Modulation de la néovascularisation post-ischémique en présence de facteurs de risque cardiovasculaire

Turgeon, Julie

02 1900

L’athérosclérose est la principale cause d’infarctus du myocarde, de mort subite d’origine cardiaque, d’accidents vasculaires cérébraux et d’ischémie des membres inférieurs. Celle-ci cause près de la moitié des décès dans les pays industrialisés. Lorsque les obstructions artérielles athérosclérotiques sont tellement importantes que les techniques de revascularisation directe ne peuvent être effectuées avec succès, la sévérité de l’ischémie tissulaire résiduelle dépendra de l’habilité de l’organisme à développer spontanément de nouveaux vaisseaux sanguins (néovascularisation). La néovascularisation postnatale est le résultat de deux phénomènes : la formation de nouveaux vaisseaux à partir de la vasculature existante (angiogenèse) et la formation de vaisseaux à partir de cellules souches progénitrices (vasculogenèse). Notre laboratoire a démontré que plusieurs facteurs de risque associés aux maladies cardiovasculaires (tabagisme, vieillissement, hypercholestérolémie) diminuaient également la réponse angiogénique suite à une ischémie. Cependant, les mécanismes précis impliqués dans cette physiopathologie sont encore inconnus. Un point commun à tous ces facteurs de risque cardiovasculaire est l’augmentation du stress oxydant. Ainsi, le présent ouvrage visait à élucider l’influence de différents facteurs de risque cardiovasculaire et du stress oxydant sur la néovascularisation. Nos résultats démontrent que l’exposition à la fumée de cigarette et le vieillissement sont associés à une diminution de la néovascularisation en réponse à l’ischémie, et que ceci est au moins en partie causé par une augmentation du stress oxydant. De plus, nous démontrons que les acides gras dérivés de la diète peuvent affecter la réponse à l’ischémie tissulaire. La première étude du projet de recherche visait à évaluer l’impact de l’exposition à la fumée de cigarette sur la néovascularisation post-ischémique, et l’effet d’une thérapie antioxydante. L’exposition à la fumée de cigarette a été associée à une réduction significative de la récupération du flot sanguin et de la densité des vaisseaux dans les muscles ischémiques. Cependant, une récupération complète de la néovascularisation a été démontrée chez les souris exposées à la fumée de cigarette et traitées au probucol ou aux vitamines antioxydantes. Nous avons démontré qu’une thérapie antioxydante administrée aux souris exposées à la fumée de cigarette était associée à une réduction significative des niveaux de stress oxydant dans le plasma et dans les muscles ischémiques. De plus, les cellules endothéliales progénitrices (EPCs) exposées à de l’extrait de fumée de cigarette in vitro présentent une diminution significative de leur activité angiogénique (migration, adhésion et incorporation dans les tissus ischémiques) qui a été complètement récupérée par le probucol et les vitamines antioxydantes. La deuxième étude avait pour but d’investiguer le rôle potentiel de la NADPH oxydase (Nox2) pour la modulation de la néovascularisation post-ischémique dans le contexte du vieillissement. Nous avons trouvé que l’expression de la Nox2 est augmentée par le vieillissement dans les muscles ischémiques des souris contrôles. Ceci est associé à une réduction significative de la récupération du flot sanguin après l’ischémie chez les vieilles souris contrôles comparées aux jeunes. Nous avons aussi démontré que la densité des capillaires et des artérioles est significativement réduite dans les muscles ischémiques des animaux vieillissants alors que les niveaux de stress oxydant sont augmentés. La déficience en Nox2 réduit les niveaux de stress oxydant dans les tissus ischémiques et améliore la récupération du flot sanguin et la densité vasculaire chez les animaux vieillissants. Nous avons aussi démontré que l’activité fonctionnelle des EPCs (migration et adhésion à des cellules endothéliales matures) est significativement diminuée chez les souris vieillissantes comparée aux jeunes. Cependant, la déficience en Nox2 est associée à une récupération de l’activité fonctionnelle des EPCs chez les animaux vieillissants. Nous avons également démontré une augmentation pathologique du stress oxydant dans les EPCs isolées d’animaux vieillissants. Cette augmentation de stress oxydant dans les EPCs n’est pas présente chez les animaux déficients en Nox2. La troisième étude du projet de recherche a investigué l’effet des acides gras dérivés de la diète sur la néovascularisation postnatale. Pour ce faire, les souris ont reçu une diète comprenant 20% d’huile de maïs (riche en oméga-6) ou 20% d’huile de poisson (riche en oméga-3). Nos résultats démontrent qu’une diète riche en oméga-3 améliore la néovascularisation post-ischémique au niveau macro-vasculaire, micro-vasculaire et clinique comparée à une diète riche en oméga-6. Cette augmentation de la néovascularisation postnatale est associée à une réduction du ratio cholestérol total/cholestérol HDL dans le sérum et à une amélioration de la voie VEGF/NO dans les tissus ischémiques. De plus, une diète riche en acides gras oméga-3 est associée à une augmentation du nombre d’EPCs au niveau central (moelle osseuse) et périphérique (rate). Nous démontrons aussi que l’activité fonctionnelle des EPCs (migration et incorporation dans des tubules de cellules endothéliales matures) est améliorée et que le niveau de stress oxydant dans les EPCs est réduit par la diète riche en oméga-3. En conclusion, nos études ont permis de déterminer l’impact de différents facteurs de risque cardiovasculaire (tabagisme et vieillissement) et des acides gras dérivés de la diète (oméga-3) sur la néovascularisation post-ischémique. Nous avons aussi identifié plusieurs mécanismes qui sont impliqués dans cette physiopathologie. Globalement, nos études devraient contribuer à mieux comprendre l’effet du tabagisme, du vieillissement, des oméga-3, et du stress oxydant sur l’évolution des maladies vasculaires ischémiques. / Atherosclerosis is the main cause of myocardial infarction, sudden cardiac death, stroke and lower limb ischemia. It is responsible for nearly half of all deaths in industrialized countries. When atherosclerotic arterial obstructions are so important that direct revascularization techniques cannot be successfully performed, the severity of residual tissue ischemia depends on the ability of the organism to spontaneously develop new blood vessels (neovascularization). Postnatal neovascularization is the result of two phenomena: the formation of new bloods vessels from the existing vasculature (angiogenesis) and vessel formation from progenitor cells (vasculogenesis). Our laboratory has demonstrated that several cardiovascular risk factors (smoking, aging, and hypercholesterolemia) also impair the angiogenic response after ischemia. However, the precise mechanisms involved in that pathophysiology are still unknown. A common feature of all the cardiovascular risk factors is increased oxidative stress. Therefore, the purpose of the present work was to elucidate the influence of cardiovascular risk factors and oxidative stress on neovascularization. Our results demonstrate that exposure to cigarette smoke and aging are associated with impaired neovascularization in response to ischemia, and that this is at least in part due to increased oxidative stress. In addition, we demonstrate that fatty acids derived from the diet can modulate the response to tissue ischemia. The first study of the research project evaluated the effect of cigarette smoke exposure on neovascularization in response to ischemia, and the effect of an antioxidant therapy. Exposure to cigarette smoke was associated with a significant reduction in the recovery of blood flow perfusion and vessel density in ischemic muscles. However, a complete recovery of neovascularization was demonstrated in mice exposed to cigarette smoke that were treated with probucol or antioxidant vitamins. We found that antioxidant therapy in mice exposed to cigarette smoke was associated with a significant reduction of oxidative stress levels in the plasma and in ischemic muscles. In addition, endothelial progenitor cells (EPCs) exposed to cigarette smoke extracts in vitro showed a significant decrease in their angiogenic activities (migration, adhesion and homing into ischemic tissues) that was completely rescued by probucol and antioxidants vitamins. The goal of the second study was to investigate the potential role of NADPH oxidase (Nox2) in the modulation of ischemia-induced neovascularization in the context of aging. We found that the expression of Nox2 is increased by aging in ischemic muscles of control mice. This is associated with a significant reduction of blood flow recovery after ischemia in older compared to young control mice. We also demonstrated that the density of capillaries and arterioles is significantly reduced in ischemic muscles of older animals, whereas oxidative stress levels are increased. Nox-2 deficiency reduces oxidative stress levels in ischemic tissues and improves blood flow recovery and vascular densities in older animals. We also demonstrated that the functional activities of EPCs (migration and adhesion to mature endothelial cells) were significantly reduced in older compared to young mice. However, Nox2 deficiency is associated with preserved EPCs functional activities in older animals. We also demonstrated an age-dependent pathological increase of oxidative stress in EPCs that is not found in Nox2-deficient animals. The third study of the research project investigated the effect of fatty acids derived from the diet on postnatal neovascularization. To this end, mice received a diet containing either 20% corn oil (rich in omega-6) or 20% fish oil (rich in omega-3). Our results demonstrate that an omega-3 rich diet increases neovascularization in response to ischemia at the macrovascular, microvascular and clinical level compared to an omega-6 rich diet. This increased postnatal neovascularization is associated with decreased total cholesterol/HDL cholesterol ratio in the serum and improved VEGF/NO pathway in ischemic tissues. In addition, the omega-3 rich diet is associated with a significant increase of central (bone marrow) and peripheral (spleen) EPCs. We also show that the functional activities of EPCs (migration and incorporation into tubules) are improved and oxidative stress level in EPCs is reduced by the omega-3 rich diet. In conclusion, our studies have clarified the impact of cardiovascular risk factors (smoking and aging) and fatty acids derived from the diet (omega-3) on ischemia-induced neovascularization. We have also identified several mechanisms involved in that physiopathology. Globally, our studies should contribute to a better understanding of the effects of cigarette smoking, aging and omega-3 on the evolution of ischemic vascular diseases.

