Long Noncoding RNA EGOT Negatively Affects the Antiviral Response and Favors HCV Replication

Overview

Journal EMBO Rep

Specialty Molecular Biology

Date 2016 Jun 11

PMID 27283940

Citations 71

Authors

Elena Carnero

Marina Barriocanal

Celia Prior

Juan Pablo Unfried

Victor Segura

Elizabeth Guruceaga

Monica Enguita

Cristian Smerdou

Pablo Gastaminza

Puri Fortes

Affiliations

Soon will be listed here.

Abstract

The role of long noncoding RNAs (lncRNAs) in viral infection is poorly studied. We have identified hepatitis C virus (HCV)-Stimulated lncRNAs (CSRs) by transcriptome analysis. Interestingly, two of these CSRs (PVT1 and UCA1) play relevant roles in tumorigenesis, providing a novel link between HCV infection and development of liver tumors. Expression of some CSRs seems induced directly by HCV, while others are upregulated by the antiviral response against the virus. In fact, activation of pathogen sensors induces the expression of CSR32/EGOT RIG-I and the RNA-activated kinase PKR sense HCV RNA, activate NF-κB and upregulate EGOT EGOT is increased in the liver of patients infected with HCV and after infection with influenza or Semliki Forest virus (SFV). Genome-wide guilt-by-association studies predict that EGOT may function as a negative regulator of the antiviral pathway. Accordingly, EGOT depletion increases the expression of several interferon-stimulated genes and leads to decreased replication of HCV and SFV Our results suggest that EGOT is a lncRNA induced after infection that increases viral replication by antagonizing the antiviral response.

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