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依普黄酮不会改变成年雄性大鼠的骨磷灰石晶体结构。

Ipriflavone does not alter bone apatite crystal structure in adult male rats.

作者信息

Ghezzo C, Civitelli R, Cadel S, Borelli G, Maiorino M, Bufalino L, Bongrani S

机构信息

Dipartimento di Scienze della Terra, Università di Siena, Italy.

出版信息

Calcif Tissue Int. 1996 Dec;59(6):496-9. doi: 10.1007/BF00369217.

Abstract

We have previously found that a short-term treatment with high doses of ipriflavone increased bone density and improved the biomechanical properties of adult male rat bones, without altering their mineral composition. To determine whether this effect can be associated with alterations of bone crystal structure, we have performed X-ray diffraction analysis of bones obtained from rats treated with ipriflavone at doses that were effective in inducing favorable changes on bone density and biomechanics. Eighteen-week-old male Sprague Dawley rats were treated by oral route with either ipriflavone (200 or 400 mg/kg/day), or its vehicle for 12 weeks. The treatment was well tolerated and body weight increased to the same extent in all animals. As a measure of bone crystallinity, we examined the (310) and (002) reflections of the X-ray diffraction patterns, corresponding to the directions perpendicular and parallel to the c-axis of the crystals, respectively. No major differences were observed between ipriflavone-treated and control animals for the broadening parameter beta(1/2) for (310) and (002) peaks, as well as for lattice parameters. Therefore, a 12-week treatment with ipriflavone at high doses does not induce significant modifications of bone "crystallinity." Thus, the positive effect of ipriflavone on bone mineral density appears to be associated with an increased apatite crystal formation rather than an increase of crystal size. These results provide further evidence for the safety and usefulness of ipriflavone in the treatment of osteoporotic syndromes.

摘要

我们之前发现,高剂量的依普黄酮短期治疗可增加成年雄性大鼠的骨密度并改善其骨骼的生物力学性能,而不会改变其矿物质组成。为了确定这种作用是否与骨晶体结构的改变有关,我们对用依普黄酮治疗的大鼠的骨骼进行了X射线衍射分析,所用依普黄酮的剂量能有效诱导骨密度和生物力学的有利变化。18周龄的雄性Sprague Dawley大鼠通过口服途径接受依普黄酮(200或400mg/kg/天)或其赋形剂治疗12周。治疗耐受性良好,所有动物的体重均有同等程度的增加。作为骨结晶度的一项指标,我们检查了X射线衍射图谱中的(310)和(002)反射,它们分别对应于与晶体c轴垂直和平行的方向。在依普黄酮治疗组和对照组动物之间,未观察到(310)和(002)峰的展宽参数β(1/2)以及晶格参数有重大差异。因此,高剂量依普黄酮12周治疗不会引起骨“结晶度”的显著改变。因此,依普黄酮对骨矿物质密度的积极作用似乎与磷灰石晶体形成增加有关,而非晶体尺寸增加。这些结果为依普黄酮在治疗骨质疏松综合征方面的安全性和有效性提供了进一步的证据。

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