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Prediction of the tissue-specificity of selective estrogen receptor modulators by using a single biochemical method

机译:使用单一的生化方法预测选择性雌激素受体调节剂的组织特异性

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摘要

Here, we demonstrate that a single biochemical assay is able to predict the tissue-selective pharmacology of an array of selective estrogen receptor modulators (SERMs). We describe an approach to classify estrogen receptor (ER) modulators based on dynamics of the receptor-ligand complex as probed with hydrogen/deuterium exchange (HDX) mass spectrometry. Differential HDX mapping coupled with cluster and discriminate analysis effectively predicted tissue-selective function in most, but not all, cases tested. We demonstrate that analysis of dynamics of the receptor–ligand complex facilitates binning of ER modulators into distinct groups based on structural dynamics. Importantly, we were able to differentiate small structural changes within ER ligands of the same chemotype. In addition, HDX revealed differentially stabilized regions within the ligand-binding pocket that may contribute to the different pharmacology phenotypes of the compounds independent of helix 12 positioning. In summary, HDX provides a sensitive and rapid approach to classify modulators of the estrogen receptor that correlates with their pharmacological profile.
机译:在这里,我们证明了单个生化分析能够预测一系列选择性雌激素受体调节剂(SERMs)的组织选择性药理作用。我们描述了一种基于受体-配体复合物的动力学对雌激素受体(ER)调节剂进行分类的方法,该动力学是用氢/氘交换(HDX)质谱探测的。差异化HDX映射结合聚类和判别分析可以在大多数(但不是全部)受测病例中有效预测组织选择性功能。我们证明,对受体-配体复合物的动力学分析有助于根据结构动力学将ER调节剂分为不同的组。重要的是,我们能够区分相同化学型的ER配体内的微小结构变化。此外,HDX揭示了配体结合袋内的差异化稳定区域,可能与化合物的螺旋线12定位无关,导致了化合物的不同药理表型。总之,HDX提供了一种灵敏而快速的方法来对雌激素受体的调节剂进行分类,这些调节剂与其药理作用有关。

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