Endogenous Retrovirus-Derived Long Noncoding RNA Enhances Innate Immune Responses via Derepressing RELA Expression

Author:

Zhou Bin12,Qi Fei2,Wu Fangyi2,Nie Hongbo1,Song Yifan1,Shao Lu3,Han Jingxuan2,Wu Zhen1,Saiyin Hexige1,Wei Gang1,Wang Penghua4,Ni Ting1,Qian Feng2

Affiliation:

1. State Key Laboratory of Genetic Engineering & MOE Key Laboratory of Contemporary Anthropology, Collaborative Innovation Center of Genetics and Development, Human Phenome Institute, School of Life Sciences and Huashan Hospital, Fudan University, Shanghai, People’s Republic of China

2. Ministry of Education Key Laboratory of Contemporary Anthropology, Human Phenome Institute, School of Life Sciences, Fudan University, Shanghai, People’s Republic of China

3. Shanghai Vocational College of Agriculture and Forestry, Shanghai, People’s Republic of China

4. Department of Immunology, School of Medicine, UConn Health, Farmington, Connecticut, USA

Abstract

Endogenous retroviruses are transposable genetic elements comprising 8% to 10% of the human and mouse genomes. Although most ERVs have been inactivated due to deleterious mutations, some are still transcribed. However, the biological functions of transcribed ERVs are largely unknown. Here, we identified a full-length ERV-derived lncRNA, designated lnc-EPAV, as a positive regulator of host innate immune responses. We found that silencing lnc-EPAV impaired virus-induced cytokine production, resulting in increased viral replication in cells. The lnc-EPAV-deficient mice exhibited enhanced susceptibility to viral challenge. We also found that lnc-EPAV regulated expression of RELA, an NF-κB subunit that plays a critical role in antiviral responses. ERV-derived lncRNA coordinated with a transcription repressor, SFPQ, to control Rela transcription. Our report provides new insights into the previously unrecognized immune gene regulatory mechanism of ERV-derived lncRNAs.

Publisher

American Society for Microbiology

Subject

Virology,Microbiology

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