A Cysteine-Reactive Alkyl Hydroquinone Modifies Topoisomerase IIα, Enhances DNA Breakage, and Induces Apoptosis in Cancer Cells

被引:4
|
作者
Lin, Ting-Yu [1 ]
Huang, Cheng-Po [2 ]
Au, Lo-Chun [3 ]
Chang, Ya-Wen [1 ,4 ]
Hu, Chung-Yi [1 ,4 ]
Lin, Shwu-Bin [1 ,2 ]
机构
[1] Natl Taiwan Univ, Dept Clin Lab Sci & Med Biotechnol, Taipei 10764, Taiwan
[2] Double Crane Biotechnol Co, Lingzhi Biomed Inst, New Taipei City, Taiwan
[3] Taipei Vet Gen Hosp, Dept Med Res & Educ, Taipei, Taiwan
[4] Natl Taiwan Univ Hosp, Dept Lab Med, Taipei, Taiwan
关键词
ANTICANCER; IDENTIFICATION; INHIBITOR; CLEAVAGE; GROWTH;
D O I
10.1021/tx3002302
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
We previously reported that the anticancer activity of a botanical compound 10'(Z),13'(E),15'(E)-heptadecatrienylhydroquinone [HQ17(3)] was attributed to topoisomerase (Topo) II alpha poisoning and the induction of oxidative damage. HQ17(3) irreversibly inhibits Topo II alpha activity in vitro and is more cytotoxic in leukemia HL-60 cells than in Topo II alpha-deficient variant HL-60/MX2 cells, which suggests that Topo II alpha is a cellular target of HQ17(3). This study further characterizes the molecular mechanisms of the anticancer activity of HQ17(3). Proteomic analyses indicated that HQ17(3) reacted with Cys-427, Cys-733, and Cys-997 of recombinant Topo II alpha in vitro, whereas it reacted with Cys-427 of cellular Topo II alpha in Huh7 hepatoma cells. The modification of HQ17(3) inhibited Topo II alpha catalytic activity, increased the Topo II alpha-DNA cleavage complex, and caused the accumulation of DNA breakage. In Huh7 cells, HQ17(3) treatment caused prompt inhibition of DNA synthesis and consequently induced the expression of DNA damage-related genes DDIT3, GADD45A, and GADD45G. Topo II alpha inhibition, apoptosis, and oxidative stress were found to account for cytotoxicity caused by HQ17(3). Pretreatment of Huh7 cells with N-acetylcysteine (NAC) partially attenuated mitochondrial membrane damage, DNA breakage, and caspase activation. However, NAC pretreatment did not diminish HQ17(3)-induced cell death. These results suggest that the anticancer activity of HQ17(3) is attributed significantly to Topo II alpha poisoning. The structural feature of HQ17(3) can be used as a model for the design of Topo II alpha inhibitors and anticancer drugs.
引用
收藏
页码:2340 / 2351
页数:12
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