Please use this identifier to cite or link to this item: http://hdl.handle.net/1942/33210
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dc.contributor.authorCassano, M.-
dc.contributor.authorBERARDI, Emanuele-
dc.contributor.authorCrippa, S.-
dc.contributor.authorToelen, J.-
dc.contributor.authorBarthelemy, I.-
dc.contributor.authorMicheletti, R.-
dc.contributor.authorChuah, M.-
dc.contributor.authorVandendriessche, T.-
dc.contributor.authorDebyser, Z.-
dc.contributor.authorBlot, S.-
dc.contributor.authorSampaolesi, M.-
dc.date.accessioned2021-01-28T15:29:56Z-
dc.date.available2021-01-28T15:29:56Z-
dc.date.issued2012-
dc.date.submitted2021-01-26T10:10:02Z-
dc.identifier.citationCELL TRANSPLANTATION, 21 (9) , p. 1945 -1967-
dc.identifier.urihttp://hdl.handle.net/1942/33210-
dc.description.abstractAmong the animal models of Duchenne muscular dystrophy (DMD). the Golden Retriever muscular dystrophy (GRMD) dog is considered the best model in terms of size and pathological onset of the disease. As in human patients presenting with DMD or Becker muscular dystrophies (BMD), the GRMD is related to a spontaneous X-linked mutation of dystrophin and is characterized by myocardial lesions. In this respect. GRMD is a useful model to explore cardiac pathogenesis and for the development of therapeutic protocols. To investigate whether cardiac progenitor cells (CPCs) isolated from healthy and GRMD dogs may differentiate into myocardial cell types and to test the feasibility of cell therapy for cardiomyopathies in a preclinical model of DMD. CPCs were isolated from cardiac biopsies of healthy and GRMD dogs. Gene profile analysis revealed an active cardiac transcription network in both healthy and GRMD CPCs. However, GRMD CPCs showed impaired self-renewal and cardiac differentiation. Population doubling and telomerase analyses highlighted earlier senescence and proliferation impairment in progenitors isolated from GRMD cardiac biopsies. Immunofluorescence analysis revealed that only wt CPCs showed efficient although not terminal cardiac differentiation, consistent with the upregulation of cardiac-specific proteins and microRNAs. Thus, the pathological condition adversely influences the cardiomyogenic differentiation potential of cardiac progenitors. Using PiggyBac transposon technology we marked CPCs for nuclear dsRed expression, providing a stable nonviral gene marking method for in vivo tracing of CPCs. Xenotransplantation experiments in neonatal immunodeficient mice revealed a valuable contribution of CPCs to cardiomyogenesis with homing differences between wt and dystrophic progenitors. These results suggest that cardiac degeneration in dystrophinopathies may account for the progressive exhaustion of local cardiac progenitors and shed light on cardiac sternness in physiological and pathological conditions. Furthermore, we provide essential information that canine CPCs may he used to alleviate cardiac involvement in a large preclinical model of DMD.-
dc.description.sponsorshipWe thank Gianpaolo Papaccio and Mark Guns for critical discussion and Shea Carter for the editing of the manuscript. We thank Ermira Samara-Kuko and Rudi Micheletti for the technical assistance, Christina Vochten for the professional secretarial service, and Paolo Luban for a kind donation. This work was supported by the Nash Avery Stem Cell Research–Wicka Fund, University of Minnesota; the Fonds Wetenschappelijk Onderzoek Odysseus Program grant G.0907.08; Research Council of the University of Leuven grant OT/09/053; Cardio Repair European Multidisciplinary Initiative grant 242038 FP7-EC; the Italian Ministry of University and Scientific Research grant 2008RFNT8T_003 (Progetto di Ricerca di Interesse Nazionale 2008); and EC (CARE-MI) FP7-HEALTH-2011.1.4-2-two-stage and Cariplo grants 2007.5639 and 2008.2005 to M. Sampaolesi. The authors declare no potential conflict of interest.-
dc.language.isoen-
dc.publisherSAGE PUBLICATIONS INC-
dc.rights2012 Cognizant Comm. Corp.-
dc.subject.otherCardiac progenitor-
dc.subject.otherMuscular dystrophy-
dc.subject.otherGRMD model-
dc.subject.otherCell therapy-
dc.titleAlteration of Cardiac Progenitor Cell Potency in GRMD Dogs-
dc.typeJournal Contribution-
dc.identifier.epage1967-
dc.identifier.issue9-
dc.identifier.spage1945-
dc.identifier.volume21-
local.bibliographicCitation.jcatA1-
local.publisher.place2455 TELLER RD, THOUSAND OAKS, CA 91320 USA-
local.type.refereedRefereed-
local.type.specifiedArticle-
dc.identifier.doi10.3727/096368912X638919-
dc.identifier.isiWOS:000312431600011-
local.provider.typeCrossRef-
local.uhasselt.uhpubno-
item.fullcitationCassano, M.; BERARDI, Emanuele; Crippa, S.; Toelen, J.; Barthelemy, I.; Micheletti, R.; Chuah, M.; Vandendriessche, T.; Debyser, Z.; Blot, S. & Sampaolesi, M. (2012) Alteration of Cardiac Progenitor Cell Potency in GRMD Dogs. In: CELL TRANSPLANTATION, 21 (9) , p. 1945 -1967.-
item.fulltextWith Fulltext-
item.contributorCassano, M.-
item.contributorBERARDI, Emanuele-
item.contributorCrippa, S.-
item.contributorToelen, J.-
item.contributorBarthelemy, I.-
item.contributorMicheletti, R.-
item.contributorChuah, M.-
item.contributorVandendriessche, T.-
item.contributorDebyser, Z.-
item.contributorBlot, S.-
item.contributorSampaolesi, M.-
item.accessRightsRestricted Access-
crisitem.journal.issn0963-6897-
crisitem.journal.eissn1555-3892-
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