Department of Epidemiology and Preventive Medicine, Monash University, Melbourne, Australia.
Cardiovasc Ther. 2012 Dec;30(6):342-50. doi: 10.1111/j.1755-5922.2011.00283.x. Epub 2011 May 25.
The increased thrombotic cardiovascular (CV) risk in trials of cyclo-oxygenase-2 (COX-2) inhibitors versus placebo, and the apparent similar risk with nonsteroidal antiinflammatory drugs (NSAIDs), may be related to their potential to elevate blood pressure (BP).
We evaluated the relationship between baseline BP and change in BP on CV events (CVEs) in patients receiving NSAIDs or COX-2 inhibitors in the prospective randomized, double-blind, Multinational Etoricoxib and Diclofenac Arthritis Long-term Program (N = 34,701) comparing etoricoxib 60 or 90 mg or diclofenac 150 mg daily for a mean duration of 18 months. The main outcome measure was confirmed thrombotic CVEs. The Antiplatelet Trialists' Collaboration endpoint, all-cause mortality, CV/congestive heart failure (CHF) mortality, and CHF incidence were similarly evaluated.
We found that baseline systolic BP (SBP) was associated with significantly higher risk of all events (P < 0.001). Baseline diastolic BP (DBP) was inversely and significantly associated with risk of all events (P < 0.001 to P = 0.016) except CV/CHF mortality (P = 0.054). There was no significant differential effect between etoricoxib and diclofenac in relation to CVEs, except for confirmed CHF, for which the risk was significantly higher with etoricoxib (P = 0.019). Only CHF risk (P = 0.020 for both SBP and DBP change), but not thrombotic endpoints, was significantly associated with change in BP from months 0 to 4. These findings were not meaningfully altered after covariate adjustment for baseline CV risk.
Baseline BP, but not change in BP, was significantly associated with risk of thrombotic CVEs through 18 months. The CV risk of COX-2s and NSAIDs did not appear to be related to the BP-elevating effects of these agents, although such analyses, i.e., from randomized controlled trials, are unable to definitively exclude such a relationship.
环氧化酶-2(COX-2)抑制剂与安慰剂相比,血栓性心血管(CV)风险增加,而非甾体抗炎药(NSAIDs)的风险似乎也增加,这可能与它们升高血压(BP)的潜力有关。
我们评估了基线 BP 与接受 NSAIDs 或 COX-2 抑制剂的患者 CV 事件(CVE)中 BP 变化之间的关系,在前瞻性随机、双盲、多国依特立昔布和双氯芬酸关节炎长期计划(N=34701)中,比较依特立昔布 60 或 90 mg 或双氯芬酸 150 mg 每日一次,平均持续 18 个月。主要观察终点为证实的血栓性 CVEs。同样评估了抗血小板试验者协作终点、全因死亡率、CV/充血性心力衰竭(CHF)死亡率和 CHF 发生率。
我们发现,基线收缩压(SBP)与所有事件的风险显著相关(P<0.001)。基线舒张压(DBP)与所有事件的风险呈负相关且显著相关(P<0.001 至 P=0.016),除 CV/CHF 死亡率(P=0.054)外。依特立昔布和双氯芬酸在 CVE 方面没有显著的差异效应,除了证实的 CHF,依特立昔布的风险显著更高(P=0.019)。只有 CHF 风险(SBP 和 DBP 变化的 P=0.020),而不是血栓终点,与 0 至 4 个月期间 BP 的变化显著相关。这些发现在校正基线 CV 风险的协变量后并没有明显改变。
基线 BP 与 18 个月内血栓性 CVE 的风险显著相关,而 BP 的变化则没有。COX-2s 和 NSAIDs 的 CV 风险似乎与这些药物的升压作用无关,尽管这种分析,即来自随机对照试验,无法明确排除这种关系。
