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BST-2 expression in human hepatocytes is inducible by all three types of interferons and restricts production of hepatitis C virus 期刊论文

编号：

a01b1f02-104f-4808-b666-1f5c5b32f9a8
作者：

Amet, Tohti[0]^[1] Byrd, Daniel J.[1]^[1] Hu, Ningjie[2]^[2] Sun, Qiangming[3]^[3] Li, F.[4]^[4] Zhao, Yongna[5]^[4] Hu, Sishun[6]^[5] Grantham, Ayslinn[7]^[1] Yu, Qigui[8]^[6]
地址：

[1]Indiana University School of Medicine Indianapolis, Department of Microbiology and Immunology,Indianapolis,United States
[2]Indiana University School of Medicine Indianapolis, Center for AIDS Research,Indianapolis,United States
[3]Chinese Academy of Medical Sciences, Molecular Epidemiology Joint Laboratory,Beijing,China
[4]Fudan University School of Life Sciences, Zhejiang Provincial Key Laboratory for Technology and Application of Model Organisms,Shanghai,China
[5]University of California, Los Angeles, Department of Medicine,Los Angeles,United States
[6]Indiana University School of Medicine Indianapolis, Center for AIDS Research and Department of Microbiology and Immunology,Indianapolis,United States
语种：

英文
期刊：

Current Molecular Medicine ISSN：1566-5240 2014 年 14 卷 3 期 (349 - 360)
收录：
关键词：

BST-2 HCV Host restriction factor Huh7.5.1 cell Interferon Lipid droplet
摘要：

Bone marrow stromal cell antigen 2 (BST-2, also known as tetherin, CD317, or HM1.24) has recently been identified as a host restriction factor against diverse families of enveloped viruses. However, the effects of BST-2 on the life cycle of hepatitis C virus (HCV), an enveloped RNA virus, remain unclear and controversial. Here we demonstrated that human hepatocytes including Huh7.5.1 cells, primary human hepatocytes (PHHs), and HepG2 cells constitutively expressed low to moderate levels of endogenous BST-2 on the cell surface, which could be robustly up-regulated by all three types of interferons (IFNs) such as IFN-α, IFN-γ, and IFN-λ. IFN-α and IFN-γ showed a synergistic effect in induction of BST-2 expression on human hepatocytes. Over-expression of BST-2 by BST-2-expressing vector transfection or up-regulation of BST-2 by IFN stimulation markedly suppressed HCV production, whereas shRNA-mediated depletion of endogenous BST-2 significantly enhanced HCV production in infected Huh7.5.1 cells. IFN-mediated anti-HCV activity was partially but significantly diminished by shRNA-mediated knockdown of BST-2 expression, indicating that BST- 2 upregulation is directly involved in IFN-mediated inhibition of HCV production. We also found that both BST-2 and HCV core co-localized with intracellular lipid droplets (LDs), suggesting that BST-2-HCV interaction may take place around LDs as LDs constitute an important intracellular organelle for HCV assembly and replication. Taken together, our data suggest that BST-2 is a host restriction factor against HCV, and induction of BST-2 in hepatocytes could be one of the mechanisms by which current HCV standard therapy (IFN-α plus ribavirin) achieves a sustained virological response (SVR). © 2014 Bentham Science Publishers.
推荐引用方式
GB/T 7714：

Amet Tohti/6506575505[0],Byrd Daniel J./35298775900[1],Hu Ningjie/26663452600[2], et al. BST-2 expression in human hepatocytes is inducible by all three types of interferons and restricts production of hepatitis C virus [J].Current Molecular Medicine,2014,14(3):349-360.
APA：

Amet Tohti/6506575505[0],Byrd Daniel J./35298775900[1],Hu Ningjie/26663452600[2],Sun Qiangming/35081294000[3],&Yu Qigui/7402947490[8].(2014).BST-2 expression in human hepatocytes is inducible by all three types of interferons and restricts production of hepatitis C virus .Current Molecular Medicine,14(3):349-360.
MLA：

Amet Tohti/6506575505[0], et al. "BST-2 expression in human hepatocytes is inducible by all three types of interferons and restricts production of hepatitis C virus" .Current Molecular Medicine 14,3(2014):349-360.

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