Nature Communications (Nov 2024)

Base-editing corrects metabolic abnormalities in a humanized mouse model for glycogen storage disease type-Ia

  • Irina Arnaoutova,
  • Yvonne Aratyn-Schaus,
  • Lisa Zhang,
  • Michael S. Packer,
  • Hung-Dar Chen,
  • Cheol Lee,
  • Sudeep Gautam,
  • Francine M. Gregoire,
  • Dominique Leboeuf,
  • Steven Boule,
  • Thomas P. Fernandez,
  • Victoria Huang,
  • Lo-I Cheng,
  • Genesis Lung,
  • Brianna Bannister,
  • Jeremy Decker,
  • Thomas Leete,
  • Lan S. Shuang,
  • Caroline Bock,
  • Prachi Kothiyal,
  • Phil Grayson,
  • Ka W. Mok,
  • Jeffrey J. Quinn,
  • Lauren Young,
  • Luis Barrera,
  • Giuseppe Ciaramella,
  • Brian C. Mansfield,
  • Janice Y. Chou

DOI
https://doi.org/10.1038/s41467-024-54108-1
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 18

Abstract

Read online

Abstract Glycogen storage disease type-Ia patients, deficient in the G6PC1 gene encoding glucose-6-phosphatase-α, lack blood glucose control, resulting in life-threatening hypoglycemia. Here we show our humanized mouse model, huR83C, carrying the pathogenic G6PC1-R83C variant displays the phenotype of glycogen storage disease type-Ia and dies prematurely. We evaluate the efficacy of BEAM-301, a formulation of lipid nanoparticles containing a newly-engineered adenine base editor, to correct the G6PC1-R83C variant in huR83C mice and monitor phenotypic correction through one year. BEAM-301 can correct up to ~60% of the G6PC1-R83C variant in liver cells, restores blood glucose control, improves metabolic abnormalities of the disease, and confers long-term survival to the mice. Interestingly, just ~10% base correction is therapeutic. The durable pharmacological efficacy of base editing in huR83C mice supports the development of BEAM-301 as a potential therapeutic for homozygous and compound heterozygous glycogen storage disease type-Ia patients carrying the G6PC1-R83C variant.