Myosin isoenzymes in human hypertrophic hearts. Shift in atrial myosin heavy chains and in ventricular myosin light chains

Schaub, Marcus C.; Tuchschmid, C. R.; Srihari, Thota; Hirzel, H

doi:10.1093/eurheartj/5.suppl_f.85

Cited by 39 publications

(20 citation statements)

References 20 publications

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“…26 In addition, a number of cases of altered MLC1 ventricular expression in chronic cardiovascular disease states may be associated with significant functional consequences. Hypertrophied left ventricles of patients with ischemic, dilated, and hypertrophic cardiomyopathy express small amounts of atrial MLC1, [27][28][29] not normally present in the adult ventricle. Postsurgical return to a normal hemodynamic state decreased this ventricular expression of atrial MLC1.…”

Section: Discussionmentioning

confidence: 99%

Proteomic Analysis of Pharmacologically Preconditioned Cardiomyocytes Reveals Novel Phosphorylation of Myosin Light Chain 1

Arrell

Neverova

Fraser

et al. 2001

Circulation Research

102

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Abstract-Proteomic analysis of rabbit ventricular myocytes revealed a novel posttranslational modification to myosin light chain 1 (MLC1), consisting of phosphorylation at two sites. Subproteomic extraction to isolate myofilamentenriched fractions enabled determination of the extent of phosphorylation, which increased from 25.7Ϯ1.6% to 34.0Ϯ2.7% (meanϮSE, nϭ4; PϽ0.05) after adenosine treatment at levels sufficient to pharmacologically precondition the myocytes (100 mol/L). Mass spectrometry of MLC1 tryptic digests identified two peptide fragments modified by phosphorylation. These two phosphopeptides were characterized by peptide mass fingerprinting to determine the phosphorylation sites within rabbit ventricular MLC1, which correspond to Thr69 and Ser200 of rat MLC1, and to

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Section: Discussionmentioning

confidence: 99%

Proteomic Analysis of Pharmacologically Preconditioned Cardiomyocytes Reveals Novel Phosphorylation of Myosin Light Chain 1

Arrell

Neverova

Fraser

et al. 2001

Circulation Research

102

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show abstract

“…Permeabilized fiber studies from these mice showed a change in cardiac fiber function such that the incorporation of either ELC1 v or RLC2 v into atrial fibers caused decreased unloaded shortening velocity (787). Interestingly, myosin light-chain isoform switching, where the ventricular isoforms convert to the atrial light chains, has been documented in various human heart failure cases such as in congestive heart failure or in DCM (26, 601,794), suggesting important and divergent physiological roles in cardiac muscle for the ventricular versus atrial myosin light chains. The precise role of the different cardiac muscle MLC isoforms in cardiac function is not fully known.…”

Section: The Myosin Essential (Mlc-1/elc) and Regulatory (Mlc-2/ Rlc)mentioning

confidence: 99%

Designing Heart Performance by Gene Transfer

Davis¹,

Westfall²,

Townsend³

et al. 2008

Physiological Reviews

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The birth of molecular cardiology can be traced to the development and implementation of high-fidelity genetic approaches for manipulating the heart. Recombinant viral vector-based technology offers a highly effective approach to genetically engineer cardiac muscle in vitro and in vivo. This review highlights discoveries made in cardiac muscle physiology through the use of targeted viral-mediated genetic modification. Here the history of cardiac gene transfer technology and the strengths and limitations of viral and nonviral vectors for gene delivery are reviewed. A comprehensive account is given of the application of gene transfer technology for studying key cardiac muscle targets including Ca2+handling, the sarcomere, the cytoskeleton, and signaling molecules and their posttranslational modifications. The primary objective of this review is to provide a thorough analysis of gene transfer studies for understanding cardiac physiology in health and disease. By comparing results obtained from gene transfer with those obtained from transgenesis and biophysical and biochemical methodologies, this review provides a global view of cardiac structure-function with an eye towards future areas of research. The data presented here serve as a basis for discovery of new therapeutic targets for remediation of acquired and inherited cardiac diseases.

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“…Therefore, this protein has been designated the embryonic myosin light chain (MLC) (16). The expression of this isoform was detected in the hypertrophied human ventricle (17). The hypertrophied right ventricle of children with tetralogy of Fallot (18) and the hemodynamically overloaded left ventricle of patients with valvular disease (19,20) also express a large amount of ALC 1 .…”

Section: Myofibrillar Assembly In Cardiac Hypertrophymentioning

confidence: 99%

“…Although ALC 1 becomes re-expressed in the overloaded human ventricle (17,19,20,22,74), β-MHC may combine with either ALC 1 and/or ventricular light chain 1 (VLC 1 ) to form two homodimers and one heterodimer in diseased human ventricles (23). The main consequence of ALC 1 re-expression in the ventricle is the increase of Ca 2+ sensitivity of the contractile apparatus (74).…”

Section: Myofibrillar Assembly In Congestive Hfmentioning

confidence: 99%

Myofibrillar remodelling in cardiac hypertrophy, heart failure and cardiomyopathies

Macháčková¹,

Barta²,

Dhalla³

2006

Canadian Journal of Cardiology

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Myosin isoenzymes in human hypertrophic hearts. Shift in atrial myosin heavy chains and in ventricular myosin light chains

Abstract: (J Clin Invest 1982; 69: 816-825

Cited by 39 publications

References 20 publications

Proteomic Analysis of Pharmacologically Preconditioned Cardiomyocytes Reveals Novel Phosphorylation of Myosin Light Chain 1

Proteomic Analysis of Pharmacologically Preconditioned Cardiomyocytes Reveals Novel Phosphorylation of Myosin Light Chain 1

Designing Heart Performance by Gene Transfer

Myofibrillar remodelling in cardiac hypertrophy, heart failure and cardiomyopathies

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