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跨膜4超家族蛋白CD81(TAPA-1)、CD82、CD63和CD53与整合素α4β1(CD49d/CD29)特异性相关。

Transmembrane-4 superfamily proteins CD81 (TAPA-1), CD82, CD63, and CD53 specifically associated with integrin alpha 4 beta 1 (CD49d/CD29).

作者信息

Mannion B A, Berditchevski F, Kraeft S K, Chen L B, Hemler M E

机构信息

Dana-Farber Cancer Institute, Harvard Medical School, Boston, MA 02115, USA.

出版信息

J Immunol. 1996 Sep 1;157(5):2039-47.

PMID:8757325
Abstract

Anti-alpha 4 integrin mAb coprecipitated CD81 (TAPA-1), a 25-kDa cell surface protein, from various alpha 4 beta1 -positive hemopoietic cell lines, including Molt4, Jurkat, Ramos, and alpha 4-transfected K562 (KX4C4) cells. In reciprocal experiments, the integrin alpha 4 beta 1 (VLA4, CD49d/CD29) could be reprecipitated from CD81 immunoprecipitates. Anti-alpha 4 integrin mAb also coprecipitated CD81 from the alpha 4 beta 7-positive B cell line RPMI 8866. In contrast, no CD81 was identified in alpha 2 beta 1, alpha 5 beta 1, or alpha L beta 2 immunoprecipitates. Abs to other members of the transmembrane-4 superfamily, including CD53, CD63, and CD82, also coprecipitated alpha 4 beta 1. As shown by confocal microscopy, CD81 and CD82 colocalized with alpha 4 beta 1 in cell surface clusters. The cytoplasmic domain of the alpha 4 integrin was not necessary for alpha 4 beta 1/CD81 association, nor was the association influenced by divalent cations, EDTA, integrin-activating mAb, or alpha 4 subunit cleavage. Notably, two independent alpha 4 adhesion-deficient mutants (D346E and D408E) were deficient in their ability to associate with CD81. Thus, CD81 and other transmembrane-4 superfamily members may participate in functionally relevant interactions with alpha 4 beta 1 and other integrins.

摘要

抗α4整合素单克隆抗体能从多种α4β1阳性造血细胞系中共同沉淀出CD81(TAPA - 1),一种25 kDa的细胞表面蛋白,这些细胞系包括Molt4、Jurkat、Ramos以及α4转染的K562(KX4C4)细胞。在反向实验中,整合素α4β1(VLA4,CD49d/CD29)可从CD81免疫沉淀物中再次沉淀出来。抗α4整合素单克隆抗体也能从α4β7阳性B细胞系RPMI 8866中共同沉淀出CD81。相比之下,在α2β1、α5β1或αLβ2免疫沉淀物中未鉴定出CD81。针对跨膜4超家族其他成员的抗体,包括CD53、CD63和CD82,也能共同沉淀出α4β1。如共聚焦显微镜所示,CD81和CD82在细胞表面簇中与α4β1共定位。α4整合素的胞质结构域对于α4β1/CD81的结合并非必需,这种结合也不受二价阳离子、EDTA、整合素激活单克隆抗体或α4亚基裂解的影响。值得注意的是,两个独立的α4黏附缺陷突变体(D346E和D408E)与CD81结合的能力存在缺陷。因此,CD81和其他跨膜4超家族成员可能参与与α4β1和其他整合素的功能相关相互作用。

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