Diminished Inotropic Response to Amrinone in Ventricular Myocytes from Myopathic Hamsters Is Linked to Depression of High-Gain Ca<sup>2+</sup>-Induced Ca<sup>2+</sup>Release

Xiong, Wei; Ferrier, Gregory R.; Howlett, Susan E.

doi:10.1124/jpet.103.064873

Cited by 7 publications

(9 citation statements)

References 27 publications

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“…Inotropic responses to selective PDE inhibitors are reduced in heart failure [4,10,33,36]. The present study is the first to suggest that these changes can be attributed directly to sympathetic overactivation and abnormalities in signal transduction, rather than to diffuse myocardial damage and contractile dysfunction.…”

Section: Discussionmentioning

confidence: 67%

“…However, most studies performed to date have described PDE-inhibitor-mediated effects in heart failure where cardiac changes may occur that are not necessarily consequences of a downregulation of the β-AR-cAMP system. Indeed, intrinsic alterations in Ca 2+ cycling [15,36] and profound myocardial damage [24], as well as myocyte dysfunction [1,9], could potentially contribute to a reduction in PDE-inhibitor-induced responsiveness. Therefore, whether reduced PDE-inhibitor-induced contractile responses are attributed to sympathetic activation and subsequent alterations in signal transduction systems or to diffuse myocardial damage and dysfunction is unclear.…”

Section: Introductionmentioning

confidence: 99%

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Contractile responses to selective phosphodiesterase inhibitors following chronic β-adrenoreceptor activation

Osadchii

Woodiwiss

Norton

2005

Pflugers Arch - Eur J Physiol

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Contractile responses to phosphodiesterase (PDE) inhibitors are attenuated in heart failure, an effect limiting the clinical value of these agents. In this study, we sought to determine whether abnormalities in the beta-adrenoreceptor (beta-AR)-cyclic adenosine monophosphate (cAMP) signal transduction are sufficient to account for downregulation of PDE inhibitor-induced inotropic responses following chronic sympathetic activation. Sustained beta-AR activation produced by administration of isoproterenol (ISO) (50 microg kg(-1) day(-1) i.p. for 1 month) to rats resulted in cardiac hypertrophy, but did not affect baseline cardiac systolic function, as assessed in vivo by echocardiography and ex vivo under controlled loading conditions and heart rate (left ventricular systolic pressure-volume and stress-strain relations). Moreover, chronic ISO administration did not alter the baseline myocardial norepinephrine release or inotropic responses to incremental concentrations of Ca(2+) in isolated, perfused heart preparations. However, left ventricular contractile responses to ISO, the PDE III inhibitor amrinone, and the PDE IV inhibitor rolipram were attenuated following chronic beta-AR activation. Myocardial cAMP concentrations after stimulation with amrinone and rolipram were similar in ISO-treated and control rats. However, in ISO-treated rats, a marked decrease in contractile responsiveness to the cell-permeable, PDE-resistant cAMP analogue, 8-bromoadenosine cAMP, was noted. In conclusion, these data suggest that in cardiac disease, sustained beta-AR activation, without producing ventricular systolic dysfunction or enhanced myocardial norepinephrine release, is sufficient to account for the downregulation of contractile responses to PDE inhibitors. This effect appears to be largely mediated through abnormalities in signal transduction between cAMP and Ca(2+)-induced Ca(2+) release.

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Section: Discussionmentioning

confidence: 67%

Section: Introductionmentioning

confidence: 99%

Contractile responses to selective phosphodiesterase inhibitors following chronic β-adrenoreceptor activation

Osadchii

Woodiwiss

Norton

2005

Pflugers Arch - Eur J Physiol

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“…Selective PDE3 inhibitors-induced I Ca2+ stimulation was shown to be significantly larger in human as compared to rabbit atrial myocytes [95]. In contrast, amrinone, a selective PDE3 inhibitor, reduced rather than increased I Ca2+ amplitude in isolated hamster ventricular myocytes [119]. Collectively, these findings suggest species-related differences in PDE inhibitors effect on I Ca2+ amplitude under resting conditions.…”

Section: Stimulation Of I Ca2+mentioning

confidence: 94%

“…Indeed, in isolated hamster ventricular myocytes, amrinone, a selective PDE3 inhibitor, stimulates sarcoplasmic reticulum voltage-sensitive Ca 2+ release mechanism, an effect occurring independently of changes in I Ca2+ amplitude [112,119]. Furthermore, PDE3 inhibitors are capable of to increase Ca 2+ stores in sarcoplasmic reticulum [119,124], and directly promote sarcoplasmic reticulum Ca 2+ release via ryanodine-sensitive mechanism [98,104,125,126]. There is some evidence to indicate that PDE3 inhibitors could promote Na + -Ca 2+ exchange [105] and increase myocardial membrane Ca 2+ -ATPase activity [127].…”

Section: Effects On Ca 2+ Handlingmentioning

confidence: 99%

Myocardial Phosphodiesterases and Regulation of Cardiac Contractility in Health and Cardiac Disease

