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Treanor, B.B-cell receptor: From resting state to activate

机译:Treanor,B.B细胞受体:从静止状态到活化

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B-cell activation is triggered by the binding of antigen to the B-cell receptor (BCR). The early molecular events triggered by BCR binding of ligand have been well-characterized both biochemically and using optical microscopy techniques to visualize B-cell activation as it happens. However, we understand much less about the BCR before activation. For this reason, this review will address recent advances in our view of the structure, organization and dynamics of the resting, unstimulated BCR. These parameters have important implications for our understanding of the initiation of B-cell activation and will be discussed in the context of current models for BCR activation. These models include the conformation-induced oligomerization model, in which binding of antigen to monomeric BCR induces a pulling or twisting force causing conformational unmasking of a clustering interface in the Cμ4 domain. Conversely, the dissociation activation model proposes that BCRs exist in auto-inhibitory oligomers on the resting B-cell surface and binding of antigen promotes the dissociation of the BCR oligomer exposing phosphorylation residues within Igα/Igβ. Finally, the collision coupling model suggests that BCR are segregated from activating co-receptors or kinases and activation is associated with changes in BCR mobility on the cell surface, which allows for the functional interaction of these elements.
机译:抗原与B细胞受体(BCR)结合可触发B细胞活化。由BCR配体的结合触发的早期分子事件已在生化和使用光学显微镜技术中很好地表征了B细胞的激活情况。但是,在激活之前,我们对BCR的了解很少。因此,本综述将探讨我们在静止,无刺激的BCR的结构,组织和动力学方面的最新进展。这些参数对于我们对B细胞活化的启动的理解具有重要意义,并将在当前BCR活化模型的背景下进行讨论。这些模型包括构象诱导的寡聚模型,其中抗原与单体BCR的结合诱导拉力或扭曲力,从而引起Cμ4结构域中聚类界面的构象未掩盖。相反,解离激活模型提出,BCRs存在于静止的B细胞表面的自抑制寡聚体中,抗原的结合促进了BCR寡聚体的解离,从而暴露了Igα/Igβ中的磷酸化残基。最后,碰撞耦合模型表明BCR与激活的共受体或激酶分离,并且激活与细胞表面BCR迁移率的变化相关,这允许这些元素的功能相互作用。

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