作者
Massimo Levrero, V De Laurenzi, A Costanzo, S Sabatini, J Gong, JYJ Wang, G Melino
发表日期
2000/5/15
来源
Journal of cell science
卷号
113
期号
10
页码范围
1661-1670
出版商
The Company of Biologists Ltd
简介
The p53 gene is the most frequently mutated gene in human cancer. The identification of two homologues, p63 and p73, revealed that p53 is a member of a family of related transcription factors. Given that they share amino acid sequence identity reaching 63% in the DNA-binding domain, p53, p63 and p73 should have redundant functions in the regulation of gene expression. Indeed, p73 can activate p53-regulated genes and suppress growth or induce apoptosis. Moreover, p53 and p73 are both induced by DNA damage – albeit through distinct mechanisms. Other evidence, however, suggests that p63 and p73 are important for regulation of normal development. An extended C-terminal region, not found in p53, is alternatively spliced in p63 and p73. Within this C-terminal extension is a sterile alpha motif (SAM) previously found in other proteins that regulate development. The p63-deficient mice showed …
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