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尽管经过 1 年英夫利昔单抗治疗,类风湿关节炎患者存在 MMP-3 异常或 CRP 水平升高,但仍出现与临床相关的关节破坏放射学进展。

Clinically relevant radiographic progression in joint destruction in RA patients with abnormal MMP-3 or high levels of CRP despite 1-year treatment with infliximab.

机构信息

a The First Department of Internal Medicine , University of Occupational and Environmental Health , Kitakyushu , Japan.

出版信息

Mod Rheumatol. 2016 Nov;26(6):807-812. doi: 10.3109/14397595.2016.1158386. Epub 2016 Apr 26.

DOI:10.3109/14397595.2016.1158386
PMID:26915532
Abstract

OBJECTIVE

Identify the independently related factors of joint destruction progression in RA patients despite of infliximab treatment.

METHODS

The subjects were cases who underwent infliximab treatment for one year or longer in our department (n = 244). Patients in which modified total sharp score (mTSS), joint erosion (JE), and joint space narrowing (JSN) had advanced to the standard value (3.0) or more for one year were defined as mTSS- Clinically-Relevant-Rapid Progression (CRRP) (n = 20), JE-CRRP (n = 20), and JSN-CRRP (n = 23), and the respective related factors at baseline and week 54 were defined by multiple logistic regression.

RESULTS

The median disease duration was 24 months and median mTSS 9.0 at baseline. The median DAS28, CRP, and yearly progression of mTSS improved from 5.8 to 2.6, 1.2 to 0.1 mg/dL, and 4.4 to 0.0 point/year, respectively. The related factor in each of mTSS-CRRP, JE-CRRP, and JSN-CRRP was high CRP levels at baseline. At week 54, the related factor of mTSS-CRRP and JSN-CRRP was high MMP-3 titer; however, the related factor of JE-CRRP was high CRP levels.

CONCLUSION

High CRP levels at baseline were an independent predictive factor of joint destruction advancement during infliximab treatment. Moreover, it was believed that abnormal MMP-3 at week 54 was the index for mTSS and JSN advancement, while high CRP levels were the index for JE advancement.

摘要

目的

确定类风湿关节炎患者在接受英夫利昔单抗治疗的情况下关节破坏进展的独立相关因素。

方法

本研究对象为在我院接受英夫利昔单抗治疗 1 年或以上的病例(n=244)。将改良总Sharp 评分(mTSS)、关节侵蚀(JE)和关节间隙狭窄(JSN)在 1 年内进展到标准值(3.0)或更高的患者定义为 mTSS-临床相关快速进展(CRRP)(n=20)、JE-CRRP(n=20)和 JSN-CRRP(n=23),并通过多元逻辑回归确定基线和第 54 周的相关因素。

结果

中位疾病持续时间为 24 个月,基线 mTSS 中位数为 9.0。基线时 DAS28、CRP 和 mTSS 每年进展的中位数分别从 5.8 降至 2.6、从 1.2 降至 0.1mg/dL 和从 4.4 降至 0.0 点/年。在 mTSS-CRRP、JE-CRRP 和 JSN-CRRP 中,各有一个相关因素为基线时 CRP 水平较高。在第 54 周,mTSS-CRRP 和 JSN-CRRP 的相关因素是较高的 MMP-3 滴度,而 JE-CRRP 的相关因素是 CRP 水平较高。

结论

基线时 CRP 水平较高是英夫利昔单抗治疗期间关节破坏进展的独立预测因素。此外,我们认为第 54 周时 MMP-3 异常是 mTSS 和 JSN 进展的指标,而 CRP 水平较高是 JE 进展的指标。

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