The mitochondrial theory of aging proposes that reactive oxygen species (ROS) generated inside the cell will lead, with time, to increasing amounts of oxidative damage to various cell components. The main site for ROS production is the respiratory chain inside the mitochondria and accumulation of mtDNA mutations, and impaired respiratory chain function have been associated with degenerative diseases and aging. The theory predicts that impaired respiratory chain function will augment ROS production and thereby increase the rate of mtDNA mutation accumulation, which, in turn, will further compromise respiratory chain function. Previously, we reported that mice expressing an error-prone version of the catalytic subunit of mtDNA polymerase accumulate a substantial burden of somatic mtDNA mutations, associated with premature aging phenotypes and reduced lifespan. Here we show that these mtDNA mutator mice accumulate mtDNA mutations in an approximately linear manner. The amount of ROS produced was normal, and no increased sensitivity to oxidative stress-induced cell death was observed in mouse embryonic fibroblasts from mtDNA mutator mice, despite the presence of a severe respiratory chain dysfunction. Expression levels of antioxidant defense enzymes, protein carbonylation levels, and aconitase enzyme activity measurements indicated no or only minor oxidative stress in tissues from mtDNA mutator mice. The premature aging phenotypes in mtDNA mutator mice are thus not generated by a vicious cycle of massively increased oxidative stress accompanied by exponential accumulation of mtDNA mutations. We propose instead that respiratory chain dysfunction per se is the primary inducer of premature aging in mtDNA mutator mice.mitochondria ͉ mtDNA mutator mice T he free radical theory of aging, formulated 50 years ago by Harman (1), proposes that aging and associated degenerative diseases can be attributed to deleterious effects of reactive oxygen species (ROS). Intracellular ROS are primarily generated by the mitochondrial electron transport chain, making the mitochondrial network a prime target of oxidative damage. Building on this, the mitochondrial theory of aging predicts that a vicious cycle contributes to the aging process. (i) Normal metabolism causes ROS production by the electron transport chain. (ii) ROS production induces damage to lipids, proteins, and nucleic acids in mitochondria. (iii) ROS-induced mtDNA mutations lead to the synthesis of functionally impaired respiratory chain subunits, causing respiratory chain dysfunction and augmented ROS production (2). (iv) This vicious cycle is proposed to cause an exponential increase of mtDNA mutations over time, resulting in aging and associated degenerative diseases. A substantial amount of correlative data from morphological, bioenergetic, biochemical, and genetic studies of mammalian tissues supports this theory (3). Mitochondria are larger and fewer in older individuals, and mitochondrial abnormalities such as vacuoles, abnormal cristae, and paracrystalline inclusions...
