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The riddle of the dual expression of IgM and IgD.

机译:IgM和IgD双重表达之谜。

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摘要

Signalling through the B cell antigen receptor (BCR) is required for peripheral B lymphocyte maturation, maintenance, activation and silencing. In mature B cells, the antigen receptor normally consists of two isotypes, membrane IgM and IgD (mIgM, mIgD). Although the signals initiated from both isotypes differ in kinetics and intensity, in vivo, the BCR of either isotype seems to be able to compensate for the loss of the other, reflected by the mild phenotypes of mice deficient for mIgM or mIgD. Thus, it is still unclear why mature B cells need expression of mIgD in addition to mIgM. In the current review we suggest that the view that IgD has a simply definable function centred around the basic signalling function should be replaced by the assumption that IgD fine tunes humoral responses, modulates B cell selection and homeostasis and thus shapes the B cell repertoire, defining IgD to be a key modulator of the humoral immune response.
机译:外周血B淋巴细胞的成熟,维持,激活和沉默需要通过B细胞抗原受体(BCR)发出信号。在成熟的B细胞中,抗​​原受体通常由两种同种型组成,即膜IgM和IgD(mIgM,mIgD)。尽管从两种同种型启动的信号在动力学和强度上都不同,但在体内,两种同种型的BCR似乎都能补偿另一种的损失,这可通过mIgM或mIgD缺陷小鼠的轻度表型反映出来。因此,目前尚不清楚为什么成熟的B细胞除mIgM外还需要表达mIgD。在当前的综述中,我们建议以IgD微调体液反应,调节B细胞选择和体内平衡从而改变B细胞组成,定义IgD具有围绕基本信号功能简单定义的功能的观点来代替IgD是体液免疫反应的关键调节剂。

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