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Enantiomer discrimination illustrated by high-resolution crystal structures of the human nuclear receptor hRARγ

机译:人类核受体hRARγ的高分辨率晶体结构说明了对映体识别

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The human retinoic acid receptor (hRAR) is a member of the nuclear receptor superfamily that regulates the transcription of target genes in a ligand-dependent manner. The three hRAR isotypes are targets for retinoids that are used in the treatment of various diseases, including breast cancer and skin diseases. Drug efficiency and safety depend on the pharmacological activity of enantiomers. which can differ because of the chiral environment generated by the target. We report the crystal structures of the hRARγ, ligand- binding domain bound to two enantiomers, the active BMS270394 and the inactive BMS270395, solved at 1.6 A and 1.7 A resolution. respectively. The crystal structures reveal that in both enantiomers, the hydroxyl moiety attached to the chiral center forms a hydrogen bond to the Met-272 sulfur atom. thus imposing a conformation of BMS270395 that differs significantly from that observed for BMS270394 and other known retinoids. BMS270395 adopts an energetically unfavorable conformation, accounting for its inac- tivity; in contrast, the conformation of BMS270394 is close to an energy minimum. Our high-resolution data allow rationalization of enantiomer discrimination by the receptor and provide a model system for the pharmacological properties of enantiomeric pairs.
机译:人视黄酸受体(hRAR)是核受体超家族的成员,该家族以配体依赖性方式调节靶基因的转录。三种hRAR亚型是类维生素A的靶标,可用于治疗多种疾病,包括乳腺癌和皮肤病。药物效率和安全性取决于对映异构体的药理活性。由于目标产生的手性环境,这可能会有所不同。我们报告了hRARγ的晶体结构,配体结合域绑定到两个对映异构体,活性BMS270394和非活性BMS270395,在1.6 A和1.7 A的分辨率下解析。分别。晶体结构表明,在两种对映异构体中,连接于手性中心的羟基部分均与Met-272硫原子形成氢键。因此强加了BMS270395的构象,该构象与BMS270394和其他已知类维生素A的构象明显不同。 BMS270395采用了一种在能量上不利的构象,这说明了它的不活动性。相反,BMS270394的构型接近最低能量。我们的高分辨率数据可通过受体合理化对映体识别,并为对映体对的药理特性提供模型系统。

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