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首页> 外文期刊>Experimental Gerontology >Advances in endocrinology of aging research, 2005-2006.
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Advances in endocrinology of aging research, 2005-2006.

机译:衰老内分泌学研究进展,2005-2006年。

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摘要

The purpose of this brief review is to highlight some of the more important advances in endocrinology of aging research over the past year. Four advances were chosen and briefly described. First, exploration of the early steps in the generation of the internal steroidal hormonal signal involved in lifespan extension via the insulin/IGF-like signaling pathway in the nematode by two research groups revealed that the product of cholestanoic acid derivatives metabolized by a cytochrome P-450-like protein activates a protein with homology to the mammalian nuclear receptor superfamily, a process strikingly similar to the steroid hormone signaling pathway documented in mammalian systems. Second is the discovery that sirtuins, proteins that regulate lifespan in model organisms, enhance pancreatic insulin secretion in mice following a glucose challenge, suggesting the potential to regulate mammalian lifespan through regulation of the insulin signaling pathway. Third, the newly discovered hormone klotho, which also plays a role in regulating lifespan, in this case in mice, is reported to not only negatively affect insulin sensitivity but, perhaps more importantly, significantly affects calcium and phosphate metabolism as a required cofactor of Fgf-23 signaling. Finally the gonadotropin FSH is shown to directly affect bone density in mice separate from any direct effect of estrogen, suggesting that reproductive hormones other than estrogen can directly impact menopause-associated pathophysiology in non-reproductive tissues.
机译:这篇简短回顾的目的是强调过去一年来衰老研究的内分泌学方面一些更重要的进展。选择并简要描述了四个方面。首先,两个研究小组探索了通过线虫中胰岛素/ IGF样信号通路延长寿命的内部甾体激素信号生成的早期步骤,发现胆甾烷酸衍生物的产物被细胞色素P-代谢了。 450样蛋白激活与哺乳动物核受体超家族具有同源性的蛋白,这一过程与哺乳动物系统中记录的类固醇激素信号传导途径极为相似。第二个发现是,sirtuins是调节模型生物寿命的蛋白质,在葡萄糖激发后会增强小鼠胰腺的胰岛素分泌,这表明可能通过调节胰岛素信号通路来调节哺乳动物的寿命。第三,据报道,在这种情况下,新发现的荷尔蒙klotho在调节寿命方面也起着作用,在小鼠中不仅对胰岛素敏感性产生负面影响,而且可能更重要的是,它作为Fgf必需的辅因子显着影响钙和磷酸盐的代谢。 -23信令。最终,促性腺激素FSH被证明可直接影响小鼠的骨密度,而不受雌激素的任何直接作用,这表明除雌激素外,生殖激素还可直接影响非生殖组织中与更年期相关的病理生理。

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