一种致癌形式的p53赋予一种显性的功能获得性表型,这种表型会破坏纺锤体检查点控制。
An oncogenic form of p53 confers a dominant, gain-of-function phenotype that disrupts spindle checkpoint control.
作者信息
Gualberto A, Aldape K, Kozakiewicz K, Tlsty T D
机构信息
Life Sciences Division, Lawrence Berkeley National Laboratory, Berkeley, CA 94720, USA.
出版信息
Proc Natl Acad Sci U S A. 1998 Apr 28;95(9):5166-71. doi: 10.1073/pnas.95.9.5166.
Abstract
Although it is well-established that p53 functions as a tumor suppressor gene, certain mutations exhibit gain-of-function activities that increase oncogenic transformation. We have found a common class of p53 missense mutation that exhibits a dominant, gain-of-function activity that generates genomic instability. Fibroblasts from Li-Fraumeni syndrome heterozygotes with such mutations generate polyploid cells when exposed to spindle depolymerizing agents. Expression of such mutant alleles in normal fibroblasts yields the same phenotype. This class of dominant, gain-of-function p53 mutation (p53(RSC), relaxed spindle checkpoint allele) does not require the transcriptional activation function of p53 for this behavior. Thus p53 mutations can contribute to progression of a cancer cell not only by absence of p53 tumor suppressor activity but also by the presence of an activity that promotes genetic instability.
摘要
尽管p53作为一种肿瘤抑制基因的功能已得到充分证实,但某些突变会表现出功能获得性活性,从而增加致癌转化。我们发现了一类常见的p53错义突变,其表现出显性的功能获得性活性,可导致基因组不稳定。患有此类突变的李-弗劳梅尼综合征杂合子的成纤维细胞在暴露于纺锤体解聚剂时会产生多倍体细胞。在正常成纤维细胞中表达此类突变等位基因会产生相同的表型。这类显性的、功能获得性p53突变(p53(RSC),松弛纺锤体检查点等位基因)的这种行为并不需要p53的转录激活功能。因此,p53突变不仅可通过缺乏p53肿瘤抑制活性,还可通过存在促进基因不稳定的活性来促进癌细胞的进展。
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