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骨关节炎的特征以及开发个性化疾病修饰药物疗法的潜力。

The hallmarks of osteoarthritis and the potential to develop personalised disease-modifying pharmacological therapeutics.

作者信息

Tonge D P, Pearson M J, Jones S W

机构信息

Faculty of Computing, Engineering and Sciences, Staffordshire University, Stoke-on-Trent ST4 2DF, UK.

MRC-ARUK Centre for Musculoskeletal Ageing Research, School of Immunity and Infection, University of Birmingham, Birmingham B15 2WB, UK.

出版信息

Osteoarthritis Cartilage. 2014 May;22(5):609-21. doi: 10.1016/j.joca.2014.03.004. Epub 2014 Mar 12.

DOI:10.1016/j.joca.2014.03.004
PMID:24632293
Abstract

Osteoarthritis (OA) is an age-related condition and the leading cause of pain, disability and shortening of adult working life in the UK. The incidence of OA increases with age, with 25% of the over 50s population having OA of the knee. Despite promising preclinical data covering various molecule classes, there is regrettably at present no approved disease-modifying OA drugs (DMOADs). With the advent of next generation sequencing technologies, other therapeutic areas, in particular oncology, have experienced a paradigm shift towards defining disease by its molecular composition. This paradigm shift has enabled high resolution patient stratification and supported the emergence of personalised or precision medicines. In this review we evaluate the potential for the development of OA therapeutics to undergo a similar paradigm shift given that OA is increasingly being recognised as a heterogeneous disease affecting multiple joint tissues. We highlight the evidence for the role of these tissues in OA pathology as different "hallmarks" of OA biology and review the opportunities to identify and develop targeted disease-modifying pharmacological therapeutics. Finally, we consider whether it is feasible to expect the emergence of personalised disease-modifying medicines for patients with OA and how this might be achieved.

摘要

骨关节炎(OA)是一种与年龄相关的病症,也是英国疼痛、残疾以及成年人工作寿命缩短的主要原因。OA的发病率随年龄增长而增加,50岁以上人群中有25%患有膝关节OA。尽管涵盖各种分子类别的临床前数据很有前景,但遗憾的是,目前尚无获批的改善病情的骨关节炎药物(DMOADs)。随着新一代测序技术的出现,其他治疗领域,尤其是肿瘤学,经历了从根据疾病分子组成来定义疾病的范式转变。这种范式转变实现了高分辨率的患者分层,并支持了个性化或精准药物的出现。在本综述中,鉴于OA越来越被认为是一种影响多个关节组织的异质性疾病,我们评估了OA治疗学发生类似范式转变的可能性。我们强调了这些组织在OA病理学中作为OA生物学不同“特征”所起作用的证据,并综述了识别和开发靶向改善病情的药物治疗方法的机会。最后,我们考虑期望为OA患者出现个性化改善病情药物是否可行以及如何实现这一点。

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