ATPase Copper Transporting Beta (ATP7B) Is a Novel Target for Improving the Therapeutic Efficacy of Docetaxel by Disulfiram/Copper in Human Prostate Cancer.

IF 5.3 2区 医学 Q1 ONCOLOGY Molecular Cancer Therapeutics Pub Date : 2024-06-04 DOI:10.1158/1535-7163.MCT-23-0876
Liankun Song, Vyvyan Nguyen, Jun Xie, Shang Jia, Christopher J Chang, Edward Uchio, Xiaolin Zi
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Abstract

Docetaxel has been the standard first-line chemotherapy for lethal metastatic prostate cancer (mPCa) since 2004, but resistance to docetaxel treatment is common. The molecular mechanisms of docetaxel resistance remain largely unknown and could be amenable to interventions that mitigate resistance. We have recently discovered that several docetaxel-resistant mPCa cell lines exhibit lower uptake of cellular copper and uniquely express higher levels of a copper exporter protein ATP7B. Knockdown of ATP7B by silencing RNAs (siRNA) sensitized docetaxel-resistant mPCa cells to the growth-inhibitory and apoptotic effects of docetaxel. Importantly, deletions of ATP7B in human mPCa tissues predict significantly better survival of patients after their first chemotherapy than those with wild-type ATP7B (P = 0.0006). In addition, disulfiram (DSF), an FDA-approved drug for the treatment of alcohol dependence, in combination with copper, significantly enhanced the in vivo antitumor effects of docetaxel in a docetaxel-resistant xenograft tumor model. Our analyses also revealed that DSF and copper engaged with ATP7B to decrease protein levels of COMM domain-containing protein 1 (COMMD1), S-phase kinase-associated protein 2 (Skp2), and clusterin and markedly increase protein expression of cyclin-dependent kinase inhibitor 1 (p21/WAF1). Taken together, our results indicate a copper-dependent nutrient vulnerability through ATP7B exporter in docetaxel-resistant prostate cancer for improving the therapeutic efficacy of docetaxel.

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ATP酶铜转运β(ATP7B)是通过双硫仑/铜改善多西他赛对人类前列腺癌疗效的新靶点。
自2004年以来,多西他赛一直是治疗致死性转移性前列腺癌(mPCa)的标准一线化疗药物,但多西他赛治疗耐药的情况却很普遍。多西他赛耐药的分子机制在很大程度上仍不为人所知,但可以通过干预来减轻耐药性。我们最近发现,几种多西他赛耐药的 mPCa 细胞系对细胞铜的吸收率较低,并且独特地表达较高水平的铜输出蛋白 ATP7B。通过沉默 RNA(siRNA)敲除 ATP7B 可使耐多西他赛的 mPCa 细胞对多西他赛的生长抑制和凋亡效应敏感。重要的是,人mPCa组织中ATP7B的缺失预示着患者首次化疗后的生存率明显高于ATP7B野生型患者(P = 0.0006)。此外,美国 FDA 批准用于治疗酒精依赖的药物双硫仑(DSF)与铜联合使用,可在多西他赛耐药异种移植肿瘤模型中显著增强多西他赛的体内抗肿瘤效果。我们的分析还显示,DSF 和铜与 ATP7B 相互作用,降低了 COMM domain-containing protein 1 (COMMD1)、S 期激酶相关蛋白 2 (Skp2) 和 clusterin 的蛋白水平,并明显增加了细胞周期蛋白依赖性激酶抑制剂 1 (p21/WAF1) 的蛋白表达。综上所述,我们的研究结果表明,在多西他赛耐药的PCa中,铜通过ATP7B输出端依赖于营养易损性,从而提高了多西他赛的疗效。
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来源期刊
CiteScore
11.20
自引率
1.80%
发文量
331
审稿时长
3 months
期刊介绍: Molecular Cancer Therapeutics will focus on basic research that has implications for cancer therapeutics in the following areas: Experimental Cancer Therapeutics, Identification of Molecular Targets, Targets for Chemoprevention, New Models, Cancer Chemistry and Drug Discovery, Molecular and Cellular Pharmacology, Molecular Classification of Tumors, and Bioinformatics and Computational Molecular Biology. The journal provides a publication forum for these emerging disciplines that is focused specifically on cancer research. Papers are stringently reviewed and only those that report results of novel, timely, and significant research and meet high standards of scientific merit will be accepted for publication.
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