Abstract
Worldwide, 71 million individuals are chronically infected with Hepatitis C Virus (HCV). Chronic HCV infection can lead to potentially fatal outcomes including liver cirrhosis and hepatocellular carcinoma. HCV-specific immune responses play a major role in viral control and may explain why approximately 20% of infections are spontaneously cleared before the establishment of chronicity. Chronic infection, associated with prolonged antigen exposure, leads to immune exhaustion of HCV-specific T cells. These exhausted T cells are unable to control the viral infection. Before the introduction of direct acting antivirals (DAAs), interferon (IFN)-based therapies demonstrated successful clearance of viral infection in approximately 50% of treated patients. New effective and well-tolerated DAAs lead to a sustained virological response (SVR) in more than 95% of patients regardless of viral genotype. Researchers have investigated whether treatment, and the subsequent elimination of HCV antigen, can reverse this HCV-induced exhausted phenotype. Here we review literature exploring the restoration of HCV-specific immune responses following antiviral therapy, both IFN and DAA-based regimens. IFN treatment during acute HCV infection results in greater immune restoration than IFN treatment of chronically infected patients. Immune restoration data following DAA treatment in chronically HCV infected patients shows varied results but suggests that DAA treatment may lead to partial restoration that could be improved with earlier administration. Future research should investigate immune restoration following DAA therapies administered during acute HCV infection.
Highlights
We provide background on Hepatitis C Virus (HCV) immune dysfunction and review literature exploring the restoration of HCV-specific immune responses with antiviral therapy, both IFN-based and more recent direct acting antivirals (DAAs) therapies
Peptide-expanded HCV-specific CD8+ T cells derived from patients at the completion of DAA therapy exhibited increased IFN-γ production compared to baseline suggesting some immune restoration in patients following DAA treatment of chronic HCV
IFN-based treatment during acute HCV infection has demonstrated an improved likelihood of immune restoration compared to patients treated in chronic HCV infection
Summary
The World Health Organization (WHO) estimates the prevalence of chronic hepatitis C virus (HCV) infection to be 71 million people worldwide [1]. 39,000 deaths are attributed to HCV infection [1]. These deaths are predominantly caused by outcomes of chronic infection including cirrhosis and hepatocellular carcinoma [1]. 15%–45% of those infected with HCV spontaneously clear viremia with the remaining 55%–85% advancing to chronic Hepatitis C (CHC) [2]. There is no preventative or therapeutic vaccine and treatment targets patients who are in the chronic phase of HCV infection and generally not those recently infected with HCV [4]
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