Ethanol withdrawal increases blood pressure and vascular oxidative stress: a role for angiotensin type 1 receptors

Q1 Medicine

Journal of The American Society of Hypertension Pub Date : 2018-07-01 DOI:10.1016/j.jash.2018.03.012

Natália A. Gonzaga PhD , Gabriel T. do Vale PhD , Juliana M. Parente MSc , Rodrigo Yokota MSc , Bruno S. De Martinis PhD , Dulce E. Casarini PhD , Michele M. Castro PhD , Carlos R. Tirapelli PhD

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引用次数: 7

Abstract

We evaluated the possible mechanisms underlying the oxidative stress induced by ethanol withdrawal. With this purpose, we verified the role of AT₁ receptors in such response. Male Wistar rats were treated with ethanol 3%–9% (vol./vol.) for 21 days. Ethanol withdrawal was induced by abrupt discontinuation of the treatment. Experiments were performed 48 hours after ethanol discontinuation. Increased plasma levels of angiotensin II were detected after ethanol withdrawal. Losartan (10 mg/kg; p.o. gavage), a selective AT₁ receptor antagonist, impeded the increase in blood pressure induced by ethanol withdrawal. Increased lipoperoxidation and superoxide anion (O₂⁻) levels were detected in aortas after ethanol withdrawal, and losartan prevented these responses. Decreased hydrogen peroxide and nitrate/nitrite concentration were detected in aortas after ethanol withdrawal, and losartan prevented these effects. Nitrotyrosine immunostaining in the rat aorta was increased after ethanol withdrawal, and AT₁ blockade impeded this response. Increased expression of PKCδ and p47^phox was detected after ethanol withdrawal, and treatment with losartan prevented these responses. Our study provides novel evidence that ethanol withdrawal increases vascular oxidative stress and blood pressure through AT₁-dependent mechanisms. These findings highlight the importance of angiotensin II in ethanol withdrawal–induced increase in blood pressure and vascular oxidative damage.

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乙醇戒断增加血压和血管氧化应激:血管紧张素1型受体的作用

我们评估了乙醇戒断诱导氧化应激的可能机制。为此，我们验证了AT1受体在这种反应中的作用。雄性Wistar大鼠以3% ~ 9%(体积/体积)乙醇处理21 d。乙醇戒断是由突然停止治疗引起的。实验在乙醇停药48小时后进行。乙醇戒断后检测到血浆血管紧张素II水平升高。氯沙坦(10mg /kg;选择性AT1受体拮抗剂(p.o. gavage)可抑制乙醇戒断引起的血压升高。乙醇戒断后，主动脉中检测到脂质过氧化和超氧阴离子(O2−)水平升高，氯沙坦阻止了这些反应。乙醇戒断后主动脉过氧化氢和硝酸盐/亚硝酸盐浓度降低，氯沙坦可阻止这些影响。乙醇戒断后大鼠主动脉的硝基酪氨酸免疫染色增加，AT1阻断阻断了这种反应。乙醇戒断后检测到PKCδ和p47phox的表达增加，氯沙坦治疗阻止了这些反应。我们的研究提供了新的证据，证明乙醇戒断通过at1依赖机制增加血管氧化应激和血压。这些发现强调了血管紧张素II在乙醇戒断诱导的血压升高和血管氧化损伤中的重要性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of The American Society of Hypertension PERIPHERAL VASCULAR DISEASE-

CiteScore

4.80

自引率

0.00%

发文量

审稿时长

6.6 weeks

期刊介绍： Cessation. The Journal of the American Society of Hypertension (JASH) publishes peer-reviewed articles on the topics of basic, applied and translational research on blood pressure, hypertension and related cardiovascular disorders and factors; as well as clinical research and clinical trials in hypertension. Original research studies, reviews, hypotheses, editorial commentary and special reports spanning the spectrum of human and experimental animal and tissue research will be considered. All research studies must have been conducted following animal welfare guidelines. Studies involving human subjects or tissues must have received approval of the appropriate institutional committee charged with oversight of human studies and informed consent must be obtained.

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