骨关节炎的发病机制涉及骨、软骨和滑膜炎症:雌激素可能是灵丹妙药吗?

Menopause international Pub Date : 2012-12-01 Epub Date: 2012-09-28 DOI:10.1258/mi.2012.012025
M A Karsdal, A C Bay-Jensen, K Henriksen, C Christiansen
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引用次数: 47

摘要

女性多关节骨关节炎(OA)的优势,特别是绝经后女性OA的显著增加,表明女性性激素可能参与软骨稳态的维持。这一观点启发了许多研究小组研究雌激素在软骨稳态调节中的作用,最终目的是阐明雌激素替代疗法(ERT)是否可以预防绝经后妇女OA患病率的迅速上升。在不同的实验模型中研究了ERT和选择性雌激素受体调节剂对关节的影响。在临床上,雌激素的作用已经通过使用软骨和骨降解生化标志物的临床试验中的事后分析来评估。最后,妇女健康倡议试验(WHI)调查了雌激素对关节和关节置换的影响。尽管确切的作用方式仍有待阐明,但其影响涉及整个关节病理生理的直接和间接机制。一些动物模型已经证明了雌激素的结构性益处,以及对关节炎症的显著影响。这与使用关节降解生化标志物的临床数据完全一致,该数据显示约50%的软骨破坏被抑制。这些发现最近在WHI得到了证实,在WHI中,服用雌激素的妇女关节置换术明显减少。综上所述,雌激素对多种不同组织的多效性作用可能在某些重要方面与OA的复杂病因相匹配。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The pathogenesis of osteoarthritis involves bone, cartilage and synovial inflammation: may estrogen be a magic bullet?

The female predominance of polyarticular osteoarthritis (OA), and in particular the marked increase of OA in women after the menopause points to a likely involvement of female sex hormones in the maintenance of cartilage homeostasis. This perception has inspired many research groups to investigate the role of estrogens in the modulation of cartilage homeostasis with the ultimate aim to clarify whether estrogen replacement therapy (ERT) could provide benefits in preventing the rapid rise in the prevalence of OA in postmenopausal women. The effects of ERT and selective estrogen-receptor modulators on the joint in various experimental models have been investigated. Clinically, the effects of estrogens have been evaluated by post hoc analysis in clinical trials using biochemical markers of cartilage and bone degradation. Lastly, the Women's Health Initiative trial (WHI) investigated the effects of estrogens on the joint and joint replacements. Even though the exact mode of action still needs to be elucidated, the effect involves both direct and indirect mechanisms on the whole joint pathophysiology. Several animal models have demonstrated structural benefits of estrogens, as well as significant effects on joint inflammation. This is in complete alignment with clinical data using biochemical markers of joint degradation which demonstrated approximately 50% inhibition of cartilage destruction. These finding were recently validated in WHI, where women taking estrogens had significantly less joint replacement. In conclusion, the pleiotropic effect of estrogens on several different tissues may match the complicated aetiology of OA in some important aspects.

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