突变体
基因
癌变
生物
转录因子
DNA
抄写(语言学)
抑制器
基因表达
抑癌基因
分子生物学
基因表达调控
突变
细胞生物学
遗传学
语言学
哲学
作者
Scott E. Kern,Jennifer A. Pietenpol,Sam Thiagalingam,A. E. Seymour,Kenneth W. Kinzler,Bert Vogelstein
出处
期刊:Science
[American Association for the Advancement of Science (AAAS)]
日期:1992-05-08
卷期号:256 (5058): 827-830
被引量:729
标识
DOI:10.1126/science.1589764
摘要
Mutant forms of the gene encoding the tumor suppressor p53 are found in numerous human malignancies, but the physiologic function of p53 and the effects of mutations on this function are unknown. The p53 protein binds DNA in a sequence-specific manner and thus may regulate gene transcription. Cotransfection experiments showed that wild-type p53 activated the expression of genes adjacent to a p53 DNA binding site. The level of activation correlated with DNA binding in vitro. Oncogenic forms of p53 lost this activity. Moreover, all mutants inhibited the activity of coexpressed wild-type p53, providing a basis for the selection of such mutants during tumorigenesis.
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