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CD20 同源寡聚体与 B 细胞抗原受体发生物理缔合。受体结合以及磷蛋白和钙调蛋白结合蛋白募集时会发生解离。

CD20 homo-oligomers physically associate with the B cell antigen receptor. Dissociation upon receptor engagement and recruitment of phosphoproteins and calmodulin-binding proteins.

作者信息

Polyak Maria J, Li Haidong, Shariat Neda, Deans Julie P

机构信息

Department of Biochemistry and Molecular Biology, Faculty of Medicine, University of Calgary, Calgary, Alberta T2N 4N1, Canada.

出版信息

J Biol Chem. 2008 Jul 4;283(27):18545-52. doi: 10.1074/jbc.M800784200. Epub 2008 May 12.

DOI:10.1074/jbc.M800784200
PMID:18474602
Abstract

B cell antigen receptor (BCR) signaling initiates sustained cellular calcium influx necessary for the development, differentiation, and activation of B lymphocytes. CD20 is a B cell-restricted tetraspanning protein organized in the plasma membrane as multimeric molecular complexes involved in BCR-activated calcium entry. Using coprecipitation of native CD20 with tagged or truncated forms of the molecule, we provide here direct evidence of CD20 homo-oligomerization into tetramers. Additionally, the function of CD20 was explored by examining its association with surface-labeled and intracellular proteins before and after BCR signaling. Two major surface-labeled proteins that coprecipitated with CD20 were identified as the heavy and light chains of cell surface IgM, the antigen-binding components of the BCR. After activation, BCR-CD20 complexes dissociated, and phosphoproteins and calmodulin-binding proteins were transiently recruited to CD20. These data provide new evidence of the involvement of CD20 in signaling downstream of the BCR and, together with the previously described involvement of CD20 in calcium influx, the first evidence of physical coupling of the BCR to a calcium entry pathway.

摘要

B细胞抗原受体(BCR)信号传导引发持续的细胞钙内流,这对于B淋巴细胞的发育、分化和激活是必需的。CD20是一种B细胞限制性的四次跨膜蛋白,在质膜中组织成多聚体分子复合物,参与BCR激活的钙内流。通过将天然CD20与该分子的标记或截短形式进行共沉淀,我们在此提供了CD20同源寡聚化为四聚体的直接证据。此外,通过检测BCR信号传导前后CD20与表面标记和细胞内蛋白的关联,探讨了CD20的功能。与CD20共沉淀的两种主要表面标记蛋白被鉴定为细胞表面IgM的重链和轻链,即BCR的抗原结合成分。激活后,BCR - CD20复合物解离,磷酸化蛋白和钙调蛋白结合蛋白被短暂募集到CD20。这些数据为CD20参与BCR下游信号传导提供了新证据,并且与先前描述的CD20参与钙内流一起,首次证明了BCR与钙内流途径的物理偶联。

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