting in rear 10 days.
Use above-mentioned model, the therapeutic effect of Chebulagic acid is carried out interior evaluating.Use mice to be SPF level ICR mice, 10 ages in days, male and female half and half.At first, lumbar injection MP10 virus is carried out viral infection to mice, infect pneumoretroperitoneum injection in 2 hours and give Chebulagic acid or normal saline, the Chebulagic acid physiological saline solution, its dosage is respectively 0.2 mg/kg of body weight/day, 1 mg/kg of body weight/day, 5 mg/kgs of body weight/day, and every group of mice quantity is 30; Every day is administration at twice, and interval 12 hours continued medication 5 days.From viral infection, continue to observe 14 days, record body weight, symptom and the survival rate of mice, estimate Chebulagic acid to the therapeutic effect of EV71 viral infection.
Result as shown in Figure 2, Fig. 2 result shows: give the Chebulagic acid of 1 mg/kg of body weight dosage every day, continued medication 5 days, the symptom of infecting mouse weakens, and the mortality rate of mice is down to 60%, and the model group mouse death rate is 100%; Illustrate that Chebulagic acid has therapeutic effect preferably for the EV71 infecting mouse.
Embodiment 3 Chebulagic acids are for the impact of virus load in EV71 virus infected mice tissue
Described virus load refers to the viral load in the Unit Weight tissue, is used for the virus replication situation of reflection tissue.
The purpose of this experiment is to detect Chebulagic acid for the impact of virus load in EV71 virus infected mice different tissues, with the inhibitory action of verifying that Chebulagic acid copies in vivo for EV71 virus.
The described EV71 virus infected mice of Application Example 2 model is measured the virus load in Chebulagic acid treatment EV71 virus infected mice different tissues.Use mice to be SPF level ICR mice, 10 ages in days, male and female half and half.Through lumbar injection MP10 virus, mice is infected, infect 2 and as a child gave Chebulagic acid or normal saline through lumbar injection, Chebulagic acid physiological saline solution, its dosage are 1 mg/kg of body weight/day.Administration every day 2 times, interval 12 hours continued medication 5 days.After viral infection the 6th day, mice is taken off neck puts to death, get respectively blood, cerebral tissue and muscular tissue, carry out the detection of virus load with the qRT-PCR method, its testing result as shown in Figure 3, Fig. 3 vertical coordinate is the viral copy number of the Log(of every milligram of tissue).
Fig. 3 result shows: the Chebulagic acid that gives 1 mg/kg of body weight dosage every day, continued medication 5 days, compare with giving the normal saline group, the virus load in each group of administration group mice obviously reduces, and illustrate: Chebulagic acid can obviously suppress viral copying in vivo.
The above is only the preferred embodiment of the present invention; should be pointed out that for those skilled in the art, under the prerequisite that does not break away from the principle of the invention; can also make some improvements and modifications, these improvements and modifications also should be considered as protection scope of the present invention.

Claims (3)

1. the application of Chebulagic acid in the medicine of the disease that the infection of preparation treatment human enterovirus 71 causes.
2. application according to claim 1, is characterized in that, described Chebulagic acid is Chebulagic acid monomer and/or chebule hydrochlorate.
3. the described application of any one according to claim 1 and 2, it is characterized in that, it is hand-foot-mouth disease, herpangina, viral meningitis, viral encephalitis, slowness paralysis, pulmonary edema or viral myocarditis that described human enterovirus 71 infects the disease that causes.
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Non-Patent Citations (2)

* Cited by examiner, † Cited by third party
Title
仓艳红: "《EV71 型重症手足口病的临床观察与护理》", 《河北医药》 *
沙磊等: "《RP - HPLC法测定余甘子中诃黎勒酸、没食子酸、粘酸-2-o没食子酸酯的含量》", 《药物分析杂志》 *

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