Objective: To investigate the correlation between serum CCL20 level and disease severity in patients with rheumatoid arthritis (RA). Methods: From July 2018 to July 2019, a cross-sectional study was conducted in the Department of Rheumatology and Immunology, the Third Affiliated Hospital of Southern Medical University. The observation group consisted of 105 outpatients and inpatients diagnosed with RA, while the control group was 90 healthy people with age and gender matched physical examination in the Third Affiliated Hospital of Southern Medical University. According to Steinbroker classification, RA patients were divided into Steinbroker grade 2 group (n=35), Steinbroker grade 3 group (n=38) and steinbroker grade 4 group (n=32); according to DAS28 score, RA patients were divided into remission group (DAS28<2.6)(n=39), mild active group (DAS28 2.6-3.2)(n=25), moderate active stage group (DAS28 3.2-5.1)(n=20) and severe active stage group (DAS28 ≥ 5.1)(n=21). The levels of chemokine ligand 20 (CCL20), erythrocyte sedimentation rate (ESR) and C-reactive protein (CRP) were detected by ELISA. The levels of CCL20 in each group were compared, and the correlation between CCL20 and other indicators was analyzed. The receiver operating characteristic (ROC) curve of CCL20 in diagnosis of RA was analyzed to explore the correlation between CCL20 and disease severity of RA patients. Results: Compared with the normal control group, the serum CCL20 level in RA patients was significantly increased [(48.1±16.7) pg/ml vs (17.6±5.9) pg/ml, t=19.39, P<0.001]. In addition, serum CCL20 in steinbroker grade 4 group was significantly higher than that in Steinbroker grade 3 group [(59.5±10.1) pg/ml vs (47.4±17.5) pg/ml, t=3.472, P<0.001], and the serum CCL20 level in steinbroker grade 3 group was significantly higher than that in steinbroker grade 2 group [(47.4±17.5) pg/ml vs (38.4±14.6) pg/ml, t=2.370, P<0.001], CCL20 level in steinbroker grade 2 group was significantly higher than that in normal control group [(38.4±14.6) pg/ml vs (17.6±5.9) pg/ml, t=7.738, P<0.001]. In addition, serum CCL20 level was significantly positively correlated with steinbroker score (r=0.505, P<0.001); CCL20 level in active RA patients was significantly higher than that in remission RA patients [(57.2±13.2) pg/ml vs (32.7±8.9) pg/ml, t=10.31, P<0.001]. The serum CCL20 level in severe activity group was significantly higher than that in moderate activity group [(60.6±10.9) pg/ml vs (51.7±16.2) pg/ml, t=0.212, P=0.040], and the serum CCL20 level in moderate activity group was significantly higher than that in mild activity group [(51.7±16.2) pg/ml vs (40.5±18.6) pg/ml, t=0.217, P=0.037]. In addition, there was a significant positive correlation between serum CCL20 level and DAS28 score (r=0.451, P<0.001). In addition, serum CCL20 level was positively correlated with serum CRP (r=0.332, P<0.001). According to the ROC curve, the specificity of steinbroker grade 2 group was 0.53, and the sensitivity was 0.74, AUC was 0.659; the sensitivity of steinbroker grade 3 group was 0.78, and the specificity was 0.69, AUC was 0.734; the sensitivity of mild vs medium stage was 0.64, and the specificity was 0.70, AUC was 0.699; the sensitivity of medium stage vs severe stage was 0.57, and the specificity was 0.68,AUC was 0.678. Conclusion: Serum CCL20 level in RA patients is significantly increased and positively correlated with disease severity, which may be used as a marker to observe and evaluate the progression of RA.
目的: 探讨类风湿性关节炎患者(RA)血清趋化因子配体20(CCL20)水平与疾病严重程度的相关性。 方法: 采用横断面研究,选取2018年7月至2019年7月南方医科大学第三附属医院风湿免疫科门诊及住院诊断的RA患者105 例,对照组是同期年龄、性别相匹配的在同院进行体检的健康人90名。根据Steinbrocker分级,将RA患者分成Steinbrocker 2级组(35例)、Steinbrocker 3级组(38例)、Steinbrocker 4级组(32例);根据 DAS28 评分,将RA患者分成缓解期组(DAS<2.6)(39例)、轻度活动期组(DAS28 2.6~3.2)(25例)、中度活动期组(DAS28 3.2~5.1)(20例)及重度活动期组(DAS28≥5.1)(21例)。采用ELISA法检测CCL20、红细胞沉降率(ESR)和C反应蛋白(CRP)。比较各组CCL20水平,分析CCL20与其他指标的相关性,并做CCL20诊断 RA 的受试者工作(ROC)曲线。 结果: RA 患者组与对照组相比,血清CCL20水平显著升高,差异有统计学意义[(48.1±16.7)pg/ml vs (17.6±5.9)pg/ml, t=19.39, P<0.001]。RA患者Steinbrocker 4级组血清CCL20显著高于Steinbrocker 3级组[(59.5±10.1)pg/ml vs (47.4±17.5)pg/ml, t=3.472, P<0.001],Steinbrocker 3级组血清CCL20水平显著高于Steinbrocker 2级组[(47.4±17.5)pg/ml vs (38.4±14.6)pg/ml, t=2.370,P=0.021],Steinbrocker 2级组CCL20水平显著高于对照组[(38.4±14.6)pg/ml vs (17.6±5.9)pg/ml, t=7.738,P<0.001]。此外,血清CCL20水平与Steinbrocker评分具有显著正相关性(r=0.505,P<0.001);活动期RA患者CCL20水平显著高于缓解期RA患者[(57.2±13.2)pg/ml vs (32.7±8.9)pg/ml,t=10.31, P<0.001]。重度活动度组血清CCL20水平显著高于中度活动度组[(60.6±10.9)pg/ml vs (51.7±16.2)pg/ml, t=0.212,P=0.040],中度活动度组血清CCL20水平显著高于轻度活动度组[(51.7±16.2)pg/ml vs (40.5±18.6)pg/ml, t=0.217,P=0.037]。血清CCL20水平与DAS28评分具有显著正相关性(r=0.451, P<0.001)。血清CCL20水平与血清CRP具有正相关性(r=0.332, P<0.001)。根据ROC曲线,Steinbrocker 2级组向Steinbrocker 3级进展,特异度为0.53,敏感度为0.74,曲线下面积为0.659;Steinbrocker 3级组向Steinbrocker 4级进展,敏感度为0.78,特异度为0.66,曲线下面积为0.734;疾病活动度轻度期vs疾病活动度中度期:敏感度为0.64,特异度为0.70,曲线下面积为0.699;疾病活动度中度期vs疾病活动度重度期:敏感度为0.57,特异度为0.68,曲线下面积为0.678。 结论: RA患者血清CCL20水平显著升高并与疾病严重程度呈正相关,可能是一种监测和评价RA疾病进展的生物标志物。.