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National Repository of Grey Literature

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Role of endothelial and vascular smooth muscle cells in the origin, progression and therapy of vascular diseases Chlupáč, Jaroslav ; Bačáková, Lucie (advisor) ; Piťha, Jan (referee) ; Sedmera, David (referee) Introduction: Vascular surgery for atherosclerosis is confronted by the lack of a suitable bypass material. Synthetic vascular prostheses include polyethylene terephthalate (PET) and expanded polytetrafluoroethylene (ePTFE). However, these materials become thrombosed in small-caliber applications (<6 mm) because of the lack of an endothelium. The objectives of this study were to make modifications to clinically-used PET vascular prostheses with tissue-engineered surfaces to improve their bio-compatibility towards vascular smooth muscle cells (VSMC) and endothelial cells (EC). Methods: Blood coagulation protein fibrin (Fb) and extracellular matrix proteins collagen (Co), laminin (LM) and fibronectin (FN) were used. Cell adhesive assemblies were prepared: Co, Co/LM, Co/FN, Co/Fb, Co/Fb/FN. Cell culture experiments were performed: (1) planar static, (2) planar dynamic with simulation of blood flow, (3) tubular dynamic, and (4) animal porcine implantation. Results: The growth of EC and VSMC on commercial prostheses (ePTFE, PET and PET/Co) was low. The growth of both cell types was lower on PET/Co than on PET. After modification with protein assemblies, the highest numbers of EC were reached on PET/Co and on PET/Co +Co/Fb. There was no difference in the densities of VSMC among various assemblies. The... Detailed record

Role of endothelial and vascular smooth muscle cells in the origin, progression and therapy of vascular diseases Chlupáč, Jaroslav ; Bačáková, Lucie (advisor) ; Piťha, Jan (referee) ; Sedmera, David (referee) Introduction: Vascular surgery for atherosclerosis is confronted by the lack of a suitable bypass material. Synthetic vascular prostheses include polyethylene terephthalate (PET) and expanded polytetrafluoroethylene (ePTFE). However, these materials become thrombosed in small-caliber applications (<6 mm) because of the lack of an endothelium. The objectives of this study were to make modifications to clinically-used PET vascular prostheses with tissue-engineered surfaces to improve their bio-compatibility towards vascular smooth muscle cells (VSMC) and endothelial cells (EC). Methods: Blood coagulation protein fibrin (Fb) and extracellular matrix proteins collagen (Co), laminin (LM) and fibronectin (FN) were used. Cell adhesive assemblies were prepared: Co, Co/LM, Co/FN, Co/Fb, Co/Fb/FN. Cell culture experiments were performed: (1) planar static, (2) planar dynamic with simulation of blood flow, (3) tubular dynamic, and (4) animal porcine implantation. Results: The growth of EC and VSMC on commercial prostheses (ePTFE, PET and PET/Co) was low. The growth of both cell types was lower on PET/Co than on PET. After modification with protein assemblies, the highest numbers of EC were reached on PET/Co and on PET/Co +Co/Fb. There was no difference in the densities of VSMC among various assemblies. The... Detailed record

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