Institution of Public Health and Clinical Medicine/Rheumatology, University Hospital, Umeå, 901 85, Sweden.
Arthritis Res Ther. 2011 Aug 15;13(4):R131. doi: 10.1186/ar3442.
Co-morbidity and mortality due to cardiovascular disease (CVD) are increased in patients with rheumatoid arthritis (RA). Most published studies in this field are retrospective or cross sectional. We investigated the presence of traditional and disease related risk factors for CVD at the onset of RA and during the first five years following diagnosis. We also evaluated their potential for predicting a new cardiovascular event (CVE) during the five-year follow-up period and the modulatory effect of pharmacological treatment.
All patients from the four northern-most counties of Sweden with early RA are, since December 1995, consecutively recruited at diagnosis (T0) into a large survey on the progress of the disease. Information regarding cardiovascular co-morbidity and related predictors was collected from clinical records and supplemented with questionnaires. By April 2008, 700 patients had been included of whom 442 patients had reached the five-year follow-up (T5).
Among the 442 patients who reached T5 during the follow-up period, treatment for hypertension increased from 24.5 to 37.4% (P < 0.001)), diagnosis of diabetes mellitus (DM) from 7.1 to 9.5% (P < 0.01) whilst smoking decreased from 29.8 to 22.4% (P < 0.001) and the BMI from 26.3 to 25.8 (P < 0.05), respectively. By T5, 48 patients had suffered a new CVE of which 12 were fatal. A total of 23 patients died during the follow-up period. Age at disease onset, male sex, a previous CVE, DM, treatment for hypertension, triglyceride level, cumulative disease activity (area under the curve (AUC) disease activity score (DAS28)), extra-articular disease, corticosteroid use, shorter duration of treatment with disease modifying anti-rheumatic drugs (DMARDs) and use of COX-2 inhibitors increased the hazard rate for a new CVE. A raised erythrocyte sedimentation rate (ESR) at inclusion and AUC DAS28 at six months increased the hazard rate of CVE independently whilst DMARD treatment was protective in multiple Cox extended models adjusted for sex and CV risk factors. The risk of a CVE due to inflammation was potentiated by traditional CV risk factors.
The occurrence of new CV events in very early RA was explained by traditional CV risk factors and was potentiated by high disease activity. Treatment with DMARDs decreased the risk. The results may have implications for cardio-protective strategies in RA.
心血管疾病(CVD)的合并症和死亡率在类风湿关节炎(RA)患者中增加。该领域的大多数已发表研究都是回顾性或横断面研究。我们调查了 RA 发病时和诊断后五年内传统和疾病相关 CVD 危险因素的存在情况。我们还评估了它们在五年随访期间预测新心血管事件(CVE)的潜力,以及药物治疗的调节作用。
自 1995 年 12 月以来,瑞典最北部四个县的所有早期 RA 患者均在诊断时(T0)连续纳入一项关于疾病进展的大型调查。从临床记录中收集有关心血管合并症和相关预测因素的信息,并通过问卷进行补充。截至 2008 年 4 月,已有 700 名患者被纳入,其中 442 名患者达到了五年随访(T5)。
在随访期间达到 T5 的 442 名患者中,高血压治疗的比例从 24.5%增加到 37.4%(P < 0.001),糖尿病(DM)的诊断从 7.1%增加到 9.5%(P < 0.01),而吸烟率从 29.8%下降到 22.4%(P < 0.001),体重指数从 26.3 下降到 25.8(P < 0.05)。到 T5 时,48 名患者发生了新的 CVE,其中 12 例为致命性的。在随访期间,共有 23 名患者死亡。发病年龄、男性、既往 CVE、DM、高血压治疗、甘油三酯水平、累积疾病活动度(曲线下面积(AUC)疾病活动评分(DAS28))、关节外疾病、皮质类固醇使用、改变病情的抗风湿药物(DMARDs)治疗时间缩短以及使用 COX-2 抑制剂均增加了新发 CVE 的危险率。纳入时升高的红细胞沉降率(ESR)和六个月时的 AUC DAS28 独立增加了 CVE 的危险率,而 DMARD 治疗在调整性别和 CV 危险因素的多个 Cox 扩展模型中具有保护作用。炎症引起的 CVE 风险被传统的 CV 危险因素所放大。
在非常早期的 RA 中,新的 CV 事件的发生可以用传统的 CV 危险因素来解释,并被高疾病活动所放大。DMARD 治疗降低了风险。结果可能对 RA 的心脏保护策略具有重要意义。
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