B cell signaling and autoimmune diseases: CD19/CD22 loop as a B cell signaling device to regulate the balance of autoimmunity
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概要
- 論文の詳細を見る
Autoimmune diseases, including connective tissue diseases and bullous diseases, may be life-threatening. Recent clinical and experimental approaches have demonstrated that B cells play critical roles in the manifestation of autoimmune disease not only by well-established autoantibody-mediated mechanisms but also by a variety of other functions. These B cell functions are under the regulation of B cell antigen receptor (BCR)-induced signals and by specialized cell surface coreceptors, or "response regulators", which inform B cells of their microenvironment. These response regulators include CD19 and CD22. CD19 and CD22 do not merely regulate BCR signals independently, but they have their own regulatory network. CD19 regulates CD22 phoshorylation by augmenting Lyn kinase activity, while CD22 inhibits CD19 phosphorylation via SHP-1. Importantly, this "CD19/CD22 loop" is significantly related to an autoimmune phenotype in mice. Thus, the CD19/CD22 loop may be a potential therapeutic target in autoimmune disease for modulating B cell signaling. © 2006 Japanese Society for Investigative Dermatology.
- Elsevier BVの論文
- 2007-04-01
著者
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FUJIMOTO Manabu
Department of Dermatology, Kanazawa University Hospital
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Fujimoto Manabu
Department Of Dermatology Kanazawa University Graduate School Of Medical Science
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Fujimoto Manabu
Department Of Cardiology Kanazawa National Hospital
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SATO SHINICHI
Departments of Internal Medicine, Sakura National Hospital
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Sato Shinichi
Department Of Dermatology Nagasaki University Graduate School Of Biomedical Sciences
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Sato Shinichi
Department Of Dermatology Faculty Of Medicine University Of Tokyo
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Sato Shinichi
Department Of Applied Biology Faculty Of Textile Science Kyoto Institute Of Technology
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