1. Academic Validation
  2. Novel histone deacetylase inhibitor CG200745 induces clonogenic cell death by modulating acetylation of p53 in cancer cells

Novel histone deacetylase inhibitor CG200745 induces clonogenic cell death by modulating acetylation of p53 in cancer cells

  • Invest New Drugs. 2012 Apr;30(2):435-42. doi: 10.1007/s10637-010-9568-2.
Eun-Taex Oh 1 Moon-Taek Park Bo-Hwa Choi Seonggu Ro Eun-Kyung Choi Seong-Yun Jeong Heon Joo Park
Affiliations

Affiliation

  • 1 Department of Microbiology, Center for Advanced Medical Education by BK21 Project, College of Medicine, Inha University, Shinheung-Dong, Jung-Gu, Inchoen 400-712, South Korea.
Abstract

Histone deacetylase (HDAC) plays an important role in Cancer onset and progression. Therefore, inhibition of HDAC offers potential as an effective Cancer treatment regimen. CG200745, (E)-N(1)-(3-(dimethylamino)propyl)-N(8)-hydroxy-2-((naphthalene-1-loxy)methyl)oct-2-enediamide, is a novel HDAC Inhibitor presently undergoing a phase I clinical trial. Enhancement of p53 acetylation by HDAC inhibitors induces cell cycle arrest, differentiation, and Apoptosis in Cancer cells. The purpose of the present study was to investigate the role of p53 acetylation in the Cancer cell death caused by CG200745. CG200745-induced clonogenic cell death was 2-fold greater in RKO cells expressing wild-type p53 than in p53-deficient RC10.1 cells. CG200745 treatment was also cytotoxic to PC-3 human prostate Cancer cells, which express wild-type p53. CG200745 increased acetylation of p53 lysine residues K320, K373, and K382. CG200745 induced the accumulation of p53, promoted p53-dependent transactivation, and enhanced the expression of MDM2 and p21(Waf1/Cip1) proteins, which are encoded by p53 target genes. An examination of CG200745 effects on p53 acetylation using cells transfected with various p53 mutants showed that cells expressing p53 K382R mutants were significantly resistant to CG200745-induced clonogenic cell death compared with wild-type p53 cells. Moreover, p53 transactivation in response to CG200745 was suppressed in all cells carrying mutant forms of p53, especially K382R. Taken together, these results suggest that acetylation of p53 at K382 plays an important role in CG200745-induced p53 transactivation and clonogenic cell death.

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