| Literature DB >> 20531295 |
S-H Lee1, G-N Shen, Y S Jung, S-J Lee, J-Y Chung, H-S Kim, Y Xu, Y Choi, J-W Lee, N-C Ha, G Y Song, B-J Park.
Abstract
p53 is frequently mutated by genetic alternation or suppressed by various kinds of cellular signaling pathways in human cancers. Recently, we have revealed that p53 is suppressed and eliminated from cells by direct binding with oncogenic K-Ras-induced Snail. On the basis of the fact, we generated specific inhibitors against p53-Snail binding (GN25 and GN29). These chemicals can induce p53 expression and functions in K-Ras-mutated cells. However, it does not show cytotoxic effect on normal cells or K-Ras-wild-type cells. Moreover, GN25 can selectively activate wild-type p53 in p53(WT/MT) cancer cells. But single allelic mt p53 containing cell line, Panc-1, does not respond to our chemical. In vivo xenograft test also supports the antitumor effect of GN25 in K-Ras-mutated cell lines. These results suggest that our compounds are strong candidate for anticancer drug against K-Ras-initiated human cancers including pancreatic and lung cancers.Entities:
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Year: 2010 PMID: 20531295 DOI: 10.1038/onc.2010.208
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867