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Unité de recherche
INNOSUISSE
Numéro de projet
8793.1;4 LSPP-LS
Titre du projet
Development of epigenetic regulators and vectors for use in stem cells and cell therapies
Titre du projet anglais
Development of epigenetic regulators and vectors for use in stem cells and cell therapies

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 AllemandFrançaisItalienAnglais
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Résumé des résultats (Abstract)
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Textes saisis


CatégorieTexte
Description succincte
(Anglais)
Development of epigenetic regulators and vectors for use in stem cells and cell therapies
Description succincte
(Français)
Development of epigenetic regulators and vectors for use in stem cells and cell therapies
Résumé des résultats (Abstract)
(Anglais)
Expression of recombinant proteins in mammalian cell is limited by gene silencing effects that hinder the development of many gene- or cell-based therapies, especially for human genetic diseases. Notably, the differentiation of stem cells in vivo is often accompanied by the loss of transgene expression. Therefore, the identification of epigenetic regulators that would counteract gene silencing in vivo are urgently needed. We previously identified epigenetic regulators called MARs elements from the human genome using bioinformatics and demonstrated their usefulness to produce recombinant proteins in bioreactors. In this project, we plan to improve gene transfer techniques and to identify small epigenetic regulators that would prevent gene silencing in both undifferentiated cells cultured in vitro and after differentiation in vivo, for cell or tissue therapies.
Résumé des résultats (Abstract)
(Français)
Expression of recombinant proteins in mammalian cell is limited by gene silencing effects that hinder the development of many gene- or cell-based therapies, especially for human genetic diseases. Notably, the differentiation of stem cells in vivo is often accompanied by the loss of transgene expression. Therefore, the identification of epigenetic regulators that would counteract gene silencing in vivo are urgently needed. We previously identified epigenetic regulators called MARs elements from the human genome using bioinformatics and demonstrated their usefulness to produce recombinant proteins in bioreactors. In this project, we plan to improve gene transfer techniques and to identify small epigenetic regulators that would prevent gene silencing in both undifferentiated cells cultured in vitro and after differentiation in vivo, for cell or tissue therapies.