肾素-血管紧张素与交感神经系统在压力过载心肌肥厚大鼠模型中的相互作用

Autonomic and Autacoid Pharmacology Pub Date : 2009-09-09 DOI:10.1111/j.1474-8665.2009.00445.x

H. A. Rathore, A. S. Munavvar, N. A. Abdullah, A. H. Khan, B. Fathihah, M. H. NurJannah, N. A. Raisa, K. R. L. Anand Swarup, M. H. Abdullah, I. M. Salman, E. J. Johns

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引用次数: 12

摘要

心脏负荷增加会激活神经激素，从而增加肌肉量并使收缩力沿弗兰克-斯塔林曲线向右移动。2本研究探讨了SNS和RAS在主动脉束带导致心脏肥厚后血管反应性的相互作用。取Sprague Dawley大鼠3只(180 ~ 200 g)，分为6组;正常、假手术、主动脉束带(AB)、氯沙坦治疗的主动脉束带(ABLOS)、6-羟多巴胺治疗的主动脉束带(ABSYMP)和氯沙坦和6-羟多巴胺治疗的主动脉束带(ABSYMPLOS)。第0天在肾上主动脉周围行缩窄带，第37天至第44天给予药物治疗。在第45天测量血管加压素对去甲肾上腺素、苯肾上腺素、甲氧胺和血管紧张素II的反应。4 . MAP对所有血管活性药物的反应大小(以百分比变化表示)在正常组和假手术组相似，但在AB组有所降低。ABLOS组对ANGII的反应减弱，而ABSYM组的所有反应均增强。5观察到两个系统之间的正相互作用，α 1a -肾上腺素受体被确定为SNS的主要成分和RAS的AT1受体诱导血管加压作用。

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Interaction between renin–angiotensin and sympathetic nervous systems in a rat model of pressure overload cardiac hypertrophy

1 A raised cardiac workload activates neurohormones which will increase muscle mass and shift contractility to the right along the Frank-Starling curve.

2 This study examined the interaction between the SNS and RAS in contributing to vascular responsiveness following the development of cardiac hypertrophy due to aortic banding.

3 Sprague Dawley rats (180–200 g) were assigned to one of six groups; Normal, Sham-operated, Aortic Banded (AB), Aortic Banded treated with losartan (ABLOS), Aortic Banded treated with 6-hydroxydopamine (ABSYMP) and Aortic banded treated with both losartan and 6-hydroxydopamine (ABSYMPLOS). A constricting band was placed around the supra renal aorta on day zero with drug treatment from day 37 to day 44. Vasopressor responses to noradrenaline, phenylephrine, methoxamine and angiotensin II were measured on day 45.

4 The magnitudes of the MAP responses to all vasoactive agents, expressed as percentage changes, were similar in Normal and Sham groups, but reduced in the AB group. ABLOS group showed attenuated response to ANGII whereas all responses were enhanced in the ABSYM group.

5 A positive interaction between the two systems was observed with α_1A-adrenoceptors identified as a major component of SNS and AT₁ receptors of RAS to induce vasopressor effects.

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Autonomic and Autacoid Pharmacology

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