A cell protection screen reveals potent inhibitors of multiple stages of the hepatitis C virus life cycle

Chockalingam, Karuppiah; Simeon, Rudo; Rice, Charles M.; Chen, Zhilei

doi:10.1073/pnas.0915117107

Cited by 71 publications

(79 citation statements)

References 37 publications

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“…Upon HCV infection and cleavage of the NS3/4A protease SEAP is released into the cell culture supernatant. Cell lines were also engineered to express the pro-apoptotic factor n4mBid, where NS3-dependent cleavage and activation led to an easily measurable cytopathic effect (Chockalingam, Simeon et al 2010). Although HCV infects mainly hepatocytes, there is evidence for the existence of non-hepatic reservoirs suggesting that the virus might have a broader cell tropism.…”

Section: Permissive Host Cellsmentioning

confidence: 99%

Cell Culture Systems for Hepatitis C Virus

Steinmann

Pietschmann

2013

Current Topics in Microbiology and Immunology

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Due to the obligatory intracellular life style of viruses, cell culture systems for efficient viral propagation are crucial to obtain a detailed understanding of the virus host cell interaction. For hepatitis C virus (HCV) the development of permissive and authentic culture models has been and continues to be a challenging task. The first ef forts to culture HCV had limited success and range back to before the virus was molecularly cloned in 1989. Since then several major breakthroughs have gradually overcome limitations in culturing the virus and sequentially permitted analysis of viral RNA replication, cell entry and ultimately the complete replication cycle in cultured cells in 2005. Until today, basic and applied HCV research greatly benefit from these tremendous efforts which spurred multiple com plementary cell based model systems for distinct steps of the HCV replication cycle. When used in combination they now permit deep insights into the fascinating biology of HCV and its interplay with the host cell. In fact drug development has been much facilitated and our understanding of the molecular determinants of HCV replication has grown in parallel to these advances. Building on this ground work and further refining our cellular models to better mimic the ar chitecture, polarization and differentiation of natural hepatocytes should reveal novel unique aspects of HCV replication. Ultimately, models to culture primary HCV isolates across all genotypes may teach us important new lessons about viral functional adaptations that have evolved in exchange with its human host and that may ex plain the variable natural course of hepatitis C.

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Section: Permissive Host Cellsmentioning

confidence: 99%

Cell Culture Systems for Hepatitis C Virus

Steinmann

Pietschmann

2013

Current Topics in Microbiology and Immunology

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“…Reporter viruses make such assays adaptable to high-throughput screening, with obvious advantages for antiviral research [76,126,[129][130][131]. Figure 4 illustrates a possible assay setup based on a dual reporter system, typically the Gaussia/Renilla and firefly luciferases.…”

Section: The Cell-cultured Hcv (Hcvcc) System and Derivativesmentioning

confidence: 99%

Entry and replication of recombinant hepatitis C viruses in cell culture

Vièyres

Pietschmann

2013

Methods

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“…Additionally, in the course of this study, antiviral activities of 6 against hepatitis C virus (HCV) and simian immunodeficiency virus (SIV) were reported [34,35]. Dual infection with HIV and HCV confers a higher rate of viral resistance and higher susceptibility to death compared with solely HIV-infected patients [36].…”

Section: Introductionmentioning

confidence: 89%

Introduction

Mizuhara

2013

Development of Novel Anti-Hiv Pyrimidobenzothiazine Derivatives

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A cell protection screen reveals potent inhibitors of multiple stages of the hepatitis C virus life cycle

Cited by 71 publications

References 37 publications

Cell Culture Systems for Hepatitis C Virus

Cell Culture Systems for Hepatitis C Virus

Entry and replication of recombinant hepatitis C viruses in cell culture

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