Asymmetric RNA Distribution among Cells and Their Secreted Exosomes: Biomedical Meaning and Considerations on Diagnostic Applications

Ragusa, Marco; Barbagallo, Cristina; Cirnigliaro, Matilde; Battaglia, Rosalia; Brex, Duilia; Caponnetto, A; Barbagallo, Davide; Pietro, Cinzia Di; Purrello, Michele

doi:10.3389/fmolb.2017.00066

Cited by 41 publications

(32 citation statements)

References 153 publications

(183 reference statements)

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“…The mechanisms for differential enrichment of particular miRNAs into ADEVs following ATP, TNFα, or IL-1β are less clear. Previous studies have reported differential sorting of miRNA into EVs 43 , and several mechanisms for miRNA loading into EVs including lipid-mediated RNA loading, RNA-binding protein-assisted RNA loading, loading by non-templated 3′-end uridylation of microRNAs 44 – 46 . However, mechanisms regulating stimulus-dependent inclusion/exclusion of particular miRNA cargo are currently unknown.…”

Section: Discussionmentioning

confidence: 99%

TNFα and IL-1β modify the miRNA cargo of astrocyte shed extracellular vesicles to regulate neurotrophic signaling in neurons

et al. 2018

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Astrocytes are known to be critical regulators of neuronal function. However, relatively few mediators of astrocyte to neuron communication have been identified. Recent advancements in the biology of extracellular vesicles have begun to implicate astrocyte derived extracellular vesicles (ADEV) as mediators of astrocyte to neuron communication, suggesting that alterations in the release and/or composition of ADEVs could influence gliotransmission. TNFα and IL-1β are key mediators of glial activation and neuronal damage, but the effects of these cytokines on the release or molecular composition of ADEVs is unknown. We found that ADEVs released in response to IL-1β (ADEV-IL-1β) and TNFα (ADEV-TNFα) were enriched with miRNAs that target proteins involved in neurotrophin signaling. We confirmed that miR-125a-5p and miR-16-5p (both enriched in ADEV-IL-1β and ADEV-TNFα) targeted NTKR3 and its downstream effector Bcl2. Downregulation of these targets in neurons was associated with reductions in dendritic growth, dendritic complexity, reduced spike rates, and burst activity. Molecular interference of miR-125a-5p and miR-16-5p prevented ADEV-IL-1β from reducing dendritic complexity, spike, and burst rates. These findings suggest that astrocytes respond to inflammatory challenge by modifying the miRNA cargo of ADEVs to diminish the activity of target neurons by regulating the translational expression of proteins controlling programs essential for synaptic stability and neuronal excitability.

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Section: Discussionmentioning

confidence: 99%

TNFα and IL-1β modify the miRNA cargo of astrocyte shed extracellular vesicles to regulate neurotrophic signaling in neurons

et al. 2018

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“…This opposite deregulation would suggest that the oncogenic function of UCA1 is crucial for tumor progression, inducing tumor cells to retain the lncRNA by limiting its secretion through exosomes. 58 …”

Section: Discussionmentioning

confidence: 99%

LncRNA UCA1, Upregulated in CRC Biopsies and Downregulated in Serum Exosomes, Controls mRNA Expression by RNA-RNA Interactions

