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Organelle aging:Lessons from model organisms

Organelle aging:Lessons from model organisms
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摘要 Most cellular processes descend into failure during aging. While a large collection of longevity pathways has been identified in the past decades, the mechanism for age-related decline of cellular homeostasis and organelle function remains largely unsolved. It is known that many organelles undergo structural and functional changes during normal aging, which significantly contributes to the decline of tissue function at old ages. Since recent studies have revealed an emerging role of organelles as regulatory hubs in maintaining cellular homeostasis, understanding of organelle aging will provide important insights into the cellular basis of organismal aging. Here we review current progress on the characterization of age-dependent structural and functional alterations in the more well-studied organelles, as well as the known mechanisms governing organelle aging in model organisms, with a special focus on the fruit fly Drosophila melanogaster. Most cellular processes descend into failure during aging. While a large collection of longevity pathways has been identified in the past decades, the mechanism for age-related decline of cellular homeostasis and organelle function remains largely unsolved. It is known that many organelles undergo structural and functional changes during normal aging, which significantly contributes to the decline of tissue function at old ages. Since recent studies have revealed an emerging role of organelles as regulatory hubs in maintaining cellular homeostasis, understanding of organelle aging will provide important insights into the cellular basis of organismal aging. Here we review current progress on the characterization of age-dependent structural and functional alterations in the more well-studied organelles, as well as the known mechanisms governing organelle aging in model organisms, with a special focus on the fruit fly Drosophila melanogaster.
机构地区 Department of Genetics
出处 《Journal of Genetics and Genomics》 SCIE CAS CSCD 2019年第4期171-185,共15页 遗传学报(英文版)
基金 supported by US National Institutes of Health (NIH)/National Institute on Aging (NIA), R00AG048016 and R01AG058741 to H.B. Glenn Foundation/American Federation for Aging Research (AFAR) Scholarships for Research in the Biology of Aging to K.H.
关键词 LONGEVITY Mitochondria NUCLEUS AUTOPHAGOSOME LYSOSOME PROTEASOME Cell membrane Longevity Mitochondria Nucleus Autophagosome Lysosome Proteasome Cell membrane
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