Cell therapy using bone marrow-derived mesenchymal stem cells (MSCs) seems to be a new alternative for the treatment of neurodegenerative diseases. Despite several promising results with their use, possible side effects are still unknown. In a previous work, we have shown that MSC-conditioned medium is toxic to hippocampal slice cultures and aggravates cell death induced by oxygen and glucose deprivation. In this work, we investigated whether the inflammatory response and/or reactive species formation could be involved in that toxicity. Rat organotypic hippocampal cultures were exposed for 24 h to conditioned medium from MSCs isolated from rat bone marrow. A marked glial activation was observed after exposure of cultures to MSC-conditioned medium, as evidenced by glial fibrillary acid protein (GFAP) and isolectin B4 increase. Tumor necrosis factor-α and interleukin-6 levels were increased in the culture medium, and 2,7-dihydrodichlorofluorescein diacetate oxidation (indicating reactive species generation) and inducible nitric oxide synthase (iNOS) immunocontent were also higher after exposure of cultures to MSC-conditioned medium. Antioxidants (ascorbic acid and TROLOX®), Nω-nitro-l-arginine methyl ester hydrochloride, and anti-inflammatory drugs (indomethacin and dexamethasone) reduced cell death in hippocampal organotypic cultures after their exposure to MSC-conditioned medium. The results obtained here suggest that MSC-secreted factors trigger reactive species generation and neuroinflammation in organotypic cultures of hippocampus, introducing a note of caution in the use of these cells for neurological application.
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References
1.
PriceD. 1999. New order from neurological disorders. Nature, 399:A3–A5.
2.
SriramK, O'CallaghanJP. 2007. Divergent roles of tumor necrosis factor-α in the brain. J Neuroimmune Pharmacol, 2:140–153.
3.
ParkKW, LeeHG, JinBK, LeeYB. 2007. Interleukin-10 endogenously expressed in microglia prevents lipopolysaccharide-induced neurodegeneration in the rat cerebral cortex in vivo. Exp Mol Med, 39:812–819.
4.
ChoppM, LiY. 2002. Treatment of neural injury with marrow stromal cells. Lancet Neurol, 1:92–100.
KanI, MelamedE, OffenD. 2007. Autotransplantation of bone marrow-derived stem cells as a therapy for neurodegenerative diseases. Handb Exp Pharmacol, 180:219–242.
FazelSS, AngoulvantD, ButanyJ, WeiselRD, LiR-K. 2008. Mesenchymal stem cells engineered to overexpress stem cell factor improve cardiac function but have malignant potential. J Thorac Cardiovasc Surg, 136:1388–1389.
15.
NorabergJ, PoulsenFR, BlaabjergM, KristensenBW, BondeC, MonteroM, MeyerM, GramsbergenJB, ZimmerJ. 2005. Organotypic hippocampal slice cultures for studies of brain damage, neuroprotection and neurorepair. Curr Drug Targets CNS Neurol Disord, 4:435–452.
16.
GähwilerBH, CapognaM, DebanneD, MckinneyRA, ThompsonSM. 1997. Organotypic slice cultures: a technique has come of age. Trends Neurosci, 20:471–477.
17.
TavaresA, CimarostiH, ValentimL, SalbegoC. 2001. Profile of phosphoprotein labelling in organotypic slice cultures of rat hippocampus. Neuroreport, 12:2705–2709.
18.
ValentimLM, RodnightR, GeyerAB, HornAP, TavaresA, CimarostiH, NettoCA, SalbegoCG. 2003. Changes in heat shock protein 27 phosphorylation and immunocontent in response to preconditioning to oxygen and glucose deprivation in organotypic hippocampal cultures. Neuroscience, 118:379–386.
19.
HornAP, GerhardtD, GeyerAB, ValentimL, CimarostiH, TavaresA, HornF, LenzG, SalbegoC. 2005. Cellular death in hippocampus in response to PI3-K pathway inhibition and oxygen and glucose deprivation. Neurochem Res, 30:355–361.
20.
HornAP, FrozzaRL, GrudzinskiP, GerhardtD, HoppeJB, BrunoAN, ChagastellesP, NardiNB, LenzG, SalbegoC. 2009. Conditioned medium from mesenchymal stem cells induces cell death in organotypic cultures of rat hippocampus and aggravates lesion in a model of oxygen and glucose deprivation. Neurosci Res, 63:35–41.
21.
FrozzaRL, HornAP, HoppeJB, SimãoF, GerhardtD, ComiranRA, SalbegoCG. 2009. A comparative study of β-amyloid peptides Aβ1-42 and Aβ25-35 toxicity in organotypic hippocampal slice cultures. Neurochem Res, 34:295–303.
