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Hypoxia Inducible Factor-1α Potentiates Jagged 1-Mediated Angiogenesis by Mesenchymal Stem Cell-Derived Exosomes.

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TLDR
Exosomes derived from MSCs stably overexpressing HIF‐1α have an increased angiogenic capacity in part via an increase in the packaging of Jagged1, which could have potential applications for the treatment of ischemia‐related disease.
Abstract
Insufficient vessel growth associated with ischemia remains an unresolved issue in vascular medicine. Mesenchymal stem cells (MSCs) have been shown to promote angiogenesis via a mechanism that is potentiated by hypoxia. Overexpression of hypoxia inducible factor (HIF)-1α in MSCs improves their therapeutic potential by inducing angiogenesis in transplanted tissues. Here, we studied the contribution of exosomes released by HIF-1α-overexpressing donor MSCs (HIF-MSC) to angiogenesis by endothelial cells. Exosome secretion was enhanced in HIF-MSC. Omics analysis of miRNAs and proteins incorporated into exosomes pointed to the Notch pathway as a candidate mediator of exosome communication. Interestingly, we found that Jagged1 was the sole Notch ligand packaged into MSC exosomes and was more abundant in HIF-MSC than in MSC controls. The addition of Jagged1-containing exosomes from MSC and HIF-MSC cultures to endothelial cells triggered transcriptional changes in Notch target genes and induced angiogenesis in an in vitro model of capillary-like tube formation, and both processes were stimulated by HIF-1α. Finally, subcutaneous injection of Jagged 1-containing exosomes from MSC and HIF-MSC cultures in the Matrigel plug assay induced angiogenesis in vivo, which was more robust when they were derived from HIF-MSC cultures. All Jagged1-mediated effects could be blocked by prior incubation of exosomes with an anti-Jagged 1 antibody. All together, the results indicate that exosomes derived from MSCs stably overexpressing HIF-1α have an increased angiogenic capacity in part via an increase in the packaging of Jagged1, which could have potential applications for the treatment of ischemia-related disease. Stem Cells 2017;35:1747-1759.

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Citations
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Autophagy: a promising therapeutic target for improving mesenchymal stem cell biological functions.

TL;DR: The role of autophagy regulation by various physical and chemical factors on the biological functions of MSCs in vitro and in vivo is focused on, and some strategies for enhancing the therapeutic efficacy of M SCs are provided.
Journal ArticleDOI

Exosomes secreted from mesenchymal stem cells mediate the regeneration of endothelial cells treated with rapamycin by delivering pro-angiogenic microRNAs.

TL;DR: It is indicated that MSC-derived exosomes could be ingested into umbilical vein endothelial cells (HUVECs) and significantly enhanced cell proliferation rate, migratory and tube-forming capabilities in vitro and inhibited the apoptosis of HUV ECs induced by rapamycin.
Journal ArticleDOI

State of the Field: Cellular Therapy Approaches in Microvascular Regeneration.

TL;DR: The state of the field in terms of common therapeutic cell population isolation techniques, their unique characteristics and their advantages and disadvantages, common molecular mechanisms of cell therapies to restore vascularization and/or vascular function, and arguments for and against allogenic vs. autologous applications ofcell therapies are discussed.
Journal ArticleDOI

Dental pulp stem cells from human teeth with deep caries displayed an enhanced angiogenesis potential in vitro.

TL;DR: In this paper, the angiogenic potential of dental pulp stem cells from human normal and infected human teeth with deep caries was investigated and compared to dental pulp cells from normal human teeth.
Journal ArticleDOI

Hypoxia-induced HIF1α activation regulates small extracellular vesicle release in human embryonic kidney cells

TL;DR: In this article , the authors investigated the requirement of HIF pathway activation for extracellular vesicles (EVs) release in Human Embryonic Kidney Cells (HEK293) and found that EV release increased concomitantly with sustained HIF1α and HIF2α activation following the onset of hypoxia.
References
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Journal ArticleDOI

Notch Signaling: Cell Fate Control and Signal Integration in Development

TL;DR: Notch signaling defines an evolutionarily ancient cell interaction mechanism, which plays a fundamental role in metazoan development, providing a general developmental tool to influence organ formation and morphogenesis.
Journal ArticleDOI

Isolation and Characterization of Exosomes from Cell Culture Supernatants and Biological Fluids

TL;DR: This unit describes different approaches for exosome purification from various sources, and discusses methods to evaluate the purity and homogeneity of the purified exosomes preparations.
Journal ArticleDOI

Membrane vesicles as conveyors of immune responses

TL;DR: The role of membrane vesicles, in particular exosomes, in the communication between immune cells, and between tumour and immune cells is focused on.
Journal ArticleDOI

Tumour exosome integrins determine organotropic metastasis

TL;DR: It is demonstrated that exosomes from mouse and human lung-, liver- and brain-tropic tumour cells fuse preferentially with resident cells at their predicted destination, namely lung fibroblasts and epithelial cells, liver Kupffer cells and brain endothelial cells.
Journal ArticleDOI

Concise review: mesenchymal stem/multipotent stromal cells: the state of transdifferentiation and modes of tissue repair--current views.

TL;DR: Critically evaluate the literature describing the plasticity of MSCs and offer insight into how the molecular and functional heterogeneity of this cell population, which reflects the complexity of marrow stroma as an organ system, may confound interpretation of their transdifferentiation potential.
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