Gene expression profiling of the aging mouse cardiac myocytes
AUTOR(ES)
Bodyak, Natalya
FONTE
Oxford University Press
RESUMO
Heart disease remains the most frequent cause of death in the general population with increasing incidence in the elderly population. The pathologic failure of the aging heart may be related to structural and functional alterations in cardiac muscle cells. However, the molecular mechanisms underlying the aging-related decline in cardiac muscle function are largely unknown. To provide the first analysis of cardiac aging at the level of gene expression, we established and compared cDNA libraries from apparently healthy young and aged mouse ventricular cardiac muscle cells. We report the identification of genes that exhibit aging-related changes of mRNA levels. Aging expression profiles in aged hearts indicate decreased cellular adaptation and protection against stress-induced injury together with the development of contractile dysfunction. The data suggest reduced activity of the mitochondrial electron transport system and reduced levels of cardiac-specific transcription regulators. The cardiomyocyte aging profile of gene expression displays similarities with known heart disorders. Genes whose mRNA levels change with aging in cardiomyocytes might profoundly affect pathological changes in the heart.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=137419Documentos Relacionados
- Gene expression profiling in Werner syndrome closely resembles that of normal aging
- Profiling gene expression in growth-arrested mouse embryos in diapause
- Evaluation of gene expression profiling in a mouse model of L-gulonolactone oxidase gene deficiency
- Electrophysiological properties of neonatal mouse cardiac myocytes in primary culture.
- Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate
