Identification of Oral Bioavailable Coumarin Derivatives as Potential AR Antagonists Targeting Prostate Cancer.

IF 6.8 1区医学 Q1 CHEMISTRY, MEDICINAL Journal of Medicinal Chemistry Pub Date : 2024-11-04 DOI:10.1021/acs.jmedchem.4c01752

Jinbiao Liao, Jianing Liao, Minkui Zhang, Yanzhen Yu, Lvtao Cai, Kaixin Le, Weitao Fu, Yiyang Qin, Tingjun Hou, Dan Li, Rong Sheng

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Abstract

Androgen receptor (AR) is a crucial driver of prostate cancer (PCa), but acquired resistance to AR antagonists significantly undermines their clinical efficacy. We previously discovered coumarin derivative 1, which is capable of disrupting AR ligand-binding domain dimers, offering the potential for overcoming resistance. However, its poor oral bioavailability limited further development. In this study, comprehensive structure optimizations led to compound 4a (IC₅₀ = 0.051 μM), which exhibited comparable AR antagonistic activity to enzalutamide (IC₅₀ = 0.060 μM) and demonstrated excellent selectivity over other nuclear receptors in vitro. Especially, 4a showed superior efficacy against AR^F876L/T877A and AR^W741C mutants compared to darolutamide and enzalutamide. Moreover, 4a exhibited favorable pharmacokinetic profiles (F = 66.24%) in vivo and significant tumor growth inhibition in an LNCaP xenograft mouse model upon oral administration. These results highlight the potential of 4a as a promising oral AR antagonist for overcoming drug resistance in PCa.

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鉴定可口服生物利用的香豆素衍生物作为针对前列腺癌的潜在 AR 拮抗剂。

雄激素受体（AR）是前列腺癌（PCa）的重要驱动因素，但AR拮抗剂的获得性抗药性大大削弱了其临床疗效。我们之前发现了香豆素衍生物 1，它能够破坏 AR 配体结合域二聚体，为克服耐药性提供了可能。然而，其口服生物利用度较低，限制了进一步的开发。在这项研究中，通过全面的结构优化，化合物 4a （IC50 = 0.051 μM）表现出与恩扎鲁胺（IC50 = 0.060 μM）相当的 AR 拮抗活性，并在体外对其他核受体表现出优异的选择性。特别是，与达罗鲁胺和恩扎鲁胺相比，4a 对 ARF876L/T877A 和 ARW741C 突变体具有更高的疗效。此外，4a 在体内表现出良好的药代动力学特征（F = 66.24%），口服后可显著抑制 LNCaP 异种移植小鼠模型的肿瘤生长。这些结果凸显了4a作为一种有前途的口服AR拮抗剂克服PCa耐药性的潜力。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Medicinal Chemistry 医学-医药化学

CiteScore

4.00

自引率

11.00%

发文量

804

审稿时长

1.9 months

期刊介绍： The Journal of Medicinal Chemistry is a prestigious biweekly peer-reviewed publication that focuses on the multifaceted field of medicinal chemistry. Since its inception in 1959 as the Journal of Medicinal and Pharmaceutical Chemistry, it has evolved to become a cornerstone in the dissemination of research findings related to the design, synthesis, and development of therapeutic agents. The Journal of Medicinal Chemistry is recognized for its significant impact in the scientific community, as evidenced by its 2022 impact factor of 7.3. This metric reflects the journal's influence and the importance of its content in shaping the future of drug discovery and development. The journal serves as a vital resource for chemists, pharmacologists, and other researchers interested in the molecular mechanisms of drug action and the optimization of therapeutic compounds.