摘要
背景:腹主动脉瘤(AAA)是一种慢性退行性炎症性疾病,遗传、环境、生活方式等多种因素决定了动脉瘤的发生和发展。目前,外科治疗仍然是唯一有效的动脉瘤治疗方法,但目前尚无药物治疗可以限制AAAS的进一步扩大和胎儿的破裂。 目的:综述血管紧张素Ⅱ(AngⅡ)及其1型受体(AT1)在AAA发病机制中的作用及AT1受体阻滞剂(ARB)治疗临床AAA的可能机制。 结果:虽然许多途径或分子与AAA的形成和进展有关,但越来越多的证据表明肽激素AngⅡ及其受体AT1在AAA发病中最重要,提示AT1靶向抑制在治疗临床AAA疾病中具有重要的借鉴价值。本文综述了AT1缺乏症和药理学arb治疗对实验性AAAs的影响,并讨论了AAA患者用药是否及如何改变临床AAAS的自然过程,包括动脉瘤增大率、破裂率和AAA特异性死亡率,并提供了两个已登记的临床试验资料,即替米沙坦和缬沙坦在限制小型AAA增大方面的疗效。 结论:AngⅡ/AT1通路在动脉瘤的发病过程中起着重要作用,通过ARB靶向AT1有助于建立限制小AAAS持续增大的新的药理治疗方法。
关键词: 腹主动脉瘤,血管紧张素Ⅱ1型受体,血管紧张素受体阻滞剂,动脉瘤发病机制,血管外科,药物治疗。
图形摘要
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