Aging is a complex process of progressive decline in overall physiological functions, resulting in a diminished capacity to withstand internal and external damage and an increased susceptibility to diseases and risk of death. The process of aging is controlled by many factors including genetic and environmental influences, and many theories have been proposed to explain the phenomenon of aging. Recent studies have implicated mitochondrial dysfunction and oxidative stress in the aging process and in the pathogenesis of age-associated diseases. It is hypothesized that damage to mitochondria including mitochondrial DNA (mtDNA) caused by the production of reactive oxygen species (ROS) during cellular respiration is one of the drivers of aging. These theories (the free radical theory and the mitochondrial vicious cycle theory of aging) provide an important conceptual framework and have led to interventions aimed at decreasing the level of ROS for health benefits. However, there is an increasing body of evidence challenging these theories, which has led to the emergence of new hypotheses on how age-associated mitochondrial dysfunction may lead to aging. The gradual ROS response theory of aging proposes that ROS act as signaling molecules to induce endogenous defense mechanisms to promote stress resistance and longevity, which provides a new interpretation of studies previously found to have a conceptual conflict with the mitochondrial and free radical theories of aging. In this chapter, we provide an overview of the relationship between ROS-induced damage, mitochondria dysfunction and aging.

ROS are highly reactive molecules that include superoxide anion, hydroxyl radical and hydrogen peroxide. ROS are produced as by-products of aerobic metabolism in cells, and mitochondria are the major sites of ROS generation. In humans, more than 90% of oxygen is consumed by mitochondria, and 1-5% of the consumed oxygen is transformed into superoxide because of electron leakage of the electron transport chain (ETC). Superoxide generated in mitochondria is then converted to hydrogen peroxide either spontaneously or catalyzed by superoxide dismutase (SOD) [1]. Hydrogen peroxide is membrane permeable and diffusible. It can either be broken down into water by glutathione peroxidase, thioredoxin peroxidase and catalase, or undergo Fenton's reaction in the presence of divalent cations such as Fe²⁺ and Cu²⁺ to produce more aggressive hydroxyl radicals [2, 3]. In addition to mitochondria, peroxi-somes also participate in ROS generation and scavenging. Peroxisomes are involved in several metabolic functions that use oxygen. Oxygen consumption in the peroxi-somes leads to hydrogen peroxide production, which is then used to oxidize a variety of molecules [4]. Apart from being generated during cellular metabolism, ROS can be produced by excessive stimulation of nicotinamide adenine dinucleotide phosphate oxidases [5] or in response to different environmental stimuli such as growth factors, inflammatory cytokines, ionizing radiation, UV, chemical oxidants, toxins, chemotherapeutics, hyperoxia, and transition metals [6-20].

Accumulation of ROS and oxidative damage is one of the cellular hallmarks of aging. In the 1950s, Denham Harman proposed the free radical theory of aging, which postulates that the production of intracellular ROS and its deleterious effects on various cellular components are the major determinants of life span [35]. This landmark theory initiates the molecular era of aging research. In addition to being a main sou...