首页> 外文期刊>Scandinavian journal of immunology. >On how the immune system preferentially interacts with antigen‐specific molecules bound to antigen over unbound molecules, with emphasis on B cell receptor signalling
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On how the immune system preferentially interacts with antigen‐specific molecules bound to antigen over unbound molecules, with emphasis on B cell receptor signalling

机译:关于免疫系统如何优先与在未结合分子上结合抗原的抗原特异性分子相互作用,重点是B细胞受体信号传导

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Abstract Antigen‐specific molecules of the immune system, namely antibodies, the membrane immunoglobulins (mIgs) of B cells and T cell receptors (TcRs), can all signal their interaction with antigen. There are different mechanisms by which this signalling could occur. These mechanisms can be divided into two general categories: allosteric and non‐allosteric. In allosteric mechanisms, the monovalent binding of the antigen to the receptor triggers a conformational change at the binding site that is propagated to an invariant part of the receptor, a change recognized by a sensing unit. We argue allosteric mechanisms are implausible. Non‐allosteric mechanisms depend on steric effects due to the antigen's size and/or multivalency. We consider two non‐allosteric mechanisms by which the mIg of B cells has been envisaged to signal its interaction with antigen: the popular cross‐linking model and the dissociation activation model. We argue, on the basis of both experimental observations and physiological considerations, that the dissociation activation model, developed by Reth and his colleagues, is uniquely plausible.
机译:摘要免疫系统的特异性分子,即抗体,B细胞和T细胞受体(TCRS)的膜免疫球蛋白(MIG),可以所有信号与抗原的相互作用。存在可能发生这种信令的不同机制。这些机制可分为两种一般类别:变构和非变构。在变构机制中,对受体的抗原的一价结合触发了传播到受体的不变部分的结合位点的构象变化,该变化由传感单元识别。我们认为争辩机制是难以置信的。由于抗原的尺寸和/或多价,非变构机制取决于空间效应。我们考虑了两种非变构机制,其中已经设想了B细胞的MIG以发出与抗原的相互作用:流行的交联模型和解离激活模型。我们在实验观察和生理考虑的基础上争辩说,由RETH和他的同事制定的解离激活模型是独特的。

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