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雷洛昔芬类似物(盐酸LY117018)对去卵巢大鼠骨质减少的预防和干预作用

The preventive and interventional effects of raloxifene analog (LY117018 HCL) on osteopenia in ovariectomized rats.

作者信息

Li X, Takahashi M, Kushida K, Inoue T

机构信息

Department of Orthopedic Surgery, Hamamatsu University School of Medicine, Japan.

出版信息

J Bone Miner Res. 1998 Jun;13(6):1005-10. doi: 10.1359/jbmr.1998.13.6.1005.

Abstract

The effects of LY117018 HCL (LY) treatment on bone metabolism, spine bone mineral density (BMD), bone mineral content (BMC), and serum cholesterol were studied in ovariectomized (OVX) rats. Experiment 1 was designed to observe the preventive effects of LY on bone loss due to ovariectomy (OVX; prevention study). The rats were divided into three groups: sham group, OVX + vehicle, and OVX + LY. LY was administrated at the same time of OVX. Experiment 2 was designed to investigate the interventional effects of LY on OVX rats with osteopenia (intervention study). The rats were divided into the sham and OVX groups, first. The OVX rats were allowed to lose bone for 6 weeks. At 6 weeks post-OVX, the OVX rats were divided into two groups: OVX + vehicle and OVX + LY. The longitudinal effects of LY on bone were studied by dual-energy X-ray absorptiometry and biochemical markers including urinary pyridinoline (Pyr), deoxypyridinoline (Dpyr), and serum osteocalcin. Urinary Pyr and Dpyr increased maximally at 6 weeks post-OVX, decreased at 12 and 18 weeks post-OVX, although the OVX rats had significantly higher levels of Pyr and Dpyr than the sham group during the experiment. LY was a very potent inhibitor of Pyr and Dpyr excretion while at the same time only partially reducing the bone loss in the high turnover phase at 6 weeks postovariectomy. However, at the later time points at 12 and 18 weeks, no further bone loss occurred in rats treated with LY, while the vehicle-treated group lost another 10% in spine BMD and BMC. LY also completely blocked further bone loss when used in an intervention protocol. LY significantly reduced serum cholesterol levels in OVX rats. The results suggest that LY is not fully protective during the early rapid bone loss phase, but the compound is fully protective during the later slow phase of bone loss in both the protocols.

摘要

在去卵巢(OVX)大鼠中研究了盐酸LY117018(LY)治疗对骨代谢、脊柱骨密度(BMD)、骨矿物质含量(BMC)和血清胆固醇的影响。实验1旨在观察LY对去卵巢所致骨丢失的预防作用(预防研究)。大鼠被分为三组:假手术组、OVX + 赋形剂组和OVX + LY组。LY在去卵巢的同时给药。实验2旨在研究LY对患有骨质减少的OVX大鼠的干预作用(干预研究)。大鼠首先被分为假手术组和OVX组。OVX大鼠被允许骨质流失6周。在去卵巢后6周,OVX大鼠被分为两组:OVX + 赋形剂组和OVX + LY组。通过双能X线吸收法和生化标志物(包括尿吡啶啉(Pyr)、脱氧吡啶啉(Dpyr)和血清骨钙素)研究LY对骨的纵向影响。尿Pyr和Dpyr在去卵巢后6周时达到最高值,在去卵巢后12周和18周时下降,尽管在实验期间OVX大鼠的Pyr和Dpyr水平显著高于假手术组。LY是Pyr和Dpyr排泄的非常有效的抑制剂,同时在去卵巢后6周的高转换期仅部分减少骨丢失。然而,在12周和18周的后期时间点,用LY治疗的大鼠没有进一步的骨丢失,而赋形剂治疗组的脊柱BMD和BMC又损失了10%。当在干预方案中使用时,LY也完全阻止了进一步的骨丢失。LY显著降低了OVX大鼠的血清胆固醇水平。结果表明,在两种方案中,LY在早期快速骨丢失阶段不是完全保护性的,但在后期缓慢骨丢失阶段是完全保护性的。

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