Priviero Fernanda B M, Teixeira Cleber E, Claudino Mário A, De Nucci Gilberto, Zanesco Angelina, Antunes Edson
Department of Pharmacology, Faculty of Medical Sciences, State University of Campinas, P.O. Box 6111, 13084-971, Campinas, São Paulo, Brazil.
Eur J Pharmacol. 2007 Oct 1;571(2-3):189-96. doi: 10.1016/j.ejphar.2007.05.060. Epub 2007 Jun 13.
Long-term propranolol treatment reduces arterial blood pressure in hypertensive individuals mainly by reducing peripheral vascular resistance, but mechanisms underlying their vasodilatory effect remain poorly investigated. This study aimed to investigate whether long-term propranolol administration ameliorates the impairment of relaxing responses of aorta and mesenteric artery from rats made hypertensive by chronic nitric oxide (NO) deficiency, and underlying mechanisms mediating this phenomenon. Male Wistar rats were treated with N(omega)-Nitro-L-arginine methyl ester (L-NAME; 20 mg/rat/day) for four weeks. DL-Propranolol (30 mg/rat/day) was given concomitantly to L-NAME in the drinking water. Treatment with L-NAME markedly increased blood pressure, an effect largely attenuated by DL-propranolol. In phenylephrine-precontracted aortic rings, the reduction of relaxing responses for acetylcholine (0.001-10 microM) in L-NAME group was not modified by DL-propranolol, whereas in mesenteric rings the impairment of acetylcholine-induced relaxation by L-NAME was significantly attenuated by DL-propranolol. In mesenteric rings precontracted with KCl (80 mM), DL-propranolol failed to attenuate the impairment of acetylcholine-induced relaxation by L-NAME. The contractile responses to extracellular CaCl2 (1-10 mM) were increased in L-NAME group, and co-treatment with DL-propranolol reduced this response in both preparations in most Ca2+ concentrations used. The NO2/NO3 plasma levels and superoxide dismutase (SOD) activity were reduced in L-NAME-treated rats, both of which were significantly prevented by DL-propranolol. In conclusion, propranolol-induced amplification of the relaxation to acetylcholine in mesenteric arteries from L-NAME-treated rats is sensitive to depolarization. Additional mechanisms involving blockade of Ca2+ entry in the vascular smooth muscle and increase in NO bioavailability contributes to beneficial effects of long-term propranolol treatment.
长期使用普萘洛尔治疗主要通过降低外周血管阻力来降低高血压患者的动脉血压,但其血管舒张作用的潜在机制仍未得到充分研究。本研究旨在探讨长期给予普萘洛尔是否能改善慢性一氧化氮(NO)缺乏所致高血压大鼠主动脉和肠系膜动脉舒张反应的损害,以及介导这一现象的潜在机制。雄性Wistar大鼠用N(ω)-硝基-L-精氨酸甲酯(L-NAME;20mg/大鼠/天)治疗四周。在饮用水中同时给予L-NAME和DL-普萘洛尔(30mg/大鼠/天)。L-NAME治疗显著升高血压,DL-普萘洛尔可大大减弱这一作用。在去氧肾上腺素预收缩的主动脉环中,L-NAME组对乙酰胆碱(0.001-10μM)舒张反应的降低未被DL-普萘洛尔改变,而在肠系膜环中,L-NAME所致乙酰胆碱诱导的舒张损害被DL-普萘洛尔显著减弱。在氯化钾(80mM)预收缩的肠系膜环中,DL-普萘洛尔未能减弱L-NAME所致乙酰胆碱诱导的舒张损害。L-NAME组对细胞外氯化钙(1-10mM)的收缩反应增强,在大多数使用的钙离子浓度下,联合使用DL-普萘洛尔可降低两种制剂中的这种反应。L-NAME处理的大鼠血浆中NO2/NO3水平和超氧化物歧化酶(SOD)活性降低,两者均被DL-普萘洛尔显著预防。总之,普萘洛尔诱导L-NAME处理大鼠肠系膜动脉对乙酰胆碱舒张反应的增强对去极化敏感。涉及阻断血管平滑肌钙离子内流和增加NO生物利用度的其他机制有助于长期普萘洛尔治疗的有益效果。
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