Abstract
Hepatitis C virus (HCV) represents a challenging global health threat to ~200 million infected individuals. Clinical data suggest that only ~10–15% of acutely HCV-infected individuals will achieve spontaneous viral clearance despite exuberant virus-specific immune responses, which is largely attributed to difficulties in recognizing the pathognomonic symptoms during the initial stages of exposure to the virus. Given the paucity of a suitable small animal model, it is also equally challenging to study the early phases of viral establishment. Further, the host factors contributing to HCV chronicity in a vast majority of acutely HCV-infected individuals largely remain unexplored. The last few years have witnessed a surge in studies showing that HCV adopts myriad mechanisms to disconcert virus-specific immune responses in the host to establish persistence, which includes, but is not limited to viral escape mutations, viral growth at privileged sites, and antagonism. Here we discuss a few hitherto poorly explained mechanisms employed by HCV that are believed to lead to chronicity in infected individuals. A better understanding of these mechanisms would aid the design of improved therapeutic targets against viral establishment in susceptible individuals.
Highlights
Hepatitis C virus (HCV), first identified in 1989 as the causative agent of hepatitis C infection, is an RNA virus belonging to the genus Hepacivirus of the Flaviviridae family [1]
We proposed that accumulation of exhausted HCV-specific CD8+ and CD4+ T-cell subsets during chronic HCV infection results in considerable loss of protective functional immune responses likely contributing to HCV persistence [62]
In one of our recent investigations, we found that MAIT cells in chronic HCV patients express high levels of CD57 besides PD-1, CD38 and HLA-DR
Summary
Hepatitis C virus (HCV), first identified in 1989 as the causative agent of hepatitis C infection, is an RNA virus belonging to the genus Hepacivirus of the Flaviviridae family [1]. Due to the existence of several variants of HCV, the levels of potential persistence in the host and the susceptibility attributes to antiviral drugs may vary [9]. The biology of HCV chronicity and the potential mechanisms that harness viral persistence are poorly understood. Certain mechanisms have been postulated based onfindings from other chronic viral infections, such as human immunodeficiency virus (HIV) and hepatitis B virus (HBV). We discuss certain hitherto poorly explored aspects of mechanisms employed by HCV in order to establish persistent infection, and the potential strategies for preventing and reversing the immunological cues to favor viral control
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