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Clinically translatable mitochondrial gene therapy in muscle using tandem mtZFN architecture.

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Peer-reviewed

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https://www.repository.cam.ac.uk/handle/1810/385544

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Article

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Authors

Powell, Christopher A  ORCID logo  https://orcid.org/0000-0001-7501-0586
Van Haute, Lindsey  ORCID logo  https://orcid.org/0000-0001-7809-1473

Abstract

Mutations in the mitochondrial genome (mtDNA) often lead to clinical pathologies. Mitochondrially-targeted zinc finger nucleases (mtZFNs) have been successful in reducing the levels of mutation-bearing mtDNA both in vivo and in vitro, resulting in a shift in the genetic makeup of affected mitochondria and subsequently to phenotypic rescue. Given the uneven distribution in the mtDNA mutation load across tissues in patients, and a great diversity in pathogenic mutations, it is of interest to develop mutation-specific, selective gene therapies that could be delivered to particular tissues. This study demonstrates the effectiveness of in vivo mitochondrial gene therapy using a novel mtZFN architecture on skeletal muscle using adeno-associated viral (AAV) platforms in a murine model harboring a pathogenic mtDNA mutation. We observed effective reduction in mutation load of cardiac and skeletal muscle, which was accompanied by molecular phenotypic rescue. The gene therapy treatment was shown to be safe when markers of immunity and inflammation were assessed. These results highlight the potential of curative approaches for mitochondrial diseases, paving the way for targeted and effective treatments.

Description

Acknowledgements: This research has been unded by UKRI Medical Research Council grants MC_UU_00015/4 and MC_UU_00028/3 (PAN, KMT, CAP, LVH, PS-P, PAG, and MM), UKRI MRC award MC_PC_21046 to the National Mouse Genetics Network Mitochondria Cluster (MitoCluster) (PAN, PS-P, KMT, CAP, LVH, and MM), The Lily Foundation (PAN), The Champ Foundation (PS-P), CRUK SI Core Funding A31287 (PAG), A_BICR_1920_Gammage (PAG). We acknowledge the significant contribution to model development made by Dr. James B. Stewart (Newcastle University, UK) and Prof. Nils-Goran Larsson (Karolinska Institute, Stockholm, Sweden), which was essential to this work. We are grateful to the personnel at Phenomics Animal Care Facility and The Anne McLaren Building for their technical support in managing the mouse colonies. We are grateful to Martin Rice, Phenomics Animal Care Facility, Cambridge, for technical assistance with viral administration. The FACS experiments were performed by the CIMR Flow facility to whom we are very grateful.


Funder: The Lily Foundation


Funder: Champ Foundation (The Champ Foundation); doi: http://dx.doi.org/10.13039/100016422


Funder: A_BICR_1920_Gammage

Keywords

Adeno-Associated Viruses (AAV), Gene Therapy, Skeletal Muscle, Zinc Finger Nuclease (mtZFN), mtDNA Heteroplasmy Modification, Genetic Therapy, Animals, Muscle, Skeletal, Dependovirus, Mice, DNA, Mitochondrial, Zinc Finger Nucleases, Mitochondrial Diseases, Disease Models, Animal, Genetic Vectors, Mitochondria, Humans, Mutation

Journal Title

EMBO Mol Med

Conference Name

Journal ISSN

1757-4676
1757-4684

Volume Title

17

Publisher

Springer Nature

Publisher DOI

https://doi.org/10.1038/s44321-025-00231-5

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Except where otherwised noted, this item's license is described as http://creativecommons.org/licenses/by/4.0/
Sponsorship
Medical Research Council (MC_UU_00015/7)
MRC (MC_UU_00028/3)
MRC (via University College London (UCL)) (MC_PC_21046)

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