急性肾血管性高血压犬肾内钾likrein-kinin活性。

Renal physiology Pub Date : 1988-01-01 DOI:10.1159/000173140

P S Verma, J A Gagnon, R L Miller

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引用次数: 5

摘要

在肾动脉收缩引起的肾血管性高血压急性期和替普肽抑制肾动激酶II期间，研究了肾内钾likrein- kininin系统。通过激肽原酶和溶脂试验测定的钾likrein样活性在肾动脉收缩时升高(p < 0.5)和(p < 0.01)。替普罗肽组进一步增加肾皮质钾化钾素样活性，抑制激酶II活性(p < 0.01)。抑制激肽酶II后，血浆激肽原浓度也显著降低(p < 0.01)。这些结果表明，抑制激肽酶II可能会增加肾内和血浆激肽的水平，而激肽肽降解的减少可能对替普肽的急性高血压作用起重要作用。

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Intrarenal kallikrein-kinin activity in acute renovascular hypertension in dogs.

The intrarenal kallikrein-kinin system was studied during the acute phase of renovascular hypertension induced by renal artery constriction and during teprotide inhibition of kininase II in the dog. Kallikrein-like activity measured by both kininogenase and esterolytic assays, was increased during renal artery constriction (p less than 0.5) and (p less than 0.01). The administration of teprotide resulted in a further increase of renal cortical kallikrein-like activity and inhibited kininase II activity (p less than 0.01). Following the inhibition of kininase II, the plasma concentration of kininogen was also significantly decreased (p less than 0.01). These results suggest that kininase II inhibition may increase levels of intrarenal and plasma kinins and that decreased degradation of kinin peptides may contribute significantly to the acute hypertensive effect of teprotide.

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Renal physiology

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