B cell class switch recombination is regulated by DYRK1A through MSH6 phosphorylation

被引:0
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作者
Liat Stoler-Barak
Ethan Harris
Ayelet Peres
Hadas Hezroni
Mirela Kuka
Pietro Di Lucia
Amalie Grenov
Neta Gurwicz
Meital Kupervaser
Bon Ham Yip
Matteo Iannacone
Gur Yaari
John D. Crispino
Ziv Shulman
机构
[1] Weizmann Institute of Science,Department of Systems Immunology
[2] St. Jude Children’s Research Hospital,Department of Hematology
[3] Bar Ilan University,Faculty of Engineering
[4] Vita-Salute San Raffaele University and Division of Immunology,De Botton Institute for Proteomics
[5] Transplantation and Infectious Diseases,Experimental Imaging Center
[6] IRCCS San Raffaele Scientific Institute,undefined
[7] Grand Israel National Center for Personalized Medicine,undefined
[8] Weizmann Institute of Science,undefined
[9] IRCCS San Raffaele Scientific Institute,undefined
来源
Nature Communications | / 14卷
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摘要
Protection from viral infections depends on immunoglobulin isotype switching, which endows antibodies with effector functions. Here, we find that the protein kinase DYRK1A is essential for B cell-mediated protection from viral infection and effective vaccination through regulation of class switch recombination (CSR). Dyrk1a-deficient B cells are impaired in CSR activity in vivo and in vitro. Phosphoproteomic screens and kinase-activity assays identify MSH6, a DNA mismatch repair protein, as a direct substrate for DYRK1A, and deletion of a single phosphorylation site impaired CSR. After CSR and germinal center (GC) seeding, DYRK1A is required for attenuation of B cell proliferation. These findings demonstrate DYRK1A-mediated biological mechanisms of B cell immune responses that may be used for therapeutic manipulation in antibody-mediated autoimmunity.
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