Osadchii

2007

Cardiovasc Drugs Ther

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Phosphodiesterase (PDE) inhibitors are potent cardiotonic agents used for parenteral inotropic support in heart failure. Contractile effects of these agents are mediated through cAMP-protein kinase A-induced stimulation of I (Ca2+) which ultimately results in increased Ca(2+)-induced sarcoplasmic reticulum Ca(2+) release. A number of additional effects such as increases in sarcoplasmic reticulum Ca(2+) stores, stimulation of reverse mode Na(+)-Ca(2+) exchange, direct or cAMP-mediated effects on sarcoplasmic reticulum ryanodine receptor, stimulation of the voltage-sensitive sarcoplasmic reticulum Ca(2+) release mechanism, as well as A(1) adenosine receptor blockade could contribute to positive inotropic responses to PDE inhibitors. Moreover, some PDE inhibitors exhibit Ca(2+) sensitizer properties as they could increase the affinity of troponin C Ca(2+)-binding sites as well as reduce Ca(2+) threshold for thin myofilament sliding and facilitate cross-bridge cycling. Inotropic responses to PDE inhibitors are significantly reduced in cardiac disease, an effect largely attributed to downregulation of cAMP-mediated signalling due to sustained sympathetic activation. Four PDE isoenzymes (PDE1, PDE2, PDE3 and PDE4) are present in myocardial tissue of various mammalian species, of which PDE3 and PDE4 are particularly involved in regulation of cardiac myocyte contraction. PDE cAMP-hydrolysing activity is preserved in compensated cardiac hypertrophy but significantly reduced in animal models of heart failure. However, clinical studies have not revealed any changes in distribution profile as well as kinetic and regulatory properties of myocardial PDEs in failing human hearts. A reduction of PDE inhibitors-induced contractile responses in heart failure has therefore been ascribed to reduced cAMP synthesis due to uncoupling of adenylyl cyclase from beta-adrenoreceptor. In cardiac myocytes, PDEs are targeted to distinct subcellular compartments by scaffolding proteins such as myomegalin, mAKAP and beta-arrestins. Over subcellular microdomains, cAMP hydrolysis by PDE3 and PDE4 allows to control the activity of local pools of protein kinase A and therefore the extent of protein kinase A-mediated phosphorylation of cellular proteins.

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“…The positive inotropic effects of milrinone in guinea pig [82] and dog [83] can be attenuated by a calcium channel blocker. Interestingly, the effect of PDE3 inhibition may differ from species to species as amrinone reduced ICa in normal hamster ventricular myocytes and produced no inotropic effects in cardiomyopathic hamsters [84] . There is also evidence that PDE3 inhibitors cause positive inotropy independently of increases in ICa and are likely due to increases in cAMP and PKA function in other localized areas resulting in altered calcium handling by SR. For instance, milrinone but not enoximone stimulates Ca release from SR by RyR2 in sheep [85] .…”

Section: Phosphodiesterasementioning

confidence: 99%

Pivotal effects of phosphodiesterase inhibitors on myocyte contractility and viability in normal and ischemic hearts

Rao

2008

Acta Pharmacol Sin

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Phosphodiesterases (PDEs) are enzymes that degrade cellular cAMP and cGMP and are thus essential for regulating the cyclic nucleotides. At least 11 families of PDEs have been identified, each with a distinctive structure, activity, expression, and tissue distribution. The PDE type-3, -4, and -5 (PDE3, PDE4, PDE5) are localized to specific regions of the cardiomyocyte, such as the sarcoplasmic reticulum and Z-disc, where they are likely to influence cAMP/cGMP signaling to the end effectors of contractility. Several PDE inhibitors exhibit remarkable hemodynamic and inotropic properties that may be valuable to clinical practice. In particular, PDE3 inhibitors have potent cardiotonic effects that can be used for short-term inotropic support, especially in situations where adrenergic stimulation is insufficient. Most relevant to this review, PDE inhibitors have also been found to have cytoprotective effects in the heart. For example, PDE3 inhibitors have been shown to be cardioprotective when given before ischemic attack, whereas PDE5 inhibitors, which include three widely used erectile dysfunction drugs (sildenafil, vardenafil and tadalafil), can induce remarkable cardioprotection when administered either prior to ischemia or upon reperfusion. This article provides an overview of the current laboratory and clinical evidence, as well as the cellular mechanisms by which the inhibitors of PDE3, PDE4 and PDE5 exert their beneficial effects on normal and ischemic hearts. It seems that PDE inhibitors hold great promise as clinically applicable agents that can improve cardiac performance and cell survival under critical situations, such as ischemic heart attack, cardiopulmonary bypass surgery, and heart failure.

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Diminished Inotropic Response to Amrinone in Ventricular Myocytes from Myopathic Hamsters Is Linked to Depression of High-Gain Ca²⁺-Induced Ca²⁺Release

Cited by 7 publications

References 27 publications

Contractile responses to selective phosphodiesterase inhibitors following chronic β-adrenoreceptor activation

Contractile responses to selective phosphodiesterase inhibitors following chronic β-adrenoreceptor activation

Myocardial Phosphodiesterases and Regulation of Cardiac Contractility in Health and Cardiac Disease

Pivotal effects of phosphodiesterase inhibitors on myocyte contractility and viability in normal and ischemic hearts

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Diminished Inotropic Response to Amrinone in Ventricular Myocytes from Myopathic Hamsters Is Linked to Depression of High-Gain Ca2+-Induced Ca2+Release

Cited by 7 publications

References 27 publications

Contractile responses to selective phosphodiesterase inhibitors following chronic β-adrenoreceptor activation

Contractile responses to selective phosphodiesterase inhibitors following chronic β-adrenoreceptor activation

Myocardial Phosphodiesterases and Regulation of Cardiac Contractility in Health and Cardiac Disease

Pivotal effects of phosphodiesterase inhibitors on myocyte contractility and viability in normal and ischemic hearts

Contact Info

Product

Resources

About

Diminished Inotropic Response to Amrinone in Ventricular Myocytes from Myopathic Hamsters Is Linked to Depression of High-Gain Ca²⁺-Induced Ca²⁺Release