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B Cell-Specific Deletion of CR6-Interacting Factor 1 Drives Lupus-Like Autoimmunity by Activation of Interleukin-17, Interleukin-6, and Pathogenic Follicular Helper T Cells in a Mouse ModelB Cell–Specific Deletion of CR6-Interacting Factor 1 Drives Lupus-like Autoimmunity by Activation of Interleukin-17, Interleukin-6, and Pathogenic Follicular Helper T Cells in a Mouse Model

Other Titles
B Cell–Specific Deletion of CR6-Interacting Factor 1 Drives Lupus-like Autoimmunity by Activation of Interleukin-17, Interleukin-6, and Pathogenic Follicular Helper T Cells in a Mouse Model
Authors
Park, Jin-SilYang, SeungCheonHwang, Sun-HeeChoi, JeongWonKwok, Seung-KiKong, Young-YunYoun, JeeheeCho, Mi-LaPark, Sung-Hwan
Issue Date
Jul-2022
Publisher
John Wiley and Sons Ltd
Citation
Arthritis and Rheumatology, v.74, no.7, pp 1211 - 1222
Pages
12
Indexed
SCIE
SCOPUS
Journal Title
Arthritis and Rheumatology
Volume
74
Number
7
Start Page
1211
End Page
1222
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/203908
DOI
10.1002/art.42091
ISSN
2326-5191
2326-5205
Abstract
Objective CR6-interacting factor 1 (CRIF1) is a nuclear transcriptional regulator and a mitochondrial inner membrane protein; however, its functions in B lymphocytes have been poorly defined. This study was undertaken to investigate the effects of CRIF1 on B cell metabolic regulation, cell function, and autoimmune diseases. Methods Using mice with B cell-specific deletion of CRIF1 (Crif1(Delta CD19) mice), we assessed the relevance of CRIF1 function for lupus disease parameters, including anti-double-stranded DNA (anti-dsDNA), cytokines, and kidney pathology. RNA sequencing was performed on B cells from Crif1(Delta CD19) mice. The phenotypic and metabolic changes in immune cells were evaluated in Crif1(Delta CD19) mice. Roquin(san/+) mice crossed with Crif1(Delta CD19) mice were monitored to assess the functionality of CRIF1-deficient B cells in lupus development. Results Crif1(Delta CD19) mice showed an autoimmune lupus-like phenotype, including high levels of autoantibodies to dsDNA and severe lupus nephritis with increased mesangial hypercellularity. While loss of CRIF1 in B cells showed impaired mitochondrial oxidative function, CRIF1-deficient B cells promoted the production of interleukin-17 (IL-17) and IL-6 and was more potent in helping T cells develop into follicular helper T cells. In a mouse model of autoimmune lupus, depletion of CRIF1 in B cells exacerbated lupus severity, and CRIF1 overexpression prevented lupus development in roquin(san/san) mice. Conclusion These results demonstrated that CRIF1 negatively correlates with disease severity and that overexpression of CRIF1 ameliorates disease development. Our findings suggest that CRIF1 is essential for preventing lupus development by maintaining B cell self tolerance.
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서울 의과대학 (DEPARTMENT OF ANATOMY AND CELL BIOLOGY)
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