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四环素/氟比洛芬联合疗法对去卵巢大鼠骨重塑的调节作用:初步观察

Tetracycline/flurbiprofen combination therapy modulates bone remodeling in ovariectomized rats: preliminary observations.

作者信息

Aoyagi M, Sasaki T, Ramamurthy N S, Golub L M

机构信息

Department of Prosthodontics, School of Dentistry, Showa University, Shinagawa-ku, Tokyo, Japan.

出版信息

Bone. 1996 Dec;19(6):629-35. doi: 10.1016/s8756-3282(96)00280-3.

Abstract

The loss of trabecular bone in the ovariectomized (OVX) rat provides a useful experimental model of postmenopausal osteoporosis. In this study, two bone-modulating compounds, an NSAID (flurbiprofen: FBP) and a chemically modified nonantimicrobial tetracycline (CMT), were tested either individually or in combination in this model. Ninety days after OVX, 6-month-old female rats were distributed into the following groups: sham-operated controls, untreated OVX, CMT-treated OVX (5 mg P.O./day), FBP-treated OVX (0.3 mg P.O./day), and combination (CMT plus FBP)-treated OVX (COMBO) groups. Untreated 3-month-old rats were used as pretreatment group. After 21 days of therapy, the dissected distal femurs were processed for light and fluorescence microscopic and backscattered electron microscopic examinations. Net trabecular bone values showed that all the treatment groups lost trabecular bone over the 111 day protocol compared to pretreatment group. In the untreated OVX rats, trabecular bone volume/unit area was reduced by 56% compared to that in the sham-operated controls, this bone loss associated with increased numbers of osteoclasts (p < 0.05). Cortical bone volume was, however, not significantly reduced in OVX rats. Both FBP-alone and COMBO therapy showed marginal, but significant, (p < 0.05, p < 0.01, respectively) inhibition of trabecular bone loss, and osteoclast numbers were also decreased (p < 0.05). Both CMT alone and COMBO therapy appeared to increase bone deposition (p < 0.01) at the endosteal surfaces of cortical bone. These results suggest that, in this animal model, (a) cortical bone volume increases by CMT; (b) FBP inhibits osteoclastic bone resorption in the trabecular area, and (c) a combination of these drugs may synergistically prevent bone loss.

摘要

去卵巢(OVX)大鼠小梁骨的丢失为绝经后骨质疏松症提供了一个有用的实验模型。在本研究中,两种骨调节化合物,一种非甾体抗炎药(氟比洛芬:FBP)和一种化学修饰的非抗菌四环素(CMT),在该模型中单独或联合进行了测试。OVX术后90天,将6月龄雌性大鼠分为以下几组:假手术对照组、未治疗的OVX组、CMT治疗的OVX组(5mg口服/天)、FBP治疗的OVX组(0.3mg口服/天)和联合(CMT加FBP)治疗的OVX组(COMBO组)。未治疗的3月龄大鼠用作预处理组。治疗21天后,对解剖后的股骨远端进行光镜、荧光显微镜和背散射电子显微镜检查。净小梁骨值显示,与预处理组相比,所有治疗组在111天的实验方案中均出现小梁骨丢失。在未治疗的OVX大鼠中,小梁骨体积/单位面积比假手术对照组减少了56%,这种骨丢失与破骨细胞数量增加有关(p<0.05)。然而,OVX大鼠的皮质骨体积没有显著减少。单独使用FBP和COMBO疗法均显示对小梁骨丢失有轻微但显著的抑制作用(分别为p<0.05,p<0.01),破骨细胞数量也减少了(p<0.05)。单独使用CMT和COMBO疗法似乎都增加了皮质骨内表面的骨沉积(p<0.01)。这些结果表明,在这个动物模型中,(a)CMT可增加皮质骨体积;(b)FBP抑制小梁区域的破骨细胞骨吸收;(c)这些药物的组合可能协同预防骨丢失。

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