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The Effects of a Single Developmentally Entrained Pulse of Testosterone in Female Neonatal Mice on Reproductive and Metabolic Functions in Adult Life

机译:女性新生小鼠中睾丸激素的单一发育夹带脉冲对成年后生殖和代谢功能的影响

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摘要

Early postnatal exposures to sex steroids have been well recognized to modulate predisposition to diseases of adulthood. There is a complex interplay between timing, duration and dose of endocrine exposures through environmental or dietary sources that may alter the sensitivity of target tissues to the exogenous stimuli. In this study, we determined the metabolic and reproductive programming effects of a single developmentally entrained pulse of testosterone (T) given to female mice in early postnatal period. CD-1 female mice pups were injected with either 5 μg of T enanthate (TE) or vehicle (control [CON] group) within 24 hours after birth and followed to adult age. A total of 66% of T-treated mice exhibited irregular cycling, anovulatory phenotype, and significantly higher ovarian weights than vehicle-treated mice. Longitudinal nuclear magnetic resonance measurements revealed that TE group had greater body weight, whole-body lean, and fat mass than the CON group. Adipose tissue cellularity analysis in TE group revealed a trend toward higher size and number than their littermate CONs. The brown adipose tissue of TE mice exhibited white fat infiltration with down-regulation of several markers, including uncoupling protein 1 (UCP-1), cell death-inducing DNA fragmentation factor, α-subunit-like effector A, bone morphogenetic protein 7 as well as brown adipose tissue differentiation-related transcription regulators. T-injected mice were also more insulin resistant than CON mice. These reproductive and metabolic reprogramming effects were not observed in animals exposed to TE at 3 and 6 weeks of age. Collectively, these data suggest that sustained reproductive and metabolic alterations may result in female mice from a transient exposure to T during a narrow postnatal developmental window.
机译:产后早期暴露于性类固醇已被公认为可调节成年疾病的易感性。通过环境或饮食来源的内分泌暴露的时间,持续时间和剂量之间存在复杂的相互作用,这可能会改变目标组织对外源性刺激的敏感性。在这项研究中,我们确定了在产后早期给予雌性小鼠睾丸激素(T)单个发育夹带脉冲的代谢和生殖编程作用。在出生后24小时内,向成年CD-1雌性幼崽幼犬注射5μgT庚酸酯(TE)或赋形剂(对照组[CON]组)。总共66%的T治疗小鼠表现出不规则的循环,无排卵表型,并且卵巢重量明显高于载体治疗的小鼠。纵向核磁共振测量结果显示,TE组比CON组具有更大的体重,全身瘦身和脂肪质量。 TE组的脂肪组织细胞密度分析显示,其大小和数量均高于其同窝仔CON。 TE小鼠的棕色脂肪组织表现出白色脂肪浸润,同时下调了一些标志物,包括解偶联蛋白1(UCP-1),诱导细胞死亡的DNA片段化因子,α-亚基样效应子A,骨形态发生蛋白7等。以及棕色脂肪组织分化相关的转录调节因子。注射T的小鼠也比CON小鼠更具胰岛素抵抗性。在3周和6周龄暴露于TE的动物中未观察到这些生殖和代谢重编程作用。总的来说,这些数据表明持续的生殖和代谢改变可能导致雌性小鼠在狭窄的出生后发育窗口期间短暂暴露于T。

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