Medical College of Qingdao University, Qingdao, 266000, China.
Department of Orthopedic Surgery, Affiliated Hospital of Qingdao University, Qingdao, 266000, China.
BMC Musculoskelet Disord. 2020 Jun 2;21(1):339. doi: 10.1186/s12891-020-03329-8.
Intervertebral disc degeneration (IVDD) is a major cause of low back pain. Although the mechanism of degeneration remains unclear, aging has been recognized as a key risk factor for IVDD. Most studies seeking to identify IVDD-associated molecular alterations in the context of human age-related IVDD have focused only on a limited number of proteins. Differential proteomic analysis is an ideal method for comprehensively screening altered protein profiles and identifying the potential pathways related to pathological processes such as disc degeneration.
In this study, tandem mass tag (TMT) labeling was combined with liquid chromatography-tandem mass spectrometry (LC-MS/MS) for differential proteomic analysis of human fetal and geriatric lumbar disc nucleus pulposus (NP) tissue. Parallel reaction monitoring (PRM) and Western blotting (WB) techniques were used to identify target proteins. Bioinformatic analyses, including Gene Ontology (GO) annotation, domain annotation, pathway annotation, subcellular localization and functional enrichment analyses, were used to interpret the potential significance of the protein alterations in the mechanism of IVDD. Student's t-tests and two-tailed Fisher's exact tests were used for statistical analysis.
Six hundred forty five proteins were significantly upregulated and 748 proteins were downregulated in the geriatric group compared with the fetal group. Twelve proteins were verified to have significant differences in abundance between geriatric and fetal NP tissue; most of these have not been previously identified as being associated with human IVDD. The potential significance of the differentially expressed proteins in age-related IVDD was analyzed from multiple perspectives, especially with regard to the association of the immunoinflammatory response with IVDD.
Differential proteomic analysis was used as a comprehensive strategy for elucidating the protein alterations associated with age-related IVDD. The findings of this study will aid in the screening of new biomarkers and molecular targets for the diagnosis and therapy of IVDD. The results may also significantly enhance our understanding of the pathophysiological process and mechanism of age-related IVDD.
椎间盘退变(IVDD)是腰痛的主要原因。尽管退变的机制尚不清楚,但衰老已被认为是 IVDD 的一个关键危险因素。大多数试图在人类年龄相关性 IVDD 背景下识别与 IVDD 相关的分子改变的研究仅集中在少数几种蛋白质上。差异蛋白质组学分析是一种全面筛选改变的蛋白质谱并识别与椎间盘退变等病理过程相关的潜在途径的理想方法。
在这项研究中,串联质量标签(TMT)标记与液相色谱-串联质谱(LC-MS/MS)相结合,用于分析人胎儿和老年腰椎间盘核髓核(NP)组织的差异蛋白质组学。平行反应监测(PRM)和 Western blotting(WB)技术用于鉴定靶蛋白。生物信息学分析,包括基因本体(GO)注释、结构域注释、途径注释、亚细胞定位和功能富集分析,用于解释 IVDD 机制中蛋白质改变的潜在意义。学生 t 检验和双尾 Fisher 精确检验用于统计分析。
与胎儿组相比,老年组中有 645 种蛋白质显著上调,748 种蛋白质下调。在老年和胎儿 NP 组织之间,有 12 种蛋白质的丰度有显著差异;其中大多数以前没有被确定与人类 IVDD 相关。从多个角度分析了与年龄相关性 IVDD 相关的差异表达蛋白的潜在意义,特别是免疫炎症反应与 IVDD 的关系。
差异蛋白质组学分析被用作阐明与年龄相关性 IVDD 相关的蛋白质改变的综合策略。本研究的结果将有助于筛选 IVDD 的新生物标志物和分子靶点。研究结果还可能显著提高我们对年龄相关性 IVDD 的病理生理过程和机制的理解。
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