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首页> 外文期刊>Hypertension research: Official journal of the Japanese Society of Hypertension >Eplerenone potentiates protective effects of amlodipine against cardiovascular injury in salt-sensitive hypertensive rats.
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Eplerenone potentiates protective effects of amlodipine against cardiovascular injury in salt-sensitive hypertensive rats.

机译:依普利农可增强氨氯地平对盐敏感性高血压大鼠心血管损伤的保护作用。

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摘要

The clinical value of the combination of amlodipine and eplerenone is unclear. This study was undertaken to test whether eplerenone potentiates the protective effects of amlodipine against hypertensive cardiovascular injury. Salt-loaded Dahl salt-sensitive hypertensive rats (DS rats) were given (1) vehicle, (2) an antihypertensive dose of amlodipine, (3) a non-antihypertensive dose of eplerenone or (4) combined amlodipine and eplerenone for 6 weeks, and the effects on cardiovascular injuries were compared. There was no significant difference among the four groups regarding plasma aldosterone, urine volume or urinary electrolytes. A subpressor dose of eplerenone markedly ameliorated vascular endothelial dysfunction, cardiac inflammation and fibrosis in DS rats to a similar degree as an antihypertensive dose of amlodipine. Addition of eplerenone to amlodipine, without affecting blood pressure, enhanced the improvement by amlodipine of vascular endothelial function, cardiac inflammation, fibrosis and diastolic dysfunction in DS rats. Additive beneficial effects of eplerenone were attributed to additive potentiation of eNOS and Akt phosphorylation and additive reduction of oxidative stress. Eplerenone significantly attenuated cardiovascular NADPH oxidase activity by reducing gp91(phox) upregulation and attenuated the upregulation of cardiovascular AT1 receptor, but amlodipine failed to affect them. Thus, the normalization by eplerenone of gp91(phox) and AT1 receptor upregulation seems to be at least partially responsible for the additive benefits of eplerenone in the prevention of hypertensive cardiovascular injury. The combination of amlodipine and eplerenone may be a promising therapeutic strategy for cardiovascular disease in salt-sensitive hypertension.
机译:氨氯地平和依普利农联合的临床价值尚不清楚。进行该研究以检验依普利农是否增强氨氯地平对高血压性心血管损伤的保护作用。给予盐载Dahl盐敏感性高血压大鼠(DS大鼠)(1)媒介物,(2)抗高血压剂量的氨氯地平,(3)非抗高血压剂量的依普利农,或(4)氨氯地平和依普利农合用6周,并比较了对心血管损伤的影响。血浆醛固酮,尿量或尿电解质在四组之间没有显着差异。降压剂量的依普利农可明显改善DS大鼠的血管内皮功能障碍,心脏炎症和纤维化,其程度与氨氯地平的降压剂量相似。在不影响血压的情况下,将依普利农添加到氨氯地平中,可增强氨氯地平对DS大鼠血管内皮功能,心脏炎症,纤维化和舒张功能障碍的改善作用。依普利农的附加有益作用归因于eNOS和Akt磷酸化的加成增强作用以及氧化应激的加成降低。依普利农通过降低gp91(phox)上调显着减弱了心血管NADPH氧化酶的活性,并减弱了心血管AT1受体的上调,但氨氯地平未能影响它们。因此,依普利农对gp91(phox)的正常化和AT1受体上调似乎至少部分负责依普利农在预防高血压性心血管损伤中的附加益处。氨氯地平和依普利农的组合可能是盐敏感性高血压中心血管疾病的有前途的治疗策略。

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