Comparison of cyclic nucleotide phosphodiesterase isoenzymes in rat and rabbit ventricular myocardium: positive inotropic and phosphodiesterase inhibitory effects of Org 30029, milrinone and rolipram

Shahid, Mohammed; Nicholson, C. D.

doi:10.1007/bf00175715

Cited by 94 publications

(78 citation statements)

References 22 publications

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“…Second, in agreement with a number of previous studies, we identified PDE3 and PDE4 as critical regulators of cAMP signals in cardiac myocytes. This finding is also consistent with the predominant impact of PDE3 and PDE4 activities for the ␤-adrenergic regulation of I Ca,L in rat ventricular myocytes (20) and the positive inotropic effect of PDE3 and PDE4 inhibitors in rats (41,42).…”

Section: Discussionsupporting

confidence: 88%

Negative Feedback Exerted by cAMP-dependent Protein Kinase and cAMP Phosphodiesterase on Subsarcolemmal cAMP Signals in Intact Cardiac Myocytes

Rochais

Vandecasteele

Lefebvre

et al. 2004

Journal of Biological Chemistry

131

141

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Intracardiac cAMP levels are modulated by hormones and neuromediators with specific effects on contractility and metabolism. To understand how the same second messenger conveys different information, mutants of the rat olfactory cyclic nucleotide-gated (CNG) channel ␣-subunit CNGA2, encoded into adenoviruses, were used to monitor cAMP in adult rat ventricular myocytes. CNGA2 was not found in native myocytes but was strongly expressed in infected cells. In whole cell patchclamp experiments, the forskolin analogue L-858051 (L-85) elicited a non-selective, Mg 2؉ -sensitive current observed only in infected cells, which was thus identified as the CNG current (I CNG ). The ␤-adrenergic agonist isoprenaline (ISO) also activated I CNG , although the maximal efficiency was Ϸ5 times lower than with L-85. However, ISO and L-85 exerted a similar maximal increase of the L-type Ca 2؉ current. The use of a CNGA2 mutant with a higher sensitivity for cAMP indicated that this difference is caused by the activation of a localized fraction of CNG channels by ISO. cAMP-dependent protein kinase (PKA) blockade with H89 or PKI, or phosphodiesterase (PDE) inhibition with IBMX, dramatically potentiated ISO-and L-85-stimulated I CNG . A similar potentiation of ␤-adrenergic stimulation occurred when PDE4 was blocked, whereas PDE3 inhibition had a smaller effect (by 2-fold). ISO and L-85 increased total PDE3 and PDE4 activities in cardiomyocytes, although this effect was insensitive to H89. However, in the presence of IBMX, H89 had no effect on ISO stimulation of I CNG . This study demonstrates that subsarcolemmal cAMP levels are dynamically regulated by a negative feedback involving PKA stimulation of subsarcolemmal cAMP-PDE.Recent evidence indicates that multimolecular signaling complexes between cell surface receptors and intracellular targets are essential for the speed and specificity of signal transduction events (1, 2, 3). However, how such modules maintain specificity when small diffusible molecules are generated during the signaling cascade is difficult to investigate. This question is particularly relevant for cAMP in the heart, where this cyclic nucleotide second messenger exerts diverse effects in response to a number of different neuromediators and hormones. For instance, the ␤-adrenergic agonist isoprenaline (ISO), 1 prostaglandin E 1 (PGE 1 ), and glucagon-like peptide 1 (GLP-1) elevate intracardiac cAMP levels with different effects on contractility; ISO augments the force of contraction, PGE 1 does not, and GLP-1 exerts a negative inotropic effect (4, 5). In order to explain these results, subcellular compartmentation of cAMP was proposed more than 20 years ago (6).Localized cAMP signals may be generated by the interplay between discrete production sites and restricted diffusion within the cytoplasm. In addition to specialized membrane structures that may circumvent cAMP spreading (6, 7), degradation of cAMP into 5Ј-AMP by cyclic nucleotide phosphodiesterases (PDEs) appears critical for the formation of dynamic microdomain...

