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一种存在于脑组织中的新型GTP结合蛋白,它是百日咳毒素(胰岛激活蛋白)的特异性底物。

A new GTP-binding protein in brain tissues serving as the specific substrate of islet-activating protein, pertussis toxin.

作者信息

Katada T, Oinuma M, Kusakabe K, Ui M

出版信息

FEBS Lett. 1987 Mar 23;213(2):353-8. doi: 10.1016/0014-5793(87)81521-1.

Abstract

A new GTP-binding protein serving as the specific substrate of islet-activating protein (IAP), pertussis toxin, was purified from porcine brain membranes as an alpha beta gamma-heterotrimeric structure. The alpha-subunit of the purified protein (alpha 40 beta gamma) had a molecular mass of 40 kDa and differed from that of Gi (alpha 41 beta gamma) or Go (alpha 39 beta gamma) previously purified from brain tissues. The fragmentation patterns of limited tryptic digestion and immunological cross-reactivities among the three alpha were different from one another. However, the beta gamma-subunit resolved from the three IAP substrates similarly inhibited a membrane-bound adenylate cyclase and their beta-subunits were immunologically indistinguishable from one another. Thus, the alpha 40 beta gamma is a new IAP substrate protein different from Gi or Go, in the alpha-subunit only.

摘要

一种作为胰岛激活蛋白(IAP)(百日咳毒素)特异性底物的新型GTP结合蛋白,以αβγ异源三聚体结构从猪脑膜中纯化得到。纯化蛋白的α亚基(α40βγ)分子量为40 kDa,与先前从脑组织中纯化得到的Gi(α41βγ)或Go(α39βγ)不同。三种α亚基的有限胰蛋白酶消化片段模式和免疫交叉反应性彼此不同。然而,从三种IAP底物中解析出的βγ亚基同样抑制膜结合腺苷酸环化酶,并且它们的β亚基在免疫上无法区分。因此,α40βγ是一种仅在α亚基上不同于Gi或Go的新型IAP底物蛋白。

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