García-Becerra Rocio, Borja-Cacho Elizabeth, Cooney Austin J, Smith Carolyn L, Lemus Ana E, Pérez-Palacios Gregorio, Larrea Fernando
Department of Reproductive Biology, Instituto Nacional de Ciencias Médicas y Nutrición Salvador Zubirán, Vasco de Quiroga No. 15, Mexico City 14000, Mexico.
J Steroid Biochem Mol Biol. 2006 May;99(2-3):108-14. doi: 10.1016/j.jsbmb.2006.01.005. Epub 2006 Apr 17.
The binding of estradiol (E(2)) to estrogen receptors (ER) is followed by conformational changes resulting in coactivator or corepressor recruitment that influences gene transcription. A series of synthetic A-ring reduced 19-nortestosterone-derived progestins has the capacity to selectively bind and activate transcription through the ERalpha. Herein, the molecular mechanisms involved in ER subtype-selective interactions of these compounds as assessed by their effects upon both ERalpha and ERbeta structural conformation and their ability to induce recruitment of steroid receptor coactivator-1 (SRC-1) to ERalpha were investigated. The results demonstrated that all synthetic A-ring 3beta,5alpha-tetrahydro-reduced derivatives of 19-nortestosterone induced an ERalpha trypsin digestion pattern similar to that seen with E(2), without effects upon ERbeta. In addition, these compounds had the ability to recruit SRC-1 to the ligand-binding domain of ERalpha similar to E(2). Our data indicate that A-ring 3beta,5alpha-tetrahydro-reduced 19-nortestosterone-derived progestins behave as selective ERalpha agonists with ligand-receptor structural and functional responses similar to those induced with natural E(2).
雌二醇(E₂)与雌激素受体(ER)结合后会发生构象变化,导致共激活因子或共抑制因子的募集,进而影响基因转录。一系列合成的A环还原19-去甲睾酮衍生的孕激素能够通过ERα选择性结合并激活转录。在此,通过这些化合物对ERα和ERβ结构构象的影响以及它们诱导类固醇受体共激活因子-1(SRC-1)募集到ERα的能力,研究了这些化合物参与ER亚型选择性相互作用的分子机制。结果表明,所有19-去甲睾酮的合成A环3β,5α-四氢还原衍生物诱导的ERα胰蛋白酶消化模式与E₂相似,对ERβ无影响。此外,这些化合物与E₂相似,能够将SRC-1募集到ERα的配体结合结构域。我们的数据表明,A环3β,5α-四氢还原的19-去甲睾酮衍生的孕激素表现为选择性ERα激动剂,其配体-受体结构和功能反应与天然E₂诱导的相似。