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Section: Discussionsupporting

confidence: 88%

Negative Feedback Exerted by cAMP-dependent Protein Kinase and cAMP Phosphodiesterase on Subsarcolemmal cAMP Signals in Intact Cardiac Myocytes

Rochais

Vandecasteele

Lefebvre

et al. 2004

Journal of Biological Chemistry

131

141

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“…This was also observed in the presence of high concentration of another PDE III inhibitor milrinone (100pM) by Shahid & Nicholson (1990). In rat aorta without functional endothelium, the PDE IV inhibitors (rolipram and denbufylline) were by themselves weak relaxant agents, acting at high concentrations only.…”

Section: Discussionmentioning

confidence: 67%

Endothelium‐dependent and independent relaxation of the rat aorta by cyclic nucleotide phosphodiesterase inhibitors

Komas

Lugnier²,

Stoclet³

1991

British J Pharmacology

138

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1 The effects of selective inhibitors of adenosine 3': 5'-cyclic monophosphate (cyclic AMP) and guanosine 3': 5'-cyclic monophosphate (cyclic GMP) phosphodiesterases (PDEs) were investigated on PDEs isolated from the rat aorta and on relaxation of noradrenaline (1 pM) precontracted rat aortic rings, with and without functional endothelium. 2 Four PDE forms were isolated by DEAE-sephacel chromatography from endothelium-denuded rat aorta: a calmodulin-activated PDE (PDE I) which hydrolyzed preferentially cyclic GMP, two cyclic AMP PDEs (PDE III and PDE IV) and one cyclic GMP-specific PDE (PDE V). The latter was selectively and potently inhibited by zaprinast. The two cyclic AMP PDEs were discriminated by specific inhibitors: one was inhibited by cyclic GMP (PDE III) and by new cardiotonic agents (milrinone, CI 930, LY 195115 and SK&F 94120); the other was inhibited by denbufylline and rolipram (PDE IV). None of these drugs significantly inhibited PDE I. 3 The PDE III inhibitors caused endothelium-independent relaxations of rat aortic rings with the following EC50 values (aM concentration producing 50% relaxation) : LY 195115: 3.4, milrinone: 5.7, CI 930; 7.8, SK&F 94120: 14.7. Neither N0-monomethyl-L-arginine (L-NMMA, 300pM), an inhibitor of the Larginine-NO pathway, nor L-arginine (1 mM) modified the effect of PDE III inhibitors. However, methylene blue (1OpM) an inhibitor of soluble guanylate cyclase abolished relaxation induced by PDE III inhibitors except in the case of compound CI 930. 4 The specific PDE IV and PDE V inhibitors both produced endothelium-dependent relaxations which were inhibited by L-NMMA and by methylene blue (10piM). In the presence of L-NMMA, relaxation was restored by subsequent addition of L-arginine. 5 The relaxant effects of denbufylline and rolipram were studied in the presence of drugs stimulating either adenylate cyclase (forskolin and isoprenaline) or soluble guanylate cyclase (sodium nitroprusside, SNP), or inhibiting PDE III (milrinone). In endothelium-denuded rings, a relaxing effect of both denbufylline and rolipram was found in the presence of milrinone (EC5o values 1.7 and 12puM, respectively) or SNP (EC50 values 12.3 and 124pM, respectively), but not in the presence of forskolin or isoprenaline. However in the presence of functional endothelium, relaxations produced by PDE IV inhibitors were significantly potentiated by forskolin, isoprenaline, milrinone and SNP (respective EC50 values for denbufylline: 2, 2, 0.4 and 0.7 JM and for rolipram: 7, 13, 7 and 1.2 pM). 6 These results indicate that the relaxant effects of inhibitors of the cyclic AMP-specific PDE IV are markedly enhanced by cyclic GMP elevating agents and by the PDE III inhibitor milrinone. They support the hypothesis that cyclic GMP enhances cyclic AMP-mediated relaxation, possibly through the inhibition of the cyclic GMP-inhibited PDE III.