Néovascularisation

Cellules endothéliales progénitrices

Stress oxydant

Fumée de cigarette

Antioxydants

Vieillissement

Nox2

Oméga-3

Endothelial progenitor cells

Oxidative stress

Cigarette smoke

Antioxidants

Aging

Omega-3

Neovascularization

Traditional Chinese Medicine extracts exert angiogenic and protective effects towards human endothelial progenitor cells: from cellular function to molecular pathway

Tang, Yubo

02 July 2014

Despite intense research efforts, the repair of large bone defects is still not satisfactory and remains a major challenge in Orthopaedic Surgery. In this context bone tissue engineering has emerged as a promising strategy. However, one of the fundamental principles underlying tissue engineering approaches is that newly formed tissue must maintain sufficient vascularization to support its growth. Thus an active blood vessel network is an essential pre-requisite for scaffold constructs to integrate within existing host tissue. Currently, great efforts are made to address this problem employing transplantation of vascular cells and loading of appropriate biological factors. Endothelial progenitor cells (EPCs) are a heterogeneous subpopulation of bone marrow mononuclear progenitor cells with potential for differentiation to the endothelial lineage and thus vasculogenic capacity. However, clinical studies reported that with the increase of age, increased susceptibility to apoptosis and accelerated senescence may contribute to the numerical and functional impairments observed in EPCs, which may lead to a reduced angiogenic capacity and an increased risk of vascular disease. Hence attention has increasingly been paid to enhance mobilization and differentiation of EPCs for therapeutic purposes. A large body of evidence indicates that in Traditional Chinese Medicine (TCM) a plethora of herbs and herbal extracts are effective in the treatment of vascular diseases such as chronic wounds, diabetic retinopathy and rheumatoid arthritis. Thus, it seems rational to explore these medicinal plants as potential sources of novel angiomodulatory factors. In this thesis we demonstrated that treatment with TCM herbal extracts promote cell growth, cell migration, cell-matrix and capillary-like tube formation of BM-EPCs. Among these TCM extracts, Salidroside (SAL) and Icariin (ICAR) incubation increased VEGF and nitric oxide secretion, which in turn mediated the enhancement of angiogenic differentiation of BM-EPCs. A mechanic evaluation provided evidence that SAL stimulates the phosphorylation of Akt, mammalian target of rapamycin (mTOR) and ribosomal protein S6 kinase (p70S6K), as well as phosphorylated ERK1/2, which is associated with the cell migration and tube formation. Furthermore, a pilot in vivo study showed that SAL has the potential to enhance bone formation in a murine femoral critical-size bone defects model. Another new finding of the present study is that hydrogen peroxide (H2O2)-induced cytotoxicity is counteracted by TCM extracts. We found that SAL, Salvianolic acid B (SalB) and ICAR significantly abrogated H2O2-induced cell apoptosis, reduced the intracellular level of reactive oxygen species (ROS) and nicotinamide adenine dinucleotide phosphate-oxidase (NADPH) expression, and restored the mitochondrial membrane potential of BM-EPCs. Our data suggest that this protective effect of SalB is mediated by the activation of mTOR, p70S6K, 4EBP1, and by the suppression of MKK3/6-p38 MAPK-ATF2 and ERK1/2 signaling pathways after H2O2 stress. In addition, the investigation also demonstrates that ICAR owns the ability to inhibit apoptotic and autophagic programmed cell death via restoring the loss of mTOR and attenuation of ATF2 activity upon oxidative stress. Based on the outcomes of the present work, we propose SAL, SalB and ICAR as novel proanigiogenic and cytoprotective therapeutic agents with potential applications in the fields of systemic and site-specific tissue regeneration including ischaemic disease and extended musculoskeletal tissue defects.

