首页> 美国卫生研究院文献>Molecular Endocrinology >The Modulator of Nongenomic Actions of the Estrogen Receptor (MNAR) Regulates Transcription-Independent Androgen Receptor-Mediated Signaling: Evidence that MNAR Participates in G Protein-Regulated Meiosis in Xenopus laevis Oocytes
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The Modulator of Nongenomic Actions of the Estrogen Receptor (MNAR) Regulates Transcription-Independent Androgen Receptor-Mediated Signaling: Evidence that MNAR Participates in G Protein-Regulated Meiosis in Xenopus laevis Oocytes

机译:雌激素受体(MNAR)的非基因组作用的调节剂调节转录独立的雄激素受体介导的信号:MNAR参与非洲爪蟾卵母细胞G蛋白调节减数分裂的证据。

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摘要

Classical steroid receptors mediate many transcription-independent (nongenomic) steroid responses in vitro, including activation of Src and G proteins. Estrogen-triggered activation of Src can be regulated by the modulator of nongenomic actions of the estrogen receptor (MNAR), which binds to estrogen receptors and Src to create a signaling complex. In contrast, the mechanisms regulating steroid-induced G protein activation are not known, nor are the physiologic responses mediated by MNAR. These studies demonstrate that MNAR regulates the biologically relevant process of meiosis in Xenopus laevis oocytes. MNAR was located throughout oocytes, and reduction of its expression by RNA interference markedly enhanced testosterone-triggered maturation and activation of MAPK. Additionally, Xenopus MNAR augmented androgen receptor (AR)-mediated transcription in CV1 cells through activation of Src. MNAR and AR coimmunoprecipitated as a complex involving the LXXLL-rich segment of MNAR and the ligand binding domain of AR. MNAR and Gβ also precipitated together, with the same region of MNAR being important for this interaction. Finally, reduction of MNAR expression decreased Gβγ-mediated signaling in oocytes. MNAR therefore appears to participate in maintaining meiotic arrest, perhaps by directly enhancing Gβγ-mediated inhibition of meiosis. Androgen binding to AR might then release this inhibition, allowing maturation to occur. Thus, MNAR may augment multiple nongenomic signals, depending upon the context and cell type in which it is expressed.
机译:经典的类固醇受体在体外介导许多转录非依赖性(非基因组)类固醇反应,包括Src和G蛋白的激活。雌激素触发的Src激活可以通过雌激素受体(MNAR)的非基因组作用调节剂来调节,该受体与雌激素受体和Src结合形成信号复合物。相反,调节类固醇诱导的G蛋白活化的机制尚不清楚,MNAR介导的生理反应也不清楚。这些研究表明,MNAR调节非洲爪蟾卵母细胞减数分裂的生物学相关过程。 MNAR位于整个卵母细胞中,RNA干扰降低其表达可显着增强睾丸激素触发的成熟和MAPK的激活。此外,非洲爪蟾MNAR通过激活Src增强CV1细胞中雄激素受体(AR)介导的转录。 MNAR和AR共沉淀为复合物,涉及MNAR的富含LXXLL的片段和AR的配体结合结构域。 MNAR和Gβ也一起沉淀,而MNAR的相同区域对于这种相互作用很重要。最后,MNAR表达的减少降低了卵母细胞中Gβγ介导的信号传导。因此,MNAR似乎通过直接增强Gβγ介导的减数分裂抑制作用参与维持减数分裂停滞。然后,雄激素与AR的结合可能会释放这种抑制作用,从而导致成熟。因此,取决于表达它的背景和细胞类型,MNAR可以增加多个非基因组信号。

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