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类风湿关节炎的生物疗法与骨质流失。

Biologic therapies and bone loss in rheumatoid arthritis.

机构信息

Centro Paulista de Investigação Clínica, Rua Moreira e Costa, 342-Ipiranga, São Paulo, SP, 04266-010, Brazil.

Hospital Infantil Federico Gómez-Faculty of Medicine UNAM, Ciudad de México D.F, Mexico.

出版信息

Osteoporos Int. 2017 Feb;28(2):429-446. doi: 10.1007/s00198-016-3769-2. Epub 2016 Oct 31.

Abstract

INTRODUCTION

Rheumatoid arthritis (RA) is a common systemic autoimmune disease of unknown cause, characterized by a chronic, symmetric, and progressive inflammatory polyarthritis. One of the most deleterious effects induced by the chronic inflammation of RA is bone loss. During the last 15 years, the better knowledge of the cytokine network involved in RA allowed the development of potent inhibitors of the inflammatory process classified as biological DMARDs. These new drugs are very effective in the inhibition of inflammation, but there are only few studies regarding their role in bone protection. The principal aim of this review was to show the evidence of the principal biologic therapies and bone loss in RA, focusing on their effects on bone mineral density, bone turnover markers, and fragility fractures.

METHODS

Using the PICOST methodology, two coauthors (PC, LM-S) conducted the search using the following MESH terms: rheumatoid arthritis, osteoporosis, clinical trials, TNF- antagonists, infliximab, adalimumab, etanercept, certolizumab, golimumab, IL-6 antagonists, IL-1 antagonists, abatacept, tocilizumab, rituximab, bone mineral density, bone markers, and fractures. The search was conducted electronically and manually from the following databases: Medline and Science Direct. The search period included articles from 2003 to 2015. The selection included only original adult human research written in English. Titles were retrieved and the same two authors independently selected the relevant studies for a full text. The retrieved selected studies were also reviewed completing the search for relevant articles. The first search included 904 titles from which 253 titles were selected. The agreement on the selection among researchers resulted in a Kappa statistic of 0.95 (p < 0.000). Only 248 abstracts evaluated were included in the acronym PICOST. The final selection included only 28 studies, derived from the systematic search. Additionally, a manual search in the bibliography of the selected articles was made and included into the text and into the section of "small molecules of new agents."

CONCLUSION

Treatment with biologic drugs is associated with the decrease in bone loss. Studies with anti-TNF blocking agents show preservation or increase in spine and hip BMD and also a better profile of bone markers. Most of these studies were performed with infliximab. Only three epidemiological studies analyzed the effect on fractures after anti-TNF blocking agent's treatment. IL-6 blocking agents also showed improvement in localized bone loss not seen with anti-TNF agents. There are a few studies with rituximab and abatacept. Although several studies reported favorable actions of biologic therapies on bone protection, there are still unmet needs for studies regarding their actions on the risk of bone fractures.

摘要

简介

类风湿关节炎(RA)是一种病因不明的常见全身性自身免疫性疾病,其特征为慢性、对称和进行性炎症性多关节炎。RA 慢性炎症引起的最具危害性的影响之一是骨质流失。在过去的 15 年中,人们对参与 RA 的细胞因子网络有了更好的了解,这使得能够开发出分类为生物 DMARDs 的强效炎症过程抑制剂。这些新药在抑制炎症方面非常有效,但关于其在骨保护中的作用的研究却很少。本综述的主要目的是展示主要的生物治疗方法和 RA 中的骨质流失的证据,重点关注它们对骨矿物质密度、骨转换标志物和脆性骨折的影响。

方法

使用 PICOST 方法,两名合著者(PC、LM-S)使用以下 MESH 术语进行了搜索:类风湿关节炎、骨质疏松症、临床试验、TNF-拮抗剂、英夫利昔单抗、阿达木单抗、依那西普、塞妥珠单抗、戈利木单抗、IL-6 拮抗剂、IL-1 拮抗剂、阿巴西普、托珠单抗、利妥昔单抗、骨矿物质密度、骨标志物和骨折。搜索通过电子方式和手动方式在以下数据库中进行:Medline 和 Science Direct。搜索期包括 2003 年至 2015 年的文章。选择仅包括以英文撰写的原始成人人类研究。检索标题,然后由相同的两名作者独立选择全文进行相关研究。还对检索到的选定研究进行了回顾,以完成相关文章的搜索。第一次搜索包括 904 个标题,其中有 253 个标题被选中。研究人员之间在选择上的一致性导致 Kappa 统计量为 0.95(p<0.000)。仅评估了 248 个摘要,这些摘要包含在缩写 PICOST 中。从系统搜索中得出的最终选择仅包括 28 项研究。此外,还对选定文章的参考文献进行了手动搜索,并将其纳入文本和“新型小分子药物”部分。

结论

生物药物治疗与骨质流失减少相关。抗 TNF 阻断剂的研究显示脊柱和臀部 BMD 保持或增加,并且骨标志物的情况也更好。这些研究大多数都是用英夫利昔单抗进行的。只有三项流行病学研究分析了抗 TNF 阻断剂治疗后骨折的影响。IL-6 阻断剂也显示出局部骨质流失的改善,而不是抗 TNF 药物的改善。有几项关于利妥昔单抗和阿巴西普的研究。尽管有几项研究报告了生物治疗对骨保护的有利作用,但关于它们对骨折风险的作用仍存在未满足的研究需求。

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