Department of General Practice.
Department of Internal Medicine.
Rheumatology (Oxford). 2023 Mar 1;62(3):1286-1295. doi: 10.1093/rheumatology/keac415.
The aim of this study was to identify biomarkers for radiographic OA severity and progression acting within the inflammation and metabolic pathways.
For 3517 Rotterdam Study participants, 184 plasma protein levels were measured using Olink inflammation and cardiometabolic panels. We studied associations with severity and progression of knee, hip and hand OA and a composite overall OA burden score by multivariable regression models, adjusting for age, sex, cell counts and BMI.
We found 18 significantly associated proteins for overall OA burden, of which 5 stayed significant after multiple testing correction: circulating cartilage acidic protein 1 (CRTAC1), cartilage oligomeric matrix protein (COMP), thrombospondin 4, IL-18 receptor 1 (IL-18R1) and TNF ligand superfamily member 14. These proteins were also associated with progression of knee OA, with the exception of IL-18R1. The strongest association was found for the level of CRTAC1, with 1 s.d. increase in protein level resulting in an increase of 0.09 (95% CI 0.06, 0.12) in the overall OA Kellgren-Lawrence sum score (P = 2.9 × 10-8) in the model adjusted for age, sex, BMI and cell counts. This association was also present with the severity of OA in all three joints and progression of knee OA and was independent of BMI. We observed a stronger association for CRTAC1 with OA than for the well-known OA biomarker COMP.
We identified several compelling biomarkers reflecting the overall OA burden and the increased risk for OA progression. CRTAC1 was the most compelling and robust biomarker for OA severity and progression. Such a biomarker may be used for disease monitoring.
本研究旨在鉴定炎症和代谢途径中与放射学 OA 严重程度和进展相关的生物标志物。
在 3517 名鹿特丹研究参与者中,使用 Olink 炎症和心脏代谢面板测量了 184 种血浆蛋白水平。我们通过多变量回归模型研究了与膝关节、髋关节和手部 OA 的严重程度和进展以及整体 OA 负担综合评分的关联,调整了年龄、性别、细胞计数和 BMI。
我们发现了 18 个与整体 OA 负担显著相关的蛋白质,其中 5 个在经过多次测试校正后仍然显著:循环软骨酸性蛋白 1(CRTAC1)、软骨寡聚基质蛋白(COMP)、血小板反应蛋白 4、白细胞介素 18 受体 1(IL-18R1)和肿瘤坏死因子配体超家族成员 14。这些蛋白质也与膝关节 OA 的进展相关,除了 IL-18R1。与 CRTAC1 水平的相关性最强,蛋白水平增加 1 个标准差,导致整体 OA Kellgren-Lawrence 总和评分增加 0.09(95%CI 0.06,0.12)(调整年龄、性别、BMI 和细胞计数后的模型中,P=2.9×10-8)。这种关联在所有三个关节的 OA 严重程度和膝关节 OA 的进展中也存在,并且独立于 BMI。我们观察到 CRTAC1 与 OA 的相关性强于著名的 OA 生物标志物 COMP。
我们鉴定了几个反映整体 OA 负担和 OA 进展风险增加的有说服力的生物标志物。CRTAC1 是 OA 严重程度和进展的最有说服力和最强大的生物标志物。这种生物标志物可用于疾病监测。
