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Vutiglabridin Alleviates Cellular Senescence with Metabolic Regulation and Circadian Clock in Human Dermal Fibroblasts

Title
Vutiglabridin Alleviates Cellular Senescence with Metabolic Regulation and Circadian Clock in Human Dermal Fibroblasts
Author(s)
Heo, Jin-WoongLee, Hye-EunLee, JiminChoi, Leo SungwongShin, JaejinMun, Ji-YoungPark, Hyung-SoonPark, Sang-ChulNam, Chang-Hoon
Issued Date
2024-01
Citation
Antioxidants, v.13, no.1
Type
Article
Author Keywords
human dermal fibroblastscellular senescencecircadian clocksmetabolismmitochondrial homeostasis
Keywords
OXIDATIVE STRESSMITOCHONDRIAL DYSFUNCTIONHUMAN-CELLSDNA-DAMAGEKINASEACTIVATIONMECHANISMSBMAL1RHYTHMCONNECTIONS
ISSN
2076-3921
Abstract
The process of cellular senescence, which is characterized by stable cell cycle arrest, is strongly associated with dysfunctional cellular metabolism and circadian rhythmicity, both of which are reported to result from and also be causal to cellular senescence. As a result, modifying any of them—senescence, metabolism, or the circadian clock—may affect all three simultaneously. Obesity accelerates aging by disrupting the homeostasis of reactive oxygen species (ROS) via an increased mitochondrial burden of fatty acid oxidation. As a result, if senescence, metabolism, and circadian rhythm are all linked, anti-obesity treatments may improve metabolic regulation while also alleviating senescence and circadian rhythm. Vutiglabridin is a small molecule in clinical trials that improves obesity by enhancing mitochondrial function. We found that chronic treatment of senescent primary human dermal fibroblasts (HDFs) with vutiglabridin alleviates all investigated markers of cellular senescence (SA-β-gal, CDKN1A, CDKN2A) and dysfunctional cellular circadian rhythm (BMAL1) while remarkably preventing the alterations of mitochondrial function and structure that occur during the process of cellular senescence. Our results demonstrate the significant senescence-alleviating effects of vutiglabridin, specifically with the restoration of cellular circadian rhythmicity and metabolic regulation. These data support the potential development of vutiglabridin against aging-associated diseases and corroborate the intricate link between cellular senescence, metabolism, and the circadian clock. © 2024 by the authors.
URI
http://hdl.handle.net/20.500.11750/47978
DOI
10.3390/antiox13010109
Publisher
MDPI
Related Researcher
  • 남창훈 Nam, Chang-Hoon
  • Research Interests Protein Engineering; History and Philosophy of Science; Scientific Art; Biomaterial Development (Tissue Engineering) with modified bacteriophage; Bio Sensor Development
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Appears in Collections:
Department of New Biology Aging and Immunity Lab 1. Journal Articles

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