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首页> 外文期刊>Journal of bone and mineral research: the official journal of the American Society for Bone and Mineral Research >SRC-1 Is Necessary for Skeletal Responses to Sex Hormones in Both Males and Females.
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SRC-1 Is Necessary for Skeletal Responses to Sex Hormones in Both Males and Females.

机译:SRC-1是男性和女性对性激素的骨骼反应所必需的。

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We created SRC-1(-/-) mice by mating floxed SRC-1 mice with CMV-Cre transgenic mice. The SRC-1(-/-) mice showed high turnover osteopenia under physiological conditions and hardly responded to osteoanabolic actions of exogenous androgen and estrogen in males and females, respectively, after gonadectomies, indicating that SRC-1 is essential for the maintenance of bone mass by sex hormones. INTRODUCTION: Steroid receptor coactivator-1 (SRC-1) is the first identified coactivator of nuclear receptors. This study investigated the role of SRC-1 in skeletal tissues of males and females using the deficient (SRC-1(-/-)) mice. MATERIALS AND METHODS: SRC-1(-/-) mice were generated by mating our original floxed SRC-1 mice with CMV-Cre transgenic mice. Bone metabolism between 24-week-old SRC-1(-/-) and wildtype (WT) littermates under physiological conditions was compared in males and females by radiological, histological, and biochemical analyses. Difference of skeletal responses to steroid hormones was examined by gonadectomies and exogenous administration experiments with the hormones. Statistical analysis was performed by ANOVA determined by posthoc testing using Bonferroni's method. RESULTS AND CONCLUSIONS: Although SRC-1(-/-) mice showed no abnormality in growth or major organs, both males and females showed osteopenia with high bone turnover in the trabecular bones, but not in the cortical bones, compared with WT littermates. Their serum levels of sex hormones were upregulated, suggesting a compensatory reaction for the insensitivity to these hormones. Gonadectomies caused decreases in BMDs of SRC-1(-/-) and WT mice to the same levels; however, replacement with 5alpha-dihydrotestosterone and 17beta-estradiol in males and females, respectively, failed to restore the bone loss in SRC-1(-/-), whereas the WT bone volume was increased to the sham-operated levels. In contrast, bone loss by administered prednisolone was similarly seen in SRC-1(-/-) and WT mice. We conclude that SRC-1 is essential for the maintenance of bone mass by sex hormones, but not for the catabolic action of glucocorticoid, under both physiological and pathological conditions.
机译:我们通过将疏散的SRC-1小鼠与CMV-Cre转基因小鼠交配来创建SRC-1(-/-)小鼠。 SRC-1(-/-)小鼠在生理条件下表现出高周转性骨质减少,并且在雌雄同体切开术后分别对雄性和雌性外源雄激素和雌激素的骨代谢作用几乎没有反应,这表明SRC-1对维持骨骼至关重要性激素的质量。简介:类固醇受体共激活因子1(SRC-1)是第一个被确定的核受体共激活因子。这项研究调查了SRC-1在有缺陷的(SRC-1(-/-))小鼠的男性和女性骨骼组织中的作用。材料与方法:SRC-1(-/-)小鼠是通过将我们原始的SRC-1杂种SRC-1小鼠与CMV-Cre转基因小鼠交配而产生的。通过放射学,组织学和生化分析比较了男性和女性在生理条件下24周龄SRC-1(-/-)和野生型(WT)同窝仔之间的骨代谢。通过性腺切除术和激素的外源性给药实验检查了对类固醇激素的骨骼反应的差异。使用Bonferroni方法通过事后检验通过ANOVA进行统计分析。结果与结论:尽管SRC-1(-/-)小鼠的生长或主要器官均未见异常,但与WT同窝仔相比,雄性和雌性均显示小梁骨中骨质疏松症的骨转换率高,而皮质骨中没有。他们的性激素血清水平上调,表明对这些激素不敏感的代偿反应。阴道切开术导致SRC-1(-/-)和WT小鼠的BMD降低至相同水平;然而,在男性和女性中分别用5α-二氢睾丸激素和17β-雌二醇替代未能恢复SRC-1(-/-)的骨丢失,而WT骨量增加到了假手术水平。相反,在SRC-1(-/-)和WT小鼠中类似地观察到泼尼松龙的骨损失。我们得出结论,在生理和病理条件下,SRC-1对于通过性激素维持骨量至关重要,但对于糖皮质激素的分解代谢作用则不是必需的。

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