Major models of HCV infection

被引:3
作者
Lagaye, Sylvie [1 ]
Shen, Hong [1 ]
Rousseau, Geraldine [2 ]
Pol, Stanislas [1 ,3 ]
机构
[1] Univ Paris 05, Equipe Cycle Cellulaire Regenerat & Hepatopathies, INSERM, Inst Cochin,U1016,CNRS,UMR8104,UMR S1016, Paris, France
[2] Grp Hosp Pitie Salpetriere, APHP, Serv Chirurg Digest & Hepato Bilio Pancreat, F-75634 Paris, France
[3] Grp Hosp Cochin, APHP, Unite Hepatol, Paris, France
关键词
antiviral therapy; HCV replicon; hepatitis C virus; human liver slices; in vitro models of infection; in vivo models of infection; HEPATITIS-C-VIRUS; CELL-CULTURE SYSTEMS; NON-B-HEPATITIS; HUMAN LIVER; HUMAN HEPATOCYTES; NON-A; HEPATOCELLULAR-CARCINOMA; TUPAIA-BELANGERI; RNA REPLICATION; CHIMERIC MICE;
D O I
10.2217/FVL.13.29
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
HCV is one of the major causes of liver disease worldwide and has a high risk of progress in cirrhosis and hepatocellular carcinoma, the incidence of which is increasing. Currently, the licensed standard treatment for HCV infection is pegylated IFN-alpha and ribavirin; in HCV genotype 1-infected patients, the first-generation HCV NS3/4 protease inhibitors telaprevir and boceprevir may be added to the standard of care with higher antiviral potency. Although the sustained viral response rate of treatment has improved over the years, this therapy is not effective in all patients. In addition, several toxic side effects, complication and high cost limits patient compliance and the efficacy of the treatment. There is no easy model of HCV infection, and it is necessary to develop useful in vitro and in vivo models to study the pathobiology of HCV infection, including early events of acute infection (viral entry, immunological mechanisms and genetic predictors), as well as to evaluate the potency of the HCV antiviral drugs and vaccines. This article summarizes the in vitro and in vivo models that are currently used for the study of HCV infection, elucidating the early events of acute infection. This is a major issue that will probably allow us to reduce the risk of chronicity and aid the development of prophylactic and therapeutic vaccines.
引用
收藏
页码:493 / 506
页数:14
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