Prostaglandins and the control of blood flow in the canine myocardium.

Hintze, Thomas H.; Kaley, Gabor

doi:10.1161/01.res.40.3.313

Cited by 108 publications

(31 citation statements)

References 34 publications

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“…Furthermore, an infusion of indomethacin produced blockade of the coronary actions as well as the PGL efflux (Schror, Moncada, Ubatuba & Vane, 1978). These data corroborate previous experiments in which NSAA was administered to inhibit prostaglandin synthetase in isolated perfused or intact hearts (Minkes, Douglas & Needleman, 1973;Needleman, 1976;Hintze & Kaley, 1977). Other polyunsaturated fatty acids have also been reported to produce changes in coronary flow and in the output of PGL (Mentz & Forster, 1977).…”

Section: Introductionsupporting

confidence: 87%

Coronary Vasoconstrictor and Vasodilator Actions of Arachidonic Acid in the Isolated Perfused Heart of the Rat

Belo

Talesnik

1982

British J Pharmacology

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1 The administration of arachidonic acid (AA) to the isolated perfused heart of the rat usually produced biphasic coronary responses characterized by initial vasoconstriction followed by prolonged vasodilatation. However, some responses were predominantly vasoconstrictor or vasodilator.2 The non-steroidal anti-inflammatory agents (NSAA) indomethacin (1-5mg/l) and naproxen (12.5-25 mg/I) reversibly inhibited both phases of the response induced by AA. 3 Pretreatment of animals with indomethacin (5 mg/kg) or naproxen (25 mg/kg) daily, resulted in unaltered coronary response to AA. Subsequent addition of NSAA to the perfusate produced inhibition of the AA effect. 4 Short infusions of acetylsalicylic acid at low concentrations (2.9 Lg/ml), dipyridamole (0.6 pg/ml) and sulphinpyrazone (28.7 pg/ml) selectively inhibited the vasoconstrictor phase of the response to AA. 5 It was confirmed that metabolic coronary dilatation induced by cardiostimulation was inhibited by prolonged AA administration; this effect was prevented by NSAA pretreatment. Reactive hyperaemic responses to short lasting occlusions of coronary inflow were unaffected by NSAA. 6 Linolenic, linoleic, dihomo-y-linolenic and oleic acid usually produced decreases in coronary flow which were unaffected by NSAA, dipyridamole or sulphinpyrazone. 7 Intra-aortic injections of AA, prostacyclin (PGI2) and prostaglandin E2 (PGE2) in the intact rat produced a dose-dependent decrease in blood pressure with the AA response inhibited by indomethacin. PGI2 and PGE2 produced long lasting coronary vasodilatation in the isolated heart. 8 The coronary actions of AA appear to be due to its transformation, within the easily accessible vascular wall, into prostaglandin and thromboxane-like substances. We suggest that a vasoconstrictor thromboxane A2-like substance may be responsible for coronary vasospasm. 9 Coronary insufficiency may also result from an inhibition of compensatory metabolic coronary dilatation by increased synthesis of PGE2 within the myocardial cell.

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Section: Introductionsupporting

confidence: 87%

Coronary Vasoconstrictor and Vasodilator Actions of Arachidonic Acid in the Isolated Perfused Heart of the Rat

Belo

Talesnik

1982

British J Pharmacology

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“…Also, previous studies have shown that indomethacin does not affect coronary vascular responsiveness. 19 Our preliminary study in seven other normal rabbit hearts without any inotropic intervention showed that left ventricular peak isovolumic pressure at a constant ventricular volume at 90 and 120 minutes after an initial measurement (+0.4+10.0% and -6.2±15.4%, respectively) did not significantly differ from the initial value of 98+13 mm Hg. This indicates stability of our cross-circulated heart preparation compared with crystalloid-perfused hearts.…”

Section: Materials and Methods Animal Modelsmentioning

confidence: 75%

Decreased contractile efficiency and increased nonmechanical energy cost in hyperthyroid rabbit heart. Relation between O2 consumption and systolic pressure-volume area or force-time integral.

Goto

Slinker

LeWinter

1990

Circulation Research

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Both systolic pressure-volume area (PVA) and force-time integral (FM1) have been used as measures of oxygen consumption per beat (Vo2) in the isolated left ventricle. The reciprocal of the slope of the Vo2-PVA relation has been considered to reflect the chemomechanical energy transduction efficiency of the contractile machinery (contractile efficiency), whereas its Vo2 intercept consists of energy cost of excitation-contraction coupling and basal metabolism. To examine whether the increase in myosin isoform V1/V3 ratio in hyperthyroid rabbits decreases contractile efficiency and to determine overall mechanisms of higher oxygen consumption in hyperthyroid hearts, the Vo2-PVA and Vo2-FTI relations as well as the end-systolic pressurevolume relation were assessed in cross-circulated, isovolumically beating hearts isolated from normal, hyperthyroid, and hypothyroid rabbits. Normalized initial slopes of the rising limb of the curvilinearly fitted end-systolic pressure-volume relation (E'm., ventricular contractility index) were similar for normal and hyperthyroid groups. However, the slopes and Vo2 intercepts of the Vo2-PVA and Vo2-Fll relations were greater in hyperthyroid hearts than in normal hearts. Accordingly, in the hyperthyroid hearts, the contractile efficiency (27±6%) was lower and left ventricular Vo2 for excitation-contraction coupling (0.028±0.004 ml 02Jbeat/100 g) was higher than in normal hearts (40±4% and 0.021±0.005 ml 02/beat/100 g, respectively).This decreased contractile efficiency in the hyperthyroid hearts was attributable to myosin isoform alteration rather than to increased (-adrenoceptors because isoproterenol did not affect the slope of the Vo2-PVA relation in all groups. In contrast, the slope of the Vo2-FTI relation was significantly increased by isoproterenol in all groups. Neither the Vo2-PVA nor the Vo2-FH relations in hypothyroid hearts were different from those in normal hearts except for significantly lower Vo2 for basal metabolism. We conclude that in hyperthyroid rabbits, the left ventricle has decreased contractile efficiency and increased energy cost of excitation-contraction coupling and that the decreased contractile efficiency in hyperthyroid hearts is probably due to the increased V1NV3 ratio of the myosin isoform component. In addition, this study demonstrates that the

