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Neonatal exposure to estradiol-17β modulates tumour necrosis factor alpha and cyclooxygenase-2 expression in brain and also in ovaries of adult female rats

机译:新生儿暴露于雌二醇-17β可调节成年雌性大鼠脑内和卵巢中肿瘤坏死因子α和环氧合酶-2的表达

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摘要

The sexually dimorphic organization in perinatal rat brain is influenced by steroid hormones. Exposure to high levels of estrogen or endocrine-disrupting compounds during perinatal period may perturb this process, resulting in compromised reproductive physiology and behavior as observed in adult In our recent observation neonatal exposure of the female rats to estradiol-17β resulted in down-regulation of TNF-α, up-regulation of COX-2 and increase in SDN-POA size in pre-optic area in the adulthood. It is known that the control of reproductive performance in female involves a complex interplay of the hypothalamus, pituitary, and ovary. The present study was undertaken to understand the possible molecular mechanism involved in changes observed in the ovarian morphology and expression of selected genes in the ovary. Administration of estradiol-17β (100 μg) on day 2 and 3 after birth revealed up-regulation of ER-α, ER-β, COX-2 and down-regulation of TNF-α expression. Also the decrease in the ovarian weight, altered ovarian morphology and changes in the 2D protein profiles were also seen. This is apparently the first report documenting that neonatal estradiol exposure modulates TNF-α and COX-2 expression in the ovary as seen during adult stage. Our results permit us to suggest that cues originating from the modified brain structure due to neonatal exposure of estradiol-17β remodel the ovary at the molecular level in such a way that there is a disharmony in the reproductive function during adulthood and these changes are perennial and can lead to infertility and changes of reproductive behavior.
机译:围产期大鼠大脑中的性二形组织受到类固醇激素的影响。在成年期暴露于高水平的雌激素或破坏内分泌的化合物可能会扰乱该过程,从而导致成年后的生殖生理和行为受损。在我们最近的观察中,雌性大鼠的新生雌二醇暴露于雌二醇-17β导致其下调。成年后视前区的TNF-α,COX-2上调和SDN-POA大小增加。众所周知,女性生殖能力的控制涉及下丘脑,垂体和卵巢的复杂相互作用。进行本研究以了解可能涉及卵巢形态学变化和卵巢中所选基因表达的分子机制。出生后第2天和第3天给予雌二醇17β(100μg)显示ER-α,ER-β,COX-2上调和TNF-α表达下调。还可以看到卵巢重量的减少,卵巢形态的改变和二维蛋白质谱的变化。显然,这是第一个报道新生儿雌二醇暴露调节成年期卵巢中TNF-α和COX-2表达的报道。我们的研究结果表明,源自新生儿暴露的雌二醇-17β导致的大脑结构改变的线索在分子水平上对卵巢进行了改造,从而使成年期的生殖功能不协调,并且这些变化是多年生的。会导致不孕和生殖行为改变。

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