AT1和ETA受体拮抗剂、坎地沙坦和A-127722在doca盐高血压大鼠中的联合作用

David M Pollock , Vimal K Derebail , Tatsuo Yamamoto , Jennifer S Pollock
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引用次数: 18

摘要

最近的一些研究提供了证据,血管紧张素II (Ang II)的许多血流动力学和有丝分裂作用是由内皮素-1 (ET-1)介导的。我们假设在醋酸去氧皮质酮(DOCA)-盐模型中,Ang II和ET-1协同作用促进了恶性高血压和肾功能障碍的肾功能下降和肾纤维化的发展。通过实验确定ETA受体拮抗剂(A-127722)和AT1受体拮抗剂(坎地沙坦西列地酯)对肾纤维化发展和肾功能下降的影响。对雄性Sprague-Dawley大鼠进行手术,切除右肾并皮下植入含有DOCA的缓释颗粒。doca处理的大鼠同时给予0.9% NaCl饮水。术后恢复后,大鼠接受以下四种治疗中的一种:(1)坎地沙坦西莱西地酯(10 mg/kg/天),(2)A-127722 (10 mg/kg/天),(3)坎地沙坦西莱西地酯加A-127722,或(4)未经治疗的对照组。在3周的治疗过程中,所有组的收缩压均升高。然而,在联合使用A-127722和坎地沙坦的组中,这种增加明显减弱,而单独使用坎地沙坦则没有。肌酸酐清除率,用于GFR的测量,在使用一种或两种药物治疗的大鼠中显着更高。研究结束时,取肾髓质组织,测定TGF-β和纤维连接蛋白含量(ELISA)。无论是ETA、AT1还是ETA和AT1受体联合阻断均未降低TGF-β水平。同样,各组间纤维连接蛋白含量相似。这些研究表明,在这种非肾素依赖性高血压模型中,联合阻断ETA和AT1受体可能会对血流动力学产生一定的改善,但对肾损害的进展没有影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Combined effects of AT1 and ETA receptor antagonists, candesartan, and A-127722 in DOCA–salt hypertensive rats

Several recent studies have provided evidence that many of the hemodynamic and mitogenic actions of angiotensin II (Ang II) are mediated by endothelin-1 (ET-1). We hypothesized that Ang II and ET-1 act synergistically to promote a decline in renal function and the development of renal fibrosis in the deoxycorticosterone acetate (DOCA)-salt model of malignant hypertension and renal dysfunction. Experiments were conducted to determine the effects of ETA receptor antagonism (A-127722) and AT1 receptor antagonism (candesartan cilexetil) on the development of renal fibrosis and the decline of renal function. Surgery was conducted on male, Sprague–Dawley rats to remove the right kidney and implant subcutaneously a time-release pellet containing DOCA. DOCA-treated rats were also given 0.9% NaCl to drink. After recovery from surgery, rats received one of four treatments via the drinking solution: (1) candesartan cilexetil (10 mg/kg/day), (2) A-127722 (10 mg/kg/day), (3) candesartan cilexetil plus A-127722, or (4) untreated controls. Over the course of a 3-week treatment period, systolic arterial pressure in all groups were elevated. However, this increase was significantly attenuated in the group given combined A-127722 and candesartan, but not with candesartan alone. Creatinine clearance, used as a measure of GFR, was significantly higher in rats treated with either or both drugs. At the end of the study, renal medullary tissue was harvested for determination of TGF-β and fibronectin content (ELISA). TGF-β levels were not reduced by either ETA, AT1, or combined ETA and AT1 receptor blockade. Likewise, fibronectin content was similar among groups. These studies indicate that combined ETA and AT1 receptor blockade may produce some improvement on hemodynamics, but have no effect on progression of renal damage in this non-renin-dependent model of hypertension.

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