Histone Arg modifications and p53 regulate the expression of OKL38, a mediator of apoptosis.

AUTHORS

Yao HHongjie , Li P Pingxin , Venters BJ Bryan J , Zheng S Suting , Thompson PR Paul R , Pugh BF B Franklin , Wang Y Yanming . The Journal of biological chemistry. 2008 7 18; 283(29). 20060-8

PMID: 18499678[PubMed].
PMCID: PMC2459274.

ABSTRACT

Protein Arg methyltransferases function as coactivators of the tumor suppressor p53 to regulate gene expression. Peptidylarginine deiminase 4 (PAD4/PADI4) counteracts the functions of protein Arg methyltransferases in gene regulation by deimination and demethylimination. Here we show that the expression of a tumor suppressor gene, OKL38, is activated by the inhibition of PAD4 or the activation of p53 following DNA damage. Chromatin immunoprecipitation assays showed a dynamic change of p53 and PAD4 occupancy and histone Arg modifications at the OKL38 promoter during DNA damage, suggesting a direct role of PAD4 and p53 in the expression of OKL38. Furthermore, we found that OKL38 induces apoptosis through localization to mitochondria and induction of cytochrome c release. Together, our studies identify OKL38 as a novel p53 target gene that is regulated by PAD4 and plays a role in apoptosis.