In silico studies on the molecular interactions of steroid hormones and steroid hormone mimicking drugs in the androgen receptor binding cleft – Implications for prostate cancer treatment

IF 2.1 4区 医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY
Bridget A. Shimmin, Lydell G. Haines, Ian C. Shaw
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引用次数: 0

Abstract

Occupancy of prostate cancer (PCa) cell androgen receptors (AR) signals proliferation, therefore testosterone biosynthesis inhibitors and AR antagonists are important PCa treatments. Conversely, androgen mimics (e.g., prednisone) used in management of PCa might cause proliferation. The balance between PCa proliferation and inhibition predicts treatment success. We used in silico molecular modelling to explore interactions between ARs, androgens (testosterone, dihydrotestosterone (DHT)) and drugs used to treat (bicalutamide) and manage (dexamethasone, prednisone, hydrocortisone) PCa. We found that hydrogen (H-) bonds between testosterone, DHT and Arg752, Asn705 and Thr877 followed by ligand binding cleft hydrophobic interactions signal proliferation, whereas bicalutamide antagonism is via Phe764 interactions. Hydrocortisone, dexamethasone and prednisone H-bond Asn705 and Thr877, but not Arg752 in the absence of a water molecule. Studies with a bicalutamide agonist AR mutation showed different amino acid interactions, indicating testosterone and DHT would not promote proliferation as effectively as via the native receptor. However, hydrocortisone and bicalutamide form Arg752 and Asn705 H-bonds indicating agonism. Our results suggest that as PCa progresses the resulting mutations will change the proliferative response to androgens and their drug mimics, which have implications for the treatment of prostate cancer.

类固醇激素和类固醇激素模拟药物在雄激素受体结合缝隙中的分子相互作用的硅学研究--对前列腺癌治疗的启示
前列腺癌(PCa)细胞雄激素受体(AR)的占据是增殖的信号,因此睾酮生物合成抑制剂和 AR 拮抗剂是治疗 PCa 的重要药物。相反,用于治疗 PCa 的雄激素模拟物(如泼尼松)可能会导致增殖。PCa增殖与抑制之间的平衡预示着治疗的成功与否。我们使用硅学分子建模来探索ARs、雄激素(睾酮、双氢睾酮(DHT))和用于治疗(比卡鲁胺)和控制(地塞米松、泼尼松、氢化可的松)PCa的药物之间的相互作用。我们发现,睾酮、DHT 与 Arg752、Asn705 和 Thr877 之间的氢键(H-)以及配体结合裂隙疏水相互作用发出增殖信号,而比卡鲁胺则通过 Phe764 相互作用产生拮抗作用。氢化可的松、地塞米松和泼尼松能与 Asn705 和 Thr877 产生氢键作用,但在没有水分子的情况下不能与 Arg752 产生氢键作用。用比卡鲁胺激动剂 AR 突变体进行的研究显示了不同的氨基酸相互作用,表明睾酮和 DHT 不会像通过原生受体那样有效地促进增殖。然而,氢化可的松和比卡鲁胺形成 Arg752 和 Asn705 H 键,表明它们具有激动作用。我们的研究结果表明,随着前列腺癌的发展,所产生的突变将改变对雄激素及其药物模拟物的增殖反应,这对前列腺癌的治疗具有重要意义。
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来源期刊
Steroids
Steroids 医学-内分泌学与代谢
CiteScore
5.10
自引率
3.70%
发文量
120
审稿时长
73 days
期刊介绍: STEROIDS is an international research journal devoted to studies on all chemical and biological aspects of steroidal moieties. The journal focuses on both experimental and theoretical studies on the biology, chemistry, biosynthesis, metabolism, molecular biology, physiology and pharmacology of steroids and other molecules that target or regulate steroid receptors. Manuscripts presenting clinical research related to steroids, steroid drug development, comparative endocrinology of steroid hormones, investigations on the mechanism of steroid action and steroid chemistry are all appropriate for submission for peer review. STEROIDS publishes both original research and timely reviews. For details concerning the preparation of manuscripts see Instructions to Authors, which is published in each issue of the journal.
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