Functional role of lipid rafts in CD20 activity?

Eva Janas, Richard Priest, Rajneesh Malhotra
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引用次数: 19

Abstract

CD20 is a B-lymphocyte-specific integral membrane protein, implicated in the regulation of transmembrane calcium conductance, cell-cycle progression and B-lymphocyte proliferation. CD20 is proposed to function as a SOCC (store-operated calcium channel). SOCCs are activated by receptor-stimulated calcium depletion of intracellular stores. Sustained calcium conductivity across the plasma membrane mediated by SOCC activity is required for long-term calcium-dependent processes, such as transcriptional control and gene expression. Cross-linking of CD20 by antibodies (e.g. Rituxan) has been reported to induce a rapid redistribution of CD20 into specialized microdomains at the plasma membrane, known as lipid rafts. Recruitment of CD20 into lipid rafts and its homo-oligomerization are suggested to be crucial for CD20 activity and regulation. This review outlines recent biochemical studies characterizing the role of CD20 in calcium signalling in B-lymphocytes and evaluates an engagement of lipid rafts in the regulation of CD20-mediated calcium conductivity.

脂筏在CD20活性中的功能作用?
CD20是一种b淋巴细胞特异性整体膜蛋白,参与调节跨膜钙传导、细胞周期进程和b淋巴细胞增殖。CD20被认为是一种储运钙通道(SOCC)。SOCCs是由受体刺激的细胞内储存的钙耗尽激活的。长期的钙依赖过程(如转录控制和基因表达)需要由SOCC活性介导的钙在质膜上的持续传导。据报道,抗体(如Rituxan)的CD20交联可诱导CD20快速重新分布到质膜上的特定微域,即脂筏。脂筏中CD20的募集及其同源寡聚化被认为是CD20活性和调控的关键。本文概述了最近的生化研究,描述了CD20在b淋巴细胞钙信号传导中的作用,并评估了脂筏在CD20介导的钙传导调节中的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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