Baxter John D, Goede Patrick, Apriletti James W, West Brian L, Feng Weijun, Mellstrom Karin, Fletterick Robert J, Wagner Richard L, Kushner Peter J, Ribeiro Ralff C J, Webb Paul, Scanlan Thomas S, Nilsson Stefan
Metabolic Research Unit, University of California, San Francisco, California 94143, USA.
Endocrinology. 2002 Feb;143(2):517-24. doi: 10.1210/endo.143.2.8617.
Antagonists have been developed for several nuclear receptors but not for others, including TRs. TR antagonists may have significant clinical utility for treating hormone excess states and other conditions. A structure derived "extension hypothesis" was applied to synthesize a TR antagonist. The principal design feature was to attach an extension group to a TR agonist whose structure would perturb formation of the TR coactivator-binding surface. The compound, 3,5-dibromo-4-(3',5'-diisopropyl-4'-hydroxyphenoxy)benzoic acid, has no (TRalpha) or very weak partial (TRbeta) TR agonist activity and blocks TR binding of T3, formation of the coactivator-binding surface, and both a positive T3 response on a thyroid hormone response element and a negative T3 response on the TSHbeta promoter in cultured cells. The results suggest that 3,5-dibromo-4-(3',5'-diisopropyl-4'-hydroxyphenoxy)benzoic acid is a TR antagonist for thyroid hormone response element-mediated responses, this approach can be used more generally to generate nuclear receptor antagonists, and this compound or analogues may have medical and research utility.
已经开发出了针对几种核受体的拮抗剂,但针对包括甲状腺激素受体(TRs)在内的其他受体的拮抗剂尚未开发出来。TR拮抗剂在治疗激素过多状态和其他病症方面可能具有重要的临床应用价值。一种基于结构衍生的“延伸假说”被应用于合成TR拮抗剂。主要设计特点是将一个延伸基团连接到一个TR激动剂上,其结构会干扰TR共激活因子结合表面的形成。化合物3,5-二溴-4-(3',5'-二异丙基-4'-羟基苯氧基)苯甲酸没有(TRα)或仅有非常弱的部分(TRβ)TR激动剂活性,并且在培养细胞中能阻断T3的TR结合、共激活因子结合表面的形成,以及甲状腺激素反应元件上的T3阳性反应和促甲状腺激素β亚基(TSHβ)启动子上的T3阴性反应。结果表明,3,5-二溴-4-(3',5'-二异丙基-4'-羟基苯氧基)苯甲酸是一种针对甲状腺激素反应元件介导反应的TR拮抗剂,这种方法可更广泛地用于生成核受体拮抗剂,并且该化合物或其类似物可能具有医学和研究用途。
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