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胰高血糖素和p21 原癌基因产物增强大鼠肝细胞中相同的38千道尔顿膜蛋白的磷酸化作用。

Glucagon and p21 ras enhance the phosphorylation of the same 38-kilodalton membrane protein from rat liver cells.

作者信息

Hegde A N, Das M R

机构信息

Centre for Cellular and Molecular Biology, Hyderabad, India.

出版信息

Mol Cell Biol. 1990 Jun;10(6):2468-74. doi: 10.1128/mcb.10.6.2468-2474.1990.

Abstract

We had reported earlier the enhanced phosphorylation of a 38-kilodalton protein (p38) in rat liver plasma membrane by ras proteins. Now we show that glucagon increased the phosphorylation of the same protein. The nature and site(s) of phosphorylation were the same as those for the ras proteins. Both ATP and GTP could donate phosphate for the phosphorylation of p38. The stimulation of p38 phosphorylation by glucagon was guanine nucleotide dependent. This observation, together with our data on the stimulation of p38 phosphorylation by AIF4-, suggest the involvement of G proteins in the reaction. We also showed that glucagon stimulates the phosphorylation of p38 in vivo.

摘要

我们之前曾报道过,ras蛋白可增强大鼠肝细胞膜中一种38千道尔顿蛋白(p38)的磷酸化作用。现在我们发现,胰高血糖素可增加同一蛋白的磷酸化。磷酸化的性质和位点与ras蛋白相同。ATP和GTP均可为p38的磷酸化提供磷酸基团。胰高血糖素对p38磷酸化的刺激作用依赖于鸟嘌呤核苷酸。这一观察结果,连同我们关于AIF4-刺激p38磷酸化的数据,提示G蛋白参与了该反应。我们还发现,胰高血糖素在体内可刺激p38的磷酸化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/df2f/360603/f807add016d0/molcellb00042-0039-a.jpg

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