Department of Endocrinology, Institute of Zoology, Jagiellonian University, Gronostajowa 9, 30-387 Krakow, Poland.
Domest Anim Endocrinol. 2013 May;44(4):185-94. doi: 10.1016/j.domaniend.2013.02.001. Epub 2013 Mar 16.
Recent reports have indicated a role of cell-to-cell interactions during gonadal development and functions. Numerous reports indicate that fetal hormonal disruption induces abnormalities in the developing reproductive system and, therefore, may interfere with reproductive functions later in adult life. Hence, this study investigated the effect of androgen deficiency during late prenatal periods on the gap junction-associated connexin 43 (Cx43) and the adherens junction-associated β-catenin expression in the fetal porcine gonads. Thus, pregnant gilts were injected with anti-androgen flutamide (for 7 d, 50 mg/kg BW per day) or corn oil (control groups) starting at 83 (GD90) or 101 (GD108) gestational day. On GD90 and GD108 the fetuses were excised and fetal gonads were obtained. To assess Cx43 and β-catenin expression real-time PCR and immunohistochemistry were performed. In fetal testes, Cx43 was localized between Leydig cells, whereas β-catenin was observed mainly within the seminiferous tubules. In fetal ovaries, Cx43 was detected between interstitial cells and between granulosa cells of forming follicles, whereas β-catenin was found within egg nests, in oocytes' membrane, and in granulosa cells of forming follicles. Immunohistochemistry showed decreased Cx43 and β-catenin expression in fetal gonads from flutamide-treated pigs compared with respective controls. However, the ovaries from animals treated with flutamide on GD108 showed increased Cx43 expression. The changes of Cx43 and β-catenin expression after prenatal flutamide treatment were confirmed at the mRNA level. These findings suggest that androgen deficiency during late gestation may lead to disturbed intercellular interactions in fetal porcine testes affecting testicular functions, as well as impaired follicular formation in fetal ovaries. Our results further signify the role of androgens in the regulation of cell-to-cell interactions within fetal porcine gonads.
最近的报告表明,细胞间相互作用在性腺发育和功能中起作用。大量报告表明,胎儿激素紊乱会导致发育中生殖系统的异常,因此可能会干扰成年后的生殖功能。因此,本研究调查了晚期产前雄激素缺乏对胎儿猪性腺中缝隙连接相关连接蛋白 43(Cx43)和黏着连接相关β-连环蛋白表达的影响。因此,妊娠母猪从第 83 天(GD90)或第 101 天(GD108)开始每天注射 50mg/kgBW 的抗雄激素氟他胺(7d)或玉米油(对照组)。在 GD90 和 GD108 时取出胎儿,获得胎儿性腺。为了评估 Cx43 和β-连环蛋白的表达,进行了实时 PCR 和免疫组织化学分析。在胎儿睾丸中,Cx43 定位于 Leydig 细胞之间,而β-连环蛋白主要存在于生精小管中。在胎儿卵巢中,Cx43 存在于间质细胞之间和正在形成的卵泡的颗粒细胞之间,而β-连环蛋白存在于卵巢中、卵母细胞的膜中和正在形成的卵泡的颗粒细胞中。免疫组织化学显示,与相应对照组相比,氟他胺处理的胎儿性腺中 Cx43 和β-连环蛋白的表达减少。然而,在第 108 天用氟他胺处理的动物的卵巢中,Cx43 的表达增加。产前氟他胺处理后 Cx43 和β-连环蛋白表达的变化在 mRNA 水平上得到了证实。这些发现表明,妊娠晚期雄激素缺乏可能导致胎儿猪睾丸中细胞间相互作用紊乱,影响睾丸功能,以及胎儿卵巢中卵泡形成受损。我们的研究结果进一步表明,雄激素在调节胎儿猪性腺细胞间相互作用中起作用。
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