Gene Therapy for retinal diseases

Our group works on engineering approaches to solve neurodegeneration with a particular focus on the retina.

  • Three axes of research that depend on a new generation of AAV vectors :

1. Engineering the ATPase domain

Modularity has allowed for the evolution of complex multi-functional genes. The same semi-autonomous functional modules emerge across lineages to enable the function of large proteins such as pumps and transporters.

The nucleotide-binding domains of the ATPase unit is just one very abundant example. We are designing a generic module for correction of ATPase-dependent genes.

Our current target of interest is the ATPase-binding cassette transporter (ABCA4), a causal gene in the juvenile maculopathy, Stargardts disease


2. Engineering the retinal glia

In inflammatory diseases such as Age-related macular degeneration (AMD) microglial cells have a largely protective role early on in the disease.

We are engineering these cells to restrict expression of checkpoint regulator chemokine genes so as to keep these cells in a protective state and limit disease progression.

Non-activating, chemically modified vectors and rationally designed promoters are essential for targetting immunomodulatory transgene expression in these cells.

3. Modelling disease states

Rodent models offer enormous insight into the effects of a mutation. However, these models are limited when evaluating therapies targetting the macula, the source of functional human vision. We are using yucatan pig models for AMD research, characterizing end-points that can be used to measure preclinical efficacy of therapeutic candidates.

Our patient retinal organoids  allow us to model visual cycle dyanamics in Stargardts disease research, a juvenile form of macular degeneration (In collaboration with Institut de la vision, Paris) .

The vector

All three axes of research depend on novel AAVs that are both safe and can transduce refractory cell types such as microglia.
Working with the vector innovation group we are testing chemically-modified vectors that broaden the scope of transduction
while shielding the vector from signalling an immune response.

Clinical Proof Of Concept for Gene therapy

The team has extensive experience in the field of translational gene therapy for inherited retinal dystrophies.

In particular, the group has performed preclinical gene therapy P.O.C. for Leber's amaurosis related to RPE65 protein deficiency and PDE6β retinal dystrophy enable development of two Phase I/II clinical trials.

This team has been selected by 

to support one of its research programmes.

Team members

CLINICAL:

Alumni

  • Fabienne Rolling, PhD
  • Baptiste Ameline, PhD
  • Kizito Tshilenge, PhD
  • Nathalie Provost
  • Carolina Isiegas, PhD
  • Alexandra Mendes-Medeira
  • Noémien Maillard, Ms
  • Minja Velimirovic, Ms
  • Ragnar Gautier, Ms
  • Jean-Baptiste Deltour, Ms
  • Betty Dupas, Ms
Mis à jour le 22 May 2024.
https://umr1089.ppksup.univ-nantes.fr/en/research/gene-therapy-for-retinal-diseases