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腹主动脉瘤药物流行病学研究

Abdominal Aortic Aneurysms Pharmacoepidemiological Studies.

作者信息

Wemmelund Holger

出版信息

Dan Med J. 2017 May;64(5).

PMID:28552095
Abstract

An abdominal aortic aneurysm (AAA) is an enlargement of the abdominal aorta. It is a common disease in the elderly, with a prevalence of 1-5%. An AAA is normally asymptomatic, and the diagnosis is often incidental, identified when a patient is examined for other conditions. The major risk of having an AAA is sudden rupture and death caused by massive hemorrhaging. As rupture risk increases with increasing AAA diameter, the current management strategies include regular imaging surveillance and elective repair before rupture occurs. Ruptured AAA (rAAA) carries high mortality, and an identification of a drug or compound with the potential to halt the growth of an AAA and/or reduce the risk of a rAAA is needed. Thus, the aims of this thesis were to examine the clinical impact of treatment with statins (Study I), reninangiotensin system (RAS) blockers (Study II), and low-dose aspirin (ASA)(Study III) on the risk of rAAA and case fatality following rAAA. The thesis is based on three nation-wide, combined case-control and follow-up studies using data from Danish population-based health-care and administrative registries. In Study I (1996-2008), we included 3,691 patients with an incident diagnosis of rAAA (cases). For the risk analyses, we matched 3,584 rAAA cases to 3,584 age- and sex-matched patients with an incident diagnosis of AAA (controls). Current statin use was associated with a lower risk of rAAA, adjusted odds ratio (OR): 0.73 (95% CI: 0.61;0.86), compared to never use of statins. Furthermore, current statin use was associated with a lower 30-day case fatality following rAAA, adjusted mortality rate ratio (MRR): 0.80 (95% CI: 0.68;0.95). In Study II (1996-2012), we identified 4,052 rAAA cases and 10,549 AAA controls. We were unable to demonstrate any association between the current use of either angiotensin-converting enzyme (ACE) inhibitors or angiotensin receptor blockers and the risk of rAAA, adjusted ORs: 0.96 (95% CI: 0.85;1.07) and 0.93 (95% CI: 0.79;1.09), respectively. The results were robust in supplemental propensity score matched analyses. Likewise, no association between current use of RAS-blockers and 30-day case fatality was found. In Study III (1996-2012), 4,055 rAAA cases were included. The adjusted OR for the risk of rAAA in ASA users compared to non-users was 0.97 (95% CI: 0.86;1.08). However, ASA use was associated with an unfavorable 30-day case fatality, adjusted MRR 1.17 (95% CI: 1.06;1.28), corresponding to an excessive rAAA case fatality in ASA users of nearly 20%. In conclusion, we found an approximately 25% lower risk of rAAA and 20% lower 30-day case fatality in statin-treated patients. Furthermore, we found an almost 20% higher 30-day case fatality following rAAA in ASA treated patients. No association between the use of RAS-blockers and the risk of rAAA or case fatality following rAAA was found. Similarly, we found no association between the use of ASA and the risk of rAAA.

摘要

腹主动脉瘤(AAA)是腹主动脉的扩张。它是老年人中的常见疾病,患病率为1%-5%。腹主动脉瘤通常无症状,诊断往往是偶然的,在患者因其他疾病接受检查时被发现。腹主动脉瘤的主要风险是突然破裂和因大量出血导致的死亡。由于破裂风险随着腹主动脉瘤直径的增加而增加,目前的管理策略包括定期影像学监测和在破裂发生前进行择期修复。破裂性腹主动脉瘤(rAAA)的死亡率很高,因此需要确定一种有可能阻止腹主动脉瘤生长和/或降低rAAA风险的药物或化合物。因此,本论文的目的是研究他汀类药物治疗(研究I)、肾素-血管紧张素系统(RAS)阻滞剂(研究II)和低剂量阿司匹林(ASA)(研究III)对rAAA风险以及rAAA后病死率的临床影响。本论文基于三项全国性的病例对照和随访研究,使用了丹麦基于人群的医疗保健和行政登记数据。在研究I(1996 - 2008年)中,我们纳入了3691例初次诊断为rAAA的患者(病例组)。为了进行风险分析,我们将3584例rAAA病例与3584例年龄和性别匹配的初次诊断为AAA的患者(对照组)进行匹配。与从未使用他汀类药物相比,当前使用他汀类药物与rAAA风险降低相关,调整后的优势比(OR)为0.73(95%置信区间:0.61;0.86)。此外,当前使用他汀类药物与rAAA后30天病死率降低相关,调整后的死亡率比(MRR)为0.80(95%置信区间:0.68;0.95)。在研究II(1996 - 2012年)中,我们确定了4052例rAAA病例和10549例AAA对照。我们未能证明当前使用血管紧张素转换酶(ACE)抑制剂或血管紧张素受体阻滞剂与rAAA风险之间存在任何关联,调整后的OR分别为0.96(95%置信区间:0.85;1.07)和0.93(95%置信区间:0.79;1.09)。在补充的倾向评分匹配分析中,结果是稳健的。同样,未发现当前使用RAS阻滞剂与30天病死率之间存在关联。在研究III(1996 - 2012年)中,纳入了4055例rAAA病例。与未使用者相比,ASA使用者发生rAAA风险的调整后OR为0.97(95%置信区间:0.86;1.08)。然而,使用ASA与不良的30天病死率相关,调整后的MRR为1.17(95%置信区间:1.06;1.28),这相当于ASA使用者中rAAA病例病死率过高近20%。总之,我们发现他汀类药物治疗的患者发生rAAA的风险降低约25%,30天病死率降低20%。此外,我们发现ASA治疗的患者rAAA后30天病死率几乎高出20%。未发现使用RAS阻滞剂与rAAA风险或rAAA后病死率之间存在关联。同样,我们未发现使用ASA与rAAA风险之间存在关联。

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