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人类胎盘芳香化酶的高级组织结构。

Higher order organization of human placental aromatase.

机构信息

Department of Pharmacology, State University of New York Upstate Medical University, Syracuse, NY 13210, USA.

出版信息

Steroids. 2011 Jul;76(8):753-8. doi: 10.1016/j.steroids.2011.02.030. Epub 2011 Mar 8.

Abstract

Aromatase (CYP19A1) is an integral membrane enzyme that catalyzes the removal of the 19-methyl group and aromatization of the A-ring of androgens. All human estrogens are synthesized from their androgenic precursors by this unique cytochrome P450. The crystal structure of active aromatase purified from human placenta has recently been determined in complex with its natural substrate androstenedione in the high-spin ferric state of heme. Hydrogen bond forming interactions and tight packing hydrophobic side chains closely complement puckering of the steroid backbone, thereby providing the molecular basis for the androgenic specificity of aromatase. In the crystal, aromatase molecules are linked by a head-to-tail intermolecular interaction via a surface loop between helix D and helix E of one aromatase molecule that penetrates the heme-proximal cavity of the neighboring, crystallographically related molecule, thus forming in tandem a polymeric aromatase chain. This intermolecular interaction is similar to the aromatase-cytochrome P450 reductase coupling and is driven by electrostatics between the negative potential surface of the D-E loop region and the positively charged heme-proximal cavity. This loop-to-proximal site link in aromatase is rather unique--there are only a few of examples of somewhat similar intermolecular interactions in the entire P450 structure database. Furthermore, the amino acids involved in the intermolecular contact appear to be specific for aromatase. Higher order organization of aromatase monomers may have implications in lipid integration and catalysis.

摘要

芳香酶(CYP19A1)是一种完整的膜酶,可催化雄激素 A 环的 19-甲基去除和芳构化。所有人类雌激素都是通过这种独特的细胞色素 P450 从其雄激素前体合成的。最近,已从人胎盘纯化的活性芳香酶与天然底物雄烯二酮在血红素的高自旋铁状态下的复合物中确定了其晶体结构。形成氢键的相互作用和紧密堆积的疏水性侧链与甾体骨架的卷曲紧密互补,从而为芳香酶的雄激素特异性提供了分子基础。在晶体中,芳香酶分子通过一个分子间的头尾相互作用连接,该相互作用通过一个分子的 D 螺旋和 E 螺旋之间的表面环穿透相邻的、晶体学相关分子的血红素近端腔,从而形成串联的聚合芳香酶链。这种分子间相互作用类似于芳香酶-细胞色素 P450 还原酶偶联,由 D-E 环区域的负电势表面和带正电荷的血红素近端腔之间的静电相互作用驱动。芳香酶中的这种环到近端位点连接相当独特——在整个 P450 结构数据库中只有少数几个类似的分子间相互作用的例子。此外,参与分子间接触的氨基酸似乎对芳香酶具有特异性。芳香酶单体的高级组织可能对脂质整合和催化有影响。

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