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Dual role of the tyrosine activation motif of the Ig-alpha protein during signal transduction via the B cell antigen receptor.

机译:在通过B细胞抗原受体进行信号转导过程中Ig-alpha蛋白的酪氨酸激活基序具有双重作用。

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摘要

The B cell antigen receptor (BCR) is a multimeric protein complex consisting of the ligand binding immunoglobulin molecule and the Ig-alpha/beta heterodimer that mediates intracellular signalling by coupling the receptor to protein tyrosine kinases (PTKs). Transfection of the Ig-alpha deficient myeloma cell line J558L microns with expression vectors coding for mutated Ig-alpha allowed us to test the function of the tyrosines in the cytoplasmic region of Ig-alpha in the context of the BCR. Furthermore we expressed Ig-alpha mutations as chimeric CD8-Ig-alpha molecules on K46 B lymphoma cells and tested their signalling capacity in terms of PTK activation and release of calcium. We show here that the conserved tyrosine residues in the cytoplasmic portion of Ig-alpha have a dual role. First, they are required for efficient activation of PTKs during signal induction and second, one of them is subject to phosphorylation by activated src-related PTKs. Phosphorylation on tyrosine in the cytoplasmic portion of Ig-alpha is discussed as a possible mechanism to couple the BCR to SH2 domain-carrying molecules.
机译:B细胞抗原受体(BCR)是由配体结合免疫球蛋白分子和Ig-alpha /β异二聚体组成的多聚体蛋白复合物,通过将受体与蛋白酪氨酸激酶(PTK)偶联来介导细胞内信号传导。用编码突变的Ig-alpha的表达载体转染Ig-alpha缺陷型骨髓瘤细胞系J558L微米使我们能够在BCR的背景下测试酪氨酸在Ig-alpha胞质区域中的功能。此外,我们在K46 B淋巴瘤细胞上将Ig-alpha突变表达为嵌合CD8-Ig-alpha分子,并根据PTK激活和钙释放测试了其信号传导能力。我们在这里显示,Ig-alpha的细胞质部分中的保守酪氨酸残基具有双重作用。首先,它们是在信号诱导过程中有效激活PTK所必需的,其次,其中一个被激活的src相关的PTK磷酸化。讨论了Ig-alpha胞质部分酪氨酸上的磷酸化是将BCR与携带SH2结构域的分子偶联的可能机制。

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