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“…The surprisingly large responses of IBMX may be due to its additional effects, all of which may increase contractility. These include its competitive reversible effect on inhibitory adenosine (Bohm et al, 1988b), its possible activation of the sarcoplasmic reticulum calcium release channels and sensitization of the myofilaments to calcium (Scholz & Meyer, 1986), reduction of the activity of inhibitory guanine nucleotide protein (Gi) function (Parsons et al, 1988) or additional effects on other PDE isoenzymes, see Shahid & Nicholson (1990).…”

Section: Discussionmentioning

confidence: 99%

Incomplete reversal of β‐adrenoceptor desensitization in human and guinea‐pig cardiomyocytes by cyclic nucleotide phosphodiesterase inhibitors

Wynne

Poole‐Wilson

Harding

1993

British J Pharmacology

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1 The decreased response to P-adrenoceptor stimulation seen in heart failure may be related to a defect in cyclic AMP production. The inotropic effects of the selective phosphodiesterase (PDE) III inhibitors, SK&F 94120 and SK&F 94836, and the non-selective PDE inhibitor, 3-isobutyl-1-methylxanthine (IBMX), alone and when combined synergistically with isoprenaline, were studied in control and P-adrenoceptor-desensitized ventricular myocytes.2 Myocytes isolated from noradrenaline-treated guinea-pigs had a reduced maximum response to isoprenaline compared with control animals (60.0 ± 2.5%, n = 42 vs 79.5 ± 1.7% maximum calcium: n = 46, P <0.001). Together with an approximately 20 fold increase in the isoprenaline EC", this is indicative of ,-adrenoceptor desensitization as a result with chronic infusion with noradrenaline. 3 The maximum inotropic response of IBMX was depressed following noradrenaline treatment, from 74.9 ± 4.6% (n = 7) in control, to 61.7 ± 2.70% (n = 6), as a percentage of maximum calcium in noradrenaline-treated guinea-pig ventricular myocytes (P<0.02). The pD2 value for IBMX was also reduced (P <0.02). No significant differences in the inotropic effects of SK&F 94120 and SK&F 94836 were seen between control and P-adrenoceptor desensitized myocytes.4 Threshold inotropic concentrations of SK&F 94120 and SK&F 94836 caused a five fold decrease in the EC50 of control myocytes for isoprenaline, and an 11 fold decrease in the noradrenaline-treated guinea-pig ventricular myocytes. 5 The maximum response to isoprenaline in myocytes isolated from normal guinea-pigs was unaffected by PDE inhibition; either at threshold or maximum inotropic concentrations, or by CPT cyclic AMP, an analogue of cyclic AMP. 6 A significant potentiation of the maximum isoprenaline response by threshold inotropic concentrations was observed with SK&F 94120 (P<0.05), but not with IBMX or SK&F 94836, in myocytes isolated from noradrenaline-treated guinea-pig hearts. This potentiation, however, did not completely restore the response to levels seen in control myocytes. 7 The extent of potentiation of the maximum isoprenaline response by maximum inotropic concentrations of either IBMX or CPT cyclic AMP, was no greater than that by threshold concentrations of IBMX, in myocytes isolated from noradrenaline-treated guinea-pig hearts. 8 In cardiac myocytes isolated from the explanted hearts of 16 patients with heart failure, threshold concentrations of IBMX and SK&F 94120 decreased the isoprenaline EC50 by a factor of four and six, respectively, but potentiation of the maximum isoprenaline response occurred only with SK&F 94120. The attenuated isoprenaline response was increased from 60.3 ± 4.5% to 74.3 ± 4.2% as a % maximum calcium (P<0.05, n = 6), but remained substantially lower than the 116 ± 7% (P<0.001, n = 6) seen in myocytes isolated from non-failing hearts. 9 We conclude that the reduced maximum contraction amplitude with isoprenaline in cardiac myocytes from either patients in end-stage failure, or noradrenaline-treated guin...

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Comparison of cyclic nucleotide phosphodiesterase isoenzymes in rat and rabbit ventricular myocardium: positive inotropic and phosphodiesterase inhibitory effects of Org 30029, milrinone and rolipram

Cited by 94 publications

References 22 publications

Negative Feedback Exerted by cAMP-dependent Protein Kinase and cAMP Phosphodiesterase on Subsarcolemmal cAMP Signals in Intact Cardiac Myocytes

Negative Feedback Exerted by cAMP-dependent Protein Kinase and cAMP Phosphodiesterase on Subsarcolemmal cAMP Signals in Intact Cardiac Myocytes

Endothelium‐dependent and independent relaxation of the rat aorta by cyclic nucleotide phosphodiesterase inhibitors

Incomplete reversal of β‐adrenoceptor desensitization in human and guinea‐pig cardiomyocytes by cyclic nucleotide phosphodiesterase inhibitors

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