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  Enhanced cardiomyocyte Ca(2+) cycling precedes terminal AV-block in mitochondrial cardiomyopathy Mterf3 KO mice

Andersson, D. C., Fauconnier, J., Park, C. B., Zhang, S. J., Thireau, J., Ivarsson, N., et al. (2011). Enhanced cardiomyocyte Ca(2+) cycling precedes terminal AV-block in mitochondrial cardiomyopathy Mterf3 KO mice. Antioxid Redox Signal, 15(9), 2455-64. doi:10.1089/ars.2011.3915.

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Item Permalink: https://hdl.handle.net/21.11116/0000-000B-B403-6 Version Permalink: https://hdl.handle.net/21.11116/0000-000B-B404-5
Genre: Journal Article

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 Creators:
Andersson, D. C., Author
Fauconnier, J., Author
Park, C. B., Author
Zhang, S. J., Author
Thireau, J., Author
Ivarsson, N., Author
Larsson, N.G.1, Author           
Westerblad, H., Author
Affiliations:
1Department Larsson - Mitochondrial Biology, Max Planck Institute for Biology of Ageing, Max Planck Society, ou_1942286              

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Free keywords: Aconitate Hydratase/genetics/metabolism Animals Atrioventricular Block/genetics/*metabolism Blotting, Northern Blotting, Western Calcium/*metabolism Cardiomyopathies/genetics/*metabolism Cells, Cultured Citrate (si)-Synthase/genetics/metabolism Electrocardiography Membrane Potential, Mitochondrial/genetics/physiology Mice Mice, Knockout Mitochondrial Myopathies/genetics/*metabolism Mitochondrial Proteins/genetics/*metabolism Myocytes, Cardiac/*metabolism Reactive Oxygen Species/metabolism Superoxide Dismutase/genetics Transcription Factors/genetics/*metabolism
 Abstract: AIMS: Heart disease is commonly associated with altered mitochondrial function and signs of oxidative stress. This study elucidates whether primary cardiac mitochondrial dysfunction causes changes in cardiomyocyte handling of reactive oxygen species (ROS) and Ca(2+). We used a mouse model with a tissue-specific ablation of the recently discovered mtDNA transcription regulator Mterf3 (Mterf3 KO). These mice display a cardiomyopathy with severe respiratory chain dysfunction, cardiac hypertrophy, and shortened lifespan. ROS and Ca(2+) handling were measured using fluorescent indicators and confocal microscopy. RESULTS: Mterf3 KO hearts displayed no signs of increased ROS production or oxidative stress. Surprisingly, Mterf3 KO cardiomyocytes showed enlarged Ca(2+) transient amplitudes, faster sarcoplasmic reticulum (SR) Ca(2+) reuptake, and increased SR Ca(2+) load, resembling increased adrenergic stimulation. Furthermore, spontaneous releases of Ca(2+) were frequent in Mterf3 KO cardiomyocytes. Electrocardiography (measured with telemetry in freely moving mice) showed a terminal state in Mterf3 KO mice with gradually developing bradycardia and atrioventricular block. CONCLUSION: In conclusion, mitochondrial dysfunction induced by Mterf3 KO leads to a cardiomyopathy without signs of oxidative stress but with increased cardiomyocyte Ca(2+) cycling and an arrhythmogenic phenotype. These findings highlight the complex interaction between mitochondrial function, cardiomyocyte contractility, and compensatory mechanisms, such as activation of adrenergic signaling.

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 Dates: 2011-11-012011-03-09
 Publication Status: Issued
 Pages: -
 Publishing info: -
 Table of Contents: -
 Rev. Type: -
 Identifiers: Other: 21381862
DOI: 10.1089/ars.2011.3915
ISSN: 1523-0864
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Title: Antioxid Redox Signal
  Alternative Title : Antioxidants & redox signaling
Source Genre: Journal
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Pages: - Volume / Issue: 15 (9) Sequence Number: - Start / End Page: 2455 - 64 Identifier: -