Arterial function in nitric oxide-deficient hypertension: influence of long-term angiotensin II receptor antagonism

doi:10.1016/S0008-6363(98)00346-0

Cardiovascular Research 1999 42(3):773-782; doi:10.1016/S0008-6363(98)00346-0
© 1999 by European Society of Cardiology

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Arterial function in nitric oxide-deficient hypertension: influence of long-term angiotensin II receptor antagonism

Jarkko Kalliovalkama^a^,*, Pasi Jolma^a, Jari-Petteri Tolvanen^a^,b, Mika Kähönen^a^,c, Nina Hutri-Kähönen^a^,d, Xiumin Wu^a, Päivi Holm^a and Ilkka Pörsti^a^,e

^aUniversity of Tampere Medical School, Department of Pharmacological Sciences, P.O. Box 607, FIN-33101 Tampere, Finland
^bDepartment of Clinical Chemistry, Tampere University Hospital, Tampere, Finland
^cDepartment of Clinical Physiology, Tampere University Hospital, Tampere, Finland
^dDepartment of Pediatrics, Tampere University Hospital, Tampere, Finland
^eDepartment of Internal Medicine, Tampere University Hospital, Tampere, Finland

^* Corresponding author. Tel.: +358-3-215-6111; fax: +358-3-215-6170. E-mail address: jarkko.kalliovalkama@uta.fi (J. Kalliovalkama)

Objective: Since the effects of angiotensin II receptor antagonismon arterial function in nitric oxide (NO)-deficient hypertensionare unknown, we investigated the influence of losartan therapy(20 mg kg^–1 day^–1) on the control of arterial tonein N^G-nitro-L-arginine methyl ester (L-NAME; 20 mg kg^–1day^–1)-induced hypertension. Methods: Forty Wistar ratswere divided into four groups: control, losartan, L-NAME, andlosartan+L-NAME. The responses of isolated mesenteric arterialrings were examined in standard organ chambers after 8 treatmentweeks. Results: Losartan therapy prevented the development ofL-NAME-induced hypertension and the associated impairments ofendothelium-independent relaxations to nitroprusside, isoprenaline,and cromakalim, vasodilators acting via the formation of NO,activation of β-adrenoceptors and opening of K⁺ channels,respectively. In addition, endothelium-dependent relaxationsof noradrenaline-precontracted rings to acetylcholine duringNO synthase inhibition in vitro were decreased in L-NAME rats,and clearly improved by losartan therapy. The inhibition ofcyclooxygenase by diclofenac improved the responses to acetylcholinemore effectively in L-NAME than losartan+L-NAME rats, but therelaxations remained decreased in L-NAME rats when comparedwith losartan+L-NAME rats. When hyperpolarization of smoothmuscle was prevented by precontractions induced by high concentrationof KCl, the responses to acetylcholine during combined NO synthaseand cyclooxygenase inhibition were similar and almost abolishedin all groups. Furthermore, superoxide dismutase, a scavengerof superoxide anions, enhanced the acetylcholine-induced relaxationsmore effectively in L-NAME than losartan+L-NAME rats, althoughplasma antioxidant capacity was similar in all study groups.Conclusion: Chronic L-NAME-induced hypertension was associatedwith attenuated arterial relaxation via endothelium-dependentand -independent mechanisms, both of which were improved bythe losartan treatment. The mechanisms whereby losartan enhancedarterial relaxation in this model of experimental hypertensionmay have included enhanced hyperpolarization and increased sensitivityto NO in smooth muscle, and decreased vascular production ofsuperoxide and vasoconstrictor prostanoids.

KEYWORDS Antihypertensive agents; Endothelial factors; Hypertension; Nitric oxide; Smooth muscle

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