Angiogenese

oxidativer Stress

reaktive Sauerstoffspezies

4EBP1

ATF2

Traditional Chinese Medicine extracts

human endothelial progenitor cells

angiogenesis

oxidative stress

reactive oxygen species

4EBP1

ATF2

ddc:610

rvk:YU 4004

Characterization of bone marrow stromal clonal populations derived from osteoarthritis patients

Mareddy, Shobha R.

January 2008

This work is concerned with the characterization of mesenchymal stem cells (MSC) specifically from bone marrow samples derived from patients with osteoarthritis (OA). The multilineage potential of mesenchymal stem cells as well as their ease of exvivo expansion makes these cells an attractive therapeutic tool for applications such as autologous transplantation and tissue engineering. Bone marrow is considered a source of MSC. However, there is a general assumption that the occurrence of MSCs and their activity in bone marrow diminishes with age and disease. This prompted us to isolate and identify multipotential and self-renewing cells from patients with the degenerative disease osteoarthritis, with the view of using these cells for autologous cell therapies. It is therefore of great potential benefit to investigate the isolation and characterization of stem cell/progenitors from bone marrow samples of patients with osteoarthritis in greater detail. We employed a single cell clone culture method in order to develop clonal cell populations from three bone marrow samples and characterized them based on their proliferation and differentiation capabilities. The clonal populations were grouped into fast-growing and slow-growing clones based on their proliferation rates. The fastgrowing clones displayed 20-30% greater proliferation rate than the slow-growing clones. The study also revealed that the proliferation rates were directly proportional to their differentiation capacities. Most of the fast-growing clones were found to be tripotential for osteogenic, chondrogenic and adipogenic lineages, whereas the slow growing clones were either uni or bipotential. Flow cytometry analysis for the phenotype determination using putative MSC surface markers did not reveal any difference between the two clonal populations indicating a need for further molecular studies. Two approaches were employed to further investigate the molecular processes involved in the existence of such varying populations. In the first method gene expression studies were performed between the fast-growing (n=3) and slow-growing (n=3) clonal populations to identify potential genetic markers associated with cell 'sternness' using the Stem Cell RT2 ProfilerTM PCR Array comprising a series of 84 genes related to stem cell pathways. Ten genes were identified to be commonly and significantly over represented in the fast-growing stem cell clones when compared to slow-growing clones. This included expression of transcripts beyond MSC lineage specification such as SOX2, NOTCH1 and FOXA2 which signified that stem cell maintenance requires a coordinated regulation by multiple signalling pathways. The second study involved an extensive protein expression profiling of the fast growing (n=2) and slow growing (n=2) clonal populations using off-line Two Dimensional Liquid Chromatography (2D-LC)/Matrix-Assisted Laser Desorption/Ionization (MALDI) Mass Spectrometry (MS). A total of 67 proteins were identified, of which 11 were expressed at significantly different levels between the subpopulations. Protein ontology revealed these proteins to be associated with cellular organization, cytokinesis, signal transduction, energy pathways and cell stress response. Of particular interest was the differential presentation of the proteins calmodulin, tropomyosin and caldesmon between fast- and slow-growing clones. Based on their reported roles in the regulation of cell proliferation and maintenance of cell integrity, we draw an association between their expression and the altered status in which the subpopulations exist. Based on our observations, these proteins may be prospective molecular markers to distinguish between the fast-growing and slow-growing subpopulations. In summary, this study demonstrated the existence of potential stem cells of therapeutic importance in spite of a supposedly smaller stem cell compartment in patients with osteoarthritis. Furthermore, the differentially expressed genes between the sub-populations highlight the 'sternness' of the potential clones, an observation supported by the expression of proteins which act as effective modulators in the maintenance of cell integrity and cell cycle regulation. This study provides a basis for more detailed investigations in search of selective cell surface markers

Desenvolvimento de um substituto nanoestruturado a ser utilizado em associação com células-tronco para a terapia vascular em doença arterial periférica

