Functional characterisation of cardiac progenitors from patients with ischaemic heart disease

Zhang, Huajun

January 2013

Ischaemic heart disease (IHD) is the leading cause of death worldwide. Currently, even optimal medical therapies do not attenuate deterioration of the left ventricular (LV) function completely. Stem cell therapies, and recently cardiac stem cell therapies, have emerged as potential novel treatments for IHD. However, clinical evidence from randomised controlled studies has shown mixed results. Thus understanding what patient-related factors may affect the therapeutic performance of the cells may help improving treatment outcomes. The studies described in this thesis aim to understand how cardiac progenitor cells (CPCs) can re-vascularise ischaemic myocardium and promote functional repair of the heart. Resident CPCs were isolated and expanded from the right atrial appendage of 68 patients following the ‘cardiosphere’ method (cardiosphere-derived cells or CDCs). They resemble mesenchymal progenitors as they lack the expression of endothelial and haematopoietic cell surface markers but express mesenchymal progenitor cell markers (e.g. CD105, CD90). Cell function was evaluated by support of angiogenesis, mesenchymal lineage differentiation potential in vitro, and improvement in heart function in vivo. Notably in vitro, CDC from different patients differed in their angiogenic supportive and differentiation potentials. In a rodent model of myocardial infarction (MI), transplantation of CDC reduced infarct size significantly (p<0.05). However, only those CDCs with a robust pro-angiogenic ability in vitro improved vessel density and heart systolic function (p<0.05) in vivo. A multiple regression model, which accounted for 51% of the variability observed, identified New York Heart Association (NYHA) class, smoking, hypertension, type of ischaemic disease and diseased vessel as independent predictors of angiogenesis. In addition, gene expression analyses revealed that differential gene expression of several extracellular matrix components (e.g. CUX1, COL1A2, BMP1 genes and microRNA-29b) could explain the differences observed in CDC’s vascular supportive function. In summary, this is the first description of variability in the pro-angiogenic and differentiation potential of CDCs and its correlation with their therapeutic potential. This study indicates that patient stratification may need to be included in the design of future trials to improve the efficacy of cell-based therapies.

616.1

Déformation myocardique et remodelage cardiaque / Myocardial deformation and cardiac remodelling

Altman, Mikhail

24 November 2014

Le remodelage myocardique est une réponse du myocarde à une altération des contraintes pariétales générée par une agression aiguë (ischémie myocardique) ou chronique (surcharge en pression, surcharge en volume, anomalie métabolique). En effet, le cœur est un organe capable de modifier en fonction de ses conditions de travail l’expression de ses fonctions moléculaires et cellulaires pour aboutir à des changements de taille,de morphologie et de fonction. Le remodelage myocardique est un mécanisme adaptatif initialement bénéfique, car en modifiant sa géométrie, le ventricule gauche s’adapte aux modifications de stress pariétal et préserve le volume d’éjection systolique. / Not transmitted

Cardiopathie ischémique

Déformation myocardique

Strain

Viabilité

Speckle tracking echocardiographie

Cardiopathie métabolique

Ischaemic cardiomyopathy

Myocardial deformation

Strain

Viability

Speckle tracking echocardiography

Diabetic cardiomyopathy

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