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用于预测膝关节骨关节炎影像学进展的血浆生物标志物的质谱分析

Mass spectrometry assays of plasma biomarkers to predict radiographic progression of knee osteoarthritis.

作者信息

Ritter Susan Y, Collins Jamie, Krastins Bryan, Sarracino David, Lopez Mary, Losina Elena, Aliprantis Antonios O

出版信息

Arthritis Res Ther. 2014 Oct 7;16(5):456. doi: 10.1186/s13075-014-0456-6.

Abstract

INTRODUCTION

Biomarkers to identify osteoarthritis (OA) patients at risk for disease progression are needed. As part of a proteomic analysis of knee synovial fluid from normal and OA patients, differentially expressed proteins were identified that could represent potential biomarkers for OA. This study aimed to use mass spectrometry assays to identify representative peptides from several proteins in synovial fluid and peripheral blood, and assess their levels as biomarkers of OA progression.

METHODS

Multiplexed high throughput selected reaction monitoring (SRM) assays were developed to measure tryptic peptides representative of 23 proteins in matched serum and synovial fluid samples from late OA subjects at the time of joint replacement. Subsequently plasma samples from the baseline visit of 173 subjects in an observational OA cohort were tested by SRM for peptides from nine of these proteins: afamin, clusterin, cartilage oligomeric matrix protein, hepatocyte growth factor, kallistatin, insulin-like growth factor binding protein, acid labile subunit, lubricin, lumican, and pigment epithelium-derived factor. Linear regression was used to determine the association between the peptide biomarker level at baseline and change in joint space width (ΔJSW) from baseline to 30 months, adjusting for age and sex.

RESULTS

In the matched cohort, 17 proteins could be identified in synovial fluid and 16 proteins were detected in serum. For the progression cohort, the average age was 62 and average ΔJSW over 30 months was 0.68 mm. A high correlation between different peptides from individual proteins was observed, indicating our assays correctly measured their target proteins. Peptides representative of clusterin, lumican and lubricin showed statistically significant associations with joint space narrowing after adjustment for age and sex. Partial R2 values showed clusterin FMETVAEK and lubricin LVEVNPK peptide biomarkers explains about 2 to 3% of the variability of ΔJSW, similar to that explained by age. A biomarker score combining normalized data for both lubricin and clusterin peptides increased the model R2 to 0.079.

CONCLUSIONS

Our results suggest that when combined, levels of peptides representative of clusterin and lubricin in plasma are as predictive of OA progression as age. Replication of these findings in other prospective OA cohorts is planned.

摘要

引言

需要能够识别骨关节炎(OA)疾病进展风险患者的生物标志物。作为对正常人和OA患者膝关节滑液进行蛋白质组分析的一部分,已鉴定出差异表达的蛋白质,这些蛋白质可能代表OA的潜在生物标志物。本研究旨在使用质谱分析来鉴定滑液和外周血中几种蛋白质的代表性肽段,并评估它们作为OA进展生物标志物的水平。

方法

开发了多重高通量选择反应监测(SRM)分析方法,以测量来自晚期OA受试者在关节置换时匹配的血清和滑液样本中代表23种蛋白质的胰蛋白酶肽段。随后,通过SRM对观察性OA队列中173名受试者基线访视时的血浆样本进行检测,以分析其中9种蛋白质的肽段:载脂蛋白A、簇集蛋白、软骨寡聚基质蛋白、肝细胞生长因子、抑肽素、胰岛素样生长因子结合蛋白、酸性不稳定亚基、润滑素、核心蛋白聚糖和色素上皮衍生因子。使用线性回归来确定基线时肽生物标志物水平与从基线到30个月时关节间隙宽度变化(ΔJSW)之间的关联,并对年龄和性别进行校正。

结果

在匹配队列中,滑液中可鉴定出17种蛋白质,血清中检测到16种蛋白质。对于进展队列,平均年龄为62岁,30个月内的平均ΔJSW为0.68毫米。观察到来自单个蛋白质的不同肽段之间具有高度相关性,表明我们的分析方法正确测量了其目标蛋白质。在校正年龄和性别后,代表簇集蛋白、核心蛋白聚糖和润滑素的肽段与关节间隙变窄具有统计学上的显著关联。偏R2值显示,簇集蛋白FMETVAEK和润滑素LVEVNPK肽生物标志物解释了约2%至3%的ΔJSW变异性,与年龄所解释的变异性相似。结合润滑素和簇集蛋白肽段标准化数据的生物标志物评分使模型R2提高到0.079。

结论

我们的结果表明,血浆中代表簇集蛋白和润滑素的肽段水平联合起来对OA进展的预测能力与年龄相当。计划在其他前瞻性OA队列中重复这些发现。

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