Frontiers in Genetics (Mar 2023)

Early postnatal administration of an AAV9 gene therapy is safe and efficacious in CLN3 disease

  • Tyler B. Johnson,
  • Tyler B. Johnson,
  • Jon J. Brudvig,
  • Jon J. Brudvig,
  • Shibi Likhite,
  • Melissa A. Pratt,
  • Katherine A. White,
  • Jacob T. Cain,
  • Jacob T. Cain,
  • Clarissa D. Booth,
  • Derek J. Timm,
  • Samantha S. Davis,
  • Brandon Meyerink,
  • Ricardo Pineda,
  • Cassandra Dennys-Rivers,
  • Brian K. Kaspar,
  • Kathrin Meyer,
  • Jill M. Weimer,
  • Jill M. Weimer,
  • Jill M. Weimer

DOI
https://doi.org/10.3389/fgene.2023.1118649
Journal volume & issue
Vol. 14

Abstract

Read online

CLN3 disease, caused by biallelic mutations in the CLN3 gene, is a rare pediatric neurodegenerative disease that has no cure or disease modifying treatment. The development of effective treatments has been hindered by a lack of etiological knowledge, but gene replacement has emerged as a promising therapeutic platform for such disorders. Here, we utilize a mouse model of CLN3 disease to test the safety and efficacy of a cerebrospinal fluid-delivered AAV9 gene therapy with a study design optimized for translatability. In this model, postnatal day one administration of the gene therapy virus resulted in robust expression of human CLN3 throughout the CNS over the 24-month duration of the study. A range of histopathological and behavioral parameters were assayed, with the therapy consistently and persistently rescuing a number of hallmarks of disease while being safe and well-tolerated. Together, the results show great promise for translation of the therapy into the clinic, prompting the launch of a first-in-human clinical trial (NCT03770572).

Keywords