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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Colocalization of the B Cell Receptor and CD20 Followed by Activation-Dependent Dissociation in Distinct Lipid Rafts.
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Colocalization of the B Cell Receptor and CD20 Followed by Activation-Dependent Dissociation in Distinct Lipid Rafts.

机译:B细胞受体和CD20的共定位,然后在不同的脂质筏中进行活化依赖性解离。

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摘要

The B cell Ag receptor (BCR) and CD20, a putative calcium channel, inducibly associate with cholesterol-dependent membrane microdomains known as lipid rafts. A functional association between the BCR and CD20 is suggested by the effects of CD20-specific mAbs, which can modulate cell cycle transitions elicited by BCR signaling. Using immunofluorescence microscopy we show here that the BCR and CD20 colocalize after receptor ligation and then rapidly dissociate at the cell surface before endocytosis of the BCR. After separation, surface BCR and CD20 were detected in distinct lipid rafts isolated as low density, detergent-resistant membrane fragments. Pretreatment with methyl-beta-cyclodextrin, which we have previously shown to enhance receptor-mediated calcium mobilization, did not prevent colocalization of the BCR and CD20, but slowed their dissociation. The data demonstrate rapid dynamics of the BCR in relation to CD20 at the cell surface. Activation-dependent dissociation of the BCR from CD20 occurs before receptor endocytosis and appears to require in part the integrity of lipid rafts.
机译:B细胞银受体(BCR)和CD20(一个推测的钙通道)可诱导性地与胆固醇依赖性膜微区(称为脂质筏)相关。 CD20特异性mAb的作用表明了BCR和CD20之间的功能性关联,它可以调节由BCR信号传导引起的细胞周期转换。使用免疫荧光显微镜,我们在这里显示BCR和CD20在受体连接后共定位,然后在BCR内吞之前迅速在细胞表面解离。分离后,在分离的脂筏中检测到了表面BCR和CD20,脂筏为低密度,耐洗涤剂的膜碎片。我们之前已经证明可以增强受体介导的钙动员作用的甲基-β-环糊精预处理不能阻止BCR和CD20的共定位,但可以减缓它们的离解。数据证明了BCR相对于细胞表面CD20的快速动力学。 BCR从CD20的活化依赖性解离发生在受体内吞之前,并且似乎部分需要脂质筏的完整性。

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