Structural and Dynamic Elucidation of a Non-acid PPARγ Partial Agonist: SR1988.

Rebecca L Frkic, Benjamin S Chua, Youseung Shin, Bruce D Pascal, Scott J Novick, Theodore M Kamenecka, Patrick R Griffin, John B Bruning
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引用次数: 5

Abstract

Targeting peroxisome proliferator-activated receptor γ (PPARγ) by synthetic compounds has been shown to elicit insulin sensitising properties in type 2 diabetics. Treatment with a class of these compounds, the thiazolidinediones (TZDs), has shown adverse side effects such as weight gain, fluid retention, and congestive heart failure. This is due to their full agonist properties on the receptor, where a number of genes are upregulated beyond normal physiological levels. Lessened transactivation of PPARγ by partial agonists has proved beneficial in terms of reducing side effects, while still maintaining insulin sensitising properties. However, some partial agonists have been associated with unfavourable pharmacokinetic profiles due to their acidic moieties, often causing partitioning to the liver. Here we present SR1988, a new partial agonist with favourable non-acid chemical properties. We used a combination of X-ray crystallography and hydrogen/deuterium exchange (HDX) to elucidate the structural basis for reduced activation of PPARγ by SR1988. This structural analysis reveals a mechanism that decreases stabilisation of the AF2 coactivator binding surface by the ligand.

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非酸性PPARγ部分激动剂SR1988的结构和动力学解析。
合成化合物靶向过氧化物酶体增殖物激活受体γ (PPARγ)已被证明可引起2型糖尿病患者的胰岛素增敏特性。用一类这类化合物,噻唑烷二酮类(TZDs)治疗,已显示出不良副作用,如体重增加、液体潴留和充血性心力衰竭。这是由于它们在受体上的完全激动剂特性,其中许多基因被上调超过正常的生理水平。部分激动剂减少PPARγ的转激活已被证明在减少副作用方面是有益的,同时仍保持胰岛素致敏特性。然而,一些部分激动剂由于其酸性部分而与不利的药代动力学特征相关,通常导致肝脏分区。在这里,我们提出了SR1988,一种新的部分激动剂,具有良好的非酸性化学性质。我们使用x射线晶体学和氢/氘交换(HDX)的组合来阐明SR1988降低PPARγ活化的结构基础。这种结构分析揭示了一种机制,降低了配体对AF2辅激活剂结合表面的稳定性。
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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