神经降压素对一氧化氮生成的负向调节作为SR 48692对大鼠利尿作用的一种潜在机制。

Negative modulation of nitric oxide production by neurotensin as a putative mechanism of the diuretic action of SR 48692 in rats.

作者信息

Croci T, Landi M, Gully D, Maffrand J P, Le Fur G, Manara L

机构信息

Sanofi-Midy Research Center, Milan, Italy.

出版信息

Br J Pharmacol. 1997 Apr;120(7):1312-8. doi: 10.1038/sj.bjp.0701016.

DOI:10.1038/sj.bjp.0701016

PMID:9105707

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1564587/

Abstract

We investigated the effect of the non-peptide neurotensin (NT) antagonist SR 48692 on renal function in rats and the involvement of nitric oxide (NO) in the diuretic action of this compound. 2. In fed animals, SR 48692 dose-dependently (0.5 to 12.5 mg kg-1, p.o., 0.03 to 1 mg kg-1, i.p. and 0.1 to 1 microgram/rat, i.c.v.) increased urine output and urinary excretion of Na+, K+ and Cl- and reduced urine osmolality. The diuretic activity was also evident in water-deprived, fasted animals and in fasted, water-loaded rats. 3. NT (0.1 microgram/rat, i.c.v.) had no effect on urine output in fed rats, but reduced the diuretic action of SR 48692 (1 microgram/rat, i.c.v.). The opposite result was obtained in fasted, water-loaded animals: NT dose-dependently (0.01 and 0.1 microgram/rat, i.c.v.) inhibited diuresis and this effect was significantly inhibited by i.c.v. SR 48692. In this experimental condition, SR 48692 did not further increase the on-going diuresis. 4. The NO synthesis inhibitor N(1)-nitro-L-arginine methyl ester (L-NAME; 30 mg kg-1, i.p.) alone had no effect on urine output in fed rats but prevented the diuretic action of i.c.v. or i.p. SR 48692; L-arginine (1 g kg-1, i.p.) but not D-arginine (1 g kg-1, i.p.) restored the SR 48692-dependent increase in diuresis, L-NAME had no effect on furosemide-stimulated diuresis. 5. Systemically administered L-NAME or i.c.v. NT in fasted, water-loaded rats significantly reduced water diuresis but this effect was no longer seen in animals given i.p. L-arginine. Rats receiving i.c.v. NT, whose diuresis was significantly reduced, also excreted less nitrates and nitrites in urine. 6. Increased diuresis after central or systemic administration of SR 48692 to fed rats was paralleled by increased urinary excretion of nitrates and nitrites, this being consistent with peripheral enhancement of NO production after NT-receptor blockade by SR 48692. The increase in diuresis after furosemide also involved an increase of nitrates and nitrites in urine, but this effect was about half that attained with an equipotent diuretic dose of SR 48692. 7. In fed rats, the NO donor isosorbide-dinitrate, reduced systolic blood pressure (unlike SR 48692 which did not affect blood pressure) but also dose-dependently (1 and 5 mg kg-1, i.p.) stimulated urine output. 8. The overall effects of SR 48692 strongly support a link between the actions of endogenous NT, AVP and peripheral NO production in the modulation of renal excretion of water, Na+, K+ and Cl-.

摘要

我们研究了非肽类神经降压素（NT）拮抗剂SR 48692对大鼠肾功能的影响，以及一氧化氮（NO）在该化合物利尿作用中的参与情况。2. 在进食的动物中，SR 48692剂量依赖性地（口服0.5至12.5 mg/kg，腹腔注射0.03至1 mg/kg，脑室内注射0.1至1 μg/只大鼠）增加尿量以及Na+、K+和Cl-的尿排泄量，并降低尿渗透压。在缺水、禁食的动物以及禁食、水负荷的大鼠中，利尿活性也很明显。3. NT（脑室内注射0.1 μg/只大鼠）对进食大鼠的尿量没有影响，但减弱了SR 48692（脑室内注射1 μg/只大鼠）的利尿作用。在禁食、水负荷的动物中得到了相反的结果：NT剂量依赖性地（脑室内注射0.01和0.1 μg/只大鼠）抑制利尿，并且这种作用被脑室内注射SR 48692显著抑制。在这种实验条件下，SR 48692没有进一步增加正在进行的利尿作用。4. NO合成抑制剂N(1)-硝基-L-精氨酸甲酯（L-NAME；腹腔注射30 mg/kg）单独对进食大鼠的尿量没有影响，但阻止了脑室内或腹腔注射SR 48692的利尿作用；L-精氨酸（腹腔注射1 g/kg）而非D-精氨酸（腹腔注射1 g/kg）恢复了SR 48692依赖性的利尿增加，L-NAME对呋塞米刺激的利尿没有影响。5. 在禁食、水负荷的大鼠中，全身给予L-NAME或脑室内注射NT显著减少水利尿，但在给予腹腔注射L-精氨酸的动物中不再出现这种作用。接受脑室内注射NT且利尿显著减少的大鼠，其尿中硝酸盐和亚硝酸盐的排泄也较少。6. 对进食大鼠中枢或全身给予SR 48692后利尿增加，同时尿中硝酸盐和亚硝酸盐的排泄也增加，这与SR 48692阻断NT受体后外周NO生成增强一致。呋塞米后利尿增加也涉及尿中硝酸盐和亚硝酸盐的增加，但这种作用约为等效利尿剂量SR 48692所达到作用的一半。7. 在进食大鼠中，NO供体异山梨醇二硝酸酯降低收缩压（与不影响血压的SR 48692不同），但也剂量依赖性地（腹腔注射1和5 mg/kg）刺激尿量。8. SR 48692的总体作用有力地支持了内源性NT、抗利尿激素（AVP）的作用与外周NO生成之间在调节水、Na+、K+和Cl-的肾排泄中的联系。