Literature DB >> 21324974

Microvesicles derived from human adult mesenchymal stem cells protect against ischaemia-reperfusion-induced acute and chronic kidney injury.

Stefano Gatti1, Stefania Bruno, Maria Chiara Deregibus, Andrea Sordi, Vincenzo Cantaluppi, Ciro Tetta, Giovanni Camussi.   

Abstract

BACKGROUND: Several studies demonstrated that mesenchymal stem cells (MSCs) reverse acute kidney injury (AKI) by a paracrine mechanism rather than by MSC transdifferentiation. We recently demonstrated that microvesicles (MVs) released from MSCs may account for this paracrine mechanism by a horizontal transfer of messenger RNA and microRNA.
METHODS: MVs isolated from MSCs were injected intravenously in rats (30 μg/rat) immediately after monolateral nephrectomy and renal artery and vein occlusion for 45 min. To evaluate the MV effects on AKI induced by ischaemia-reperfusion injury (IRI), the animals were divided into different groups: normal rats (n = 4), sham-operated rats (n = 6), IRI rats (n = 6), IRI + MV rats (n = 6), and IRI + RNase-MV rats (n = 6), and all animals were sacrificed at Day 2 after the operation. To evaluate the chronic kidney damage consequent to IRI, the rats were divided into different groups: sham-operated rats (n = 6) and IRI rats (n = 6), IRI + MV rats (n = 6), and all animal were sacrificed 6 months after the operation.
RESULTS: We found that a single administration of MVs, immediately after IRI, protects rats from AKI by inhibiting apoptosis and stimulating tubular epithelial cell proliferation. The MVs also significantly reduced the impairment of renal function. Pretreatment of MVs with RNase to inactivate their RNA cargo abrogated these protective effects. Moreover, MVs by reducing the acute injury also protected from later chronic kidney disease.
CONCLUSION: MVs released from MSCs protect from AKI induced by ischaemia reperfusion injury and from subsequent chronic renal damage. This suggest that MVs could be exploited as a potential new therapeutic approach.

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Year:  2011        PMID: 21324974     DOI: 10.1093/ndt/gfr015

Source DB:  PubMed          Journal:  Nephrol Dial Transplant        ISSN: 0931-0509            Impact factor:   5.992


  313 in total

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2.  hucMSC Exosome-Derived GPX1 Is Required for the Recovery of Hepatic Oxidant Injury.

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Review 3.  Applying horizontal gene transfer phenomena to enhance non-viral gene therapy.

Authors:  Jacob J Elmer; Matthew D Christensen; Kaushal Rege
Journal:  J Control Release       Date:  2013-08-30       Impact factor: 9.776

4.  Microvesicles derived from human bone marrow mesenchymal stem cells promote U2OS cell growth under hypoxia: the role of PI3K/AKT and HIF-1α.

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6.  Extracellular vesicles from bone marrow-derived mesenchymal stem cells protect against murine hepatic ischemia/reperfusion injury.

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7.  Therapeutic effects of human mesenchymal stem cell microvesicles in an ex vivo perfused human lung injured with severe E. coli pneumonia.

Authors:  Jeonghyun Park; Seonguk Kim; Hyungsun Lim; Airan Liu; Shuling Hu; JaeHoon Lee; Hanjing Zhuo; Qi Hao; Michael A Matthay; Jae-W Lee
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8.  Apparent Diffusion Coefficient is a Useful Biomarker for Monitoring Adipose-Derived Mesenchymal Stem Cell Therapy of Renal Ischemic-Reperfusion Injury.

Authors:  Sheung-Fat Ko; Hon-Kan Yip; Chen-Chang Lee; Chia-Chang Lee; Chia-Hao Su; Chung-Cheng Huang; Shu-Hang Ng; Yi-Ling Chen; Min-Chi Chen
Journal:  Mol Imaging Biol       Date:  2018-10       Impact factor: 3.488

Review 9.  Angiogenesis and hypoxia in the kidney.

Authors:  Tetsuhiro Tanaka; Masaomi Nangaku
Journal:  Nat Rev Nephrol       Date:  2013-03-05       Impact factor: 28.314

Review 10.  A systematic review of preclinical studies on the therapeutic potential of mesenchymal stromal cell-derived microvesicles.

Authors:  Celine Akyurekli; Yevgeniya Le; Richard B Richardson; Dean Fergusson; Jason Tay; David S Allan
Journal:  Stem Cell Rev Rep       Date:  2015-02       Impact factor: 5.739

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