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首页> 外文期刊>The Prostate >A novel hydroxysuberamide derivative potentiates MG132-mediated anticancer activity against human hormone refractory prostate cancers - The role of histone deacetylase and endoplasmic reticulum stress
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A novel hydroxysuberamide derivative potentiates MG132-mediated anticancer activity against human hormone refractory prostate cancers - The role of histone deacetylase and endoplasmic reticulum stress

机译:新型羟基亚氨基酰胺衍生物增强了MG132介导的抗人激素难治性前列腺癌的抗癌活性-组蛋白脱乙酰基酶和内质网应激的作用

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BACKGROUND Histone deacetylase (HDAC) inhibitors are successful for treatment of advanced cutaneous T-cell lymphoma but only show modest effect in solid tumors. Approaches for HDAC inhibitors to improve activity against solid tumors are necessary. METHODS Sulforhodamine B assay and flow cytometric analysis detected cell proliferation and cell-cycle progression, respectively. Protein expression was determined by Western blotting. Comet assay and DNA end-binding activity of Ku proteins detected DNA damage and DNA repair activity, respectively. siRNA technique was used for knockdown of specific cellular target. RESULTS WJ25591 displayed inhibitory activity against HDAC1 and cell proliferation in human hormone-refractory prostate cancers PC-3 and DU-145. WJ25591 caused an arrest of cell-cycle at both G1- and G2-phase and increased protein expressions of p21 and cyclin E, followed by cell apoptosis. WJ25591-induced Bcl-2 down-regulation and activation of caspase-9, -8, and -3, suggesting apoptotic execution through both intrinsic and extrinsic apoptotic pathways. WJ25591 also significantly inhibited DNA repair activity but not directly induced DNA damage. Moreover, the proteasome inhibitor MG-132 dramatically sensitized WJ25591-induced cell apoptosis. The siRNA technique demonstrated that endoplasmic reticulum (ER) stress, in particular CHOP/GADD153 up-regulation, contributed to the synergistic effect. CONCLUSIONS The data suggest that WJ25591 inhibited HDAC activity, leading to cell-cycle arrest and inhibition of DNA repair. Caspase cascades are subsequently triggered to execute cell apoptosis. MG-132 dramatically sensitizes WJ25591-mediated apoptosis, at least partly, through ER stress response. The data also reveal that combination of HDAC inhibitors and proteasome inhibitors may be a potential strategy against hormone-refractory prostate cancers.
机译:背景技术组蛋白脱乙酰基酶(HDAC)抑制剂可成功治疗晚期皮肤T细胞淋巴瘤,但在实体瘤中仅显示适度的作用。 HDAC抑制剂改善对实体瘤的活性的方法是必要的。方法磺胺大黄素B测定和流式细胞仪分析分别检测细胞增殖和细胞周期进程。通过蛋白质印迹确定蛋白质表达。 Ku蛋白的彗星试验和DNA末端结合活性分别检测出DNA损伤和DNA修复活性。 siRNA技术被用于敲除特定的细胞靶标。结果WJ25591在人激素难治性前列腺癌PC-3和DU-145中显示出对HDAC1的抑制活性和细胞增殖。 WJ25591导致G1和G2期细胞周期停滞,p21和cyclin E蛋白表达增加,随后细胞凋亡。 WJ25591诱导的Bcl-2下调和激活caspase-9,-8和-3,这表明通过内在和外在凋亡途径进行凋亡执行。 WJ25591还显着抑制DNA修复活性,但不直接诱导DNA损伤。此外,蛋白酶体抑制剂MG-132使WJ25591诱导的细胞凋亡显着敏化。 siRNA技术证明内质网(ER)应激,特别是CHOP / GADD153上调,起到了协同作用。结论数据表明WJ25591抑制HDAC活性,导致细胞周期停滞并抑制DNA修复。随后触发半胱天冬酶级联反应以执行细胞凋亡。 MG-132至少部分通过ER应激反应显着地敏化WJ25591介导的细胞凋亡。数据还显示,HDAC抑制剂和蛋白酶体抑制剂的组合可能是抵抗激素难治性前列腺癌的潜在策略。

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