| Literature DB >> 35665306 |
Amrita Sahu1,2, Zachary J Clemens2, Sunita N Shinde1, Sruthi Sivakumar1,3, Abish Pius1,4, Ankit Bhatia5, Silvia Picciolini6, Cristiano Carlomagno6, Alice Gualerzi6, Marzia Bedoni6, Bennett Van Houten7, Mita Lovalekar8, Nicholas F Fitz2, Iliya Lefterov2, Aaron Barchowsky2,7, Radosveta Koldamova2, Fabrisia Ambrosio1,2,3,9.
Abstract
Heterochronic blood exchange (HBE) has demonstrated that circulating factors restore youthful features to aged tissues. However, the systemic mediators of those rejuvenating effects remain poorly defined. We show here that the beneficial effect of young blood on aged muscle regeneration was diminished when serum was depleted of extracellular vesicles (EVs). Whereas EVs from young animals rejuvenate aged cell bioenergetics and skeletal muscle regeneration, aging shifts EV subpopulation heterogeneity and compromises downstream benefits on recipient cells. Machine learning classifiers revealed that aging shifts the nucleic acid, but not protein, fingerprint of circulating EVs. Alterations in sub-population heterogeneity were accompanied by declines in transcript levels of the pro-longevity protein, α-Klotho, and injection of EVs improved muscle regeneration in a Klotho mRNA-dependent manner. These studies demonstrate that EVs play a key role in the rejuvenating effects of HBE and that Klotho transcripts within EVs phenocopy the effects of young serum on aged skeletal muscle.Entities:
Year: 2021 PMID: 35665306 PMCID: PMC9165723 DOI: 10.1038/s43587-021-00143-2
Source DB: PubMed Journal: Nat Aging ISSN: 2662-8465