Braghirolli, Daikelly Iglesias

January 2017

Atualmente, existe uma grande necessidade médica por enxertos vasculares de pequeno calibre (< 6 mm), que possam ser utilizados em cirurgias de reconstrução vascular. Nesse trabalho, dois tipos de biomateriais vasculares foram desenvolvidos pela técnica de electrospinning: biomateriais de policaprolactona (PCL) e biomateriais de poli(carbonato de trimetileno – co – ácido lático) (PTMCLLA). Os biomateriais de PCL foram funcionalizados com heparina e com VEGF (PCL/Hep/VEGF). Os biomateriais de PTMCLLA foram desenvolvidos a partir de três razões de carbonato de trimetileno/ ácido lático: 20/80, 30/70 e 40/60. Os biomateriais de PCL apresentaram taxa de degradação lenta e alta elasticidade. A funcionalização dos biomateriais preveniu a coagulação do sangue e também favoreceu o crescimento de células-tronco mesenquimais (CTMs) e de células progenitoras endoteliais (CPEs) nessas estruturas. A análise de PCR demonstrou que o VEGF adsorvido aos biomateriais não foi suficiente para diferenciar as CTMs em células endoteliais. O cultivo das CPEs sobre os biomateriais aumentou a expressão de VE-caderina e a presença de VEGF nas estruturas manteve o nível de expressão de CD31 e CD34 nessas células. Após essas análises, os biomateriais de PCL/Hep/VEGF foram fabricados em formato tubular. As CPEs foram semeadas no lúmen do biomaterial, através de biorreatores de parede rotatória (BPR), e mantidas em cultivo, por biorreatores de perfusão (BP). O BPR favoreceu a distribuição homogênea das CPEs na parede luminal dos biomateriais enquanto que o BP estimulou seu crescimento e otimizou seu metabolismo energético. Os biomateriais produzidos a partir dos copolímeros de PTMCLLA 30/70 e 40/60 exibiram uma alta flexibilidade. Porém, os biomateriais de PTMCLLA 40/60 tiveram um grande enrugamento. Os biomateriais de PTMCLLA 30/70 suportaram a adesão e o crescimento de CTMs, de CPEs e de células musculares lisas. Os resultados obtidos no presente estudo demonstram que biomateriais de PCL/Hep/VEGF apresentam características físico-químicas compatíveis para o uso vascular. Ainda, previnem a formação de trombos em sua superfície e propiciam o desenvolvimento da camada endotelial em seu lúmen. Os biomateriais de PTMCLLA 30/70 exibem alta flexibilidade e suportam o desenvolvimento de células vasculares e de células-tronco mesenquimais. De acordo com esses resultados, é possível concluir que biomateriais de PCL/Hep/VEGF e de PTMCLLA 30/70 são candidatos promissores para aplicação como enxertos vasculares. / Currently, there is a great medical need for small caliber vascular grafts (<6 mm), which can be used in vascular replacement surgeries. In this work, two types of vascular biomaterials were developed by the electrospinning technique: biomaterials of polycaprolactone (PCL) and biomaterials of poly(trimethylene carbonate-co-L-lactide) (PTMCLLA). PCL biomaterials were functionalized with heparin and VEGF (PCL / Hep/VEGF). The PTMCLLA biomaterials were developed from three ratios of trimethylene carbonate/lactide: 20/80, 30/70 and 40/60. The PCL biomaterials presented a slow degradation rate and high elasticity. The functionalization of the biomaterials prevented the blood from clotting and also favored the growth of mesenchymal stem cells (MSCs) and endothelial progenitor cells (EPCs) in these structures. PCR analysis demonstrated that VEGF adsorbed by the biomaterials was not sufficient to differentiate the MSCs into endothelial cells. The cultivation of CPEs on the biomaterials increased their expression of VE-cadherin and the presence of VEGF in the structures maintained the cell expression of CD34 and CD31. After these analyzes, the PCL/Hep/VEGF biomaterials were produced in a tubular geometrical form. The CPEs were seeded into their lumen by rotating bioreactors (RB) and maintained in culture by perfusion bioreactors (PB). The RB favored the homogeneous distribution of the CPEs in the luminal wall of the biomaterials while the BP stimulated their growth and optimized their energetic metabolism. The biomaterials produced from the PTMCLLA 30/70 and 40/60 copolymers exhibited high flexibility. However, the PTMCLLA 40/60 biomaterials exhibited substantial wrinkling. The PTMCLLA 30/70 biomaterials supported the adhesion and growth of MSCs, CPEs and smooth muscle cells. This study has demonstrated that PCL/Hep/VEGF biomaterials have physicochemical characteristics compatible with vascular use. Furthermore, they prevent thrombus formation on their surfaces and promote the development of the endothelial layer in their lumen. Biomaterials of PTMCLLA 30/70 exhibit high flexibility and support the development of vascular and mesenchymal stem cells. According to these results, it can be concluded that PCL/Hep/VEGF and PTMCLLA 30/70 biomaterials are promising candidates for use as vascular grafts.

Células-tronco

Materiais biocompatíveis

Doença arterial periférica

Engenharia tecidual

Vascular tissue engineering

Poly(caprolactone)

Endothelial progenitor cells

Vascular biomaterials

Implication de la sérotonine et des récepteurs 5-HT 2A/2B dans le remodelage des valves cardiaques et des bioprothèses valvulaires / Involvement of serotonin and 5-HT2A/2B receptors in cardiac valve and bioprosthetic remodeling

Ayme-Dietrich, Estelle

29 January 2016

L’hypothèse d’un lien entre valvulopathies et surexpression du système sérotoninergique fait suite aux lésions valvulaires observées lors de tumeurs carcinoïdes (taux sanguins de 5-HT élevés) et lors de l’utilisation chronique d’agonistes sérotoninergiques 5-HT2 (comme les dérivés de l’ergot de seigle, les fenfluramines). Le dogme actuel repose sur un effet prolifératif de la sérotonine, activant des cellules résidentes valvulaires, mais ne suffit pas à expliquer la dégénérescence de bioprothèses acellulaires. Nos travaux ont permis d’identifier des cellules progénitrices endothéliales (CD34+/CD309+), exprimant les récepteurs 5-HT2A et 5-HT2B, au sein de lésions valvulaires humaines aortiques et mitrales, quelle que soit l’étiologie de leur dégénérescence. Ils ont permis de mettre en évidence un rôle double de la sérotonine dans la dégénérescence valvulaire : 1) la stimulation des récepteurs 5-HT2B contribue à la mobilisation sanguine des progéniteurs CD34+ (recrutés à partir de la moelle osseuse, et migrant dans le tissu valvulaire), 2) le rôle des récepteurs 5-HT2 dans la transdifférenciation des progéniteurs endothéliaux en cellules activées, au sein de la matrice valvulaire. La suite de ce travail permettra de développer 1) un biomarqueur prédictif d’atteinte valvulaire, dans des populations à haut risque, 2) de développer un modèle cellulaire de valvulopathie pour étudier les mécanismes impliqués dans le remodelage valvulaire et leurs voies de signalisation, et 3) de déterminer des cibles thérapeutiques autour du système sérotoninergique, permettant de ralentir la progression des lésions et retarder l’exérèse chirurgicale, seule alternative actuelle.Abstract / Several studies have established an association between some cardiac valve injuries and overexpression of the serotonergic system. Valve lesions are observed following carcinoid tumours (with high blood levels of 5-HT) and during the chronic use of 5-HT2 serotonergic agonists (ergot derivatives or fenfluramines). The current dogma is based on a mitogenic effect of serotonin, by activating 5-HT2B receptors, leading to resident valvular cells proliferation, but does not explain the degeneration of acellular cardiac bioprosthesis. Our work identified endothelial progenitor cells (CD34 + / CD309 +), expressing 5-HT2A and 5-HT2B receptors, in human aortic and mitral valve lesions, regardless of the etiology of their degeneration. Our work highlights the dual role of serotonin in valvular degeneration: 1) stimulation of the 5-HT2B receptor contributes to blood mobilization of CD34+ progenitors (recruited from the bone marrow, and migrating in the valve tissue), 2) the role of 5-HT2 receptors in the transdifferentiation of endothelial progenitor cells in activated valvular cells. The results of this work could drive to the development of 1) a predictive biomarker of cardiac valve injuries in high-risk populations, 2) a model to study heart valve disease cellular and molecular mechanisms, and 3) identify therapeutic targets around the serotonergic system, to slower the progression of the lesions and delay surgical replacement, the only current alternative.

