Aging as a Mitochondria‐Mediated Atavistic Program: Can Aging Be Switched Off?

1 December 2005

journal article
Published by Wiley in Annals of the New York Academy of Sciences

Vol. 1057 (1) , 145-164
https://doi.org/10.1196/annals.1356.009

Abstract

Programmed death phenomena have been demonstrated on subcellular (mitoptosis), cellular (apoptosis), and supracellular (collective apoptosis) levels. There are numerous examples of suicide mechanisms at the organismal level (phenoptosis). In yeast, it was recently shown that the death of aging cells is programmed. Many of the steps of programmed cell death are shown to be common for yeast and animals, including mammals. In particular, generation of the mitochondrial reactive oxygen species (ROS) is involved in the suicide programs. Aging of higher animals is accompanied by an increase in damage induced by mitochondrial ROS. Perhaps prevention of such damage by scavenging of mitochondrial ROS might slow down or even switch off the aging programs.

Keywords

This publication has 96 references indexed in Scilit:

Programmed and altruistic ageing
Nature Reviews Genetics, 2005
Inhibitory effects of anticancer peptide from Mercenaria on the BGC‐823 cells and several enzymes
FEBS Letters, 2005
Cardiac disease due to random mitochondrial DNA mutations is prevented by cyclosporin A
Biochemical and Biophysical Research Communications, 2004
Genes that act downstream of DAF-16 to influence the lifespan of Caenorhabditis elegans
Nature, 2003
Genetics and the Specificity of the Aging Process
Science, 2003
Programmed death in yeast as adaptation?
FEBS Letters, 2002
Sex, kings and serial killers and other group-selected human traits
Medical Hypotheses, 2000
Population Viscosity and the Evolution of Altruism
Journal of Theoretical Biology, 2000
A C. elegans mutant that lives twice as long as wild type
Nature, 1993
Aging: A Theory Based on Free Radical and Radiation Chemistry
Journal of Gerontology, 1956