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外文期刊>The journal of immunology
>Cognate B Cell Signaling via MHC Class II: Differential Regulation of B Cell Antigen Receptor and MHC Class II/Ig-αβ Signaling by CD22
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Cognate B Cell Signaling via MHC Class II: Differential Regulation of B Cell Antigen Receptor and MHC Class II/Ig-αβ Signaling by CD22
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机译:通过MHC II类的同源B细胞信号转导:CD22对B细胞抗原受体和MHC II /Ig-αβ信号的差异调节
Recent studies demonstrate that MHC class II molecules can signal via associated Ig-αβ dimers, signal transducers previously thought to function only in B cell Ag receptor (BCR) signaling. Surprisingly, the biologic outputs of MHC class II and BCR ligation (by thymus-dependent Ags) differ, e.g., MHC class II signaling leads to robust proliferation and extension of pseudopods. It seemed possible that these differences might be due, at least in part, to differential use of inhibitory coreceptors thought to modulate membrane Ig signals. In this study, we demonstrate that CD22, an inhibitory BCR coreceptor, neither associates with nor functions in MHC class II/Ig-αβ signaling. Interestingly, CD22 is actively excluded from cell surface MHC class II aggregates.
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机译:最近的研究表明,MHC II类分子可以通过相关的Ig-αβ二聚体发出信号,以前认为这些信号转导仅在B细胞Ag受体(BCR)信号中起作用。令人惊讶地,II类MHC和BCR连接的生物学输出(通过胸腺依赖性Ag)不同,例如,II类MHC信号传导导致假足的强健增殖和延伸。这些差异似乎可能至少部分地是由于不同地使用被认为可调节膜Ig信号的抑制性共受体而引起的。在这项研究中,我们证明CD22,一种抑制性BCR受体,既不与MHC II /Ig-αβ信号传导相关,也没有其功能。有趣的是,CD22被积极地从细胞表面MHC II类聚集体中排除。
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