Sérotonine

Valvulopathies

Cellules progénitrices endothéliales

Mobilisation

Transition endothélio-mésenchymateuse

Serotonin

5-HT2A and 5-HT2B receptors

Valvulopathy

Endothelial progenitor cells

Mobilization

Mesenchymal-endothelial transition

572.8

615.58

616.12

Desenvolvimento de um substituto nanoestruturado a ser utilizado em associação com células-tronco para a terapia vascular em doença arterial periférica

Braghirolli, Daikelly Iglesias

January 2017

Atualmente, existe uma grande necessidade médica por enxertos vasculares de pequeno calibre (< 6 mm), que possam ser utilizados em cirurgias de reconstrução vascular. Nesse trabalho, dois tipos de biomateriais vasculares foram desenvolvidos pela técnica de electrospinning: biomateriais de policaprolactona (PCL) e biomateriais de poli(carbonato de trimetileno – co – ácido lático) (PTMCLLA). Os biomateriais de PCL foram funcionalizados com heparina e com VEGF (PCL/Hep/VEGF). Os biomateriais de PTMCLLA foram desenvolvidos a partir de três razões de carbonato de trimetileno/ ácido lático: 20/80, 30/70 e 40/60. Os biomateriais de PCL apresentaram taxa de degradação lenta e alta elasticidade. A funcionalização dos biomateriais preveniu a coagulação do sangue e também favoreceu o crescimento de células-tronco mesenquimais (CTMs) e de células progenitoras endoteliais (CPEs) nessas estruturas. A análise de PCR demonstrou que o VEGF adsorvido aos biomateriais não foi suficiente para diferenciar as CTMs em células endoteliais. O cultivo das CPEs sobre os biomateriais aumentou a expressão de VE-caderina e a presença de VEGF nas estruturas manteve o nível de expressão de CD31 e CD34 nessas células. Após essas análises, os biomateriais de PCL/Hep/VEGF foram fabricados em formato tubular. As CPEs foram semeadas no lúmen do biomaterial, através de biorreatores de parede rotatória (BPR), e mantidas em cultivo, por biorreatores de perfusão (BP). O BPR favoreceu a distribuição homogênea das CPEs na parede luminal dos biomateriais enquanto que o BP estimulou seu crescimento e otimizou seu metabolismo energético. Os biomateriais produzidos a partir dos copolímeros de PTMCLLA 30/70 e 40/60 exibiram uma alta flexibilidade. Porém, os biomateriais de PTMCLLA 40/60 tiveram um grande enrugamento. Os biomateriais de PTMCLLA 30/70 suportaram a adesão e o crescimento de CTMs, de CPEs e de células musculares lisas. Os resultados obtidos no presente estudo demonstram que biomateriais de PCL/Hep/VEGF apresentam características físico-químicas compatíveis para o uso vascular. Ainda, previnem a formação de trombos em sua superfície e propiciam o desenvolvimento da camada endotelial em seu lúmen. Os biomateriais de PTMCLLA 30/70 exibem alta flexibilidade e suportam o desenvolvimento de células vasculares e de células-tronco mesenquimais. De acordo com esses resultados, é possível concluir que biomateriais de PCL/Hep/VEGF e de PTMCLLA 30/70 são candidatos promissores para aplicação como enxertos vasculares. / Currently, there is a great medical need for small caliber vascular grafts (<6 mm), which can be used in vascular replacement surgeries. In this work, two types of vascular biomaterials were developed by the electrospinning technique: biomaterials of polycaprolactone (PCL) and biomaterials of poly(trimethylene carbonate-co-L-lactide) (PTMCLLA). PCL biomaterials were functionalized with heparin and VEGF (PCL / Hep/VEGF). The PTMCLLA biomaterials were developed from three ratios of trimethylene carbonate/lactide: 20/80, 30/70 and 40/60. The PCL biomaterials presented a slow degradation rate and high elasticity. The functionalization of the biomaterials prevented the blood from clotting and also favored the growth of mesenchymal stem cells (MSCs) and endothelial progenitor cells (EPCs) in these structures. PCR analysis demonstrated that VEGF adsorbed by the biomaterials was not sufficient to differentiate the MSCs into endothelial cells. The cultivation of CPEs on the biomaterials increased their expression of VE-cadherin and the presence of VEGF in the structures maintained the cell expression of CD34 and CD31. After these analyzes, the PCL/Hep/VEGF biomaterials were produced in a tubular geometrical form. The CPEs were seeded into their lumen by rotating bioreactors (RB) and maintained in culture by perfusion bioreactors (PB). The RB favored the homogeneous distribution of the CPEs in the luminal wall of the biomaterials while the BP stimulated their growth and optimized their energetic metabolism. The biomaterials produced from the PTMCLLA 30/70 and 40/60 copolymers exhibited high flexibility. However, the PTMCLLA 40/60 biomaterials exhibited substantial wrinkling. The PTMCLLA 30/70 biomaterials supported the adhesion and growth of MSCs, CPEs and smooth muscle cells. This study has demonstrated that PCL/Hep/VEGF biomaterials have physicochemical characteristics compatible with vascular use. Furthermore, they prevent thrombus formation on their surfaces and promote the development of the endothelial layer in their lumen. Biomaterials of PTMCLLA 30/70 exhibit high flexibility and support the development of vascular and mesenchymal stem cells. According to these results, it can be concluded that PCL/Hep/VEGF and PTMCLLA 30/70 biomaterials are promising candidates for use as vascular grafts.

Células-tronco

Materiais biocompatíveis

Doença arterial periférica

Engenharia tecidual

Vascular tissue engineering

Poly(caprolactone)

Endothelial progenitor cells

Vascular biomaterials

Expansão ex vivo das células-tronco hematopoiéticas do sangue do cordão umbilical: análise comparativa da proliferação celular em cocultura de células-troco mesenquimais provenientes do endotélio vascular do cordão umbilical e do tecido adiposo / Cord blood hematopoietic stem cells ex vivo expansion: comparative analysis of cell proliferation promoted by adipose tissue and umbilical cord endothelium mesenchymal stem cells in coculture system

