OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages

Upon viral infection, the 2′, 5′-oligoadenylate synthetase (OAS)-ribonuclease L (RNaseL) system works to cleave viral RNA, thereby blocking viral replication. However, it is unclear whether OAS proteins have a role in regulating gene expression. Here, we show that OAS1 and OAS3 act as negative regul...

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Autores principales: Lee, Wook-Bin, Choi, Won Young, Lee, Dong-Hyun, Shim, Hyeran, Kim-Ha, Jeongsil, Kim, Young-Joon
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Korean Society for Biochemistry and Molecular Biology 2019
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Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6443328/
https://www.ncbi.nlm.nih.gov/pubmed/30078389
http://dx.doi.org/10.5483/BMBRep.2019.52.2.129
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author Lee, Wook-Bin
Choi, Won Young
Lee, Dong-Hyun
Shim, Hyeran
Kim-Ha, Jeongsil
Kim, Young-Joon
author_facet Lee, Wook-Bin
Choi, Won Young
Lee, Dong-Hyun
Shim, Hyeran
Kim-Ha, Jeongsil
Kim, Young-Joon
author_sort Lee, Wook-Bin
collection PubMed
description Upon viral infection, the 2′, 5′-oligoadenylate synthetase (OAS)-ribonuclease L (RNaseL) system works to cleave viral RNA, thereby blocking viral replication. However, it is unclear whether OAS proteins have a role in regulating gene expression. Here, we show that OAS1 and OAS3 act as negative regulators of the expression of chemokines and interferon-responsive genes in human macrophages. Clustered regularly interspaced short palindromic repeats (CRISPR)-CRISPR-associated protein-9 nuclease (Cas9) technology was used to engineer human myeloid cell lines in which the OAS1 or OAS3 gene was deleted. Neither OAS1 nor OAS3 was exclusively responsible for the degradation of rRNA in macrophages stimulated with poly(I:C), a synthetic surrogate for viral double-stranded (ds)RNA. An mRNA sequencing analysis revealed that genes related to type I interferon signaling and chemokine activity were increased in OAS1(−/−) and OAS3(−/−) macrophages treated with intracellular poly(I:C). Indeed, retinoic-acid-inducible gene (RIG)-I- and interferon-induced helicase C domain-containing protein (IFIH1 or MDA5)-mediated induction of chemokines and interferon-stimulated genes was regulated by OAS3, but Toll-like receptor 3 (TLR3)- and TLR4-mediated induction of those genes was modulated by OAS1 in macrophages. However, stimulation of these cells with type I interferons had no effect on OAS1- or OAS3-mediated chemokine secretion. These data suggest that OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages.
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spelling pubmed-64433282019-04-15 OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages Lee, Wook-Bin Choi, Won Young Lee, Dong-Hyun Shim, Hyeran Kim-Ha, Jeongsil Kim, Young-Joon BMB Rep Articles Upon viral infection, the 2′, 5′-oligoadenylate synthetase (OAS)-ribonuclease L (RNaseL) system works to cleave viral RNA, thereby blocking viral replication. However, it is unclear whether OAS proteins have a role in regulating gene expression. Here, we show that OAS1 and OAS3 act as negative regulators of the expression of chemokines and interferon-responsive genes in human macrophages. Clustered regularly interspaced short palindromic repeats (CRISPR)-CRISPR-associated protein-9 nuclease (Cas9) technology was used to engineer human myeloid cell lines in which the OAS1 or OAS3 gene was deleted. Neither OAS1 nor OAS3 was exclusively responsible for the degradation of rRNA in macrophages stimulated with poly(I:C), a synthetic surrogate for viral double-stranded (ds)RNA. An mRNA sequencing analysis revealed that genes related to type I interferon signaling and chemokine activity were increased in OAS1(−/−) and OAS3(−/−) macrophages treated with intracellular poly(I:C). Indeed, retinoic-acid-inducible gene (RIG)-I- and interferon-induced helicase C domain-containing protein (IFIH1 or MDA5)-mediated induction of chemokines and interferon-stimulated genes was regulated by OAS3, but Toll-like receptor 3 (TLR3)- and TLR4-mediated induction of those genes was modulated by OAS1 in macrophages. However, stimulation of these cells with type I interferons had no effect on OAS1- or OAS3-mediated chemokine secretion. These data suggest that OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages. Korean Society for Biochemistry and Molecular Biology 2019-02 2019-02-28 /pmc/articles/PMC6443328/ /pubmed/30078389 http://dx.doi.org/10.5483/BMBRep.2019.52.2.129 Text en Copyright © 2019 by the The Korean Society for Biochemistry and Molecular Biology This is an open-access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Articles
Lee, Wook-Bin
Choi, Won Young
Lee, Dong-Hyun
Shim, Hyeran
Kim-Ha, Jeongsil
Kim, Young-Joon
OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages
title OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages
title_full OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages
title_fullStr OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages
title_full_unstemmed OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages
title_short OAS1 and OAS3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages
title_sort oas1 and oas3 negatively regulate the expression of chemokines and interferon-responsive genes in human macrophages
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6443328/
https://www.ncbi.nlm.nih.gov/pubmed/30078389
http://dx.doi.org/10.5483/BMBRep.2019.52.2.129
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