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基于 MIEC-SVM 模型发现的一种有效的新型雄激素受体拮抗剂。

A potent new-scaffold androgen receptor antagonist discovered on the basis of a MIEC-SVM model.

机构信息

College of Pharmaceutical Sciences, Zhejiang University, Hangzhou, 310058, China.

Institute of Cancer Research and Basic Medical Sciences of Chinese Academy of Sciences, Cancer Hospital of University of Chinese Academy of Sciences, Zhejiang Cancer Hospital, Hangzhou, 310022, China.

出版信息

Acta Pharmacol Sin. 2024 Sep;45(9):1978-1991. doi: 10.1038/s41401-024-01284-x. Epub 2024 May 15.

Abstract

Prostate cancer (PCa) is the second most prevalent malignancy among men worldwide. The aberrant activation of androgen receptor (AR) signaling has been recognized as a crucial oncogenic driver for PCa and AR antagonists are widely used in PCa therapy. To develop novel AR antagonist, a machine-learning MIEC-SVM model was established for the virtual screening and 51 candidates were selected and submitted for bioactivity evaluation. To our surprise, a new-scaffold AR antagonist C2 with comparable bioactivity with Enz was identified at the initial round of screening. C2 showed pronounced inhibition on the transcriptional function (IC = 0.63 μM) and nuclear translocation of AR and significant antiproliferative and antimetastatic activity on PCa cell line of LNCaP. In addition, C2 exhibited a stronger ability to block the cell cycle of LNCaP than Enz at lower dose and superior AR specificity. Our study highlights the success of MIEC-SVM in discovering AR antagonists, and compound C2 presents a promising new scaffold for the development of AR-targeted therapeutics.

摘要

前列腺癌(PCa)是全球男性第二大常见恶性肿瘤。雄激素受体(AR)信号的异常激活已被认为是 PCa 的关键致癌驱动因素,AR 拮抗剂广泛用于 PCa 治疗。为了开发新型 AR 拮抗剂,建立了机器学习 MIEC-SVM 模型进行虚拟筛选,筛选出 51 个候选物并提交进行生物活性评估。令我们惊讶的是,在第一轮筛选中发现了一种新型骨架 AR 拮抗剂 C2,其具有与 Enz 相当的生物活性。C2 对 AR 的转录功能(IC=0.63μM)和核转位表现出明显的抑制作用,并对 LNCaP PCa 细胞系表现出显著的抗增殖和抗转移活性。此外,C2 在较低剂量下比 Enz 更能阻断 LNCaP 的细胞周期,并且具有更高的 AR 特异性。我们的研究强调了 MIEC-SVM 在发现 AR 拮抗剂方面的成功,化合物 C2 为开发针对 AR 的治疗药物提供了一个有前途的新骨架。

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