22.
HoppeJB, FrozzaRL, HornAP, ComiranRA, BernardiA, CamposMM, BattastiniAMO, SalbegoC. 2010. Amiloid-β neurotoxicity in organotypic culture is attenuatted by melatonin: involvement of GSK3β, Tau and neuroinflammation. J Pineal Res, 48:230–238.
23.
StoppiniL, BuchsPA, MullerD. 1991. A simple method for organotypic cultures of nervous tissue. J Neurosci Methods, 37:173–182.
24.
Da Silva MeirellesLS, NardiNB. 2003. Murine marrow-derived mesenchymal stem cells: isolation, in vitro expansion, and characterization. Br J Hematol, 123:702–711.
25.
NardiNB, Da Silva MeirellesL. 2006. Mesenchymal stem cells: isolation, in vitro expansion and characterization. Handb Exp Pharmacol, 174:249–282.
26.
NorabergJ, KristensenBW, ZimmerJ. 1999. Markers for neuronal degeneration in organotypic slice cultures. Brain Res Prot, 3:278–290.
27.
RockRB, GekkerG, HuS, ShengWS, CheeranM, LokensgardJR, PetersonPK. 2004. Role of microglia in central nervous system infections. Clin Microbiol Rev, 17:942–964.
28.
BrownGC. 2007. Mechanisms of inflammatory neurodegeneration: iNOS and NADPH oxidase. Biochem Soc Trans, 35:1119–1121.
29.
BuffoA, RiteI, TripathiP, LepierA, ColakD, HornAP, MoriT, GötzM. 2008. Origin and progeny of reactive gliosis: a source of multipotent cells in the injured brain. Proc Natl Acad Sci USA, 105:3581–3586.
CoyneTM, MarcusAJ, WoodburyD, BlackIB. 2006. Marrow stromal cells transplanted to the adult brain are rejected by an inflammatory response and transfer donor labels to host neurons and glia. Stem Cells, 24:2483–2492.
34.
OhtakiH, YlostaloJH, ForakeJE, RobinsonAP, RegerRL, ShiodaS, ProckopDJ. 2008. Stem/progenitor cells from bone marrow decrease neuronal death in global ischemia by modulation of inflammatory/immune responses. Proc Natl Acad Sci USA, 105:14638–14643.
35.
DjouadF, FritzV, ApparaillyF, Louis-PlenceP, BonyC, SanyJ, JorgensenC, NoëlD. 2005. Reversal of the immunosuppressive properties of mesenchymal stem cells by tumor necrosis factor α in collagen-induced arthritis. Arthritis Rheum, 52:1595–1603.
36.
EliginiS, BarbieriSS, CavalcaV, CameraM, BrambillaM, De FranceschiM, TremoliE, ColliS. 2005. Diversity and similarity in signaling events leading to rapid Cox-2 induction by tumor necrosis factor-α and phorbol ester in human endothelial cells. Cardiovasc Res, 65:683–693.
37.
HämäläinenM, LiljaR, KankaanrantaH, MoilanenE. 2008. Inhibition of iNOS expression and NO production by anti-inflammatory steroids: reversal by histone deacetylase inhibitors. Pulm Pharmacol Ther, 21:331–339.
38.
Bal-PriceA, BrownGC. 2001. Inflammatory neurodegeneration mediated by nitric oxide from activated microglia-inhibiting neuronal respiration, causing glutamate release and excitotoxicity. J Neurosci, 21:6480–6491.
39.
CombsCK, KarloJC, KaoS-C, LandrethGE. 2001. β-Amyloid stimulation of microglia and monocytes results in TNFα-dependent expression of inducible nitric oxide synthase and neuronal apoptosis. J Neurosci, 21:1179–1188.
40.
TakeuchiH, JinS, WangJ, ZhangG, KawanokuchiJ, KunoR, SonobeY, MizunoT, SuzumuraA. 2006. Tumor necrosis factor-α induces neurotoxicity via glutamate release from hemichannels of activated microglia in an autocrine manner. J Biol Chem, 281:21362–21368.
41.
BezziP, DomercqM, BrambillaL, GalliR, ScholsD, De ClercqE, VescoviA, BagettaG, KolliasG, MeldolesiJ, VolterraA. 2001. CXCR4-activated astrocyte glutamate release via TNFα: amplification by microglia triggers neurotoxicity. Nat Neurosci, 4:702–710.
42.
Da Silva MeirellesLS, ChagastellesP, NardiNB. 2006. Mesenchymal stem cells reside in virtually all postnatal organs and tissues. J Cell Sci, 119:2204–2213.
