Targeted deletion of titin N2B region leads to diastolic dysfunction and cardiac atrophy

Michael H Radke; Jun Peng; Yiming Wu; Mark McNabb; O. Lynne Nelson; Henk Granzier; Michael Gotthardt

doi:10.1073/pnas.0608543104

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Targeted deletion of titin N2B region leads to diastolic dysfunction and cardiac atrophy

Journal article

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Targeted deletion of titin N2B region leads to diastolic dysfunction and cardiac atrophy

Michael H Radke, Jun Peng, Yiming Wu, Mark McNabb, O. Lynne Nelson, Henk Granzier and Michael Gotthardt

Proceedings of the National Academy of Sciences - PNAS, Vol.104(9), pp.3444-3449

02/27/2007

DOI: https://doi.org/10.1073/pnas.0608543104

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https://hdl.handle.net/2376/103225

PMCID: PMC1805563

PMID: 17360664

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Abstract

Biological Sciences

mechanics

disease

hypertrophy

cardiac muscle

cardiology

Titin is a giant protein that is in charge of the assembly and passive mechanical properties of the sarcomere. Cardiac titin contains a unique N2B region, which has been proposed to modulate elasticity of the titin filament and to be important for hypertrophy signaling and the ischemic stress response through its binding proteins FHL2 and αB-crystallin, respectively. To study the role of the titin N2B region in systole and diastole of the heart, we generated a knockout (KO) mouse deleting only the N2B exon 49 and leaving the remainder of the titin gene intact. The resulting mice survived to adulthood and were fertile. Although KO hearts were small, they produced normal ejection volumes because of an increased ejection fraction. FHL2 protein levels were significantly reduced in the KO mice, a finding consistent with the reduced size of KO hearts. Ultrastructural analysis revealed an increased extension of the remaining spring elements of titin (tandem Ig segments and the PEVK region), which, together with the reduced sarcomere length and increased passive tension derived from skinned cardiomyocyte experiments, translates to diastolic dysfunction as documented by echocardiography. We conclude from our work that the titin N2B region is dispensable for cardiac development and systolic properties but is important to integrate trophic and elastic functions of the heart. The N2B-KO mouse is the first titin-based model of diastolic dysfunction and, considering the high prevalence of diastolic heart failure, it could provide future mechanistic insights into the disease process.

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Title: Targeted deletion of titin N2B region leads to diastolic dysfunction and cardiac atrophy
Creators: Michael H Radke - Department of Neuromuscular and Cardiovascular Cell Biology, Max-Delbrück-Center for Molecular Medicine, D-13122 Berlin-Buch, Germany; and
Jun Peng - Department of Veterinary and Comparative Anatomy, Pharmacology, and Physiology, and
Yiming Wu - Department of Veterinary and Comparative Anatomy, Pharmacology, and Physiology, and
Mark McNabb - Department of Veterinary and Comparative Anatomy, Pharmacology, and Physiology, and
O. Lynne Nelson - Department of Veterinary Clinical Sciences, Washington State University, Pullman, WA 99164
Henk Granzier - Department of Veterinary and Comparative Anatomy, Pharmacology, and Physiology, and
Michael Gotthardt - Department of Neuromuscular and Cardiovascular Cell Biology, Max-Delbrück-Center for Molecular Medicine, D-13122 Berlin-Buch, Germany; and
Publication Details: Proceedings of the National Academy of Sciences - PNAS, Vol.104(9), pp.3444-3449
Academic Unit: Integrative Physiology and Neuroscience, Department of
Publisher: National Academy of Sciences
Identifiers: 99900546650501842
Language: English
Resource Type: Journal article