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Beta 3-endonexin a novel polypeptide that interacts specifically with the cytoplasmic tail of the integrin beta 3 subunit

机译:Beta 3-endonexin一种新型多肽与整合素beta 3亚基的胞质尾特异性相互作用

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摘要

The adhesive and signaling functions of integrins are regulated through their cytoplasmic domains. We identified a novel 111 residue polypeptide, designated beta 3-endonexin, that interacted with the cytoplasmic tail of the beta 3 integrin subunit in a yeast two-hybrid system. This interaction is structurally specific, since it was reduced by 64% by a point mutation in the beta 3 cytoplasmic tail (S752-->P) that disrupts integrin signaling. Moreover, this interaction is integrin subunit specific since it was not observed with the cytoplasmic tails of the alpha IIb, beta 1, or beta 2 subunits. beta 3- Endonexin fusion proteins bound selectively to detergent-solubilized beta 3 from platelets and human umbilical vein endothelial cells, and beta 3-endonexin mRNA and protein were detected in platelets and other tissues. A related mRNA encoded a larger polypeptide that failed to bind to beta integrin tails. The apparent specificity of beta 3- endonexin for the beta 3 integrin subunit suggests potential mechanisms for selective modulation of integrin functions.
机译:整联蛋白的粘附和信号传导功能通过其胞质结构域调节。我们鉴定了一种新型的111残基多肽,称为β3-内毒素,它与酵母双杂交系统中的β3整联蛋白亚基的细胞质尾相互作用。这种相互作用在结构上是特定的,因为β3细胞质尾巴中的点突变(S752-> P)破坏了整联蛋白信号传导,使其相互作用降低了64%。此外,这种相互作用是整联蛋白亚基特异性的,因为未观察到αIIb,β1或β2亚基的胞质尾巴。 β3-内毒素融合蛋白与血小板和人脐静脉内皮细胞中去污剂增溶的β3选择性结合,在血小板和其他组织中检测到β3-内毒素mRNA和蛋白。一个相关的mRNA编码了一个较大的多肽,该多肽无法与β整联蛋白尾巴结合。 β3-内毒素对β3整联蛋白亚基的明显特异性表明了选择性调节整联蛋白功能的潜在机制。

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