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Large oncosomes mediate intercellular transfer of functional microRNA
Authors:Matteo Morello  Valentina R Minciacchi  Paola de Candia  Julie Yang  Edwin Posadas  Hyung Kim  Duncan Griffiths  Neil Bhowmick  Leland WK Chung  Paolo Gandellini  Michael R Freeman  Francesca Demichelis  Dolores Di Vizio
Abstract:Prostate cancer cells release atypically large extracellular vesicles (EVs), termed large oncosomes, which may play a role in the tumor microenvironment by transporting bioactive molecules across tissue spaces and through the blood stream. In this study, we applied a novel method for selective isolation of large oncosomes applicable to human platelet-poor plasma, where the presence of caveolin-1-positive large oncosomes identified patients with metastatic disease. This procedure was also used to validate results of a miRNA array performed on heterogeneous populations of EVs isolated from tumorigenic RWPE-2 prostate cells and from isogenic non-tumorigenic RWPE-1 cells. The results showed that distinct classes of miRNAs are expressed at higher levels in EVs derived from the tumorigenic cells in comparison to their non-tumorigenic counterpart. Large oncosomes enhanced migration of cancer-associated fibroblasts (CAFs), an effect that was increased by miR-1227, a miRNA abundant in large oncosomes produced by RWPE-2 cells. Our findings suggest that large oncosomes in the circulation report metastatic disease in patients with prostate cancer, and that this class of EV harbors functional molecules that may play a role in conditioning the tumor microenvironment.
Keywords:miRNA  prostate cancer  exosome  extracellular vesicles  microvesicle  amoeboid blebbing  filtration  large oncosome
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