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肾脏N-甲基-D-天冬氨酸受体可独立刺激近端重吸收和肾小球滤过。

Renal NMDA receptors independently stimulate proximal reabsorption and glomerular filtration.

作者信息

Deng Aihua, Thomson Scott C

机构信息

Department of Medicine, University of California School of Medicine and VASDHS, San Diego, CA 92161, USA.

出版信息

Am J Physiol Renal Physiol. 2009 May;296(5):F976-82. doi: 10.1152/ajprenal.90391.2008. Epub 2009 Mar 11.

Abstract

N-methyl-D-aspartate receptors (NMDA) are expressed in the kidney, where little is known of their functional role. Several series of micropuncture experiments were performed in hydropenic rats using the NMDA channel blocker, MK801, and the NMDA coagonist, L-glycine, to probe NMDA for effects on single-nephron glomerular filtration rate (SNGFR) and proximal reabsorption (J(prox)). During intravenous infusion of MK801 or L-glycine, Henle's loop was perfused to manipulate SNGFR via tubuloglomerular feedback (TGF), thereby facilitating analysis of glomerulotubular balance. To confirm local actions on the kidney, MK801 was delivered to the glomerulus by microperfusion past the macula densa and to the proximal tubule by microperfusion into the early S1 segment. By all measures, MK801 acted on the glomerulus to reduce SNGFR, and acted on the proximal tubule to suppress J(prox), while having no effect on the responsiveness of TGF. L-Glycine raised SNGFR, dampened the TGF response, and could not be proved to independently stimulate proximal reabsorption. NMDA exerts a tonic vasodilatory influence on the glomerulus and a proreabsorptive effect on the proximal tubule. These combined effects allow NMDA to modulate SNGFR with minimal impact on late proximal flow. The full effects of L-glycine infusion on proximal tubule and TGF response do not extrapolate from the response to NMDA blockade.

摘要

N-甲基-D-天冬氨酸受体(NMDA)在肾脏中表达,但其功能作用鲜为人知。在缺水大鼠中进行了一系列微穿刺实验,使用NMDA通道阻滞剂MK801和NMDA协同激动剂L-甘氨酸,以探究NMDA对单肾单位肾小球滤过率(SNGFR)和近端重吸收(J(prox))的影响。在静脉输注MK801或L-甘氨酸期间,通过灌注髓袢来通过管球反馈(TGF)操纵SNGFR,从而便于分析球管平衡。为了证实对肾脏的局部作用,通过微灌注将MK801输送到致密斑后的肾小球,并通过微灌注到早期S1段输送到近端小管。通过所有测量方法,MK801作用于肾小球以降低SNGFR,并作用于近端小管以抑制J(prox),而对TGF的反应性没有影响。L-甘氨酸提高了SNGFR,减弱了TGF反应,并且无法证明其能独立刺激近端重吸收。NMDA对肾小球施加持续性血管舒张影响,并对近端小管产生促重吸收作用。这些联合作用使NMDA能够调节SNGFR,同时对近端晚期流量的影响最小。L-甘氨酸输注对近端小管和TGF反应的全部影响不能从对NMDA阻断的反应中推断出来。

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