microRNA-guided immunity against respiratory virus infection in human and mouse lung cells

Author:

Shibamoto Ayaka1,Kitsu Yoshiaki1,Shibata Keiko2,Kaneko Yuka2,Moriizumi Harune2,Takahashi Tomoko12ORCID

Affiliation:

1. Saitama University 1 Department of Biochemistry and Molecular Biology, Faculty of Science , , Saitama 338-8570 , Japan

2. Graduate School of Science and Engineering, Saitama University 2 Department of Biochemistry and Molecular Biology , , Saitama 338-8570 , Japan

Abstract

ABSTRACT Viral infectivity depends on multiple factors. Recent studies showed that the interaction between viral RNAs and endogenous microRNAs (miRNAs) regulates viral infectivity; viral RNAs function as a sponge of endogenous miRNAs and result in upregulation of its original target genes, while endogenous miRNAs target viral RNAs directly and result in repression of viral gene expression. In this study, we analyzed the possible interaction between parainfluenza virus RNA and endogenous miRNAs in human and mouse lungs. We showed that the parainfluenza virus can form base pairs with human miRNAs abundantly than mouse miRNAs. Furthermore, we analyzed that the sponge effect of endogenous miRNAs on viral RNAs may induce the upregulation of transcription regulatory factors. Then, we performed RNA-sequence analysis and observed the upregulation of transcription regulatory factors in the early stages of parainfluenza virus infection. Our studies showed how the differential expression of endogenous miRNAs in lungs could contribute to respiratory virus infection and species- or tissue-specific mechanisms and common mechanisms could be conserved in humans and mice and regulated by miRNAs during viral infection.

Funder

Canon Foundation

MSD Life Science Foundation

Secom Science and Technology Foundation

Publisher

The Company of Biologists

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1. First person – Yoshiaki Kitsu;Biology Open;2024-06-15

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