In vivo Base Editing of a Pathogenic Eif2b5 Variant Improves Vanishing White Matter Phenotypes in Mice

Overview

Journal Mol Ther

Publisher Cell Press

Specialties Molecular Biology
Pharmacology

Date 2024 Mar 8

PMID 38454603

Authors

Desiree Bock

Ilma M Revers

Anastasia S J Bomhof

Anne E J Hillen

Claire Boeijink

Lucas Kissling

Sabina Egli

Miguel A Moreno-Mateos

Marjo S van der Knaap

Niek P van Til

Gerald Schwank

Affiliations

Soon will be listed here.

Abstract

Vanishing white matter (VWM) is a fatal leukodystrophy caused by recessive mutations in subunits of the eukaryotic translation initiation factor 2B. Currently, there are no effective therapies for VWM. Here, we assessed the potential of adenine base editing to correct human pathogenic VWM variants in mouse models. Using adeno-associated viral vectors, we delivered intein-split adenine base editors into the cerebral ventricles of newborn VWM mice, resulting in 45.9% ± 5.9% correction of the Eif2b5 variant in the cortex. Treatment slightly increased mature astrocyte populations and partially recovered the integrated stress response (ISR) in female VWM animals. This led to notable improvements in bodyweight and grip strength in females; however, locomotor disabilities were not rescued. Further molecular analyses suggest that more precise editing (i.e., lower rates of bystander editing) as well as more efficient delivery of the base editors to deep brain regions and oligodendrocytes would have been required for a broader phenotypic rescue. Our study emphasizes the potential, but also identifies limitations, of current in vivo base-editing approaches for the treatment of VWM or other leukodystrophies.

Citing Articles

Ovarioleukodystrophy Due to EIF2B Genes: Systematic Review and Case Report.

Escobar-Pacheco M, Luna-Alvarez M, Davila-Ortiz de Montellano D, Yescas-Gomez P, Ramirez-Garcia M Cureus. 2024; 16(7):e64497.

PMID: 39139316 PMC: 11319890. DOI: 10.7759/cureus.64497.

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