Bonde B G, Sharif M, Privalsky M L
Department of Microbiology, University of California, Davis 95616.
J Virol. 1991 Apr;65(4):2037-46. doi: 10.1128/JVI.65.4.2037-2046.1991.
The avian erythroblastosis virus v-erbA oncogene is imprecisely derived from a cellular gene (c-erbA) encoding a thyroid hormone receptor: the v-erbA protein has sustained both small terminal deletions and internal amino acid sequence changes relative to c-erbA. We report here that one of these missense differences between v- and c-erbA proteins, located in a zinc finger DNA binding domain, has dramatic effects on the biological activities of the encoded protein. Back mutation of the viral coding sequence to resemble c-erbA at this site severely impairs erythroid transformation and produces subtle changes in DNA binding by the encoded protein, suggesting that differences in DNA binding by the viral and cellular proteins may be involved in the activation of v-erbA as an oncogene.
禽成红细胞增多症病毒v-erbA癌基因是由一个编码甲状腺激素受体的细胞基因(c-erbA)不精确衍生而来:相对于c-erbA,v-erbA蛋白既有小的末端缺失,又有内部氨基酸序列变化。我们在此报告,v-erbA和c-erbA蛋白之间的这些错义差异之一,位于锌指DNA结合域,对所编码蛋白的生物学活性有显著影响。病毒编码序列在此位点的回突变使其类似于c-erbA,这严重损害了红细胞转化,并使所编码蛋白的DNA结合产生细微变化,表明病毒蛋白和细胞蛋白在DNA结合上的差异可能与v-erbA作为癌基因的激活有关。
