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化学修饰四环素CMT-8对骨质疏松状态下骨质流失及破骨细胞结构与功能的影响。

Effects of chemically modified tetracycline, CMT-8, on bone loss and osteoclast structure and function in osteoporotic states.

作者信息

Sasaki T, Ohyori N, Debari K, Ramamurthy N S, Golub L M

机构信息

Department of Anatomy and Cell Biology, Showa University Dental School, Tokyo, Japan.

出版信息

Ann N Y Acad Sci. 1999 Jun 30;878:347-60. doi: 10.1111/j.1749-6632.1999.tb07694.x.

Abstract

We examined the effects of a nonantimicrobial tetracycline analogue, CMT-8, on bone loss and osteoclasts in ovariectomized (OVX) rats. Three-month-old female rats were OVX, and, one week later, distributed into three groups: sham-operated non-OVX controls, untreated OVX controls, and CMT-8-treated OVX rats. After 145 days of daily drug administration (p.o.), the femurs were dissected and examined histologically. Ovariectomy markedly decreased trabecular and cortical bone volume in the metaphyses compared to sham-operated controls. Treating the OVX rats with CMT-8 produced a significant inhibition of trabecular and cortical bone loss and induced new bone formation, in which connectivity of the trabecular struts was increased by bridging the adjacent longitudinal bone trabeculae. Ultrastructurally, CMT-8 reduced ruffled border formation in osteoclasts, while it caused no structural impairment in osteoblasts. To further evaluate the effects of CMT-8 on the resorbing activity of osteoclasts, osteoclasts were cultured on dentine slices pretreated with CMT-8 at concentrations of 2, 10, or 50 micrograms/ml, and resorption lacuna formation on the dentine surface was found to be reduced, dose-dependently, by the bound CMT-8. Our results suggest that CMT-8 therapy effectively inhibits post-ovariectomy bone loss not only by inducing new bone formation, but also by inhibiting osteoclastic bone resorption, and that CMT-8 binding to bone may provide a prolonged release delivery of this anti-resorptive therapy.

摘要

我们研究了一种非抗菌四环素类似物CMT - 8对去卵巢(OVX)大鼠骨质流失和破骨细胞的影响。将3个月大的雌性大鼠进行去卵巢手术,一周后,分为三组:假手术未去卵巢对照组、未治疗的去卵巢对照组和CMT - 8治疗的去卵巢大鼠组。每日经口给药145天后,解剖股骨并进行组织学检查。与假手术对照组相比,去卵巢显著降低了干骺端的小梁骨和皮质骨体积。用CMT - 8治疗去卵巢大鼠可显著抑制小梁骨和皮质骨流失,并诱导新骨形成,其中通过桥接相邻的纵向骨小梁增加了小梁支柱的连通性。在超微结构上,CMT - 8减少了破骨细胞中皱褶缘的形成,而对成骨细胞没有造成结构损伤。为了进一步评估CMT - 8对破骨细胞吸收活性的影响,将破骨细胞培养在经2、10或50微克/毫升浓度的CMT - 8预处理的牙本质切片上,发现牙本质表面的吸收陷窝形成被结合的CMT - 8剂量依赖性地减少。我们的结果表明,CMT - 8治疗不仅通过诱导新骨形成,还通过抑制破骨细胞骨吸收有效抑制去卵巢后的骨质流失,并且CMT - 8与骨的结合可能为这种抗吸收治疗提供缓释给药。

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