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苯基布他松对马体内速尿的肾脏效应及排泄的抑制作用

Attenuation by phenylbutazone of the renal effects and excretion of frusemide in horses.

作者信息

Dyke T M, Hinchcliff K W, Sams R A

机构信息

Department of Veterinary Clinical Sciences, College of Veterinary Medicine, The Ohio State University, Columbus 43210-1089, USA.

出版信息

Equine Vet J. 1999 Jul;31(4):289-95. doi: 10.1111/j.2042-3306.1999.tb03819.x.

Abstract

The objectives of this study were to determine the effect of phenylbutazone premedication on the pharmacokinetics and urinary excretion of frusemide in horses; and on frusemide-induced changes in urinary electrolyte excretion. Six Standardbred mares were used in a 3-way crossover design. The pharmacokinetics and renal effects of frusemide (1 mg/kg bwt i.v.) were studied with and without phenylbutazone premedication (8.8 mg/kg bwt per os 24 h before, followed by 4.4 mg/kg bwt i.v. 30 min before frusemide administration). A control (saline) treatment was also studied. Administration of frusemide without phenylbutazone led to diuresis, natriuresis, kaliuresis and chloruresis, and altered the ratio of sodium:chloride excretion from 0.4 to 1.0 in the first hour of diuresis. When frusemide and phenylbutazone were administered, sodium and chloride excretion in the first hour were significantly (P<0.05) reduced by 40 and 32%, respectively, when compared to frusemide administrationwithout phenylbutazone. The fractional clearance of sodium and chloride was also significantly reduced. Potassium excretion, potassium fractional clearance and the ratio of sodium to chloride excretion were not affected by administration of phenylbutazone. During peak diuresis, phenylbutazone did not affect the efficiency of frusemide with respect to electrolyte excretion. The plasma disposition of frusemide was not affected by phenylbutazone. However, the renal excretion of frusemide decreased by approximately 25%. We conclude that the decreased urinary excretion of frusemide by phenylbutazone led to an attenuation of frusemide-induced increases in urinary excretion of sodium and chloride. Since the efficiency of frusemide was not affected by phenylbutazone, we conclude that phenylbutazone attenuates the renal excretion of frusemide without inhibiting the intrarenal activity of frusemide in horses.

摘要

本研究的目的是确定保泰松预处理对马体内速尿的药代动力学和尿排泄的影响;以及对速尿引起的尿电解质排泄变化的影响。采用6匹标准赛马母马进行三交叉设计。研究了在有和没有保泰松预处理(给药前24小时口服8.8mg/kg体重,随后在速尿给药前30分钟静脉注射4.4mg/kg体重)的情况下速尿(1mg/kg体重静脉注射)的药代动力学和肾脏效应。还研究了对照(生理盐水)处理。未用保泰松给予速尿导致利尿、利钠、利尿钾和利尿氯,并在利尿的第一小时将钠:氯排泄率从0.4改变为1.0。当同时给予速尿和保泰松时,与未用保泰松给予速尿相比,第一小时的钠和氯排泄分别显著(P<0.05)减少了40%和32%。钠和氯的分数清除率也显著降低。保泰松的给药不影响钾排泄、钾分数清除率以及钠与氯排泄率。在利尿高峰期,保泰松对速尿的电解质排泄效率没有影响。保泰松不影响速尿的血浆处置。然而,速尿的肾脏排泄减少了约25%。我们得出结论,保泰松使速尿的尿排泄减少,导致速尿引起的钠和氯尿排泄增加减弱。由于速尿的效率不受保泰松影响,我们得出结论,保泰松减弱了速尿的肾脏排泄,而不抑制马体内速尿的肾内活性。

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