作者
Jing Huang, Roopsha Sengupta, Alexsandra B Espejo, Min Gyu Lee, Jean A Dorsey, Mario Richter, Susanne Opravil, Ramin Shiekhattar, Mark T Bedford, Thomas Jenuwein, Shelley L Berger
发表日期
2007/9/6
期刊
Nature
卷号
449
期号
7158
页码范围
105-108
出版商
Nature Publishing Group UK
简介
p53, the tumour suppressor and transcriptional activator, is regulated by numerous post-translational modifications, including lysine methylation,. Histone lysine methylation has recently been shown to be reversible; however, it is not known whether non-histone proteins are substrates for demethylation. Here we show that, in human cells, the histone lysine-specific demethylase LSD1 (refs , ) interacts with p53 to repress p53-mediated transcriptional activation and to inhibit the role of p53 in promoting apoptosis. We find that, in vitro, LSD1 removes both monomethylation (K370me1) and dimethylation (K370me2) at K370, a previously identified Smyd2-dependent monomethylation site. However, in vivo, LSD1 shows a strong preference to reverse K370me2, which is performed by a distinct, but unknown, methyltransferase. Our results indicate that K370me2 has a different role in regulating p53 from that of K370me1 …
引用总数
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学术搜索中的文章
J Huang, R Sengupta, AB Espejo, MG Lee, JA Dorsey… - Nature, 2007