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Publication : SIRT3 reverses aging-associated degeneration.

First Author  Brown K Year  2013
Journal  Cell Rep Volume  3
Issue  2 Pages  319-27
PubMed ID  23375372 Mgi Jnum  J:269808
Mgi Id  MGI:6274009 Doi  10.1016/j.celrep.2013.01.005
Citation  Brown K, et al. (2013) SIRT3 reverses aging-associated degeneration. Cell Rep 3(2):319-27
abstractText  Despite recent controversy about their function in some organisms, sirtuins are thought to play evolutionarily conserved roles in lifespan extension. Whether sirtuins can reverse aging-associated degeneration is unknown. Tissue-specific stem cells persist throughout the entire lifespan to repair and maintain tissues, but their self-renewal and differentiation potential become dysregulated with aging. We show that SIRT3, a mammalian sirtuin that regulates the global acetylation landscape of mitochondrial proteins and reduces oxidative stress, is highly enriched in hematopoietic stem cells (HSCs) where it regulates a stress response. SIRT3 is dispensable for HSC maintenance and tissue homeostasis at a young age under homeostatic conditions but is essential under stress or at an old age. Importantly, SIRT3 is suppressed with aging, and SIRT3 upregulation in aged HSCs improves their regenerative capacity. Our study illuminates the plasticity of mitochondrial homeostasis controlling stem cell and tissue maintenance during the aging process and shows that aging-associated degeneration can be reversed by a sirtuin.
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