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Cartilage tissue engineering: molecular control of chondrocyte differentiation for proper cartilage matrix reconstruction.
Demoor, Magali; Ollitrault, David; Gomez-Leduc, Tangni; Bouyoucef, Mouloud; Hervieu, Magalie; Fabre, Hugo; Lafont, Jérôme; Denoix, Jean-Marie; Audigié, Fabrice; Mallein-Gerin, Frédéric; Legendre, Florence; Galera, Philippe.
Afiliação
  • Demoor M; Laboratoire Microenvironnement Cellulaire et Pathologies (MILPAT) EA 4652, SFR 146 ICORE, Faculty of Medicine, IBFA, University of Caen/Lower-Normandy (UCLN), France.
  • Ollitrault D; Laboratoire Microenvironnement Cellulaire et Pathologies (MILPAT) EA 4652, SFR 146 ICORE, Faculty of Medicine, IBFA, University of Caen/Lower-Normandy (UCLN), France.
  • Gomez-Leduc T; Laboratoire Microenvironnement Cellulaire et Pathologies (MILPAT) EA 4652, SFR 146 ICORE, Faculty of Medicine, IBFA, University of Caen/Lower-Normandy (UCLN), France.
  • Bouyoucef M; Laboratoire Microenvironnement Cellulaire et Pathologies (MILPAT) EA 4652, SFR 146 ICORE, Faculty of Medicine, IBFA, University of Caen/Lower-Normandy (UCLN), France.
  • Hervieu M; Laboratoire Microenvironnement Cellulaire et Pathologies (MILPAT) EA 4652, SFR 146 ICORE, Faculty of Medicine, IBFA, University of Caen/Lower-Normandy (UCLN), France.
  • Fabre H; Laboratory of Biology and Engineering of Cartilage, UMR 5305 CNRS-Univ. de Lyon, IBCP, Lyon, France.
  • Lafont J; Laboratory of Biology and Engineering of Cartilage, UMR 5305 CNRS-Univ. de Lyon, IBCP, Lyon, France.
  • Denoix JM; CIRALE (Centre d'imagerie et de recherche sur les affections locomotrices), USC INRA-ENVA (Ecole Nationale Vétérinaire d'Alfort) 957, Equipe Biomécanique et pathologie locomotrice du cheval), Imagerie et Pathologie Ostéo-Articulaire, University of Caen/Lower-Normandy, Goustranville, France.
  • Audigié F; CIRALE (Centre d'imagerie et de recherche sur les affections locomotrices), USC INRA-ENVA (Ecole Nationale Vétérinaire d'Alfort) 957, Equipe Biomécanique et pathologie locomotrice du cheval), Imagerie et Pathologie Ostéo-Articulaire, University of Caen/Lower-Normandy, Goustranville, France.
  • Mallein-Gerin F; Laboratory of Biology and Engineering of Cartilage, UMR 5305 CNRS-Univ. de Lyon, IBCP, Lyon, France.
  • Legendre F; Laboratoire Microenvironnement Cellulaire et Pathologies (MILPAT) EA 4652, SFR 146 ICORE, Faculty of Medicine, IBFA, University of Caen/Lower-Normandy (UCLN), France.
  • Galera P; Laboratoire Microenvironnement Cellulaire et Pathologies (MILPAT) EA 4652, SFR 146 ICORE, Faculty of Medicine, IBFA, University of Caen/Lower-Normandy (UCLN), France. Electronic address: philippe.galera@unicaen.fr.
Biochim Biophys Acta ; 1840(8): 2414-40, 2014 Aug.
Article em En | MEDLINE | ID: mdl-24608030
BACKGROUND: Articular cartilage defects are a veritable therapeutic problem because therapeutic options are very scarce. Due to the poor self-regeneration capacity of cartilage, minor cartilage defects often lead to osteoarthritis. Several surgical strategies have been developed to repair damaged cartilage. Autologous chondrocyte implantation (ACI) gives encouraging results, but this cell-based therapy involves a step of chondrocyte expansion in a monolayer, which results in the loss in the differentiated phenotype. Thus, despite improvement in the quality of life for patients, reconstructed cartilage is in fact fibrocartilage. Successful ACI, according to the particular physiology of chondrocytes in vitro, requires active and phenotypically stabilized chondrocytes. SCOPE OF REVIEW: This review describes the unique physiology of cartilage, with the factors involved in its formation, stabilization and degradation. Then, we focus on some of the most recent advances in cell therapy and tissue engineering that open up interesting perspectives for maintaining or obtaining the chondrogenic character of cells in order to treat cartilage lesions. MAJOR CONCLUSIONS: Current research involves the use of chondrocytes or progenitor stem cells, associated with "smart" biomaterials and growth factors. Other influential factors, such as cell sources, oxygen pressure and mechanical strain are considered, as are recent developments in gene therapy to control the chondrocyte differentiation/dedifferentiation process. GENERAL SIGNIFICANCE: This review provides new information on the mechanisms regulating the state of differentiation of chondrocytes and the chondrogenesis of mesenchymal stem cells that will lead to the development of new restorative cell therapy approaches in humans. This article is part of a Special Issue entitled Matrix-mediated cell behaviour and properties.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Cartilagem Articular / Diferenciação Celular / Condrócitos / Engenharia Tecidual / Matriz Extracelular Limite: Animals / Humans Idioma: En Ano de publicação: 2014 Tipo de documento: Article

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Cartilagem Articular / Diferenciação Celular / Condrócitos / Engenharia Tecidual / Matriz Extracelular Limite: Animals / Humans Idioma: En Ano de publicação: 2014 Tipo de documento: Article