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骨质疏松症的现有及潜在未来药物治疗方法。

Current and potential future drug treatments for osteoporosis.

作者信息

Patel S

机构信息

Department of Rheumatology, St George's Hospital, London, United Kingdom.

出版信息

Ann Rheum Dis. 1996 Oct;55(10):700-14. doi: 10.1136/ard.55.10.700.

Abstract

There has been a major interest in the drug treatment of osteoporosis and an increase in the number of drugs available in most countries. The ideal drug (one which increases or restores bone density and trabecular connectivity) is still not available. However, in patients with relatively preserved trabecular connectivity and moderately reduced bone density, several agents have shown substantial clinical benefit. Oestrogens are still the mainstay of drug treatment, but the risks of breast cancer versus the cardiovascular and skeletal benefits with long term use have to be assessed in the individual. Newer tissue specific oestrogens show some promise in this respect. The bisphosphonates and possibly fluoride are likely to be the major alternatives to oestrogens in the medium term. The newer bisphosphonates, alendronate and in the future risedronate, are likely to supersede etidronate. Calcitriol probably has a limited role, confined to those patients in whom HRT or bisphosphonates are not appropriate. Calcium supplementation, or an increase in dietary intake if deficient, irrespective of which agent is used, is also of benefit. In older patients there is considerable support for using a combination of calcium and vitamin D. Whether combination treatment, for example oestrogens, bisphosphonates, and calcium together, will result in greater efficacy remains to be conclusively shown, but may be an attractive option in younger patients with higher bone turnover. Apart from fluoride, bone formation stimulators are unlikely to have a major role until the next century, although it may be possible to use growth factors as part of an ADFR regimen (A = activate remodelling, D = depress resorption, F = free formation, and R = repeat). This is still an important theoretical approach and needs further work with newer agents to see if increased efficacy can be found. In addition sequential treatment may be necessary in view of the limited time periods over which particular agents, such as intermittent fluoride (four years), have been examined, and this will have to be individually tailored. Other approaches include trying to increase peak bone mineral density, although influencing the young to prevent a disease that may not manifest itself for half a century is daunting.

摘要

骨质疏松症的药物治疗已引起广泛关注,多数国家可选用的药物数量也有所增加。理想的药物(即能增加或恢复骨密度及骨小梁连接性的药物)目前仍未出现。然而,对于骨小梁连接性相对保留且骨密度中度降低的患者,几种药物已显示出显著的临床益处。雌激素仍是药物治疗的主要手段,但长期使用时,必须对个体评估乳腺癌风险与心血管及骨骼方面益处的平衡。新型组织特异性雌激素在这方面展现出一些前景。双膦酸盐以及可能的氟化物在中期可能成为雌激素的主要替代药物。新型双膦酸盐阿仑膦酸钠以及未来的利塞膦酸钠可能会取代依替膦酸二钠。骨化三醇的作用可能有限,仅适用于不适合使用激素替代疗法(HRT)或双膦酸盐的患者。无论使用何种药物,补充钙剂或在钙剂缺乏时增加饮食摄入量也有益处。在老年患者中,大量证据支持联合使用钙剂和维生素D。例如雌激素、双膦酸盐和钙剂联合使用是否会产生更大疗效仍有待确切证实,但对于骨转换率较高的年轻患者可能是一个有吸引力的选择。除氟化物外,在下个世纪之前骨形成刺激剂不太可能发挥主要作用,不过或许可以将生长因子作为ADFR方案(A = 激活重塑,D = 抑制吸收,F = 自由形成,R = 重复)的一部分使用。这仍是一种重要的理论方法,需要进一步研究新型药物以确定是否能提高疗效。此外,鉴于特定药物(如间歇性使用氟化物,为期四年)的研究时间有限,可能需要采用序贯治疗,且这必须根据个体情况量身定制。其他方法包括试图提高峰值骨矿物质密度,尽管要影响年轻人预防一种可能在半个世纪后才会显现的疾病颇具挑战性。

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