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建立一个实验模型以研究血压的日常变异性与主动脉僵硬度之间的关系。

Development of an Experimental Model to Study the Relationship Between Day-to-Day Variability in Blood Pressure and Aortic Stiffness.

作者信息

Bouissou-Schurtz Camille, Lindesay Georges, Regnault Véronique, Renet Sophie, Safar Michel E, Molinie Vincent, Dabire Hubert, Bezie Yvonnick

机构信息

Institut National de la Santé et de la Recherche Médicale, U955, Equipe 03 Créteil, France.

Cardiovascular Department, Institut de Recherches Servier Suresnes, France.

出版信息

Front Physiol. 2015 Dec 8;6:368. doi: 10.3389/fphys.2015.00368. eCollection 2015.

Abstract

We aimed to develop an animal model of long-term blood pressure variability (BPV) and to investigate its consequences on aortic damage. We hypothesized that day-to-day BPV produced by discontinuous treatment of spontaneously hypertensive rats (SHR) by valsartan may increase arterial stiffness. For that purpose, rats were discontinuously treated, 2 days a week, or continuously treated by valsartan (30 mg/kg/d in chow) or placebo. Telemetered BP was recorded during 2 min every 15 min, 3 days a week during 8 weeks to cover the full BP variations in response to the treatment schedule. Pulse wave velocity (PWV) and aortic structure evaluated by immunohistochemistry were investigated in a second set of rats treated under the same conditions. Continuous treatment with valsartan reduced systolic BP (SBP) and reversed the aortic structural alterations observed in placebo treated SHR (decrease of medial cross-sectional area). Discontinuous treatment with valsartan decreased SBP to a similar extent but increased the day-to-day BPV, short term BPV, diastolic blood pressure (DBP), and PWV as compared with continuous treatment. Despite no modifications in the elastin/collagen ratio and aortic thickness, an increase in PWV was observed following discontinuous treatment and was associated with a specific accumulation of fibronectin and its αv-integrin receptor compared with both groups of rats. Taken together the present results indicate that a discontinuous treatment with valsartan is able to induce a significant increase in day-to-day BPV coupled to an aortic phenotype close to that observed in hypertension. This experimental model should pave the way for future experimental and clinical studies aimed at assessing how long-term BPV increases aortic stiffness.

摘要

我们旨在建立一种长期血压变异性(BPV)的动物模型,并研究其对主动脉损伤的影响。我们假设,缬沙坦间断治疗自发性高血压大鼠(SHR)所产生的每日BPV可能会增加动脉僵硬度。为此,大鼠每周接受2天的缬沙坦间断治疗,或持续接受缬沙坦(饲料中30mg/kg/d)或安慰剂治疗。每周3天,每15分钟记录2分钟的遥测血压,持续8周,以涵盖治疗方案引起的全部血压变化。在相同条件下治疗的另一组大鼠中,研究了通过免疫组织化学评估的脉搏波速度(PWV)和主动脉结构。缬沙坦持续治疗可降低收缩压(SBP),并逆转安慰剂治疗的SHR中观察到的主动脉结构改变(中膜横截面积减小)。与持续治疗相比,缬沙坦间断治疗使SBP降低到相似程度,但增加了每日BPV、短期BPV、舒张压(DBP)和PWV。尽管弹性蛋白/胶原蛋白比率和主动脉厚度没有改变,但间断治疗后观察到PWV增加,并且与两组大鼠相比,纤连蛋白及其αv整合素受体的特异性积累有关。综上所述,目前的结果表明,缬沙坦间断治疗能够导致每日BPV显著增加,并伴有与高血压中观察到的相似的主动脉表型。该实验模型应为未来旨在评估长期BPV如何增加主动脉僵硬度的实验和临床研究铺平道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2ace/4672044/b6cbad15b6a5/fphys-06-00368-g0001.jpg

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