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腹水肝癌细胞系质膜中的内源性过度磷酸化

Endogenous hyperphosphorylation in plasma membrane from an ascites hepatocarcinoma cell line.

作者信息

Church J G, Ghosh S, Roufogalis B D, Villalobo A

机构信息

Faculty of Pharmaceutical Sciences, University of British Columbia, Vancouver, Canada.

出版信息

Biochem Cell Biol. 1988 Jan;66(1):1-12. doi: 10.1139/o88-001.

Abstract

Plasma-membrane-bound kinases of AS-30D ascites from transplantable rat hepatocarcinoma were shown to extensively catalyze the phosphorylation of plasma membrane proteins and membrane lipids, using [gamma-32P]ATP or [gamma-32P]GTP as a phosphate donor. In contrast, plasma membranes from normal adult rat liver or fast-growing regenerating liver (24 h after partial hepatectomy) produce significantly less activity for protein phosphorylation and little phosphorylation of the lipids. However, neonatal (24 h old) rat liver plasma membrane preparations show levels of phosphorylation of proteins and lipids intermediate between those in the tumor cell line and normal adult plasma membrane preparations. Phosphatidic acid was identified as one of the 32P-labelled lipids in the tumor plasma membrane chloroform-methanol (2:1, v/v) extract. Phosphorylation of protein was not affected by cAMP or cGMP. However, calcium ion (in the presence or absence of calmodulin) significantly modifies the 32P labelling of a series of proteins in normal tissue but has little effect with the neoplastic preparations. Some plasma membrane proteins were capable of nucleotide binding, instead or in addition to being phosphorylated. Finally, the presence of membrane-bound phosphoprotein phosphatase(s) was also demonstrated in all the preparations examined by means of chase experiments with nonlabelled ATP or GTP, and (or) by the use of the phosphoprotein phosphatase inhibitor, orthovanadate.

摘要

来自可移植大鼠肝癌的AS-30D腹水的质膜结合激酶,使用[γ-32P]ATP或[γ-32P]GTP作为磷酸盐供体,被证明可广泛催化质膜蛋白和膜脂的磷酸化。相比之下,正常成年大鼠肝脏或快速生长的再生肝脏(部分肝切除术后24小时)的质膜对蛋白质磷酸化的活性显著较低,对脂质的磷酸化也很少。然而,新生(24小时大)大鼠肝脏质膜制剂显示蛋白质和脂质的磷酸化水平介于肿瘤细胞系和正常成年质膜制剂之间。磷脂酸被鉴定为肿瘤质膜氯仿-甲醇(2:1,v/v)提取物中32P标记的脂质之一。蛋白质的磷酸化不受cAMP或cGMP的影响。然而,钙离子(无论有无钙调蛋白)显著改变正常组织中一系列蛋白质的32P标记,但对肿瘤制剂影响很小。一些质膜蛋白除了被磷酸化外,还能够结合核苷酸。最后,通过用未标记的ATP或GTP进行追踪实验,和(或)使用磷蛋白磷酸酶抑制剂原钒酸盐,在所有检测的制剂中也证明了膜结合磷蛋白磷酸酶的存在。

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