首页> 外文OA文献 >Pre-emptive, early, and delayed alendronate treatment in a rat model of knee osteoarthritis: effect on subchondral trabecular bone microarchitecture and cartilage degradation of the tibia, bone/cartilage turnover, and joint discomfort
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Pre-emptive, early, and delayed alendronate treatment in a rat model of knee osteoarthritis: effect on subchondral trabecular bone microarchitecture and cartilage degradation of the tibia, bone/cartilage turnover, and joint discomfort

机译:在膝关节骨性关节炎大鼠模型中预先,早期和延迟阿仑膦酸盐治疗:对软骨下骨小梁微结构和胫骨软骨退化,骨/软骨翻转和关节不适的影响

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摘要

OBJECTIVE Bisphosphonates are considered potential disease modifying osteoarthritis (OA) agents. The present study investigated the efficacy of pre-emptive, early, and delayed alendronate (ALN) treatment initiation on subchondral trabecular bone and cartilage in low-dose monosodium iodoacetate (MIA)-induced knee OA in rats. METHODS Male rats received pre-emptive (n = 12, day 0–end of week 2), early (n = 12, end of week 2–end of week 6), or delayed (n = 12, end of week 6–end of week 10) ALN treatment (30 μg/kg/week). Pre-emptive ALN-treated rats were scanned using in vivo micro-computed tomography (micro-CT) after 2 weeks and then sacrificed, early ALN-treated rats were scanned after 2 and 6 weeks and sacrificed, and the delayed ALN-treated rats were scanned after 2, 6, and 10 weeks of OA induction and sacrificed. After sacrifice, bone histomorphometry and histology of the tibia and biomarker analyses were undertaken. Changes in hind limb weight-bearing were assessed from day −1 until day 14. RESULTS MIA-induced pathological features similar to progressive human OA in the cartilage and subchondral bone. Pre-emptive ALN treatment preserved subchondral trabecular bone microarchitecture, prevented bone loss, decreased bone turnover and joint discomfort. Pre-emptive ALN treatment had moderate effects on cartilage degradation. Early and delayed ALN treatments prevented loss of trabeculae and decreased bone turnover, but had no significant effect on cartilage degradation. CONCLUSION ALN prevented increased bone turnover and preserved the structural integrity of subchondral bone in experimental OA. The time point of treatment initiation is crucial for treating OA. Treating both the subchondral bone and cartilage in OA would be clinically more beneficial.
机译:目的双膦酸盐被认为是潜在的疾病改良骨关节炎(OA)药物。本研究调查了在低剂量碘乙酸单钠(MIA)诱导的大鼠膝OA中先发性,早期和延迟阿仑膦酸盐(ALN)治疗开始对软骨下小梁骨和软骨的疗效。方法雄性大鼠先发制人(n = 12,第0天-第2周结束),提前(n = 12,第2周结束-第6周结束),或延迟接受(n = 12,第6周结束-第6周结束)。第10周末)ALN治疗(30μg/ kg /周)。 2周后使用体内微计算机断层扫描(micro-CT)扫描先发性ALN处理的大鼠,然后处死,2周和6周后扫描早期ALN处理的大鼠并处死,以及延迟的ALN处理的大鼠在OA诱导2、6和10周后扫描并处死。处死后,进行胫骨的骨组织形态测量和组织学以及生物标志物分析。从第-1天到第14天评估后肢负重的变化。结果MIA诱发的病理特征类似于软骨和软骨下骨中进行性人类OA。先发制人的ALN治疗可保留软骨下小梁骨微结构,防止骨质流失,骨转换减少和关节不适。先发制人的ALN治疗对软骨退化有中等程度的影响。早期和延迟的ALN治疗可防止小梁丢失和减少骨转换,但对软骨降解没有明显影响。结论ALN在实验性OA中防止了骨转换增加,并保留了软骨下骨的结构完整性。治疗开始的时间点对于治疗OA至关重要。在OA中治疗软骨下骨和软骨将在临床上更加有益。

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