| Literature DB >> 27135165 |
Mario Baumgart1, Steffen Priebe2, Marco Groth1, Nils Hartmann1, Uwe Menzel2, Luca Pandolfini3, Philipp Koch1, Marius Felder1, Michael Ristow4, Christoph Englert5, Reinhard Guthke2, Matthias Platzer1, Alessandro Cellerino6.
Abstract
Mutations and genetic variability affect gene expression and lifespan, but the impact of variations in gene expression within individuals on their aging-related mortality is poorly understood. We performed a longitudinal study in the short-lived killifish, Nothobranchius furzeri, and correlated quantitative variations in gene expression during early adult life with lifespan. Shorter- and longer-lived individuals differ in their gene expression before the onset of aging-related mortality; differences in gene expression are more pronounced early in life. We identified mitochondrial respiratory chain complex I as a hub in a module of genes whose expression is negatively correlated with lifespan. Accordingly, partial pharmacological inhibition of complex I by the small molecule rotenone reversed aging-related regulation of gene expression and extended lifespan in N. furzeri by 15%. These results support the use of N. furzeri as a vertebrate model for identifying the protein targets, pharmacological modulators, and individual-to-individual variability associated with aging.Entities:
Keywords: GAGE; Nothobranchius furzeri; RNA transport; RNA-seq; aging; history trait; hormesis; hourglass; life ribosome; lifespan regulation; longevity; longitudinal study; mitohormesis; rejuvenation; weighted gene coexpression network analysis (WGCNA); zebrafish
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Year: 2016 PMID: 27135165 DOI: 10.1016/j.cels.2016.01.014
Source DB: PubMed Journal: Cell Syst ISSN: 2405-4712 Impact factor: 10.304