Cardiac hypertrophy induced by sustained β-adrenoreceptor activation: pathophysiological aspects

Osadchii, Oleg E.

doi:10.1007/s10741-007-9007-4

Cited by 154 publications

(149 citation statements)

References 236 publications

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“…It is worth noting that this mechanism functions without an overall chronic activation of ␤-adrenergic pathways, that has proven detrimental to cardiac function (see Ref. 41 for review). Thus the cTnI N-terminal extension serves as a mechanism to modulate cardiac Ca 2ϩ sensitivity and cross-bridge cycling by ␤-adrenergic induced phosphorylation at Ser-23/24 or through its removal, both resulting from an alteration of its interaction with TnC to favor the closed conformation.…”

Section: Discussionmentioning

confidence: 99%

Removal of the Cardiac Troponin I N-terminal Extension Improves Cardiac Function in Aged Mice

Biesiadecki¹,

Tachampa

Yuan

et al. 2010

Journal of Biological Chemistry

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The cardiac troponin I (cTnI) isoform contains a unique N-terminal extension that functions to modulate activation of cardiac myofilaments. During cardiac remodeling restricted proteolysis of cTnI removes this cardiac specific N-terminal modulatory extension to alter myofilament regulation. We have demonstrated expression of the N-terminal-deleted cTnI (cTnI-ND) in the heart decreased the development of the cardiomyopathy like phenotype in a ␤-adrenergic-deficient transgenic mouse model. To investigate the potential beneficial effects of cTnI-ND on the development of naturally occurring cardiac dysfunction, we measured the hemodynamic and biochemical effects of cTnI-ND transgenic expression in the aged heart. Echocardiographic measurements demonstrate cTnI-ND transgenic mice exhibit increased systolic and diastolic functions at 16 months of age compared with age-matched controls. This improvement likely results from decreased Ca 2؉ sensitivity and increased cross-bridge kinetics as observed in skinned papillary bundles from young transgenic mice prior to the effects of aging. Hearts of cTnI-ND transgenic mice further exhibited decreased ␤ myosin heavy chain expression compared to age matched nontransgenic mice as well as altered cTnI phosphorylation. Finally, we demonstrated cTnI-ND expressed in the heart is not phosphorylated indicating the cTnI N-terminal is necessary for the higher level phosphorylation of cTnI. Taken together, our data suggest the regulated proteolysis of cTnI during cardiac stress to remove the unique cardiac N-terminal extension functions to improve cardiac contractility at the myofilament level and improve overall cardiac function.Troponin I (TnI), 2 the inhibitory domain of the troponin (Tn) complex, is an essential protein involved in regulation of the actin-myosin interaction responsible for striated muscle contraction. Troponin I is encoded by three muscle genes expressing fast skeletal, slow skeletal, and cardiac TnI (cTnI) isoforms (1), with the cTnI gene the most recently evolved (2). Unlike the fast and slow skeletal isoforms, the cTnI isoform has evolved to contain a unique 32 amino acid N-terminal extension with the function of modulating cardiac contraction. In response to ␤-adrenergic-induced stimulatory G-protein (G s ␣) activation of protein kinase A (PKA), Ser-23/24 of the cTnI N-terminal extension are bis-phosphorylated (3). Phosphorylation of these residues alters cTnI structure diminishing the cTnI N-terminal interaction with troponin C (TnC) to decrease Ca 2ϩ -sensitive activation of muscle contraction (4, 5) and increase myosin cross-bridge kinetics (6 -8). Functionally, this structural change in the modulatory cTnI N-terminal extension is essential to increase the rate of myocardial relaxation and maintain adequate diastolic filling during the increased heart rate of ␤-adrenergic stimulation to meet increased cardiac demand. Non-physiological truncations removing the cTnI N-terminal extension result in a cTnI molecule that exhibits similar structural and functional al...

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Section: Discussionmentioning

confidence: 99%

Removal of the Cardiac Troponin I N-terminal Extension Improves Cardiac Function in Aged Mice

Biesiadecki¹,

Tachampa

Yuan

et al. 2010

Journal of Biological Chemistry

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“…In experiments, transgenic overexpression of 1-adrenergic receptors in the murine heart causes dilated cardiomyopathy (Engelhardt et al, 1999). We also found that metoprolol, a selective 1-adrenergic antagonist, almost completely prevented cardiac hypertrophy and failure of isoproterenol-treated mice (data not shown), indicating that excessive stimulation of 1-adrenergic receptors is the primary cause of myocardial remodeling in isoproterenol-treated mice (Osadchii, 2007;Xiao et al, 2006).…”

Section: Discussionmentioning

confidence: 62%

“…In heart failure, chronic and excessive -adrenergic receptor stimulation causes remodeling of the myocardium and aggravates cardiac function (Osadchii, 2007;Rockman et al, 2002). This concept is the theoretical basis for the treatment of heart failure with -adrenergic antagonists.…”

Section: Discussionmentioning

confidence: 99%

“…Thus, development of medical treatment based on further understanding of the pathophysiology of heart failure is required to improve the quality of life of patients with heart failure. Maladaptive remodeling of ventricular excitation-contraction (EC) coupling caused by such as chronic -adrenergic receptor stimulation, and activation of the reninangiotensin-aldosterone system plays a predominant role in an impaired cardiac function in heart failure (Mann, 2008;Osadchii, 2007;Rockman et al, 2002). The underlying primary defect is a decrease in sarcoplasmic reticulum (SR) Ca 2+ content due to decreased activity and/or expression of SR Ca 2+ -ATPase 2, increased expression of sarcolemmal Na + /Ca 2+ exchangers and diastolic Ca 2+ leak from the SR via ryanodine receptors (Bers, 2008).…”

Section: Introductionmentioning

confidence: 99%

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β2-Adrenergic and M2-muscarinic receptors decrease basal t-tubular L-type Ca2+ channel activity and suppress ventricular contractility in heart failure

Kashihara

Hirose

Shimojo

et al. 2014

European Journal of Pharmacology

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L-type Ca 2+ channels (LTCC) play a crucial role in cardiac excitation-contraction coupling.We previously found that in failing ventricular myocytes of mice chronically treated with isoproterenol, basal t-tubular (TT) LTCC activity was halved by activation of protein phosphatase (PP)2A whereas basal surface sarcolemmal (SS) LTCC activity was doubled by inhibition of PP1.Interestingly, chronic treatment of these mice with pertussis toxin almost completely normalized TT and SS LTCC densities and cardiac contractility. In the present study, we therefore sought to identify the Gi/o protein-coupled receptors in cardiac myocytes (i.e. 2-adrenergic, M2-muscarinic and A1-adenosine receptors) that are responsible for these abnormalities in heart failure by chronically administrating mice a selective antagonist of each receptor (ICI118,551, atropine and 8-cyclopentyl-1,3-dipropilxanthine (DPCPX), respectively) with isoproterenol. Compared with mice treated with isoproterenol alone, mice treated with isoproterenol plus ICI118,551 or atropine, but not DPCPX showed significantly lower lung weight/tibial length, higher fractional shortening, lower left ventricular end-diastolic pressure and higher dP/dtmax and dP/dtmin. In addition, ventricular myocytes of mice treated with isoproterenol plus ICI118,551 or atropine, but not DPCPX exhibited significantly higher TT and lower SS LTCC current densities than those of mice treated with isoproterenol alone due to normalization of the PP activities. These results indicate that 2-adrenergic, M2-muscarinic, but not A1-adenosine receptors contribute to reduced ventricular 3 contractility at least partially by decreasing basal TT LTCC activity in heart failure. Therefore, antagonists of 2-adrenergic and/or M2-muscarinic receptors can be good adjuncts to 1-adrenergic receptor antagonists in the treatment of heart failure.

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“…1,3 Chronic AR stimulation promotes pathological remodeling, leading to hypertrophy and/or heart failure. 2,7,8 b 1 -AR signaling shows strong down-regulation in pathophysiological conditions, whereas a 1 -AR expression does not change. 5 Relative increases in a 1 -AR expression levels raise this receptor subtype to a more important role in the regulation of cardiac function in pathophysiological conditions.…”

mentioning

confidence: 99%

Combined blockade of β- and α1-adrenoceptors in left ventricular remodeling induced by hypertension: Beneficial or not?

Lopes

2010

Hypertens Res

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Cardiac hypertrophy induced by sustained β-adrenoreceptor activation: pathophysiological aspects

Cited by 154 publications

References 236 publications

Removal of the Cardiac Troponin I N-terminal Extension Improves Cardiac Function in Aged Mice

Removal of the Cardiac Troponin I N-terminal Extension Improves Cardiac Function in Aged Mice

β2-Adrenergic and M2-muscarinic receptors decrease basal t-tubular L-type Ca2+ channel activity and suppress ventricular contractility in heart failure

Combined blockade of β- and α1-adrenoceptors in left ventricular remodeling induced by hypertension: Beneficial or not?

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