EMBO Molecular Medicine (Mar 2024)

Fine-tuning FAM161A gene augmentation therapy to restore retinal function

  • Yvan Arsenijevic,
  • Ning Chang,
  • Olivier Mercey,
  • Younes El Fersioui,
  • Hanna Koskiniemi-Kuendig,
  • Caroline Joubert,
  • Alexis-Pierre Bemelmans,
  • Carlo Rivolta,
  • Eyal Banin,
  • Dror Sharon,
  • Paul Guichard,
  • Virginie Hamel,
  • Corinne Kostic

DOI
https://doi.org/10.1038/s44321-024-00053-x
Journal volume & issue
Vol. 16, no. 4
pp. 805 – 822

Abstract

Read online

Abstract For 15 years, gene therapy has been viewed as a beacon of hope for inherited retinal diseases. Many preclinical investigations have centered around vectors with maximal gene expression capabilities, yet despite efficient gene transfer, minimal physiological improvements have been observed in various ciliopathies. Retinitis pigmentosa-type 28 (RP28) is the consequence of bi-allelic null mutations in the FAM161A, an essential protein for the structure of the photoreceptor connecting cilium (CC). In its absence, cilia become disorganized, leading to outer segment collapses and vision impairment. Within the human retina, FAM161A has two isoforms: the long one with exon 4, and the short one without it. To restore CC in Fam161a-deficient mice shortly after the onset of cilium disorganization, we compared AAV vectors with varying promoter activities, doses, and human isoforms. While all vectors improved cell survival, only the combination of both isoforms using the weak FCBR1-F0.4 promoter enabled precise FAM161A expression in the CC and enhanced retinal function. Our investigation into FAM161A gene replacement for RP28 emphasizes the importance of precise therapeutic gene regulation, appropriate vector dosing, and delivery of both isoforms. This precision is pivotal for secure gene therapy involving structural proteins like FAM161A.

Keywords