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首页> 外文期刊>Journal of vascular research >Prevention of increases in blood pressure and left ventricular mass and remodeling of resistance arteries in young New Zealand genetically hypertensive rats: the effects of chronic treatment with valsartan, enalapril and felodipine.
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Prevention of increases in blood pressure and left ventricular mass and remodeling of resistance arteries in young New Zealand genetically hypertensive rats: the effects of chronic treatment with valsartan, enalapril and felodipine.

机译:预防年轻的新西兰遗传性高血压大鼠血压和左心室肿块的增加以及抵抗动脉的重塑:缬沙坦,依那普利和非洛地平的长期治疗效果。

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摘要

The relative efficacy of three antihypertensive drugs in the prevention of further elevation of blood pressure (BP) and cardiovascular structural remodeling in 4-week-old genetically hypertensive (GH) rats was studied by means of two complementary methods, stereology and myography. Four to 10-week-old GH rats were treated with valsartan (10 mg/kg/day), enalapril (10 mg/kg/day) or felodipine (30 mg/kg/day). Untreated GH and normotensive control rats of Wistar origin served as controls. Tail-cuff systolic SBP was measured weekly and left ventricular (LV) mass determined at the end of the experiment. Mesenteric resistance arteries (MRA) were either fixed by perfusion, embedded in Technovit and sections stained for stereological analysis, or mounted on a wire myograph for structural and functional measurements. BP and LV mass were significantly reduced by all drugs; decreases in BP and LV mass were smaller after felodipine treatment. Valsartan and enalapril caused a decrease in BP to normotensive control values. Felodipine kept BP at the 4-week level and prevented further rise with age. Valsartan caused hypotrophic outward remodeling of MRA, enalapril eutrophic outward remodeling and felodipine hypotrophic remodeling. Myograph measurements showed remodeling of the same order. While all drugs lowered the media/lumen ratio in GH to normal, the outward remodeling after valsartan and enalapril indicates that valsartan and enalapril might be more effective in reversing the inward remodeling of resistance arteries found in essential hypertension. Copyright 2000 S. Karger AG, Basel.
机译:通过两种互补的方法,立体学和肌成像,研究了三种降压药在预防4周龄遗传性高血压(GH)大鼠的血压进一步升高(BP)和心血管结构重构方面的相对功效。用缬沙坦(10 mg / kg /天),依那普利(10 mg / kg /天)或非洛地平(30 mg / kg /天)治疗4至10周大的GH大鼠。 Wistar来源的未经处理的GH和血压正常对照大鼠作为对照。每周测量尾袖收缩期SBP,并在实验结束时确定左心室(LV)质量。肠系膜阻力动脉(MRA)可以通过灌注固定,嵌入Technovit并进行染色以进行立体分析,也可以安装在钢丝肌电图仪上进行结构和功能测量。所有药物均显着降低了BP和LV的质量;非洛地平治疗后BP和LV质量的下降较小。缬沙坦和依那普利使血压降低至血压正常控制值。非洛地平将血压维持在4周的水平,并防止随着年龄的增长而进一步升高。缬沙坦引起MRA的营养不足的外向重塑,依那普利富营养的向外重塑和非洛地平的营养不足的重塑。肌电图仪测量显示相同顺序的重塑。尽管所有药物均使GH的中/腔比降低至正常水平,但缬沙坦和依那普利后的向外重塑表明缬沙坦和依那普利可能更有效地逆转了原发性高血压中抵抗性动脉的向内重塑。版权所有2000 S. Karger AG,巴塞尔。

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