期刊
EUROPEAN CELLS & MATERIALS
卷 42, 期 -, 页码 401-414出版社
AO RESEARCH INSTITUTE DAVOS-ARI
DOI: 10.22203/eCM.v042a25
关键词
Mesenchymal stem cells; cellular senescence; secretory phenotype; regenerative medicine; metabolism
资金
- Dutch Arthritis Society [16-1-201]
- NWO [P15-23]
TWIST1 influences the expansion of MSCs, and its silencing-induced senescence in MSCs is characterized by a specific SASP profile and metabolic state, different from irradiation-induced senescent MSCs.
Mesenchymal stem cells (MSCs) are promising cells for regenerative medicine therapies because they can differentiate towards multiple cell lineages. However, the occurrence of cellular senescence and the acquiring of the senescence-associated secretory phenotype (SASP) limit their clinical use. Since the transcription factor TWIST1 influences expansion of MSCs, its role in regulating cellular senescence was investigated. The present study demonstrated that silencing of TWIST1 in MSCs increased the occurrence of senescence, characterised by a SASP profile different from irradiation-induced senescent MSCs. Knowing that senescence alters cellular metabolism, cellular bioenergetics was monitored by using the Seahorse XF apparatus. Both TWIST1-silencing-induced and irradiation-induced senescent MSCs had a higher oxygen consumption rate compared to control MSCs, while TWIST1-silencing-induced senescent MSCs had a low extracellular acidification rate compared to irradiation-induced senescent MSCs. Overall, data indicated how TWIST1 regulation influenced senescence in MSCs and that TWIST1 silencing-induced senescence was characterised by a specific SASP profile and metabolic state.
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