受体亚型Y1和Y5参与神经肽Y的肾脏效应。

Receptor subtypes Y1 and Y5 are involved in the renal effects of neuropeptide Y.

作者信息

Bischoff A, Avramidis P, Erdbrügger W, Münter K, Michel M C

机构信息

Department of Medicine, University of Essen, Germany.

出版信息

Br J Pharmacol. 1997 Apr;120(7):1335-43. doi: 10.1038/sj.bjp.0701028.

DOI:10.1038/sj.bjp.0701028

PMID:9105710

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1564592/

Abstract

Systemic infusion of neuropeptide Y (NPY) reduces renal blood flow and can concomitantly increase diuresis, natriuresis and calciuresis in anaesthetized rats. The present study was designed to investigate whether the apparently contradictory NPY effects on renal blood flow and urine formation and composition are mediated by distinct NPY receptor subtypes. 2. NPY and its analogues, peptide YY (PYY), [Leu31, Pro34]NPY and NPY13-36, were infused in incremental doses of 0.3, 1 and 3 micrograms kg-1 min-1 for 45 min each and the results compared to those obtained in vehicle-infused rats. Renal blood flow was monitored in 1-5 min intervals, while urine excretion and composition were determined in 15 min collection periods. Plasma renin activity and aldosterone concentrations were measured at the end of the final infusion period. 3. Relative to vehicle NPY, PYY and [Leu31, Pro34]NPY dose-dependently reduced renal blood flow and increased diuresis, natriuresis and calciuresis with roughly similar potency; NPY13-36 slightly but significantly increased renal blood flow but had no effect on diuresis, natriuresis and calciuresis. None of the peptides significantly affected endogenous creatinine clearance or kaliuresis. 4. Plasma renin activity was significantly reduced by PYY. Quantitatively similar reductions were observed with NPY and [Leu31, Pro34]NPY but failed to reach statistical significance with the given number of experiments. NPY13-36 did not reduce plasma renin activity. None of the peptides significantly affected plasma aldosterone concentrations. 5. In another series of experiments infusion of PYY3-36 (2 micrograms kg-1 min-1 for 120 min) did not reduce renal blood flow but significantly enhanced diuresis and natriuresis to a similar extent as the NPY 2 micrograms kg-1 min-1. 6. In a final series of experiments the Y1-selective antagonist, BIBP 3226 (1 or 10 micrograms kg-1 min-1) dose-dependently antagonized reductions of renal blood flow elicited by bolus injections of NPY (0.1-30 micrograms kg-1). BIBP 3226 (10 micrograms kg-1 min-1) also inhibited the effects of a 120 min infusion of NPY (2 micrograms kg-1 min-1) on renal blood flow but had only minor inhibitory effects on enhancements of diuresis and did not significantly affect enhancements of natriuresis. 7. We conclude that NPY reduces renal blood via a classical Y1 subtype of NPY receptor. In contrast enhancements of diuresis, natriuresis and calciuresis occur via a distinct subtype which resembles the receptor that mediates NPY-induced enhancement of food intake.

摘要

对麻醉大鼠进行神经肽Y（NPY）的全身输注会减少肾血流量，同时可增加利尿、利钠和尿钙排泄。本研究旨在探究NPY对肾血流量以及尿液生成和成分的明显矛盾作用是否由不同的NPY受体亚型介导。2. 以0.3、1和3微克/千克体重·分钟的递增剂量分别输注NPY及其类似物肽YY（PYY）、[亮氨酸31，脯氨酸34]NPY和NPY13 - 36，每次输注45分钟，将结果与输注溶媒的大鼠所得结果进行比较。每隔1 - 5分钟监测肾血流量，同时在15分钟的收集期内测定尿液排泄和成分。在最后一次输注期结束时测量血浆肾素活性和醛固酮浓度。3. 相对于溶媒，NPY、PYY和[亮氨酸31，脯氨酸34]NPY剂量依赖性地减少肾血流量，并增加利尿、利钠和尿钙排泄，效力大致相似；NPY13 - 36轻微但显著增加肾血流量，但对利尿、利钠和尿钙排泄无影响。这些肽均未显著影响内生肌酐清除率或尿钾排泄。4. PYY显著降低血浆肾素活性。NPY和[亮氨酸31，脯氨酸34]NPY观察到数量上相似的降低，但在给定的实验次数下未达到统计学显著性。NPY13 - 36未降低血浆肾素活性。这些肽均未显著影响血浆醛固酮浓度。5. 在另一系列实验中，输注PYY3 - 36（2微克/千克体重·分钟，持续120分钟）未降低肾血流量，但显著增强利尿和利钠作用，程度与输注2微克/千克体重·分钟的NPY相似。6. 在最后一系列实验中，Y1选择性拮抗剂BIBP 3226（1或10微克/千克体重·分钟）剂量依赖性地拮抗大剂量注射NPY（0.1 - 30微克/千克体重）引起的肾血流量降低。BIBP 3226（10微克/千克体重·分钟）也抑制了120分钟输注NPY（2微克/千克体重·分钟）对肾血流量的影响，但对利尿增强作用仅有轻微抑制作用，且未显著影响利钠增强作用。7. 我们得出结论，NPY通过经典的NPY受体Y1亚型减少肾血流量。相比之下，利尿、利钠和尿钙排泄的增强是通过一种不同的亚型发生的，该亚型类似于介导NPY诱导食物摄入增加的受体。