Barbagallo

Brex

Caponnetto

et al. 2018

Molecular Therapy - Nucleic Acids

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161

111

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Long non-coding RNAs (lncRNAs) and circular RNAs (circRNAs) contribute to the onset of many neoplasias through RNA-RNA competitive interactions; in addition, they could be secreted by cancer cells into biological fluids, suggesting their potential diagnostic application. By analyzing the expression of 17 lncRNAs and 31 circRNAs in biopsies and serum exosomes from colorectal cancer (CRC) patients through qRT-PCR, we detected CCAT1, CCAT2, HOTAIR, and UCA1 upregulation and CDR1AS, MALAT1, and TUG1 downregulation in biopsies. In serum exosomes, UCA1 was downregulated, while circHIPK3 and TUG1 were upregulated. Combined receiver operating characteristic (ROC) curves of TUG1:UCA1 and circHIPK3:UCA1 showed high values of sensitivity and specificity. Through in vitro (i.e., RNA silencing and mitogen-activated protein kinase [MAPK] inhibition) and in silico analyses (i.e., expression correlation and RNA-RNA-binding prediction), we found that UCA1 could (1) be controlled by MAPKs through CEBPB; (2) sequester miR-135a, miR-143, miR-214, and miR-1271, protecting ANLN, BIRC5, IPO7, KIF2A, and KIF23 from microRNA (miRNA)-induced degradation; and (3) interact with mRNA 3′-UTRs, preventing miRNA binding. UCA1 and its co-regulated antisense LINC01764 could interact and reciprocally mask their own miRNA-binding sites. Functional enrichment analysis of the RNA-RNA network controlled by UCA1 suggested its potential involvement in cellular migration. The UCA1 regulatory axis would represent a promising target to develop innovative RNA-based therapeutics against CRC.

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“…Cell stressors not only promote the release of EVs, but more importantly, also promote highly specific EV-containing microRNAs (miRNAs; Gray et al, 2015 ; Lee et al, 2016 , 2017 ). Accumulating evidence indicates that a specific repertoire of miRNAs is actively selected and loaded into EVs ( Skog et al, 2008 ; Xu et al, 2013 ; Momose et al, 2016 ; Ragusa et al, 2017 ). This process involves an ATP-dependent, active sorting mechanism ( Xu et al, 2013 ) and involves RNA-binding proteins that are enriched in EVs ( Laffont et al, 2013 ; Villarroya-Beltri et al, 2013 ; Cha et al, 2015 ; McKenzie et al, 2016 ; Santangelo et al, 2016 ; Shurtleff et al, 2016 ; Teng et al, 2017 ).…”

Section: Introductionmentioning

confidence: 99%

Caveolin-1 selectively regulates microRNA sorting into microvesicles after noxious stimuli

Lee

Zhang

et al. 2019

Journal of Experimental Medicine

146

156

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Emerging evidence suggests that extracellular vesicle (EV)–containing miRNAs mediate intercellular communications in response to noxious stimuli. It remains unclear how a cell selectively sorts the cellular miRNAs into EVs. We report that caveolin-1 (cav-1) is essential for sorting of selected miRNAs into microvesicles (MVs), a main type of EVs generated by outward budding of the plasma membrane. We found that cav-1 tyrosine 14 (Y14)–phosphorylation leads to interactions between cav-1 and hnRNPA2B1, an RNA-binding protein. The cav-1/hnRNPA2B1 complex subsequently traffics together into MVs. Oxidative stress induces O-GlcNAcylation of hnRNPA2B1, resulting in a robustly altered hnRNPA2B1-bound miRNA repertoire. Notably, cav-1 pY14 also promotes hnRNPA2B1 O-GlcNAcylation. Functionally, macrophages serve as the principal recipient of epithelial MVs in the lung. MV-containing cav-1/hnRNPA2B1 complex-bound miR-17/93 activate tissue macrophages. Collectively, cav-1 is the first identified membranous protein that directly guides RNA-binding protein into EVs. Our work delineates a novel mechanism by which oxidative stress compels epithelial cells to package and secrete specific miRNAs and elicits an innate immune response.

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Asymmetric RNA Distribution among Cells and Their Secreted Exosomes: Biomedical Meaning and Considerations on Diagnostic Applications

Cited by 41 publications

References 153 publications

TNFα and IL-1β modify the miRNA cargo of astrocyte shed extracellular vesicles to regulate neurotrophic signaling in neurons

TNFα and IL-1β modify the miRNA cargo of astrocyte shed extracellular vesicles to regulate neurotrophic signaling in neurons

LncRNA UCA1, Upregulated in CRC Biopsies and Downregulated in Serum Exosomes, Controls mRNA Expression by RNA-RNA Interactions

Caveolin-1 selectively regulates microRNA sorting into microvesicles after noxious stimuli

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