In vivo haemopoietic stem cell gene therapy enabled by postnatal trafficking.

出生后造血干细胞转运促进体内造血干细胞基因治疗

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作者:Milani Michela, Fabiano Anna, Perez-Rodriguez Marta, Hernandez Raisa Jofra, Zecchillo Alessandra, Zonari Erika, Ottonello Sofia, Basso-Ricci Luca, Canepari Cesare, Volpin Monica, Iannello Valeria, Capo Valentina, Quaranta Pamela, Seffin Luca, Russo Fabio, Biffi Mauro, Ormoli Leonardo, Brombin Chiara, Carlucci Filippo, Forlino Antonella, Filibian Marta, Montini Eugenio, Scala Serena, Villa Anna, Bueren Juan Antonio, Rio Paula, Aiuti Alessandro, Cantore Alessio, Naldini Luigi
Lentiviral vector (LV)-mediated ex vivo gene therapy for haematopoietic stem and progenitor cells (HSPCs) has delivered on the promise of a 'one-and-done' treatment for several genetic diseases(1). However, ex vivo manipulation and patient conditioning before transplantation are major hurdles that could be overcome by an in vivo approach. Here we demonstrate that in vivo gene delivery to HSPCs after systemic LV administration is enabled by the substantial trafficking of these cells from the liver to the bone marrow in newborn mice. We improved gene-transfer efficiency using a phagocytosis-shielded LV, successfully reaching bona fide HSPCs capable of long-term multilineage output and engraftment after serial transplantation, as confirmed by clonal tracking. HSPC mobilization further increased gene transfer, extending the window of intervention, although permissiveness to LV transduction declined with age. We successfully tested this in vivo strategy in mouse models of adenosine deaminase deficiency, autosomal recessive osteopetrosis and Fanconi anaemia. Interestingly, in vivo gene transfer provided a selective advantage to corrected HSPCs in Fanconi anaemia, leading to near-complete haematopoietic reconstitution and prevention of bone marrow failure. Given that circulating HSPCs in humans are also most abundant shortly after birth, in vivo HSPC gene transfer holds strong translational potential across multiple diseases.

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