HIV-1 Intron-containing RNA Expression Induces Innate Immune Activation and T Cell Dysfunction

Overview

Journal Nat Commun

Specialty Biology

Date 2018 Aug 29

PMID 30150664

Citations 46

Authors

Hisashi Akiyama

Caitlin M Miller

Chelsea R Ettinger

Anna C Belkina

Jennifer E Snyder-Cappione

Suryaram Gummuluru

Affiliations

Soon will be listed here.

Abstract

Low levels of type I interferon (IFN-I) are thought to be a driving force for immune activation and T-cell exhaustion in HIV-1 infected individuals on combination antiretroviral therapy (cART), though the causative mechanisms for persistent IFN-I signaling have remained unclear. Here, we show Rev-CRM1-dependent nuclear export and peripheral membrane association of intron-containing HIV-1 RNA, independent of primary viral sequence or viral protein expression, is subject to sensing and signaling via MAVS, resulting in IFN-I-dependent pro-inflammatory responses in macrophages. Additionally, HIV-1 intron-containing-RNA-induced innate immune activation of macrophages leads to upregulation of inhibitory receptor expression and functional immune exhaustion of co-cultured T cells. Our findings suggest that persistent expression of HIV-1 intron-containing RNA in macrophages contributes to chronic immune activation and T-cell dysfunction and that use of HIV RNA expression inhibitors as adjunct therapy might abrogate aberrant inflammation and restore immune function in HIV-infected individuals on cART.

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