Andresa Forte

10 December 2014

INTRODUÇÃO: As células-tronco hematopoiéticas (CTH) do sangue do cordão umbilical (SCU) têm sido utilizadas com sucesso para o tratamento de doenças malignas e não malignas. No entanto, algumas unidades de SCU podem apresentar baixa quantidade de células nucleadas totais (CNT). Algumas abordagens têm sido sugeridas para evitar problemas em relação à baixa concentração de CTH no transplante, como a administração de duas unidades de SCU para o paciente e a expansão ex vivo de CTH. OBJETIVO: Avaliar as taxas de proliferação celular na expansão ex vivo do SCU em sistema de cocultura com células-tronco mesenquimais (CTM) obtidos a partir de diferentes fontes com alta e baixa confluência e adicionando-se ou não coquetel de citocinas no meio de cultura. MÉTODOS: Este estudo foi aprovado pelo Comitê de Ética de Pesquisa (CAPPesq) do Hospital das Clínicas da Faculdade de Medicina da USP. A coleta do SCU (n =10) foi realizada após o nascimento do bebê e expulsão da placenta. O processamento foi realizado utilizando o método de redução de volume, o qual consiste em depleção de eritrócitos. As amostras de CTM provenientes do endotélio vascular do cordão umbilical foram obtidas de doadores diferentes (n=3) e o tecido adiposo (n=3) do inventário do LIM-31. A expansão das CNT e das células com expressão de marcadores CD133+/CD34+ foram observados depois de sete dias de cultura. Além disso, o ensaio para análise de unidades de formadoras de colônias (UFC) foi realizado em todas as amostras antes e depois da expansão do SCU. Para a expansão em sistema de cocultura foi separado dois grupos para ambas as fontes de CTM (Grupo I - cocultura com adição de coquetel de citocinas vs. Grupo II - cocultura sem citocinas). RESULTADOS: Após sete dias, no grupo I com cocultura confluente, a taxa de proliferação de CNT foi duas vezes maior ao comparar com cocultura subconfluente (35 vs. 16 vezes). No mesmo grupo também foi possível evidenciar elevada taxa de proliferação de células CD133+/CD34+. O índice de proliferação das UFC no grupo I aumentou até oito vezes. A cocultura subconfluente tanto do endotélio vascular do cordão umbilical como do tecido adiposo apresentou menor rendimento em comparação as CTM confluentes. A expansão das células na presença de citocinas apresentou maior proliferação celular ao comparar às coculturas sem adição de citocinas. CONCLUSÃO: Este estudo mostrou que para alto rendimento de células do SCU, o sistema de cocultura requer adição de coquetel de citocinas e CTM confluente independentemente da fonte utilizada / INTRODUCTION: Umbilical cord blood (UCB) hematopoietic stem cells have been successfully used for the treatment of both malignant and non-malignant diseases. Nevertheless, some UCB units could have low total nucleated cells (TNC) dose. Several approaches have been suggested to avoid inadequacy problems of hematopoietic stem cells (HSC) number for transplantation, such as administration of two UCB units to the patient and HSC ex vivo expansion. OBJECTIVE: Evaluate UCB ex vivo expansion proliferative rates in a high and low mesenchymal stem cells (MSC) confluence feeder layer obtained from different MSC sources and by adding or not cytokines cocktail into the medium. METHODS: This study was approved by the Research Ethic Committee (CAPPESQ) of Hospital das Clínicas da Faculdade de Medicina da USP. The collection of UCB (n=10) was made after delivery of the infant and the expulsion of placenta. Processing was performed using volume reduction method which consists in red blood depletion. MSC samples from umbilical cord endothelium were obtained from three different donors and adipose tissue (n=3) obtained from LIM31\'s pattern inventory. The total nucleated cell (TNC), expression of hematopoietic surface markers such as CD133+/CD34+ were observed after seven days of culture. Beyond that, colony forming unit assay (CFU) was performed before and after UCB expansion. The expansion by coculture method was observed in two groups (Group I - coculture with cytokines cocktail added vs. Group II- coculture without cytokines cocktail) for both MSCs sources. RESULTS: After seven days, analysis of confluent coculture showed that TNC proliferation rate ware almost 2 times higher than in subconfluent coculture (35 vs. 16-fold) in Group I and also revealed higher proliferative rate in CD133+/CD34+ cells considering. CFU showed similar increase after seven days of culture in comparison of day 0 (up to 8-fold). Subconfluent coculture for both umbilical cord endothelium and adipose tissue showed lower yield compared with those with high MSC confluence. The expansion in the presence of cytokines showed higher cell proliferation compared to the cocultures without addition of cytokines. CONCLUSION: This study showed that coculture system may require the addition of cytokines cocktail in the media and confluent MSC regardless of source for high yield of UCB cells

Células progenitoras hematopoiéticas

Células-tronco

Células-tronco adultas

Cordão umbilical

Proliferação de células

Sangue fetal

Tecido adiposo

Técnicas de cocultura

Adipose tissue

Adult stem cells

Cell proliferation

Coculture techniques

Fetal blood

Hematopoietic progenitor cells

Stem cells

Umbilical cord

Novel Therapeutic Strategies for the Treatment of Pulmonary Arterial Hypertension

Suen, Colin

January 2017

Pulmonary arterial hypertension (PAH) is a progressive disease that results in increased pulmonary vasculature resistance, causing right ventricular (RV) remodeling, which eventually progresses into right heart failure and mortality. New and emerging therapeutic strategies involve regenerative approaches to repair the underlying vascular pathology using regenerative cell therapy and methods to alleviate RV dysfunction in the setting of fixed RV afterload. In the first section of the thesis, we investigated the role of EPC paracrine mechanisms in the treatment of PAH. We characterized the paracrine function of EPCs by demonstrating that EPC conditioned medium enhances endothelial cell migration, survival and angiogenesis in vitro. We further examined the role of secreted extracellular vesicles in the paracrine function of EPCs, which played a minor role in promoting wound healing. However, using the monocrotaline rat model of PAH, we did not demonstrate a consistent benefit on RV pressures or remodeling with EPCs or EPC conditioned medium. The lack of effect may be related to the advanced phenotype observed in our model of PAH. Survival in severe pulmonary arterial hypertension (PAH) is related to the ability of the right ventricle (RV) to adapt to increased afterload. Therefore, we explored the effect of genetic background on right ventricular adaptation and survival in a rat model of severe (PAH). Compared to the conventional Sprague-Dawley rat strain, we observed high mortality in the Fischer SUHx model of severe PAH. This was related to a strain-dependent failure of RV adaptation, as evidenced by RV dilatation, RV contractile dysfunction, decreased cardiac ouptut and decreased exercise capacity. Further analysis by gene expression microarrays and fluorescence microangiography demonstrate that failure of RV adaptation is due at least in part due to lack of adequate microvascular angiogenesis in the hypertrophied RV. This work lays the foundation for the section on RV-specific therapy that follows. Using the Fischer model of maladaptive RV remodeling, we tested whether cardiotrophin-1 (CT-1), a pro-angiogenic and cardioprotective cytokine, could improve RV adaptation. We demonstrated that as a rescue treatment, CT-1 reduced RV dilatation and function without influencing RV afterload, which suggests improved RV adaptation. These changes were associated with an increase in RV capillary density. As an early-stage preventative treatment, in addition to improving RV remodeling, CT-1 also reduced pulmonary pressures. These hemodynamic changes suggest that CT-1 may also have a direct impact on vascular tone or the underlying pulmonary vascular pathology.

