1991
DOI: 10.1111/j.1476-5381.1991.tb09834.x
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Nitric oxide is the mediator of ATP‐induced dilatation of the rabbit hepatic arterial vascular bed

Abstract: 1Livers of 10 New Zealand White rabbits were perfused in vitro with Krebs-Builbring buffer via the hepatic artery (HA) and portal vein (PV) at constant flows of 23 + 1 and 77 + 1 ml min 1 00 g' respectively. The tone of the preparation was raised with noradrenaline (concentration: 10p1M). 2 Dose-response curves for the vasodilatation produced by adenosine 5'-triphosphate (ATP), acetylcholine (ACh), adenosine, and sodium nitroprusside (SNP) were obtained following injection into the HA supply. Injections were t… Show more

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Cited by 81 publications
(53 citation statements)
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“…This contrasts with the results of our study, where the tumour :normal ratio remained raised after a 45 min infusion in some patients. It has been demonstrated that Nitric Oxide (NO) is the mediator of hepatic parenchymal vasodilatation (Mathie et al, 1991), and NO inhibition has been shown to prolong Vasopressininduced vasoconstriction and enhancement of tumour : liver blood flow ratio in the rat (Dworkin et al, 1995). Further investigation of NO induced compensatory vasodilation during Angiotensin II infusion in humans may help to elucidate the mechanisms responsible for the discrepancies seen in the small number of published studies, and also the wide variation in response seen between individual patients.…”
Section: Discussionmentioning
confidence: 99%
“…This contrasts with the results of our study, where the tumour :normal ratio remained raised after a 45 min infusion in some patients. It has been demonstrated that Nitric Oxide (NO) is the mediator of hepatic parenchymal vasodilatation (Mathie et al, 1991), and NO inhibition has been shown to prolong Vasopressininduced vasoconstriction and enhancement of tumour : liver blood flow ratio in the rat (Dworkin et al, 1995). Further investigation of NO induced compensatory vasodilation during Angiotensin II infusion in humans may help to elucidate the mechanisms responsible for the discrepancies seen in the small number of published studies, and also the wide variation in response seen between individual patients.…”
Section: Discussionmentioning
confidence: 99%
“…The proposed endothelium-derived relaxing factors (EDRFs) are NO, prostacyclin, and endothelium-derived hyperpolarizing factors (EDHFs) (Brown & Burnstock, 1981;Mathie et al, 1991;Keef et al, 1992;Malmsjo et al, 1999).…”
Section: Introductionmentioning
confidence: 99%
“…17 Although it is clear that NO controls basal resistance in the hepatic artery, [18][19][20] a functional role for eNOS in the portal circulation has been more controversial. [21][22][23] By contrast, iNOS is virtually absent in the normal liver but markedly increased in response to inflammation and a variety of oxidative stresses.…”
Section: Blood Flow Regulationmentioning
confidence: 99%