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Somatostatin Is Essential for the Sexual Dimorphism of GH Secretion Corticosteroid-Binding Globulin Production and Corticosterone Levels in Mice

机译:生长抑素对于小鼠的GH分泌雌性激素结合球蛋白和皮质酮水平的性二态化至关重要。

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摘要

Distinct male and female patterns of pituitary GH secretion produce sexually differentiated hepatic gene expression profiles, thereby influencing steroid and xenobiotic metabolism. We used a fully automated system to obtain serial nocturnal blood samples every 15 minutes from cannulated wild-type (WT) and somatostatin knockout (Sst-KO) mice to determine the role of SST, the principal inhibitor of GH release, in the generation of sexually dimorphic GH pulsatility. WT males had lower mean and median GH values, less random GH secretory bursts, and longer trough periods between GH pulses than WT females. Each of these parameters was feminized in male Sst-KO mice, whereas female Sst-KO mice had higher GH levels than all other groups, but GH pulsatility was unaffected. We next performed hepatic mRNA profiling with high-density microarrays. Male Sst-KO mice exhibited a globally feminized pattern of GH-dependent mRNA levels, but female Sst-KO mice were largely unaffected. Among the differentially expressed female-predominant genes was Serpina6, which encodes corticosteroid-binding globulin (CBG). Increased CBG was associated with elevated diurnal peak plasma corticosterone in unstressed WT females and both sexes of Sst-KO mice compared with WT males. Sst-KO mice also had exaggerated ACTH and corticosterone responses to acute restraint stress. However, consistent with their lack of phenotypic signs of excess glucocorticoids, cerebrospinal fluid concentrations of free corticosterone in Sst-KO mice were not elevated. In summary, SST is necessary for the prolonged interpulse troughs that define masculinized pituitary GH secretion. SST also contributes to sexual dimorphism of the hypothalamic-pituitary-adrenal axis via GH-dependent regulation of hepatic CBG production.
机译:垂体GH分泌的不同的男性和女性模式产生了性别差异的肝基因表达谱,从而影响了类固醇和异种生物的代谢。我们使用全自动系统每15分钟从插管的野生型(WT)和生长抑素基因敲除(Sst-KO)小鼠中获取连续的夜间血样,以确定GH释放的主要抑制剂SST在产生性二形性GH搏动。 WT雄性比WT雌性具有更低的平均GH和中值GH值,更少的随机GH分泌爆发以及更长的GH脉冲谷谷期。这些参数中的每个参数在雄性Sst-KO小鼠中都是女性化的,而雌性Sst-KO小鼠的GH水平高于所有其他组,但GH搏动性不受影响。接下来,我们用高密度微阵列进行肝脏mRNA谱分析。雄性Sst-KO小鼠表现出全球女性化的GH依赖mRNA水平的女性化模式,但雌性Sst-KO小鼠在很大程度上未受影响。在差异表达的女性主导基因中,有Serpina6,它编码皮质类固醇结合球蛋白(CBG)。与野生雄性小鼠相比,未受压力的野生雌性小鼠和雌雄同体的CBG升高与昼夜峰值血浆皮质酮水平升高有关。 Sst-KO小鼠对急性约束应激也具有夸大的ACTH和皮质酮反应。然而,与其缺乏过量糖皮质激素的表型征兆相一致,Sst-KO小鼠的脑脊髓液中游离皮质酮的浓度并未升高。总而言之,SST对于定义男性化垂体GH分泌的延长脉冲间谷是必要的。 SST还通过GH依赖的肝脏CBG产生调节作用,导致下丘脑-垂体-肾上腺轴性二态性。

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