Renal functional and metabolic studies on the role of preventive measures in experimental acute ischemic renal failure.

H J Kramer, A Neumark, S Schmidt, D Klingmüller, K Glänzer
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引用次数: 20

Abstract

In the present study 1 h of total occlusion of the left renal artery in conscious rats was chosen as experimental model of ischemic acute renal failure (ARF), while the contralateral kidney was left intact. Chronic high dietary sodium intake, acute isotonic saline infusion, or administration of saralasin did not protect from ARF. Furosemide, mannitol, and verapamil converted oliguric into non-oliguric ARF in 100%, 75%, and 60% of the animals, resp. Protection from oliguria and preservation of GFR inversely correlated with the depression of cortical ATP-concentration (control: 1.32 +/- 0.07 mumoles/g wet weight) 6 h after ischemia by 16%, 41%, and 58% in mannitol- and verapamil- treated rats and in untreated rats, resp. At this time, Na-K-ATPase enzyme activities in renal cortex and papilla were unaffected, while enzyme activity in outer medulla was suppressed from 15.4 +/- 1.4 to 9.4 +/- 1.0 mumoles Pi/mg protein h in all groups of animals. The results suggest that in this model of ARF renal ischemia not only affects cellular energy supply in renal cortex but also causes severe structural and functional impairment in the outer medulla, probably leading to tubular obstruction and depression of glomerular function. Pharmacological protection from ischemic oliguric ARF cannot be achieved by prior induction of high urine flow rates alone but depends on the degree of metabolic and functional reserve of the injured tubular epithelium.

预防措施在实验性急性缺血性肾功能衰竭中的作用的肾功能和代谢研究。
本研究选择清醒大鼠左肾动脉完全闭塞1 h作为缺血性急性肾功能衰竭(ARF)的实验模型,对侧肾脏保持完整。长期高钠饮食摄入,急性等渗生理盐水输注,或给予萨拉拉西不能预防ARF。速尿、甘露醇和维拉帕米分别在100%、75%和60%的动物中将低尿酸转化为非低尿酸ARF。甘尼醇和维拉帕米处理大鼠和未处理大鼠缺血6小时后皮质atp浓度(对照组:1.32 +/- 0.07摩尔/g湿重)下降16%,41%和58%,对少尿的保护和GFR的保存呈负相关。此时,肾皮质和乳头的na - k - atp酶活性未受影响,而外髓质酶活性从15.4 +/- 1.4抑制到9.4 +/- 1.0摩尔π /mg蛋白h。结果提示,在该ARF模型中,肾缺血不仅影响肾皮质细胞能量供应,而且引起外髓质严重的结构和功能损伤,可能导致小管梗阻和肾小球功能下降。对缺血性少尿性ARF的药理学保护不能仅仅通过预先诱导高尿流率来实现,而是取决于受损小管上皮的代谢和功能储备程度。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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