Iron homeostasis and organismal aging.

Iron is indispensable for normal body functions across species because of its critical roles in red blood cell function and many essential proteins and enzymes required for numerous physiological processes. Regulation of iron homeostasis is an intricate process involving multiple modulators at the systemic, cellular, and molecular levels. Interestingly, emerging evidence has demonstrated that many modulators of iron homeostasis contribute to organismal aging and longevity. On the other hand, the age-related dysregulation of iron homeostasis is often associated with multiple age-related pathologies including bone resorption and neurodegenerative diseases such as Alzheimer's disease. Thus, a thorough understanding on the interconnections between systemic and cellular iron balance and organismal aging may help decipher the etiologies of multiple age-related diseases, which could ultimately lead to developing therapeutic strategies to delay aging and treat various age-related diseases. Here we present the current understanding on the mechanisms of iron homeostasis. We also discuss the impacts of aging on iron homeostatic processes and how dysregulated iron metabolism may affect aging and organismal longevity. • Tight regulation of physiological Fe levels is essential for normal body functions • Complex systemic, cellular, and molecular mechanisms maintain Fe homeostasis • Age-associated Fe dyshomeostasis and cellular Fe deposition are hallmarks of aging • Fe dyshomeostasis accelerates cellular senescence and organismal aging in animals • Fe overload leads to multiple age-related pathologies in humans [ABSTRACT FROM AUTHOR]