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首页> 外文期刊>Hypertension: An Official Journal of the American Heart Association >Renoprotective effects of felodipine and/or enalapril in spontaneously hypertensive rats with and without L-NAME (published erratum appears in Hypertension 1998 Apr;31(4):1046)
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Renoprotective effects of felodipine and/or enalapril in spontaneously hypertensive rats with and without L-NAME (published erratum appears in Hypertension 1998 Apr;31(4):1046)

机译:非洛地平和/或依那普利对具有和不具有L-NAME的自发性高血压大鼠的肾保护作用(发表的勘误表见高血压1998 Apr; 31(4):1046)

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摘要

To determine the renoprotective effects of a calcium antagonist (felodipine) and an angiotensin-converting enzyme (ACE) inhibitor (enalapril), alone or in combination, 10 groups of 19-week-old spontaneously hypertensive rats (SHR) (with or without N(G)-nitro-L-arginine methyl ester [L-NAME]) were studied using renal micropuncture techniques. Group 1 (control), group 2 (felodipine, 30 mg x kg(-1) x d[-1]), group 3 (enalapril, 30 mg x kg(-1) x d[-1]), and group 4 (felodipine plus enalapril, 15 mg x kg(-1) x d(-1) each agent) were studied after 3 weeks of treatment without L-NAME. L-NAME (50 mg/L) cotreatment was administered in drinking water to groups 6 through 10 using the same doses of each agent as in groups 1 through 4: group 5 (only L-NAME), group 6 (felodipine), group 7 (enalapril), and group 8 (felodipine plus enalapril). Groups 9 and 10 received L-NAME initially for 3 weeks followed by felodipine or felodipine plus enalapril, respectively, for the subsequent 3 weeks. All three treatments resulted in reductions in mean arterial pressure and total peripheral vascular resistance (P<.001) that were associated with important structural and functional renal microcirculatory improvements. Thus, the pathological nephrosclerosis (subcapsular and juxtamedullary) glomerular and arteriolar injury scores were improved (P<.05 at least) in association with normalization of afferent and efferent arteriolar resistances, and single-nephron glomerular filtration rate, plasma flow, and blood flow were significantly improved, as well as the ultrafiltration coefficient (compared with group 5, L-NAME). Thus, the calcium antagonist felodipine, alone or in combination with an ACE inhibitor, not only prevented but also reversed L-NAME-exacerbated hypertensive nephrosclerosis in SHR.
机译:为了确定钙拮抗剂(非洛地平)和血管​​紧张素转换酶(ACE)抑制剂(依那普利)的肾脏保护作用,单独或组合使用10组19周龄的自发性高血压大鼠(SHR)(有或没有N (G)-硝基-L-精氨酸甲酯[L-NAME])使用肾脏微穿刺技术进行了研究。第1组(对照组),第2组(非洛地平30 mg x kg(-1)xd [-1]),第3组(依那普利30 mg x kg(-1)xd [-1])和第4组(非L-NAME治疗3周后,研究了非洛地平加依那普利(15 mg x kg(-1)xd(-1)每种药物)。将L-NAME(50 mg / L)协同治疗在饮用水中施用至第6至10组,使用与第1-4组相同的每种药物剂量:第5组(仅L-NAME),第6组(非洛地平),第7(依那普利)和第8组(非洛地平加依那普利)。第9组和第10组最初接受L-NAME治疗3周,然后分别接受非洛地平或非洛地平加依那普利治疗,随后3周。所有这三种治疗均导致平均​​动脉压降低和总外周血管阻力降低(P <.001),这与重要的结构和功能性肾脏微循环改善有关。因此,与传入和传出小动脉阻力的正常化以及单肾单位肾小球滤过率,血浆流量和血流量的正常化相比,病理性肾硬化(囊下和近髓)肾小球和小动脉损伤评分得以改善(至少P <.05)以及超滤系数(与第5组相比,L-NAME)均得到显着改善。因此,钙拮抗剂非洛地平单独或与ACE抑制剂联合使用不仅可以预防SHR中的L-NAME加重性高血压肾硬化,而且还可以逆转其逆转。

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