用于肿瘤学和女性健康的芳基O-氨基磺酸酯药效团的发现与开发。
Discovery and Development of the Aryl O-Sulfamate Pharmacophore for Oncology and Women's Health.
作者信息
Thomas Mark P, Potter Barry V L
机构信息
Wolfson Laboratory of Medicinal Chemistry, Department of Pharmacy and Pharmacology, University of Bath , Claverton Down, Bath BA2 7AY, United Kingdom.
Department of Pharmacology, University of Oxford , Mansfield Road, Oxford OX1 3QT, United Kingdom.
出版信息
J Med Chem. 2015 Oct 8;58(19):7634-58. doi: 10.1021/acs.jmedchem.5b00386. Epub 2015 Jun 12.
Abstract
In 1994, following work from this laboratory, it was reported that estrone-3-O-sulfamate irreversibly inhibits a new potential hormone-dependent cancer target steroid sulfatase (STS). Subsequent drug discovery projects were initiated to develop the core aryl O-sulfamate pharmacophore that, over some 20 years, have led to steroidal and nonsteroidal drugs in numerous preclinical and clinical trials, with promising results in oncology and women's health, including endometriosis. Drugs have been designed to inhibit STS, e.g., Irosustat, as innovative dual-targeting aromatase-steroid sulfatase inhibitors (DASIs) and as multitargeting agents for hormone-independent tumors, such as the steroidal STX140 and nonsteroidal counterparts, acting inter alia through microtubule disruption. The aryl sulfamate pharmacophore is highly versatile, operating via three distinct mechanisms of action, and imbues attractive pharmaceutical properties. This Perspective gives a personal view of the work leading both to the therapeutic concepts and these drugs, their current status, and how they might develop in the future.
摘要
1994年,继本实验室开展的研究工作之后,有报道称雌酮-3-O-硫酸酯胺可不可逆地抑制一种新的潜在激素依赖性癌症靶点——甾体硫酸酯酶(STS)。随后启动了药物研发项目,以开发核心芳基O-硫酸酯胺药效基团。在大约20年的时间里,该项目已研发出多种甾体和非甾体药物,并开展了大量临床前和临床试验,在肿瘤学以及包括子宫内膜异位症在内的女性健康领域取得了令人鼓舞的成果。已设计出多种抑制STS的药物,例如伊罗司他,作为创新的双靶点芳香化酶-甾体硫酸酯酶抑制剂(DASI)以及用于激素非依赖性肿瘤的多靶点药物,如甾体类的STX140及其非甾体类类似物,它们尤其通过破坏微管发挥作用。芳基硫酸酯胺药效基团具有高度的通用性,可通过三种不同的作用机制发挥作用,并具有吸引人的药学性质。本文从个人角度阐述了促成这些治疗理念和药物的研究工作、它们的当前状况以及未来可能的发展方向。
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