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新生大鼠肾脏发育的药理学探究

Pharmacologic probing of renal development in the neonatal rat.

作者信息

Gray J A, Kavlock R J

出版信息

Biol Neonate. 1986;50(4):182-91. doi: 10.1159/000242598.

Abstract

This study was designed to examine the ontogeny of renal functions in the neonatal rat using various pharmacologic agents as probes. The renal responses of 2-, 6-, and 10-day-old rats to diuretic agents known to act on proximal tubules, loops of Henle and distal tubules were assessed. These included acetazolamide, furosemide, mercaptomerin, chlorothiazide and amiloride. Following administration of a diuretic agent, urine was collected at 90-min intervals for 6 h and urine volume, osmolality, chloride and pH were measured. Acetazolamide, furosemide, chlorothiazide and amiloride induced diuresis at each age indicating that the respective reabsorptive mechanisms were present and functional by 2 days of age. At all ages furosemide evoked a maximal response in eliminating the interstitial fluid gradient as indicated by the formation of an isosmotic urine in treated pups. However, the volume of the diuresis at 2 days of age was half those at 6 and 10 days, reflecting enhanced activity of the countercurrent multiplication apparatus in the maturing pups. Administration of mercaptomerin did not produce pharmacologic diuresis, but rather resulted in acute renal failure; although the nephrotoxicity was to a lesser extent in 2-day-old pups. The ability of the neonatal rat to respond to these pharmacologic probes demonstrates that the integrity of these renal functions is established in this species early in postnatal life.

摘要

本研究旨在使用各种药理学试剂作为探针,研究新生大鼠肾功能的个体发生。评估了2日龄、6日龄和10日龄大鼠对已知作用于近端小管、髓袢和远端小管的利尿剂的肾脏反应。这些药物包括乙酰唑胺、呋塞米、汞撒利、氯噻嗪和阿米洛利。给予利尿剂后,每隔90分钟收集尿液6小时,并测量尿量、渗透压、氯化物和pH值。乙酰唑胺、呋塞米、氯噻嗪和阿米洛利在各年龄均诱导利尿,表明相应的重吸收机制在2日龄时已存在并发挥作用。在所有年龄,呋塞米在消除间质液梯度方面引起最大反应,这表现为经处理的幼崽形成等渗尿液。然而,2日龄时的尿量是6日龄和10日龄时的一半,这反映了成熟幼崽中逆流倍增装置的活性增强。汞撒利的给药并未产生药理学利尿作用,反而导致急性肾衰竭;尽管2日龄幼崽的肾毒性程度较轻。新生大鼠对这些药理学探针的反应能力表明,这些肾功能的完整性在该物种出生后早期就已建立。

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