汪晴

个人信息Personal Information

教授

博士生导师

硕士生导师

性别:男

毕业院校:日本国立九州工业大学

学位:博士

所在单位:化工学院

学科:药剂学. 药物工程

办公地点:大连理工大学制药科学与技术学院 G202

联系方式:0411-84986176

电子邮箱:qwang@dlut.edu.cn

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Selective Inhibition of Bicyclic Tetrapeptide Histone Deacetylase Inhibitor on HDAC4 and K562 Leukemia Cell

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论文类型:期刊论文

发表时间:2013-07-01

发表刊物:ASIAN PACIFIC JOURNAL OF CANCER PREVENTION

收录刊物:SCIE、PubMed、Scopus

卷号:14

期号:12

页面范围:7095-7100

ISSN号:1513-7368

关键字:Histone deacetylase inhibitor; bicyclic tetrapeptide; leukemia

摘要:Histone deacetylase (HDAC) inhibitors of cyclic peptide have been proved to be the most complex but the most stable and relative efficient inhibitors because of their large cap region. In this paper, a series of studies were carried out to evaluate the efficacy of synthetic bicyclic tetrapeptide inhibitors 1-5 containing hydroxamic acid referring molecular docking, anti-proliferation, morphology and apoptosis. Docking analysis, together with enzyme inhibitory results, verified the selective capability of inhibitor 4 to HDAC4, which might closely related to haematological tumorigenesis, with Phe227, Asp115, Pro32, His198 and Ser114 participating into hydrophobic interactions and Van der Waals force which was familiar with former study. Moreover, inhibitor 4 inhibited K562 cell line at the IC50 value of 1.22 mu M which was 51-67 times more efficient than that for U937 and HL60 cell lines. Inhibitor 4 exhibited the cell cycle-arrested capability to leukemia at S phase or G2/M phase as well as apoptosis-induced ability in different degrees. Finally, we considered that bicyclic tetrapeptide inhibitors were promising inhibitors used in cancer treatment and inhibitor 4 could prevent K562 cell line well from proliferation, arrest cell cycle and induce K562 towards apoptosis to achieve the goals of reversing cancer cells which could become a potential leukemia therapeutic agent in the future.