Preclinical lentiviral vector-mediated hematopoietic stem and progenitor cell gene therapy corrects Pompe disease-related muscle and neurological manifestations

Author:

Yoon John K.,Schindler Jeffrey W.,Loperfido Mariana,Baricordi Cristina,DeAndrade Mark P.,Jacobs Mary E.,Treleaven Christopher,Plasschaert Robert N.,Yan Aimin,Barese Cecilia N.,Dogan Yildirim,Chen Vicky Ping,Fiorini Claudia,Hull Fritz,Barbarossa Luigi,Unnisa Zeenath,Ivanov Daniel,Kutner Robert H.,Guda Swaroopa,Oborski Christine,Maiwald Tim,Michaud Véronique,Rothe Michael,Schambach Axel,Pfeifer Richard,Mason Chris,Biasco Luca,van Til Niek P.ORCID

Abstract

AbstractPompe disease, a rare genetic neuromuscular disorder, is caused by a deficiency of acid alpha-glucosidase (GAA), leading to the accumulation of glycogen in lysosomes and the progressive development of muscle weakness. The current standard treatment, enzyme replacement therapy (ERT), is not curative and demonstrates poor penetration into skeletal muscle and the central and peripheral nervous systems, susceptibility to immune responses against the recombinant enzyme, and the need for high doses and frequent infusions. To overcome these limitations, lentiviral vector-mediated hematopoietic stem and progenitor cell (HSPC) gene therapy has been proposed as a next-generation approach for treating Pompe disease. This study demonstrates the potential of lentiviral HSPC gene therapy to reverse the pathological effects of Pompe disease in a preclinical mouse model. It includes a comprehensive safety assessment via integration site analysis, along with single-cell RNA sequencing analysis of CNS samples to gain insights into the underlying mechanisms of phenotype correction.One Sentence Summary:Preclinical hematopoietic stem cell gene therapy for the treatment of Pompe disease.

Publisher

Cold Spring Harbor Laboratory

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