Litcius/Paper detail

Mitovesicles are a novel population of extracellular vesicles of mitochondrial origin altered in Down syndrome

Pasquale D’Acunzo, Rocío Pérez‐González, Yohan Kim, Tal Hargash, Chelsea Miller, Melissa J. Alldred, Hediye Erdjument‐Bromage, Sai C. Penikalapati, Monika Pawlik, Mitsuo Saito, Mariko Saito, Stephen D. Ginsberg, Thomas A. Neubert, Chris N. Goulbourne, Efrat Levy

2021Science Advances278 citationsDOIOpen Access PDF

Abstract

Mitochondrial dysfunction is an established hallmark of aging and neurodegenerative disorders such as Down syndrome (DS) and Alzheimer's disease (AD). Using a high-resolution density gradient separation of extracellular vesicles (EVs) isolated from murine and human DS and diploid control brains, we identify and characterize a previously unknown population of double-membraned EVs containing multiple mitochondrial proteins distinct from previously described EV subtypes, including microvesicles and exosomes. We term these newly identified mitochondria-derived EVs "mitovesicles." We demonstrate that brain-derived mitovesicles contain a specific subset of mitochondrial constituents and that their levels and cargo are altered during pathophysiological processes where mitochondrial dysfunction occurs, including in DS. The development of a method for the selective isolation of mitovesicles paves the way for the characterization in vivo of biological processes connecting EV biology and mitochondria dynamics and for innovative therapeutic and diagnostic strategies.

Topics & Concepts

MicrovesiclesMitochondrionExtracellular vesiclesCell biologyBiologyPopulationGeneticsmicroRNAMedicineGeneEnvironmental healthExtracellular vesicles in diseaseRNA modifications and cancerMitochondrial Function and Pathology