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Exogenous Exposure to Estradiol Benzoate or Flutamide at the Weaning Age Alters Expression of Connexin Isoforms in the Initial Segment of Male Rat

机译:断奶年龄外源性暴露于雌二醇苯甲酸酯或氟他胺改变了雄性大鼠初始节段中连接蛋白亚型的表达

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摘要

Connexin (Cx) is a complex which allows direct communication between neighboring cells via exchange of signaling molecules and eventually leads to functional harmony of cells in a tissue. The initial segment (IS) is an excurrent duct of male reproductive tract and expression of numerous genes in the IS are controlled by andevrepogens and estrogens. The effects of these steroid hormones on gene expression in the IS during postnatal development have not extensively examined. The present research investigated expressional modulation of Cx isoforms in the IS by exogenous exposure to estrogen agonist, estradiol benzoate (EB), or andevrepogen antagonist, flutamide (Flu), at weaning age. Two different doses of EB or Flu were subcutaneously administrated in 21-day old of male rats, and expressional changes of Cx isoforms in the adult IS were analyzed by quantitative real-time PCR. Treatment of a low-dose EB (0.015 μg/kg body weight) resulted in an increased expression of Cx31 gene and a decreased expression of Cx37 gene. A high-dose EB (1.5 μg/kg body weight) treatment caused an increase of Cx31 gene expression. Increased levels of Cx30.3 and Cx40 transcripts were observed with a low-dose Flu (500 μg/kg body weight) treatment. Treatment of high-dose Flu (50 mg/kg body weight) led to expressional increases of Cx30.3, 40, and 43 genes. Our previous and present findings suggest differential responsiveness on gene expression of Cx isoforms in the IS by andevrepogens and estrogens at different postnatal ages.
机译:连接蛋白(Cx)是一种复合物,可通过交换信号分子使相邻细胞之间直接通信,并最终导致组织中细胞的功能和谐。初始区段(IS)是雄性生殖道的流出管,IS中许多基因的表达受雄激素和雌激素控制。这些类固醇激素对产后发育过程中IS中基因表达的影响尚未得到广泛研究。本研究通过在断奶年龄外源性暴露于雌激素激动剂苯甲酸雌二醇(EB)或雄激素排斥剂氟他胺(Flu)来研究IS中Cx亚型的表达调节。在21日龄的雄性大鼠中皮下注射两种不同剂量的EB或Flu,并通过实时定量PCR分析成年IS中Cx亚型的表达变化。低剂量EB(0.015μg/ kg体重)的治疗导致Cx31基因表达增加和Cx37基因表达减少。大剂量EB(1.5μg/ kg体重)处理导致Cx31基因表达增加。在低剂量流感(500μg/ kg体重)处理下,观察到Cx30.3和Cx40转录物水平增加。大剂量流感(50 mg / kg体重)的治疗导致Cx30.3、40和43基因的表达增加。我们以前和现在的发现表明,在不同的产后年龄,雄激素和雌激素对IS中Cx亚型基因表达的反应不同。

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