Pulmonary hypertension

Pulmonary arterial hypertension

Stem cell

Right ventricle

Endothelial progenitor cell

Endothelium

Heart failure

Sprague dawley rat

Fischer rat

Exosome

Microvesicle

Extracellular vesicles

SU5416

Paracrine

Angiogenesis

SUHx

Cardiotrophin

CT-1

Approche physiopathologique et recherche de biomarqueurs associés aux complications neurovasculaires chez l'enfant drépanocytaire / Biomarkers associated with cerebrovascular complications in children with sickle-cell disease : a pathophysiological approach

Kossorotoff, Manoëlle

24 November 2014

L'atteinte vasculaire cérébrale est une complication grave et fréquente chez les enfants drépanocytaires, car elle impacte leur pronostic, en termes de morbidité (handicap) et de mortalité. L’accélération des vitesses mesurées par le doppler transcrânien (DTC) est prédictive du risque d'infarctus cérébral et implique une modification de la prise en charge thérapeutique. Chez l’enfant drépanocytaire, l'infarctus cérébral est d'origine multifactorielle, lié à la vasculopathie cérébrale sténotique ainsi qu'à une hypercoagulabilité et une activation cellulaire. Nous avons étudié de manière prospective l'association de marqueurs biologiques au DTC chez 108 enfants porteurs de syndrome drépanocytaire majeur et recherché des éléments prédictifs d'événement vasculaire périphérique ou cérébral. Nous avons ainsi réalisé une analyse approfondie de la fonction endothéliale, de l’activation de l’hémostase primaire et de la coagulation, de l'activation cellulaire et de la mécanique artérielle. L’atteinte vasculaire cérébrale a été estimée en considérant les données du DTC comme une variable continue plutôt que catégorielle. Le principal résultat est le rôle prédictif du nombre des cellules souches hématopoïétiques CD34+ pour la survenue d'événements cliniques vasculaires. Nous avons également mis en évidence un profil particulier de coagulation chez les enfants drépanocytaires présentant des céphalées récurrentes ou des accès migraineux. Ceci supporte l'hypothèse que les céphalées chez l'enfant drépanocytaire, et notamment celles répondant aux critères de la migraine, peuvent être le reflet d'événements ischémiques cérébraux ultra-transitoires. Elles représentent donc peut-être un indicateur indirect de risque ischémique cérébral. Nous avons par ailleurs montré que le risque hémorragique cérébral chez les enfants drépanocytaires restait proportionnellement stable par rapport au risque ischémique, malgré l'utilisation en routine de stratégies de prévention du risque ischémique. L'observation de lésions sténotiques et d'anévrismes permet de supposer que ces atteintes vasculaires cérébrales procèdent de mécanismes physiopathologiques communs. L'amélioration de la compréhension des mécanismes physiopathologiques des complications neurovasculaires et la mise en évidence de facteurs prédictifs d'événements cliniques est un pas supplémentaire vers l'amélioration de la sensibilité diagnostique de la vasculopathie cérébrale drépanocytaire, de la compréhension des mécanismes des accidents vasculaires cérébraux de ces enfants et probablement de leur pronostic neurologique en permettant une prise en charge thérapeutique adaptée plus précoce. / Cerbrovascular involvement is frequent in children with sickle-cell disease (SCD). It is severe in terms of morbidity (handicap) and mortality. Accelerated intracranial arterial blood flow velocity measured by transcranial doppler (TCD) is predictive for stroke occurrence and leads to therapeutic modifications. In SCD children, ischemic stroke results from stenotic cerebral vasculopathy associated with hypercoagulability, and cell activation. We prospectively addressed associations between biological markers and TCD velocity in 108 children with sickle-cell anemia (HbSS or HbSβ°) and looked for predictive factors for vascular peripheral or cerebral events. We performed extensive work-up of endothelial function, coagulation activation, cell activation, and arterial wall mechanics. Cerebral vasculopathy was defined using TCD velocity (continuous data) rather than the classical category classification. The main result is the demonstration of the role of hematopoietic stem cell CD34+ for the prediction of clinical vascular event occurrence. We also demonstrated an imbalanced coagulation profile in SCD children with recurrent cephalalgia or migraine. This finding supports the hypothesis that recurrent cephalalgia, especially migraine, could be a symptom of ultra-transient ischemic cerebrovascular events in SCD children. Therefore, this symptom may also indicate increased cerebrovascular ischemic risk. We demonstrated that the ratio cerebral hemorrhagic risk / cerebral ischemic risk in SCD children remains stable, despite the routine use of strategies aiming at reducing ischemic stroke risk. The concurrent observation of intracranial arterial stenotic lesions and aneurysm suggests common pathophyiological mechanisms. Improving pathophysiological understanding of cerebrovascular complications and demonstrating predictive risk factors for clinical events may help clinicians to improve early diagnosis of SCD-associated cerebral vasculopathy, to better understand stroke mechanism in this population, and probably to improve neurological outcome with earlier and more adapted management

Drépanocytose

Enfant

Vasculopathie cérébrale

AVC

Infarctus cérébral

Cellules souches hématopoïétiques

Migraine

Hémorragie cérébrale

Anévrisme

Sickle-cell disease

Children

Cerebral vasculopathy

Stroke

Ischemic stroke

Hematopoietic progenitor cell

Migraine

Cerebral hemorrhage

Aneurysm

616.152 7

Modulation du potentiel angiogène des progéniteurs endothéliaux humains par des biomarqueurs plasmatiques vasculaires / Angiogenic potential modulation of human endothelial progenitor cells by vascular plasmatic biomarkers

