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首页> 外文期刊>Annals of the New York Academy of Sciences >Restoration of Bone Mass in Hpg Mouse by Preoptic Area Grafting
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Restoration of Bone Mass in Hpg Mouse by Preoptic Area Grafting

机译:通过视前区移植修复Hpg小鼠的骨量

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摘要

Hereditary hypogonadism in the hpg mouse, caused by a deletion mutation in the gonadotropin-releasing hormone (GnRH) gene, is associated with sterility, absent ovarian development, and undetectable circulating sex steroids. Eight-month-old female hpg mice had a significantly reduced bone mineral density (BMD) at the lumbar spine, femur, and tibia. In addition, the mice showed significant reductions in liver and kidney weight, with virtually nonexistent ovaries. Successfully transplanted hpg mice with preoptic area grafts contained GnRH-positive neurons, consistent with our previous experience, and the host median eminence was innervated by GnRH immunoreactive fibers. A return of reproductive function was evident from increased ovarian weight and vaginal cornification. Of note was that grafted hpg mice showed a complete reversal to baseline of their BMD measured at all three sites. This establishes that the low bone mass that occurs in old hpg mice can be fully and rapidly ameliorated by preoptic area grafting.
机译:由促性腺激素释放激素(GnRH)基因的缺失突变引起的hpg小鼠遗传性性腺功能减退与不育,卵巢发育异常和循环性类固醇检测不到有关。八个月大的雌性hpg小鼠的腰椎,股骨和胫骨的骨矿物质密度(BMD)明显降低。此外,小鼠的肝脏和肾脏重量显着减少,卵巢几乎不存在。用视前区移植物成功移植的hpg小鼠含有GnRH阳性神经元,这与我们以前的经验一致,并且宿主中位突出是由GnRH免疫反应性纤维支配的。卵巢重量增加和阴道角质形成可明显恢复生殖功能。值得注意的是,移植的hpg小鼠在三个部位均显示出BMD基线完全逆转。这表明,通过视前区移植可以完全并迅速改善老年hpg小鼠中出现的低骨量。

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