Michael-Michalovitz D, Yehiely F, Gottlieb E, Oren M
Department of Chemical Immunology, Weizmann Institute of Science, Rehovot, Israel.
J Virol. 1991 Aug;65(8):4160-8. doi: 10.1128/JVI.65.8.4160-4168.1991.
In simian virus 40 (SV40)-transformed cells, a tight complex is formed between the viral large T antigen (large T) and p53. It has been proposed that this complex interferes with the antiproliferative activity of p53. This notion was tested in primary rat fibroblasts by assessing the ability of SV40-mediated transformation to be spared from the inhibitory effect of wild-type (wt) p53. The data indicate that relative to transformation induced by myc plus ras, SV40-plus-ras-mediated focus formation was indeed much less suppressed by p53 plasmids. A majority of the resultant cell lines made a p53 protein with properties characteristic of a wt conformation. Furthermore, cell lines expressing stably both SV40 large T and a temperature-sensitive p53 mutant continued to proliferate at a temperature at which this p53 assumes wt-like properties and normally causes a growth arrest. Surprisingly, at least partial resistance to the growth-inhibitory effect of wt p53 was also evident when transformation was mediated by an SV40 deletion mutant, encoding a large T which does not bind p53 detectably. In addition to supporting the idea that SV40 can overcome the growth-restrictive activity of wt p53, these findings strongly suggest that at least part of this effect does not require a stable association between p53 and large T.
在猿猴病毒40(SV40)转化的细胞中,病毒大T抗原(大T)与p53之间形成紧密复合物。有人提出这种复合物会干扰p53的抗增殖活性。通过评估SV40介导的转化能否免受野生型(wt)p53抑制作用的影响,在原代大鼠成纤维细胞中对这一概念进行了测试。数据表明,相对于myc加ras诱导的转化,p53质粒对SV40加ras介导的集落形成的抑制作用确实要小得多。大多数所得细胞系产生的p53蛋白具有野生型构象的特征。此外,稳定表达SV40大T和温度敏感型p53突变体的细胞系在该p53呈现野生型样特性并通常导致生长停滞的温度下仍继续增殖。令人惊讶的是,当由编码无法检测到与p53结合的大T的SV40缺失突变体介导转化时,对野生型p53的生长抑制作用也至少表现出部分抗性。这些发现除了支持SV40能够克服野生型p53的生长限制活性这一观点外,还强烈表明这种效应至少部分不需要p53与大T之间的稳定结合。
