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Androgens and estrogens in skeletal sexual dimorphism

机译:骨骼性二态性中的雄激素和雌激素

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摘要

Bone is an endocrine tissue expressing androgen and estrogen receptors as well as steroid metabolizing enzymes. The bioactivity of circulating sex steroids is modulated by sex hormone-binding globulin and local conversion in bone tissue, for example, from testosterone (T) to estradiol (E2) by aromatase, or to dihydrotestosterone by 5α-reductase enzymes. Our understanding of the structural basis for gender differences in bone strength has advanced considerably over recent years due to increasing use of (high resolution) peripheral computed tomography. These microarchitectural insights form the basis to understand sex steroid influences on male peak bone mass and turnover in cortical vs trabecular bone. Recent studies using Cre/LoxP technology have further refined our mechanistic insights from global knockout mice into the direct contributions of sex steroids and their respective nuclear receptors in osteoblasts, osteoclasts, osteocytes, and other cells to male osteoporosis. At the same time, these studies have reinforced the notion that androgen and estrogen deficiency have both direct and pleiotropic effects via interaction with, for example, insulin-like growth factor 1, inflammation, oxidative stress, central nervous system control of bone metabolism, adaptation to mechanical loading, etc., This review will summarize recent advances on these issues in the field of sex steroid actions in male bone homeostasis.
机译:骨是表达雄激素和雌激素受体以及类固醇代谢酶的内分泌组织。循环性类固醇的生物活性受性激素结合球蛋白的调节和在骨组织中的局部转化,例如,由芳香酶从睾丸激素(T)转变为雌二醇(E2),或由5α-还原酶从二氢睾丸激素转变。近年来,由于越来越多地使用(高分辨率)外围计算机断层扫描技术,我们对骨骼强度性别差异的结构基础的理解有了很大的进步。这些微架构的见解构成了了解性类固醇对男性峰值骨量和皮层与小梁骨转换率的影响的基础。最近使用Cre / LoxP技术进行的研究进一步从全球基因敲除小鼠中进一步了解了我们的机理见解,认为成骨细胞,破骨细胞,破骨细胞和其他细胞中性类固醇及其各自的核受体对男性骨质疏松症的直接贡献。同时,这些研究强化了这样一种观念,即雄激素和雌激素缺乏症通过与例如胰岛素样生长因子1,炎症,氧化应激,中枢神经系统对骨骼代谢的控制,适应等相互作用而具有直接作用和多效作用。到机械负荷等方面,本综述将总结在男性骨稳态中性类固醇作用领域中这些问题的最新进展。

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