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“…PGE 2 reportedly promotes the second phase of platelet aggregation. 23 ' 24 While it is doubtful that unregulated PGE 2 formation by spontaneous hydrolysis of PGH 2 contributes to carotid arterial thromboregulatory mechanisms, PGE 2 formed nonenzymatically could oppose platelet inhibitory effects of PGI 2 . Previous work in our laboratory, which unmasked the presence of GSH-dependent PGE 2 isomerase activity in bovine coronary artery microsomes, demonstrated the need for appropriately controlled experiments before the presence of GSH-dependent PGE 2 isomerase in vascular tissues could be definitely excluded.…”

Section: Discussionmentioning

confidence: 99%

Prostacyclin, thromboxane A2, and prostaglandin E2 formation in atherosclerotic human carotid artery.

et al. 1988

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Prostaglandin (PG) formation In 16 atherosclerotic human carotid endarterectomy specimens was compared systematically with that of normal carotid artery from seven white pigs and six rhesus monkeys. Prostacyclin (PGI2) formation (plcomoles 6-keto-PGF 1t /2 mln/100 ^9 homogenate protein plus 2 mM glutathlone [GSH]) of nonatheromatous Intlma adjacent proximal (276 ± 32, mean ± SEM) or distal (271 ± 14) to carotid plaque was comparable to that of normal carotid artery from white pig (272 ± 25, NS) and rhesus monkey (219 ± 41, NS), and was greater than stenotlc Intlma (156 ± 1 7 , p<0.01), sublntlmal plaque (168 ± 14, p < 0.01), and ulceratlon (65 ± 16, p<0.01 A rterial prostaglandin (PG) synthesis Is thought to be important in the maintenance of circulatory homeostasis by contributing to regulation of vascular tone and endothelial platelet adherence. Prostacyclin (PGy, the major product of arachidonic acid metabolism in normal vascular endothelium, is a potent vasodilator and inhibitor of platelet aggregation and adherence to the vessel wall. 1It has been hypothesized that PGI 2 counterbalances the proaggregatory and vasoconstrictive effects of predominantly platelet-synthesized thromboxane Aj (TXAj).1 Recent reports 2 ' 3 -4 suggest that atherosclerotic arteries differ from normal arterial tissues by producing substantially less PGI 2 , more PGE 2 , 4 and detectable levels of TXA 2 . 5 Such alterations in PG synthesis could create a localized imbalance between the intravascular actions of PGI 2 and TXAa, resulting in increased platelet deposition and arterial thrombogenicity at atherosclerotic sites.The underlying biochemical basis for reported alterations in arterial PG synthesis in atherosclerosis is unclear. Furthermore, it has not been demonstrated whether such changes in atherosclerotic patients are focal (localized only to plaque) or systemic (also found in nonatheromatous arterial tissues). The purpose of this study was to identify enzymatic changes in carotid endarterectomy Received May 26,1987; revision accepted September 9,1987. specimens that might account for these previously observed disturbances of eicosanoid metabolism and investigate the potential of glutathione (GSH), an endogenous antioxidant, to modulate PG synthesis. Methods Normal Carotid Artery SpecimensA single specimen of nonatherosclerotic human carotid artery (n = 1) was harvested with appropriate authorization from a brain-dead cadaver kidney donor. Fresh carotid arteries from young adult, white (cross-bred, market grade) pigs (n = 7) and rhesus monkeys (n = 6) were used as control specimens. The animal experiments conformed to principles of animal care established by the Tulane Medical Center Advisory Committee for Animal Resources, "Principles of Laboratory Animal Care," and the "Guide for the Care and Use of Laboratory Animals" (NIH publication No. 80-23, revised 1978). Atherosclerotic Carotid Artery SpecimensOcclusive atheromatous internal carotid artery plaques were removed from patients (n = 16) by standard carotid endarterecto...

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Prostaglandins and the control of blood flow in the canine myocardium.

Cited by 108 publications

References 34 publications

Coronary Vasoconstrictor and Vasodilator Actions of Arachidonic Acid in the Isolated Perfused Heart of the Rat

Coronary Vasoconstrictor and Vasodilator Actions of Arachidonic Acid in the Isolated Perfused Heart of the Rat

Decreased contractile efficiency and increased nonmechanical energy cost in hyperthyroid rabbit heart. Relation between O2 consumption and systolic pressure-volume area or force-time integral.

Prostacyclin, thromboxane A2, and prostaglandin E2 formation in atherosclerotic human carotid artery.

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