首页> 美国卫生研究院文献>BioMed Research International >Androgen Signaling Disruption during Fetal and Postnatal Development Affects Androgen Receptor and Connexin 43 Expression and Distribution in Adult Boar Prostate
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Androgen Signaling Disruption during Fetal and Postnatal Development Affects Androgen Receptor and Connexin 43 Expression and Distribution in Adult Boar Prostate

机译:胎儿和产后发育过程中的雄激素信号破坏影响成年公猪前列腺中的雄激素受体和连接蛋白43的表达和分布

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摘要

To date, limited knowledge exists regarding the role of the androgen signaling during specific periods of development in the regulation of androgen receptor (AR) and connexin 43 (Cx43) in adult prostate. Therefore, in this study we examined mRNA and protein expression, and tissue distribution of AR and Cx43 in adult boar prostates following fetal (GD20), neonatal (PD2), and prepubertal (PD90) exposure to an antiandrogen flutamide (50 mg/kg bw). In GD20 and PD2 males we found the reduction of the luminal compartment, inflammatory changes, decreased AR and increased Cx43 expression, and altered localization of both proteins. Moreover, enhanced apoptosis and reduced proliferation were detected in the prostates of these animals. In PD90 males the alterations were less evident, except that Cx43 expression was markedly upregulated. The results presented herein indicate that in boar androgen action during early fetal and neonatal periods plays a key role in the maintenance of normal phenotype and functions of prostatic cells at adulthood. Furthermore, we demonstrated that modulation of Cx43 expression in the prostate could serve as a sensitive marker of hormonal disruption during different developmental stages.
机译:迄今为止,关于雄激素信号在特定发育时期在成年前列腺中雄激素受体(AR)和连接蛋白43(Cx43)的调节中的作用的知识有限。因此,在这项研究中,我们检查了胎儿(GD20),新生儿(PD2)和青春期前(PD90)暴露于抗雄激素氟他胺(50μmg/ kg bw)后成年公猪前列腺的mRNA和蛋白表达以及AR和Cx43的组织分布)。在GD20和PD2雄性动物中,我们发现管腔区室减少,炎症改变,AR降低和Cx43表达增加以及两种蛋白质的定位发生改变。此外,在这些动物的前列腺中检测到凋亡增加和增殖减少。在PD90男性中,这种变化不太明显,除了Cx43表达明显上调。本文呈现的结果表明,在胎儿和新生儿早期的雄激素作用中,成年期在维持正常表型和前列腺细胞功能中起着关键作用。此外,我们证明了前列腺中Cx43表达的调节可作为不同发育阶段荷尔蒙破坏的敏感标志。

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