Title | RNA-Editing Enzyme ADAR1 p150 Isoform Is Critical for Germinal Center B Cell Response |
Author | |
Corresponding Author | Li,Yan; Ou,Xijun |
Publication Years | 2022-09-15
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DOI | |
Source Title | |
ISSN | 0022-1767
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EISSN | 1550-6606
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Volume | 209Issue:6Pages:1071-1082 |
Abstract | Adenosine deaminase acting on RNA (ADAR)1 is the principal enzyme for adenosine-to-inosine editing, an RNA modification-avoiding cytosolic nucleic acid sensor’s activation triggered by endogenous dsRNAs. Two ADAR1 isoforms exist in mammals, a longer IFN-inducible and mainly cytoplasm-localized p150 isoform and a shorter constitutively expressed and primarily nucleus-localized p110 isoform. Studies of ADAR1 mutant mice have demonstrated that ADAR1 is essential for multiple physiological processes, including embryonic development, innate immune response, and B and T lymphocyte development. However, it remained unknown whether ADAR1 plays a role in the humoral immune response. In this study, we conditionally delete Adar1 in activated B cells and show that ADAR1-deficient mice have a defective T cell-dependent Ab response and diminished germinal center (GC) B cells. Using various double mutant mice concurrently deficient in ADAR1 and different downstream dsRNA sensors, we demonstrate that ADAR1 regulates the GC response by preventing hyperactivation of the melanoma differentiation-associated protein 5 (MDA5) but not the protein kinase R or RNase L pathway. We also show that p150 is exclusively responsible for ADAR1’s function in the GC response, and the p110 isoform cannot substitute for the p150’s role, even when p110 is constitutively expressed in the cytoplasm. We further demonstrated that the dsRNA-binding but not the RNA-editing activity is required for ADAR1’s function in the GC response. Thus, our data suggest that the ADAR1 p150 isoform plays a crucial role in regulating the GC B cell response. |
URL | [Source Record] |
Indexed By | |
Language | English
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SUSTech Authorship | Corresponding
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Funding Project | Basic and Applied Basic Research Foundation of Guangdong Province[2020A1515010262]
; National Natural Science Foundation of China[32170882]
; Science, Technology and Innovation Commission of Shenzhen Municipality[JCYJ20190809161807432]
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ESI Research Field | IMMUNOLOGY
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Scopus EID | 2-s2.0-85138458013
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Data Source | Scopus
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Citation statistics |
Cited Times [WOS]:1
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Document Type | Journal Article |
Identifier | http://kc.sustech.edu.cn/handle/2SGJ60CL/402687 |
Department | Department of Biology 生命科学学院 |
Affiliation | 1.Harbin Institute of Technology,Harbin,China 2.Department of Biology,School of Life Sciences,Southern University of Science and Technology,Shenzhen,China 3.Singapore Immunology Network,Agency for Science,Technology and Research,Singapore 4.Department of Physiology,Yong Loo Lin School of Medicine,National University of Singapore,Singapore |
First Author Affilication | Department of Biology; School of Life Sciences |
Corresponding Author Affilication | Department of Biology; School of Life Sciences |
Recommended Citation GB/T 7714 |
Li,Yuxing,Ruan,Gui Xin,Chen,Wenjing,et al. RNA-Editing Enzyme ADAR1 p150 Isoform Is Critical for Germinal Center B Cell Response[J]. JOURNAL OF IMMUNOLOGY,2022,209(6):1071-1082.
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APA |
Li,Yuxing.,Ruan,Gui Xin.,Chen,Wenjing.,Huang,Hengjun.,Zhang,Rui.,...&Ou,Xijun.(2022).RNA-Editing Enzyme ADAR1 p150 Isoform Is Critical for Germinal Center B Cell Response.JOURNAL OF IMMUNOLOGY,209(6),1071-1082.
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MLA |
Li,Yuxing,et al."RNA-Editing Enzyme ADAR1 p150 Isoform Is Critical for Germinal Center B Cell Response".JOURNAL OF IMMUNOLOGY 209.6(2022):1071-1082.
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