Role of Nitric Oxide–cGMP Pathway in Adrenomedullin-Induced Vasodilation in the Rat | Zendy

Hiroshi Hayakawa | Zendy; Yasunobu Hirata | Zendy; Masao Kakoki | Zendy; Yasuko Suzuki | Zendy; Hiroaki Nishimatsu | Zendy; Daisuke Nagata | Zendy; Etsu Suzuki | Zendy; Kazuya Kikuchi | Zendy; Tetsuo Nagano | Zendy; Kenji Kangawa | Zendy; Hisayuki Matsuo | Zendy; Tsuneaki Sugimoto | Zendy; Masao Omata | Zendy

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Role of Nitric Oxide–cGMP Pathway in Adrenomedullin-Induced Vasodilation in the Rat

Author(s) -

Hiroshi Hayakawa,

Yasunobu Hirata,

Masao Kakoki,

Yasuko Suzuki,

Hiroaki Nishimatsu,

Daisuke Nagata,

Etsu Suzuki,

Kazuya Kikuchi,

Tetsuo Nagano,

Kenji Kangawa,

Hisayuki Matsuo,

Tsuneaki Sugimoto,

Masao Omata

Publication year - 1999

Publication title -

hypertension

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.986

H-Index - 265

eISSN - 1524-4563

pISSN - 0194-911X

DOI - 10.1161/01.hyp.33.2.689

Subject(s) - adrenomedullin , nitric oxide , chemistry , vasodilation , phenylephrine , acetylcholine , endocrinology , medicine , phosphodiesterase , zaprinast , pharmacology , cyclic gmp , biochemistry , peptide , organic chemistry , blood pressure , enzyme

We previously reported that adrenomedullin (AM), a potent vasodilator peptide discovered in pheochromocytoma cells, stimulates nitric oxide (NO) release in the rat kidney. To further investigate whether the NO-cGMP pathway is involved in the mechanisms of AM-induced vasodilation, we examined the effects of E-4021, a cGMP-specific phosphodiesterase inhibitor, on AM-induced vasorelaxation in aortic rings and perfused kidneys isolated from Wistar rats. We also measured NO release from the kidneys using a chemiluminescence assay. AM (10(-10) to 10(-7) mol/L) relaxed the aorta precontracted with phenylephrine in a dose-dependent manner. Denudation of endothelium (E) attenuated the vasodilatory action of AM (10(-7) mol/L AM: intact (E+) -25.7+/-5.2% versus denuded (E-) -7. 8+/-0.6%, P<0.05). On the other hand, pretreatment with 10(-8) mol/L E-4021 augmented AM-induced vasorelaxation in the intact aorta (-49. 0+/-7.9%, P<0.05) but not in the denuded one. E-4021 also enhanced acetylcholine (ACh)-induced vasorelaxation in the rat intact aorta (10(-7) mol/L ACh -36.6+/-8.4% versus 10(-8) mol/L E-4021+10(-7) mol/L ACh -62.7+/-3.1%, P<0.05). In perfused kidneys, AM-induced vasorelaxation was also augmented by preincubation with E-4021 (10(-9) mol/L AM -15.4+/-0.6% versus 10(-8) mol/L E-4021+10(-9) mol/L AM -23.6+/-1.2%, P<0.01). AM significantly increased NO release from rat kidneys (DeltaNO: +11.3+/-0.8 fmol. min-1. g-1 kidney at 10(-9) mol/L AM), which was not affected by E-4021. E-4021 enhanced ACh-induced vasorelaxation (10(-9) mol/L ACh -9.7+/-1.7% versus 10(-8) mol/L E-4021+10(-9) mol/L ACh -18.8+/-2.9%, P<0.01) but did not affect ACh-induced NO release from the kidneys. In the aorta and the kidney, 10(-4) mol/L of NG-nitro-L-arginine methyl ester, an NO synthase inhibitor, and 10(-5) mol/L of methylene blue, a guanylate cyclase inhibitor, reduced the vasodilatory effect of AM. These results suggest that the NO-cGMP pathway is involved in the mechanism of AM-induced vasorelaxation, at least in the rat aorta and kidney.

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