EMBO Molecular Medicine (Jul 2017)

Promoterless gene targeting without nucleases rescues lethality of a Crigler‐Najjar syndrome mouse model

  • Fabiola Porro,
  • Giulia Bortolussi,
  • Adi Barzel,
  • Alessia De Caneva,
  • Alessandra Iaconcig,
  • Simone Vodret,
  • Lorena Zentilin,
  • Mark A Kay,
  • Andrés F Muro

DOI
https://doi.org/10.15252/emmm.201707601
Journal volume & issue
Vol. 9, no. 10
pp. 1346 – 1355

Abstract

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Abstract Crigler‐Najjar syndrome type I (CNSI) is a rare monogenic disease characterized by severe neonatal unconjugated hyperbilirubinemia with a lifelong risk of neurological damage and death. Liver transplantation is the only curative option, which has several limitations and risks. We applied an in vivo gene targeting approach based on the insertion, without the use of nucleases, of a promoterless therapeutic cDNA into the albumin locus of a mouse model reproducing all major features of CNSI. Neonatal transduction with the donor vector resulted in the complete rescue from neonatal lethality, with a therapeutic reduction in plasma bilirubin lasting for at least 12 months, the latest time point analyzed. Mutant mice, which expressed about 5–6% of WT Ugt1a1 levels, showed normal liver histology and motor‐coordination abilities, suggesting no functional liver or brain abnormalities. These results proved that the promoterless gene therapy is applicable for CNSI, providing therapeutic levels of an intracellular ER membrane‐bound enzyme responsible for a lethal liver metabolic disease.

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