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阿片样肽可促进神经母细胞瘤与胶质瘤杂交细胞膜中抑制性鸟嘌呤核苷酸结合蛋白(Gi)的霍乱毒素催化的ADP核糖基化。

Opioid peptides promote cholera-toxin-catalysed ADP-ribosylation of the inhibitory guanine-nucleotide-binding protein (Gi) in membranes of neuroblastoma x glioma hybrid cells.

作者信息

Milligan G, McKenzie F R

机构信息

Department of Biochemistry, University of Glasgow, Scotland, U.K.

出版信息

Biochem J. 1988 Jun 1;252(2):369-73. doi: 10.1042/bj2520369.

Abstract

NG108-15 neuroblastoma x glioma hybrid cells express a major 45 kDa substrate for cholera toxin and a 40 kDa substrate(s) for pertussis toxin when ADP-ribosylation is performed in the presence of GTP. In the absence of exogenous GTP, however, cholera toxin was shown to catalyse incorporation of radioactivity into a 40 kDa protein as well as into the 45 kDa polypeptide. In membranes of cells which had been pretreated in vivo with pertussis toxin, the 40 kDa band was no longer a substrate for either pertussis or cholera toxin in vitro, whereas in membranes from cholera-toxin-pretreated cells the 40 kDa band was still a substrate for fresh cholera toxin in vitro and for pertussis toxin. In this cell line, opioid peptides have been shown to inhibit adenylate cyclase exclusively by interacting with Gi (inhibitory G-protein) and with no other pertussis-toxin-sensitive G-protein. Opioid agonists, but not antagonists, promoted the cholera-toxin-catalysed ADP-ribosylation of the 40 kDa polypeptide, hence demonstrating that this cholera-toxin substrate was indeed the alpha-subunit of Gi. These results demonstrate that Gi can be a substrate for either cholera or pertussis toxin under appropriate conditions.

摘要

NG108 - 15神经母细胞瘤x胶质瘤杂交细胞在GTP存在的情况下进行ADP - 核糖基化时,表达一种主要的45 kDa霍乱毒素底物和一种40 kDa百日咳毒素底物。然而,在没有外源性GTP的情况下,霍乱毒素被证明能催化放射性掺入一种40 kDa蛋白质以及45 kDa多肽中。在用百日咳毒素进行体内预处理的细胞的膜中,40 kDa条带在体外不再是百日咳毒素或霍乱毒素的底物,而在经霍乱毒素预处理的细胞的膜中,40 kDa条带在体外仍然是新鲜霍乱毒素和百日咳毒素的底物。在这种细胞系中,阿片肽已被证明仅通过与Gi(抑制性G蛋白)相互作用来抑制腺苷酸环化酶,而不与其他百日咳毒素敏感的G蛋白相互作用。阿片激动剂而非拮抗剂促进了霍乱毒素催化的40 kDa多肽的ADP - 核糖基化,因此表明这种霍乱毒素底物确实是Gi的α亚基。这些结果表明,在适当条件下,Gi可以是霍乱毒素或百日咳毒素的底物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e61f/1149154/ba5d9047aad6/biochemj00230-0061-a.jpg

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