在正常血压和高血压大鼠中,短期输注血管紧张素-(1-7)增强缓激肽的降压作用。
Potentiation of the hypotensive effect of bradykinin by short-term infusion of angiotensin-(1-7) in normotensive and hypertensive rats.
作者信息
Lima C V, Paula R D, Resende F L, Khosla M C, Santos R A
机构信息
Departamento de Fisiologia e Biofísica, Instituto de Ciências Biológicas, Universidade Federale de Minas Gerais, Belo Horizonte, Brazil.
出版信息
Hypertension. 1997 Sep;30(3 Pt 2):542-8. doi: 10.1161/01.hyp.30.3.542.
In this study we evaluated the effect of angiotensin-(1-7) on the hypotensive action of bradykinin (BK) in normotensive rats, renal hypertensive rats (RHR), and spontaneously hypertensive rats (SHR). In addition, we evaluated the effect of angiotensin-converting enzyme (ACE) inhibition with enalaprilat treatment (10 mg/kg I.V.) on the BK-potentiating activity of Ang-(1-7). Renal hypertension was produced by aorta coarctation between the origin of renal arteries. Ang-(1-7) (0.3 pmol/min) or saline (0.9% NaCl, 5 microL/min) was infused intravenously in conscious male Wistar rats, adult SHR, or RHR. Intravenous bolus injections of BK (0.1 to 1.6 nmol in RHR and SHR; 0.625 to 5 nmol in Wistar rats) were made before and within 30 and 60 minutes of Ang-(1-7) infusion. Ang-(1-7) infusion did not change mean arterial pressure (MAP) of Wistar rats (MAP=97+/-3 mm Hg), RHR (MAP=173+/-3 mm Hg), or SHR (MAP=177+/-5 mm Hg). In Wistar rats, Ang-(1-7) increased the BK hypotensive effect by 24+/-6% within 60 minutes of infusion. No significant changes were observed at 30 minutes of infusion. In additional groups of rats, Ang-(1-7) (5 pmol/min, n=5) was infused alone or combined with its selective antagonist D-Ala7-Ang-(1-7) (A-779) (5 pmol/min, n=6). The bradykinin-potentiating activity of Ang-(1-7) was completely abolished by A-779. In SHR and RHR, Ang-(1-7) significantly increased the hypotensive effect of BK by 59+/-8% and 57+/-9.8%, respectively, within 60 minutes of infusion. No significant changes were observed with saline infusion. In Wistar rats, enalaprilat treatment increased the BK-potentiating activity of Ang-(1-7) transforming the effect of 0.3 pmol/min into that observed with a rate 16-fold higher (5 pmol/min). On the other hand, in SHR enalaprilat did not change the Ang-(1-7) effect, while it abolished the BK potentiation in RHR. Our data show that the BK-potentiating activity of Ang-(1-7) is preserved and even augmented in hypertensive rats. The finding that the BK-potentiating activity of Ang-(1-7) could be demonstrated at a very low infusion rate suggests that this angiotensin can act as an endogenous modulator of the vascular actions of kinins. ACE inhibition can influence differently the BK-potentiating activity of Ang-(1-7) in normotensive and hypertensive rats.
在本研究中,我们评估了血管紧张素 -(1 - 7)对正常血压大鼠、肾性高血压大鼠(RHR)和自发性高血压大鼠(SHR)中缓激肽(BK)降压作用的影响。此外,我们评估了依那普利拉治疗(静脉注射10 mg/kg)抑制血管紧张素转换酶(ACE)对血管紧张素 -(1 - 7)增强BK活性的影响。肾性高血压通过肾动脉起始处的主动脉缩窄产生。将血管紧张素 -(1 - 7)(0.3 pmol/分钟)或生理盐水(0.9% NaCl,5 μL/分钟)静脉输注到清醒的雄性Wistar大鼠、成年SHR或RHR中。在血管紧张素 -(1 - 7)输注前以及输注后30分钟和60分钟内静脉推注BK(RHR和SHR中为0.1至1.6 nmol;Wistar大鼠中为0.625至5 nmol)。血管紧张素 -(1 - 7)输注未改变Wistar大鼠(平均动脉压[MAP]=97±3 mmHg)、RHR(MAP=173±3 mmHg)或SHR(MAP=177±5 mmHg)的平均动脉压。在Wistar大鼠中,血管紧张素 -(1 - 7)在输注60分钟内使BK的降压作用增加了24±6%。输注30分钟时未观察到显著变化。在另外几组大鼠中,单独输注血管紧张素 -(1 - 7)(5 pmol/分钟,n = 5)或与其选择性拮抗剂D - Ala7 - 血管紧张素 -(1 - 7)(A - 779)(5 pmol/分钟,n = 6)联合输注。血管紧张素 -(1 - 7)增强BK的活性被A - 779完全消除。在SHR和RHR中,血管紧张素 -(1 - 7)在输注60分钟内分别使BK的降压作用显著增加了59±8%和57±9.8%。输注生理盐水未观察到显著变化。在Wistar大鼠中,依那普利拉治疗增强了血管紧张素 -(1 - 7)增强BK的活性,将0.3 pmol/分钟的作用转变为以高16倍的速率(5 pmol/分钟)观察到的作用。另一方面,在SHR中依那普利拉未改变血管紧张素 -(1 - 7)的作用,而在RHR中它消除了BK的增强作用。我们的数据表明,血管紧张素 -(1 - 7)增强BK的活性在高血压大鼠中得以保留甚至增强。血管紧张素 -(1 - 7)在非常低的输注速率下就能增强BK活性这一发现表明,这种血管紧张素可作为激肽血管作用的内源性调节剂。ACE抑制在正常血压和高血压大鼠中对血管紧张素 -(1 - 7)增强BK活性的影响不同。
Zotero 插件