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Differential Effects of Progenitor Cell Populations on Left Ventricular Remodeling and Myocardial Neovascularization After Myocardial Infarction
Christophe Dubois ,
Xiaoshun Liu ,
Piet Claus ,
Glenn Marsboom ,
Peter Pokreisz ,
Sara Vandenwijngaert ,
Hélène Dépelteau ,
Witold Streb ,
Lertlak Chaothawee ,
Frederik Maes ,
Olivier Gheysens ,
Zeger Debyser ,
Hilde Gillijns ,
Marijke Pellens ,
Thierry Vandendriessche ,
Marinee Chuah ,
Desiré Collen ,
Erik Verbeken ,
Ann Belmans ,
Frans Van de Werf ,
Jan Bogaert ,
Stefan Janssens
May 2010
May 2010
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Abstract
We compared biological repair after acute myocardial infarction (AMI) with selected
porcine progenitor cell populations.
Cell types and mechanisms responsible for myocardial repair after AMI remain uncertain.
In a blinded, randomized study, we infused autologous late-outgrowth endothelial progenitor
cells (EPC) (n = 10, 34 +/- 22 x 10(6) CD29-31-positive, capable of tube formation),
allogeneic green fluorescent peptide-labeled mesenchymal stem cells (MSC) (n = 11,
10 +/- 2 x 10(6) CD29-44-90-positive, capable of adipogenic and osteogenic differentiation),
or vehicle (CON) (n = 12) in the circumflex artery 1 week after AMI. Systolic function
(ejection fraction), left ventricular (LV) end-diastolic and end-systolic volumes,
and infarct size were assessed with magnetic resonance imaging at 1 week and 7 weeks.
Cell engraftment and vascular density were evaluated on postmortem sections.
Recovery of LV ejection fraction from 1 to 7 weeks was similar between groups, but
LV remodeling markedly differed with a greater increase of LV end-systolic volume
in MSC and CON (+11 +/- 12 ml/m(2) and +7 +/- 8 ml/m(2) vs. -3 +/- 11 ml/m(2) in EPC,
respectively, p = 0.04), and a similar trend was noted for LV end-diastolic volume
(p = 0.09). After EPC, infarct size decreased more in segments with >50% infarct transmurality
(p = 0.02 vs. MSC and CON) and was associated with a greater vascular density (p =
0.01). Late outgrowth EPCs secrete higher levels of the pro-angiogenic placental growth
factor (733 [277 to 1,214] pg/10(6) vs. 59 [34 to 88] pg/10(6) cells in MSC, p = 0.03)
and incorporate in neovessels in vivo.
Infusion of late-outgrowth EPCs after AMI improves myocardial infarction remodeling
via enhanced neovascularization but does not mediate cardiomyogenesis. Endothelial
progenitor cell transfer might hold promise for heart failure prevention via pro-angiogenic
or paracrine matrix-modulating effects.