Literature DB >> 3814919

Purinoceptors in the rat heart.

G Fleetwood, J L Gordon.   

Abstract

The effects of an intracoronary bolus of adenosine triphosphate (ATP), alpha, beta-methylene ATP (APCPP), beta, gamma-methylene ATP (APPCP), adenosine diphosphate (ADP), adenosine monophosphate (AMP) and adenosine on coronary tone and ventricular myocardial contraction were investigated in the perfused rat heart. Adenine nucleotides, given by bolus injection were negatively inotropic in amounts greater than 3 X 10(-7) mol. The potency order was ATP greater than ADP greater than AMP. Adenosine (less than 1 X 10(-5)mol) had no effect on ventricular myocardial contraction. Adenine nucleotides and adenosine (1 X 10(-10)-1 X 10(-7) mol) reduced coronary tone. The potency order was ATP greater than ADP greater than AMP = adenosine. The ATP analogue APPCP was less active than ATP at reducing coronary tone, and APCPP had no vasodilator effect. This suggests the presence of a P2-purinoceptor, subclass P2Y, which mediates vasodilation. ATP and ADP increased the concentration of prostacyclin (measured as 6-keto prostaglandin F1 alpha) in the perfusate, but only after injection of greater than 3 X 10(-7) mol, suggesting that the vasodilator responses to ATP and ADP were not mediated by prostacyclin. AMP and adenosine had no effect, even at 1 X 10(-5) mol. At a dose of 3 X 10(-9) mol, approximately 40% of ATP and 70% of ADP was converted to AMP and adenosine whilst passing through the heart. The amounts of AMP and adenosine formed, however, were insufficient to account for the vasodilator effects of ATP and ADP. 6 Vasodilatation mediated by AMP and adenosine was inhibited by an infusion of 8-phenyltheophylline (8-PT; 2 x 10-5 M) indicating interaction with a P1-purinoceptor. Vasodilatation induced by ATP (at doses at which AMP and adenosine had no action) was also depressed by 8-PT indicating either an action of ATP on PI-purinoceptors, or an effect of 8-PT on P2y receptors. 7 Vasodilatation induced by AMP was unaltered during an infusion of alpha,beta-methylene ADP (2 x 10-6 M, which inhibited breakdown of AMP to adenosine by 54.2 +/- 1.5%, n = 4). This suggests that AMP acted directly, and it did not require conversion to adenosine to induce vasodilatation. 8 The ATP analogues APCPP (1 x 10-9_1 x 10-8 mol) and APPCP (1 x 10-8_l x 10-7mol) increased coronary tone, as did high doses (I x 10-5 mol) ofATP and ADP, indicating the presence of an additional P2-purinoceptor, subclass P2X, mediating vasoconstriction.

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Year:  1987        PMID: 3814919      PMCID: PMC1917271          DOI: 10.1111/j.1476-5381.1987.tb16843.x

Source DB:  PubMed          Journal:  Br J Pharmacol        ISSN: 0007-1188            Impact factor:   8.739


  37 in total

1.  Coronary vasodilator properties of purine and pyrimidine derivatives.

Authors:  M M WOLF; R M BERNE
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2.  5'-Nucleotidase from rat heart membranes. Inhibition by adenine nucleotides and related compounds.

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3.  Quantitative thin-layer chromatography of ATP and the products of its degradation in meat tissue.

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5.  Catabolism of adenine nucleotides by the isolated perfused rat heart.

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Review 6.  The role of adenosine in the regulation of coronary blood flow.

Authors:  R M Berne
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7.  Role of the intima in cholinergic and purinergic relaxation of isolated canine femoral arteries.

Authors:  J G De Mey; P M Vanhoutte
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9.  Mechanisms of adenosine triphosphate-, thrombin-, and trypsin-induced relaxation of rat thoracic aorta.

Authors:  R M Rapoport; M B Draznin; F Murad
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10.  Can ATP stimulate P1-receptors in guinea-pig atrium without conversion to adenosine?

Authors:  M G Collis; S J Pettinger
Journal:  Eur J Pharmacol       Date:  1982-07-30       Impact factor: 4.432

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8.  Ecto-5'-nucleotidase, CD73, is an endothelium-derived hyperpolarizing factor synthase.

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9.  Dual effect of ATP and UTP on rat atria: which types of receptors are involved?

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10.  Vasodilator actions of acetylcholine, A23187 and bradykinin in the guinea-pig isolated perfused heart are independent of prostacyclin.

Authors:  A G Stewart; P J Piper
Journal:  Br J Pharmacol       Date:  1988-10       Impact factor: 8.739

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