首页> 美国卫生研究院文献>The EMBO Journal >Acceleration of intracellular targeting of antigen by the B-cell antigen receptor: importance depends on the nature of the antigen-antibody interaction.
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Acceleration of intracellular targeting of antigen by the B-cell antigen receptor: importance depends on the nature of the antigen-antibody interaction.

机译:B细胞抗原受体加速抗原在细胞内的靶向作用:重要性取决于抗原-抗体相互作用的性质。

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摘要

The B-cell antigen receptor (BCR) internalizes bound antigen such that antigen-derived peptides become associated with emigrating major histocompatibility complex (MHC) class II molecules for presentation to T cells. Experiments with B-cell transfectants reveal that BCR confers a specificity of intracellular targeting since chimeric antigen receptors which internalize antigen by virtue of a heterologous cytoplasmic domain do not necessarily give rise to presentation. In contrast, however, previous studies have shown that antigen binding to irrelevant cell surface molecules (e.g. transferrin receptor, MHC class I) can ultimately lead to presentation. The solution to this paradox appears to be that the intracellular targeting by BCR actually reflects an acceleration of antigen delivery. Depending on the nature of the BCR-antigen interaction, this accelerated targeting can be essential in determining whether or not internalization leads to significant presentation. Physiologically, the accelerated delivery of antigen by BCR could prove of particular importance early in the immune response when antigen-BCR interaction is likely to be poor.
机译:B细胞抗原受体(BCR)将结合的抗原内在化,这样抗原衍生的肽就与主要的组织相容性复合物(MHC)II类分子迁移相关,可呈递给T细胞。 B细胞转染子的实验表明BCR赋予了细胞内靶向的特异性,因为借助异质胞质结构域使抗原内在化的嵌合抗原受体不一定会出现。然而,相反,先前的研究表明抗原结合到不相关的细胞表面分子(例如转铁蛋白受体,I类MHC)最终可以导致呈递。解决这一矛盾的方法似乎是BCR的细胞内靶向作用实际上反映了抗原递送的加速。取决于BCR抗原相互作用的性质,这种加速的靶向作用对于确定内在化是否会导致重要的表现至关重要。在生理上,当抗原与BCR的相互作用可能很弱时,BCR加速抗原的递送可能在免疫反应的早期就显得尤为重要。

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