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Dilatation by angiotensin II of the rat femoral arterial bed in vivo via pressure/flow‐induced release of nitric oxide and prostaglandins
Author(s) -
Heinemann Akos,
Wachter Christof H.,
Peskar Bernhard A.,
Holzer Peter
Publication year - 1997
Publication title -
british journal of pharmacology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.432
H-Index - 211
eISSN - 1476-5381
pISSN - 0007-1188
DOI - 10.1038/sj.bjp.0701460
Subject(s) - vasoconstriction , vasodilation , medicine , vasopressin , angiotensin ii , endocrinology , femoral artery , hexamethonium , blood pressure , atropine
1 The haemodynamic effects of angiotensin II (AII) and, for comparison, arginine vasopressin (AVP) in the femoral and superior mesenteric artery of urethane‐anaesthetized rats were analysed with the ultrasonic transit time shift technique. 2 I.v. bolus injection of AII (0.1–3 nmol kg −1 ) and AVP (0.03–1 nmol kg −1 ) increased blood pressure which was accompanied by a decrease in blood flow through the superior mesenteric artery and an increase in femoral blood flow. The femoral hyperaemia was in part due to vasodilatation as indicated by a rise of femoral vascular conductance up to 200% relative to baseline. The femoral vasodilatation caused by AVP, but not AII, was followed by vasoconstriction. 3 Blockade of angiotensin AT 1 receptors by telmisartan (0.2–20 μmol kg −1 ) prevented all haemodynamic responses to AII. 4 The femoral dilator responses to AII and AVP depended on the increase in vascular perfusion pressure since vasodilatation was reversed to vasoconstriction when blood pressure was maintained constant by means of a gravity reservoir. However, the AII‐evoked femoral vasodilatation was not due to an autonomic or neuroendocrine reflex because it was not depressed by hexamethonium (75 μmol kg −1 ), prazosin (0.25 μmol kg −1 ) or propranolol (3 μmol kg −1 ). 5 The AII‐induced femoral vasodilatation was suppressed by blockade of nitric oxide (NO) synthesis with N G ‐nitro‐ L ‐arginine methyl ester ( L ‐NAME, 40 μmol kg −1 ) and reversed to vasoconstriction when L ‐NAME was combined with indomethacin (30 μmol kg −1 ), but was left unaltered by antagonism of endothelin ET A/B receptors with bosentan (37 μmol kg −1 ). 6 These results demonstrate that the effect of AII to increase systemic blood pressure and the resulting rise of perfusion pressure in the femoral artery stimulates the formation of NO and prostaglandins and thereby dilates the femoral arterial bed. This local vasodilator mechanism is sufficient to mask the direct vasoconstrictor response to AII.British Journal of Pharmacology (1997) 122 , 975–984; doi: 10.1038/sj.bjp.0701460