MicroRNA and mRNA cargo of extracellular vesicles from porcine adipose tissue-derived mesenchymal stem cells

Eirin, Alfonso; Riester, Scott M.; Zhu, Xiang Yang; Tang, Hui; Evans, Jared M.; O’Brien, Daniel R.; Wijnen, André J. van; Lerman, Lilach O.

doi:10.1016/j.gene.2014.08.041

Cited by 233 publications

(247 citation statements)

References 60 publications

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“…Exosomes represent the release of extracellular vesicles carrying predominantly proteins, mRNAs, and microRNAs that are exchanged during cellular interactions [57]. Production of exosomes has been described for MSC to transport gene regulatory information to recipient cells that can modulate cell growth and angiogenesis by affecting a variety of cellular pathways [58]. Indeed, the CD73, CD90, and CD105 induction in the different tumor cells was observed at both the protein and mRNA levels, suggesting exchange of proteins and/or transcriptional regulators and/or mRNAs between MSC and co-cultured tumor cells.…”

Section: Discussionmentioning

confidence: 99%

Human Mesenchymal Stroma/Stem Cells Exchange Membrane Proteins and Alter Functionality During Interaction with Different Tumor Cell Lines

Yang

Otte

Hass

2015

Stem Cells and Development

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To analyze effects of cellular interaction between human mesenchymal stroma/stem cells (MSC) and different cancer cells, direct co-cultures were performed and revealed significant growth stimulation of the tumor populations and a variety of protein exchanges. More than 90% of MCF-7 and primary human HBCEC699 breast cancer cells as well as NIH:OVCAR-3 ovarian adenocarcinoma cells acquired CD90 proteins during MSC co-culture, respectively. Furthermore, SK-OV-3 ovarian cancer cells progressively elevated CD105 and CD90 proteins in co-culture with MSC. Primary small cell hypercalcemic ovarian carcinoma cells (SCCOHT-1) demonstrated undetectable levels of CD73 and CD105; however, both proteins were significantly increased in the presence of MSC. This co-culture-mediated protein induction was also observed at transcriptional levels and changed functionality of SCCOHT-1 cells by an acquired capability to metabolize 5¢cAMP. Moreover, exchange between tumor cells and MSC worked bidirectional, as undetectable expression of epithelial cell adhesion molecule (EpCAM) in MSC significantly increased after co-culture with SK-OV-3 or NIH:OVCAR-3 cells. In addition, a small population of chimeric/hybrid cells appeared in each MSC/tumor cell co-culture by spontaneous cell fusion. Immune fluorescence demonstrated nanotube structures and exosomes between MSC and tumor cells, whereas cytochalasin-D partially abolished the intercellular protein transfer. More detailed functional analysis of FACS-separated MSC and NIH:OVCAR-3 cells after co-culture revealed the acquisition of epithelial cell-specific properties by MSC, including increased gene expression for cytokeratins and epithelial-like differentiation factors. Vice versa, a variety of transcriptional regulatory genes were downmodulated in NIH:OVCAR-3 cells after co-culture with MSC. Together, these mutual cellular interactions contributed to functional alterations in MSC and tumor cells.

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Section: Discussionmentioning

confidence: 99%

Human Mesenchymal Stroma/Stem Cells Exchange Membrane Proteins and Alter Functionality During Interaction with Different Tumor Cell Lines

Yang

Otte

Hass

2015

Stem Cells and Development

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“…We have previously shown that EVs released from porcine adipose tissue-derived MSCs transport gene regulatory information to modulate angiogenesis, adipogenesis, and other cell pathways in recipient cells [4, 5]. We have also shown that EVs are enriched with proteins linked to a broad range of biological functions, including angiogenesis, inflammation, apoptosis, and extracellular matrix remodeling[5] [6].…”

Section: Introductionmentioning

confidence: 99%

The metabolic syndrome alters the miRNA signature of porcine adipose tissue‐derived mesenchymal stem cells

et al. 2017

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Background Autologous transplantation of mesenchymal stem cells (MSCs) may be a viable option for the treatment of several diseases. Evidence indicates that MSCs release extracellular vesicles (EVs) that shuttle miRNAs to damaged parenchymal cells, activating an endogenous repair program. However, whether comorbidities, such as metabolic syndrome (MetS) interfere with the packaging of cargo of MSC-derived EVs has never been explored. We hypothesized that MetS modulates the miRNA content packed within MSC-derived EVs. Methods MSCs were collected from swine abdominal adipose tissue after 16 weeks of Lean or Obese diet (n=7 each). Next-generation miRNA sequencing (miRNA-seq) was performed to identify miRNAs enriched in MSC-derived EVs, and their predicted target genes. Functional pathway analysis of the top 50 target genes of the top 4 miRNAs enriched in each group was performed using FunRich. Results Fourteen and 8 miRNAs were enriched in Lean- and MetS- EVs, respectively. Target genes of miRNAs enriched in MetS-EVs were implicated in the development of MetS and its complications, including diabetes-related pathways, validated transcriptional targets of AP1 family members Fra1 and Fra2, Class A/1 (Rhodopsin-like receptors), and Peptide ligand-binding receptors. Contrarily, miRNAs enriched in Lean EVs target primarily EphrinA-EPHA and the Rho family of GTPases. Conclusions MetS alters the miRNA content of EVs derived from porcine adipose tissue MSCs. These alterations could impair the efficacy of autologous MSCs and limit its therapeutic use in subjects with MetS. Our findings may assist in developing adequate regenerative strategies to preserve the reparative potency of MSCs in individuals with MetS.

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“…Moreover, EV-MSCs express some specific exosomal markers, such as CD107 [50,51], CD63, CD9 and CD81 [52,53].…”

Section: Characterization Of Evs Derived From Mscsmentioning

confidence: 99%

“…Recently, the characterization of RNA content of EVs obtained from porcine ASCs has been reported [53]. EVs released from ASCs preferentially express mRNAs for transcription factors (MDFIC, POU3F1, NRIP1), genes involved in angiogenesis (HGF, HES1, TCF4) and adipogenesis (KLF7), Golgi apparatus genes (ARRB1, GOLGA4), and genes involved in TGF-␤ signaling.…”

Section: Characterization Of Evs Derived From Mscsmentioning

confidence: 99%

“…Moreover, RNA-seq analyses generated reads for 386 miRNAs, but only 4 of them (miR148a, miR532-5p, miR378 and let-7f) are enriched in EVs with respect to ASCs, supporting the theory of a specific and organized package of miRNAs in EVs before their secretion. Gene ontology analyses have revealed that these miRNAs target transcription factors of genes involved in angiogenesis, cellular transport, apoptosis and proteolysis [53].…”

Section: Characterization Of Evs Derived From Mscsmentioning

confidence: 99%

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The secretome of mesenchymal stromal cells: Role of extracellular vesicles in immunomodulation

2015

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MicroRNA and mRNA cargo of extracellular vesicles from porcine adipose tissue-derived mesenchymal stem cells

Cited by 233 publications

References 60 publications

Human Mesenchymal Stroma/Stem Cells Exchange Membrane Proteins and Alter Functionality During Interaction with Different Tumor Cell Lines

Human Mesenchymal Stroma/Stem Cells Exchange Membrane Proteins and Alter Functionality During Interaction with Different Tumor Cell Lines

The metabolic syndrome alters the miRNA signature of porcine adipose tissue‐derived mesenchymal stem cells

The secretome of mesenchymal stromal cells: Role of extracellular vesicles in immunomodulation

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