| Literature DB >> 26334526 |
Peter J Quesenberry1, Jason Aliotta2, Maria Chiara Deregibus3,4, Giovanni Camussi5.
Abstract
Growing evidence suggests that transcriptional regulators and secreted RNA molecules encapsulated within membrane vesicles modify the phenotype of target cells. Membrane vesicles, actively released by cells, represent a mechanism of intercellular communication that is conserved evolutionarily and involves the transfer of molecules able to induce epigenetic changes in recipient cells. Extracellular vesicles, which include exosomes and microvesicles, carry proteins, bioactive lipids, and nucleic acids, which are protected from enzyme degradation. These vesicles can transfer signals capable of altering cell function and/or reprogramming targeted cells. In the present review we focus on the extracellular vesicle-induced epigenetic changes in recipient cells that may lead to phenotypic and functional modifications. The relevance of these phenomena in stem cell biology and tissue repair is discussed.Entities:
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Year: 2015 PMID: 26334526 PMCID: PMC4558901 DOI: 10.1186/s13287-015-0150-x
Source DB: PubMed Journal: Stem Cell Res Ther ISSN: 1757-6512 Impact factor: 6.832
Fig. 1Combined factors that modulate cell fate and functions. a Soluble growth factors may act as paracrine or autocrine mechanisms by interacting with cell receptors directly or after binding to matrix; extracellular matrix and direct cell-to-cell contact may in turn direct cell fate in a defined microenvironment. The interaction between stem and stromal cells is reciprocal. In addition, oxygen tension and metabolic products may modulate cell phenotype. Extracellular vesicles are part of this complex regulatory network of factors involved in the interaction between cells. b Schematic representation of different modes of action of extracellular vesicles. lncRNA long noncoding RNA, miRNA microRNA
Fig. 2Model of extracellular vesicle-induced modulation of cell phenotype involved in the repair of tissue injury. EV extracellular vesicle, lncRNA long noncoding RNA, miRNA microRNA