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Molecular taxonomy of osteoarthritis for patient stratification, disease management and drug development: biochemical markers associated with emerging clinical phenotypes and molecular endotypes

机译:患者分层,疾病管理和药物开发的骨关节炎的分子分类:与新出现的临床表型和分子内型相关的生化标志

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Purpose of review This review focuses on the molecular taxonomy of osteoarthritis from the perspective of molecular biomarkers. We discuss how wet biochemical markers may be used to understand disease pathogenesis and progression and define molecular endotypes of osteoarthritis and how these correspond to clinical phenotypes. Recent findings Emerging evidence suggests that osteoarthritis is a heterogeneous and multifaceted disease with multiple causes, molecular endotypes and corresponding clinical phenotypes. Biomarkers may be employed as tools for patient stratification in clinical trials, enhanced disease management in the primary care centres of the future and for directing more rational and targeted osteoarthritis drug development. Proximal molecular biomarkers (e.g synovial fluid) are more likely to distinguish between molecular endotypes because there is less interference from systemic sources of biomarker noise, including comorbidities. Summary In this review, we have focused on the molecular biomarkers of four distinct osteoarthritis subtypes including inflammatory, subchondral bone remodelling, metabolic syndrome and senescent age-related endotypes, which have corresponding phenotypes. Progress in the field of osteoarthritis endotype and phenotype research requires a better understanding of molecular biomarkers that may be used in conjunction with imaging, pain and functional assessments for the design of more effective, stratified and individualized osteoarthritis treatments.
机译:审查目的本综述着重于分子生物标志物的角度来看骨关节炎的分子分类。我们讨论湿生化标志物如何用于了解疾病发病机制和进展,并定义骨关节炎的分子内型以及这些与临床表型的分子内型。最近的发现出现的证据表明,骨关节炎是一种异质和多方面的疾病,具有多种原因,分子内型和相应的临床表型。生物标志物可作为临床试验中患者分层的工具,增强未来初级保健中心的疾病管理,并指导更合理和有针对性的骨关节炎药物发育。近端分子生物标志物(例如滑膜液)更可能区分分子内型,因为从包括合并症的生物标志物噪声的系统源的干扰较小。发明概述在本次综述中,我们专注于四种不同骨关节炎亚型的分子生物标志物,包括炎症,骨髓性骨重塑,代谢综合征和衰老年龄相关的内型,具有相应的表型。骨关节炎子型和表型研究领域的进展需要更好地理解可与成像,疼痛和功能评估一起使用的分子生物标志物,以设计更有效,分层和个体化的骨关节炎治疗。

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