2008
DOI: 10.3727/096368908786576480
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The Use of Clinically Approved Small Particles of Iron Oxide (SPIO) for Labeling of Mesenchymal Stem Cells Aggravates Clinical Symptoms in Experimental Autoimmune Encephalomyelitis and Influences Their In Vivo Distribution

Abstract: Multiple sclerosis (MS) is an inflammatory and demyelinating disease of the central nervous system (CNS).Mesenchymal stem cells (MSC) have been shown to ameliorate symptoms in experimental autoimmune encephalomyelitis (EAE), a model of MS. Using cloned MSC labeled with clinically approved small particles of iron oxide (SPIO) for treatment of EAE we analyzed the tissue localization of transferred cells. Treatment with unlabeled MSC led to disease amelioration compared to controls. In contrast, treatment with SP… Show more

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Cited by 40 publications
(40 citation statements)
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“…were initially developed to treat EAE based on the concept that substitution of one or more amino acids to change MHC or -Martin et al, 2003;Pryce et al, 2003;Zajicek et al, 2003;Ni et al, 2004;Maresz et al, 2005;Rog et al, 2005; Freeman et al, 2006;Wissel et al, 2006; Centonze et al, 2007; Collin et al, 2007;Palazuelos et al, 2008;Zhang et al, 2009) Cell-based therapies Neural stem cells Improvement (Picard-Riera et al, 2002; Einstein et al, 2003;Pluchino et al, 2003; Einstein et al, 2006;Makar et al, 2008;Pluchino et al, 2009;Yang et al, 2009) Mesenchymal stem cells Improvement (Zappia et al, 2005; Kassis et al, 2008;Schafer et al, 2008; Bai et al, 2009;Lanza et al, 2009;Lu et al, 2009;Rafei et al, 2009; Freedman et al, 2010;Gordon et al, 2010; Karussis et al, 2010;Yamout et al, 2010) BJP CS Constantinescu et al T-cell receptor (TCR) binding characteristics would induce tolerance to the native peptide through mechanisms including T-cell antagonism and partial agonism as well as cytokine deviation (Evavold and Allen, 1991;Racioppi et al, 1993) and antagonism at the T-cell activation level (De Magistris et al, 1992). Brocke et al induced EAE with a MBP87-99-specific T-cell clone and were able to induce tolerance in vivo by treating mice with an analogue of the native peptide (alanine substitution of the phenylalanine at residue 96).…”
Section: Altered Peptide Ligands Altered Peptide Ligands (Apl) Of Mbpmentioning
confidence: 99%
“…were initially developed to treat EAE based on the concept that substitution of one or more amino acids to change MHC or -Martin et al, 2003;Pryce et al, 2003;Zajicek et al, 2003;Ni et al, 2004;Maresz et al, 2005;Rog et al, 2005; Freeman et al, 2006;Wissel et al, 2006; Centonze et al, 2007; Collin et al, 2007;Palazuelos et al, 2008;Zhang et al, 2009) Cell-based therapies Neural stem cells Improvement (Picard-Riera et al, 2002; Einstein et al, 2003;Pluchino et al, 2003; Einstein et al, 2006;Makar et al, 2008;Pluchino et al, 2009;Yang et al, 2009) Mesenchymal stem cells Improvement (Zappia et al, 2005; Kassis et al, 2008;Schafer et al, 2008; Bai et al, 2009;Lanza et al, 2009;Lu et al, 2009;Rafei et al, 2009; Freedman et al, 2010;Gordon et al, 2010; Karussis et al, 2010;Yamout et al, 2010) BJP CS Constantinescu et al T-cell receptor (TCR) binding characteristics would induce tolerance to the native peptide through mechanisms including T-cell antagonism and partial agonism as well as cytokine deviation (Evavold and Allen, 1991;Racioppi et al, 1993) and antagonism at the T-cell activation level (De Magistris et al, 1992). Brocke et al induced EAE with a MBP87-99-specific T-cell clone and were able to induce tolerance in vivo by treating mice with an analogue of the native peptide (alanine substitution of the phenylalanine at residue 96).…”
Section: Altered Peptide Ligands Altered Peptide Ligands (Apl) Of Mbpmentioning
confidence: 99%
“…While most studies do not describe any significant changes in cell behavior (e. g. apoptosis rate, proliferation index, differentiation behavior) [150,151], individual studies show changes in migration behavior and the ability to form colonies [152], in cell vitality [153], in differentiation behavior [154], or in the expression pattern [152]. By the same token, the influence of cell labeling on the long-term behavior of cells and the course of disease is currently unclear [155] and must be studied more closely in the future [156]. Successful in vivo detection and migration monitoring of SPIO-labeled cells was able to be demonstrated in numerous studies, e. g. in implanted hematopoietic, mesenchymal, or neuronal stem cells in the CNS [157], heart [158], liver [159], spleen [160], bone marrow [160], kidneys [161], joints [162], and muscles [163], endothelial progenitor cells [164], transplanted islet cells [165], and lymphocytic and moncytic cells (natural killer cells in oncological cell therapies [166]).…”
Section: Cell Labeling and Cell Imaging In Mrimentioning
confidence: 99%
“…mMSCs were trypsinized, labeled with PKH26 as described previously [31], and kept on ice until transplantation. One minute before the end of myocardial ischemia (30 min), 0.5 · 10 6 mMSCs in 50 mL saline were injected intramuscularly into the apex cordis.…”
Section: Transplantation Of Mmscs Into Infarcted Heartsmentioning
confidence: 99%