Accéder au contenu
Merck

Improving the safety of human pluripotent stem cell therapies using genome-edited orthogonal safeguards.

Nature communications (2020-06-03)
Renata M Martin, Jonas L Fowler, M Kyle Cromer, Benjamin J Lesch, Ezequiel Ponce, Nobuko Uchida, Toshinobu Nishimura, Matthew H Porteus, Kyle M Loh
RÉSUMÉ

Despite their rapidly-expanding therapeutic potential, human pluripotent stem cell (hPSC)-derived cell therapies continue to have serious safety risks. Transplantation of hPSC-derived cell populations into preclinical models has generated teratomas (tumors arising from undifferentiated hPSCs), unwanted tissues, and other types of adverse events. Mitigating these risks is important to increase the safety of such therapies. Here we use genome editing to engineer a general platform to improve the safety of future hPSC-derived cell transplantation therapies. Specifically, we develop hPSC lines bearing two drug-inducible safeguards, which have distinct functionalities and address separate safety concerns. In vitro administration of one small molecule depletes undifferentiated hPSCs >106-fold, thus preventing teratoma formation in vivo. Administration of a second small molecule kills all hPSC-derived cell-types, thus providing an option to eliminate the entire hPSC-derived cell product in vivo if adverse events arise. These orthogonal safety switches address major safety concerns with pluripotent cell-derived therapies.

MATÉRIAUX
Référence du produit
Marque
Description du produit

Roche
Insuline human, recombinant (yeast)
Roche
Transferrin, from human serum