| Literature DB >> 26944433 |
Lihui Wang1, Xuefei Bao2, Jingyu Yang1, Huahuan Li1, Qifan Zhou2, Xiaorui Jiang1, Meng Li1, Xing Liu1, Xiangzhong Yuan1, Yuhong Sun1, Junli Chen1, Jingyuan Zhang3, Guoliang Chen4, Chunfu Wu5.
Abstract
A novel series of cinnamohydroxamic acid derivatives were synthesized and their biological activities against HDAC were assessed. Our results showed that the compound with more strong inhibitory activity to HDAC would exhibited more significant anti-proliferative effect on tumor cells. Among these compounds, 7e displayed clearly inhibitory effects on HDAC and tumor cell growth. Furthermore, HDAC isoforms enzyme data indicated that, compared to HDAC pan-inhibitor SAHA, 7e owned an enhanced inhibitory effect on HDAC1, 3 and 6 isoforms. Meanwhile, it also significantly suppressed cell growth of lung cancer cells compared to SAHA, but with lower toxicity in normal cells. Mechanistically, 7e prompted acetylation of histone3 and histone4, led to up-regulation of p21, and then mediated cell cycle arrest and pro-apoptosis. Moreover, the in vivo study indicated that compound 7e could retard tumor growth of A549 xenograft models. These findings support the further investigation on the anti-tumor potential of this class of compounds as HDAC inhibitor.Entities:
Keywords: Apoptosis; Cancer; Cell cycle; Histone deacetylase inhibitor
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Year: 2016 PMID: 26944433 DOI: 10.1016/j.cbi.2016.02.018
Source DB: PubMed Journal: Chem Biol Interact ISSN: 0009-2797 Impact factor: 5.192