Systematic review of biochemical biomarkers for neck and upper-extremity musculoskeletal disorders

混淆 医学 生物标志物 荟萃分析 内科学 斯科普斯 物理疗法 梅德林 肿瘤科 生物 生物化学
作者
Judith E. Gold,David Hallman,Fredrik Hellström,Martin Björklund,Albert G. Crenshaw,Mats Djupsjöbacka,Marina Heiden,Svend Erik Mathiassen,George Piligian,Mary F. Barbe
出处
期刊:Scandinavian Journal of Work, Environment & Health [Scaninavian Journal of Work, Environment, and Health]
卷期号:42 (2): 103-124 被引量:20
标识
DOI:10.5271/sjweh.3533
摘要

This study systematically summarizes biochemical biomarker research in non-traumatic musculoskeletal disorders (MSD). Two research questions guided the review: (i) Are there biochemical markers associated with neck and upper-extremity MSD? and (ii) Are there biochemical markers associated with the severity of neck and upper-extremity MSD?A literature search was conducted in PubMed and SCOPUS, and 87 studies met primary inclusion criteria. Following a quality screen, data were extracted from 44 articles of sufficient quality.Most of the 87 studies were cross-sectional and utilized convenience samples of patients as both cases and controls. A response rate was explicitly stated in only 11 (13%) studies. Less than half of the studies controlled for potential confounding through restriction or in the analysis. Most sufficient-quality studies were conducted in older populations (mean age in one or more analysis group >50 years). In sufficient-quality articles, 82% demonstrated at least one statistically significant association between the MSD and biomarker(s) studied. Evidence suggested that: (i) the collagen-repair marker TIMP-1 is decreased in fibro proliferative disorders, (ii) 5-HT (serotonin) is increased in trapezius myalgia, and (iii) triglycerides are increased in a variety of MSD. Only 5 studies showed an association between a biochemical marker and MSD severity.While some MSD biomarkers were identified, limitations in the articles examined included possible selection bias, confounding, spectrum effect (potentially heterogeneous biomarker associations in populations according to symptom severity or duration), and insufficient attention to comorbid conditions. A list of recommendations for future studies is provided.
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