d'Audigier, Clément

02 October 2013

Rationnel : L’implication établie des progéniteurs endothéliaux circulants dans les phénomènes de néovascularisation chez l’adulte a stimulé la recherche de thérapeutiques angiogènes basées sur la greffe de ces cellules. Deux types cellulaires au phénotype endothélial sont actuellement définis entre autres par leur cinétique d’apparition en culture : les progéniteurs précoces (CFU-EC ou CAC) et tardifs (ECFC). Notre équipe a montré que l’injection thérapeutique de cellules mononucléées de moelle osseuse (BM-MNC) permettait la néovascularisation du site ischémié chez des patients atteints d’artériopathie des membres inférieurs, et que les néovaisseaux formés avaient le phénotype d’ECFC. Nous avons dans un premier temps mesuré les concentrations de différentes protéines modulant l’angiogenèse, chez des patients atteints de pathologies ischémiques et cardiovasculaires, ou impliquant des anomalies vasculaires associées à la fibrose. Ainsi, le transforming growth factor - β1 (TGF-β1) dans la fibrose pulmonaire idiopathique (FPI), la thrombospondine-1 (TSP-1) dans l’artériopathie des membres inférieurs (AMI), et le placental growth factor (PlGF) chez les patients atteints de pathologies cardiovasculaires [syndrome coronarien aigu (SCA), ou patients devant subir une chirurgie de la valve ou un pontage coronarien], se sont distingués comme potentiel biomarqueur plasmatique dans ces pathologies, et ont été étudiés dans la biologie des ECFC humaines.Résultats : Le taux plasmatique de TGF-β1 est augmenté chez les patients atteints de FPI par rapport à la population contrôle ; il a un effet pro-angiogène in vivo (vascularisation des implants de Matrigel®) et in vitro (prolifération et migration des ECFC) via les récepteurs ALK-1, ALK-5 et TGF-βRII. Le taux plasmatique de TSP-1 est augmenté chez les patients artéritiques par rapport à la population contrôle. Par ailleurs les néovaisseaux formés de patients artéritiques ayant été traités par injection locale de BM-MNC expriment la TSP-1. Dans les modèles murins de Matrigel®-plugs et d’ischémie du membre inférieur (IMI), la TSP-1 induit une diminution de la vascularisation des implants ainsi qu’une diminution de la revascularisation du membre ischémié. In vitro, la TSP-1 augmente l’adhésion via un mécanisme N-Terminal dépendant, et diminue le potentiel angiogène (prolifération et migration) des ECFC via sa liaison au récepteur CD47, ce qui active la voie de signalisation SDF-1/CXCR4. Le taux plasmatique de PlGF est augmenté chez les patients atteints de SCA par rapport à 2 populations contrôles ; il est également augmenté chez les patients ayant subit une chirurgie cardiaque. Les PlGF-1 et -2 potentialisent la tubulogenèse des ECFC in vitro via la phosphorylation du récepteur VEGFR1. Cet effet est aboli lorsque le VEGFR1 est inhibé par ARN interférence ou par le composé chimique « 4321 ». De plus ce composé « 4321 » inhibe la vascularisation des implants de Matrigel®, ainsi que la revascularisation du membre ischémié dans le modèle d’IMI.Conclusions : Le TGF-β1 joue un rôle dans le remodelage vasculaire de la FPI via les ECFC ; la TSP-1 est un potentiel biomarqueur de l’angiogenèse induite par les ECFC dans l’AMI ; l’inhibition de la voie PlGF/VEGFR1 module la tubulogenèse induite par les ECFC, cellules impliquées dans la formation de nouveaux vaisseaux. Nous avons ainsi mis en évidence 3 protéines modulant l’angiogenèse dans 3 contextes pathologiques différents, caractérisés par un remodelage vasculaire et où les ECFC sont impliquées dans leurs mécanismes physiopathologiques. Ces 3 protéines se présentent donc comme de potentiels biomarqueurs plasmatiques, modulant les propriétés angiogènes des ECFC et pouvant influencer leur efficacité en tant que produit de thérapie cellulaire. Ces protéines jouent un rôle probable dans l’équilibre homéostatique au décours des pathologies concernées. / Rationale: The pro-angiogenic capacities of endothelial progenitor cells are now well established, and their involvement in neovascularization events in adults has stimulated the research in the field of angiogenic therapy based on transplant of these cells. Current data converge towards the notion of two cell types with endothelial phenotype, defined at least by their kinetics of appearance in culture: early endothelial progenitor cells (CFU-EC or CAC) and late (ECFC). Our team has shown that the therapeutic injection of bone marrow mononuclear cells (BM-MNC) led to neovascularization of the ischemic site in patients with critical limb ischemia, and that the new vessels formed bore the phenotype of ECFC. We initially measured the concentrations of different proteins modulating angiogenesis in patients with ischemic and cardiovascular diseases, or involving vascular abnormalities associated with fibrosis. Thus, the transforming growth factor - ß1 (TGF-ß1) in idiopathic pulmonary fibrosis, the thrombospondin-1 (TSP-1) in peripheral artery disease, and the placental growth factor (PlGF) in patients with cardiovascular diseases [acute coronary syndrome (ACS), patients undergoing valve surgery or coronary artery bypass surgery], emerged as potential plasmatic biomarkers in these pathological settings, and have been studied in the biology of human ECFC.Results: TGF-ß1 plasma level is increased in patients with idiopathic pulmonary fibrosis (IPF) compared to the control population; it exerts a pro-angiogenic effect in vivo (vascularization of Matrigel ®-plugs) and in vitro (proliferation and migration of ECFC) via ALK-1, ALK-5 and TGF-ßRII receptors. TSP-1 plasma level is increased in patients with peripheral artery disease (PAD) compared to the control population. In addition, the new vessels formed in PAD patients treated by local injection of BM-MNC express TSP-1. In murine models of Matrigel ®-plugs and hindlimb ischemia, TSP-1 induces a decrease in plugs vascularization and impaired revascularization of ischemic limb. In vitro, TSP-1 increases ECFC adhesion via an N-terminal dependent mechanism and reduces their angiogenic potential (proliferation and migration) via its binding to CD47 receptor, which activates the SDF-1/CXCR4 signaling pathway. PlGF plasma level is increased in ACS patients compared with the control population and stable angina patients and is also increased in patients undergoing cardiac surgery. PlGF-1 and -2 potentiate ECFC tubulogenesis in vitro via phosphorylation of the VEGFR1 receptor. This effect was abolished when the ECFC VEGFR1 is inhibited by RNA interference or by the chemical compound "4321". In addition this compound "4321" inhibits the vascularization of Matrigel ®-plugs, and revascularization of the ischemic limb in the hindlimb ischemia model.Conclusions: TGF-ß1 is involved in the IPF vascular remodeling through ECFC; TSP-1 is a potential biomarker of angiogenesis induced by ECFC in PAD; the inhibition of the PlGF/VEGFR1 pathway modulates ECFC tubulogenesis, cells involved in the formation of new vessels. We thus identified three proteins that modulate angiogenesis in three different pathological settings characterized by a vascular remodeling and where ECFC are involved in their pathophysiology. These three proteins therefore state as potential plasmatic biomarkers, modulating ECFC angiogenic properties and are able to influence their efficacy as a cell therapy product. These plasmatic biomarkers likely play a role in the homeostasis of those pathologies progress.

Progéniteurs endothéliaux circulants

Biomarqueurs plasmatiques vasculaires

Potentiel angiogène

Fibrose pulmonaire idiopathique

Artériopathie des membres inférieurs

Syndromes coronariens aigus

Thérapie cellulaire

Endothelial progenitor cells

Vascular plasmatic biomarkers

Angiogenic potential

Idiopathic pulmonary fibrosis

Peripheral artery disease

Acute coronary syndromes

Cell therapy

616.13