| Literature DB >> 31002926 |
Prashanti Patil1, Micol Falabella2, Amal Saeed2, Dayeong Lee1, Brett Kaufman2, Sruti Shiva3, Claudette St Croix4, Ben Van Houten5, Laura J Niedernhofer6, Paul D Robbins6, Joon Lee1, Sowa Gwendolyn7, Nam V Vo8.
Abstract
Cellular senescence is a phenotype characterized by irreversible growth arrest, chronic elevated secretion of proinflammatory cytokines and matrix proteases, a phenomenon known as senescence-associated secretory phenotype (SASP). Biomarkers of cellular senescence have been shown to increase with age and degeneration of human disc tissue. Senescent disc cells in culture recapitulate features associated with age-related disc degeneration, including increased secretion of proinflammatory cytokines, matrix proteases, and fragmentation of matrix proteins. However, little is known of the metabolic changes that underlie the senescent phenotype of disc cells. To assess the metabolic changes, we performed a bioenergetic analysis of in vitro oxidative stress-induced senescent (SIS) human disc cells. SIS disc cells acquire SASP and exhibit significantly elevated mitochondrial content and mitochondrial ATP-linked respiration. The metabolic changes appear to be driven by the upregulated protein secretion in SIS cells as abrogation of protein synthesis using cycloheximide decreased mitochondrial ATP-linked respiration. Taken together, the results of the study suggest that the increased energy generation state supports the secretion of senescent associated proteins in SIS disc cells.Entities:
Keywords: Aging; Bioenergetics; Cellular senescence; Intervertebral disc degeneration; Matrix homeostasis; Mitochondria
Mesh:
Year: 2019 PMID: 31002926 DOI: 10.1016/j.mad.2019.04.006
Source DB: PubMed Journal: Mech Ageing Dev ISSN: 0047-6374 Impact factor: 5.432