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纯化的gag-mil和gag-raf蛋白的丝氨酸和苏氨酸特异性蛋白激酶活性。

Serine- and threonine-specific protein kinase activities of purified gag-mil and gag-raf proteins.

作者信息

Moelling K, Heimann B, Beimling P, Rapp U R, Sander T

出版信息

Nature. 1984;312(5994):558-61. doi: 10.1038/312558a0.

Abstract

Retroviruses carry cell-derived oncogenes (v-onc) that have the potential to transform cells in culture and induce tumours in vivo. One of the few carcinoma-inducing viruses is the acutely transforming retrovirus MH2, which carries the putative oncogene v-mil and the known oncogene v-myc. Recently, a high degree of homology was discovered between v-mil and v-raf, the transforming gene of the murine retrovirus 3611 murine sarcoma virus (MSV), whereas homology to v-src is low. Both viruses express their oncogenes as the gag-fusion polyproteins p100gag-mil and p75gag-raf (of respective relative molecular mass (Mr) 100,000 and 75,000), while the myc oncogene of MH2 is expressed by means of a subgenomic messenger RNA. We have recently demonstrated that p100gag-mil is not a nuclear protein. Here we report that purified p100gag-mil and p75gag-raf exhibit protein kinase activities in vitro which, in contrast to the src-related p130gag-fps of Fujinami sarcoma virus (FSV) and all other characterized oncogene-encoded protein kinases, phosphorylate serine and threonine but not tyrosine. Both types of protein kinases phosphorylate lipids in vitro.

摘要

逆转录病毒携带源自细胞的癌基因(v-onc),这些癌基因有可能在培养中转化细胞并在体内诱发肿瘤。少数能诱发癌症的病毒之一是急性转化型逆转录病毒MH2,它携带推定的癌基因v-mil和已知的癌基因v-myc。最近,人们发现v-mil与鼠逆转录病毒3611鼠肉瘤病毒(MSV)的转化基因v-raf之间存在高度同源性,而与v-src的同源性较低。两种病毒都将其癌基因表达为gag融合多蛋白p100gag-mil和p75gag-raf(各自的相对分子质量(Mr)分别为100,000和75,000),而MH2的myc癌基因则通过亚基因组信使核糖核酸来表达。我们最近证明p100gag-mil不是核蛋白。在此我们报告,纯化的p100gag-mil和p75gag-raf在体外表现出蛋白激酶活性,与 Fujinami 肉瘤病毒(FSV)的src相关p130gag-fps以及所有其他已鉴定的癌基因编码蛋白激酶不同,它们使丝氨酸和苏氨酸磷酸化,而不使酪氨酸磷酸化。这两种蛋白激酶在体外都能使脂质磷酸化。

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