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高血压前期预处理可改善成人降压和心脏保护治疗。

Prehypertensive preconditioning improves adult antihypertensive and cardioprotective treatment.

机构信息

Department of Nephrology, Klinikum rechts der Isar, Technical University Munich, Ismaninger Str. 22, 81675 Munich, Germany.

出版信息

J Pharmacol Exp Ther. 2010 Mar;332(3):1121-6. doi: 10.1124/jpet.109.161075. Epub 2009 Nov 10.

Abstract

Transient prehypertensive treatment (TPT) causes prolonged antihypertensive and cardioprotective effects. Reduced angiotensin sensitivity has been attributed to those effects. We hypothesize that prehypertensive preconditioning by angiotensin II type 1 receptor (AT1R) blockade improves cardiovascular protection of late-onset AT1R blockade in a model of spontaneous hypertensive heart-failure rats (SHHF/Mcc-fa(cp)). TPT (4-8 weeks of age) consisted of AT1R blockade (5 mg/kg candesartan) or vehicle. Candesartan-pretreated SHHF (5 mg/kg/day candesartan; weeks 4-8) received during adulthood (20-28 weeks of age) either candesartan at a dose of 1.5 or 5 mg/kg/day or vehicle. Vehicle-pretreated SHHF received either candesartan (5 mg/kg/day) or vehicle during adulthood. Blood pressure telemetry and longitudinal echocardiography were performed between weeks 20 and 28. Final examination included cardiac and vascular morphometry and measurement of the AT1R signaling and receptor internalization (ATRAP). Combined juvenile and adult AT1R blockade caused lower mean arterial pressure (MAP) than adult AT1R blockade alone (84 +/- 5 versus 97 +/- 5 mm Hg; P < 0.05). Cardiac and vascular hypertrophy was lower. Juvenile treatments were associated with a reduced cardiovascular AT1R expression and enhanced ATRAP expression. Combined juvenile and reduced adult AT1R blockade resulted in MAP similar to that with adult AT1R blockade alone (92 +/- 3 versus 97 +/- 5 mm Hg). We conclude that prehypertensive preconditioning improves adult treatment effects in SHHF. Those effects correlate with reduced cardiovascular AT1R expression and enhanced receptor internalization, suggesting reduced angiotensin sensitivity in pretreated SHHF. Moreover, preconditioning allows a reduction of adult AT1R blockade without loss of protection. Therefore, prehypertensive preconditioning may offer a tool to improve treatment efficacy in humans.

摘要

短暂性高血压前期治疗(TPT)可引起持久的降压和心脏保护作用。这些作用归因于血管紧张素敏感性降低。我们假设,血管紧张素 II 型 1 型受体(AT1R)阻断的高血压前期预处理可改善自发性高血压心力衰竭大鼠(SHHF/Mcc-fa(cp))模型中晚期 AT1R 阻断的心血管保护作用。TPT(4-8 周龄)包括 AT1R 阻断(5mg/kg坎地沙坦)或载体。成年期(20-28 周龄)给予坎地沙坦预处理的 SHHF(5mg/kg/天坎地沙坦;4-8 周)接受 1.5 或 5mg/kg/天坎地沙坦或载体的剂量。给予载体预处理的 SHHF 在成年期接受坎地沙坦(5mg/kg/天)或载体。在 20 至 28 周之间进行血压遥测和纵向超声心动图检查。最终检查包括心脏和血管形态计量学以及 AT1R 信号和受体内化(ATRAP)的测量。青少年和成年期联合 AT1R 阻断比单独成年期 AT1R 阻断引起的平均动脉压(MAP)更低(84 +/- 5 与 97 +/- 5mmHg;P < 0.05)。心脏和血管肥大减少。青少年治疗与心血管 AT1R 表达减少和 ATRAP 表达增强相关。青少年和减少的成年期联合 AT1R 阻断导致的 MAP 与单独成年期 AT1R 阻断相似(92 +/- 3 与 97 +/- 5mmHg)。我们得出结论,高血压前期预处理可改善 SHHF 中的成年期治疗效果。这些作用与心血管 AT1R 表达减少和受体内化增强相关,提示预处理 SHHF 中的血管紧张素敏感性降低。此外,预处理允许减少成年期 AT1R 阻断而不丧失保护作用。因此,高血压前期预处理可能为改善人类治疗效果提供一种工具。

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