Mutual Antagonism between Circadian Protein Period 2 and Hepatitis C Virus Replication in Hepatocytes

6533b7d2fe1ef96bd125eb8c

RESEARCH PRODUCT

Mutual Antagonism between Circadian Protein Period 2 and Hepatitis C Virus Replication in Hepatocytes

Valerio Pazienza Francesca Rappa Manlio Vinciguerra Jude A. Oben Giorgia Benegiamo Azzura Greco Roger Williams Angelo Andriulli Gianluigi Mazzoccoli Nunzia Scibetta Francesco Cappello

subject

Male Gastroenterology and hepatology Circadian clock Hepacivirus Virus Replication Hepatitis Molecular cell biology Cellular Stress Responses Multidisciplinary Viral Core Proteins Q Mechanisms of Signal Transduction R Period Circadian Proteins Middle Aged Hepatitis C CLOCK PER2 ARNTL Infectious hepatitis Liver Medicine Infectious diseases RNA Viral Female Research Article Signal Transduction PER1 Adult Histology Feedback Regulation Genotype Science Period (gene)DNA transcription Viral diseases Genome Viral Biology Cell Line Cell Line Tumor Genetics Humans Biology Liver diseases Aged Virology Hepatocytes Period Circadian Proteins Gene expression ARNTL2

description

BackgroundHepatitis C virus (HCV) infects approximately 3% of the world population and is the leading cause of liver disease, impacting hepatocyte metabolism, depending on virus genotype. Hepatic metabolic functions show rhythmic fluctuations with 24-h periodicity (circadian), driven by molecular clockworks ticking through translational-transcriptional feedback loops, operated by a set of genes, called clock genes, encoding circadian proteins. Disruption of biologic clocks is implicated in a variety of disorders including fatty liver disease, obesity and diabetes. The relation between HCV replication and the circadian clock is unknown.MethodsWe investigated the relationship between HCV core infection and viral replication and the expression of clock genes (Rev-Erbα, Rorα, ARNTL, ARNTL2, CLOCK, PER1, PER2, PER3, CRY1 and CRY2) in two cellular models, the Huh-7 cells transiently expressing the HCV core protein genotypes 1b or 3a, and the OR6 cells stably harboring the full-length hepatitis C genotype 1b replicon, and in human liver biopsies, using qRT-PCR, immunoblotting, luciferase assays and immunohistochemistry.ResultsIn Huh-7 cells expressing the HCV core protein genotype 1b, but not 3a, and in OR6 cells, transcript and protein levels of PER2 and CRY2 were downregulated. Overexpression of PER2 led to a consistent decrease in HCV RNA replicating levels and restoration of altered expression pattern of a subset of interferon stimulated genes (ISGs) in OR6 cells. Furthermore, in liver biopsies from HCV genotype 1b infected patients, PER2 was markedly localized to the nucleus, consistent with an auto-inhibitory transcriptional feedback loop.ConclusionsHCV can modulate hepatic clock gene machinery, and the circadian protein PER2 counteracts viral replication. Further understanding of circadian regulation of HCV replication and rhythmic patterns of host-hosted relationship may improve the effectiveness of HCV antiviral therapy. This would extend to hepatic viral infections the current spectrum of chronotherapies, implemented to treat metabolic, immune related and neoplastic disease.

year	journal	country	edition	language
2013-04-01	PLoS ONE

https://doi.org/10.1371/journal.pone.0060527