PLoS ONE (Jan 2013)

AAV-mediated gene therapy for choroideremia: preclinical studies in personalized models.

  • Vidyullatha Vasireddy,
  • Jason A Mills,
  • Rajashekhar Gaddameedi,
  • Etiena Basner-Tschakarjan,
  • Monika Kohnke,
  • Aaron D Black,
  • Krill Alexandrov,
  • Shangzhen Zhou,
  • Albert M Maguire,
  • Daniel C Chung,
  • Helen Mac,
  • Lisa Sullivan,
  • Paul Gadue,
  • Jeannette L Bennicelli,
  • Deborah L French,
  • Jean Bennett

DOI
https://doi.org/10.1371/journal.pone.0061396
Journal volume & issue
Vol. 8, no. 5
p. e61396

Abstract

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Choroideremia (CHM) is an X- linked retinal degeneration that is symptomatic in the 1(st) or 2(nd) decade of life causing nyctalopia and loss of peripheral vision. The disease progresses through mid-life, when most patients become blind. CHM is a favorable target for gene augmentation therapy, as the disease is due to loss of function of a protein necessary for retinal cell health, Rab Escort Protein 1 (REP1).The CHM cDNA can be packaged in recombinant adeno-associated virus (rAAV), which has an established track record in human gene therapy studies, and, in addition, there are sensitive and quantitative assays to document REP1 activity. An animal model that accurately reflects the human condition is not available. In this study, we tested the ability to restore REP1 function in personalized in vitro models of CHM: lymphoblasts and induced pluripotent stems cells (iPSCs) from human patients. The initial step of evaluating safety of the treatment was carried out by evaluating for acute retinal histopathologic effects in normal-sighted mice and no obvious toxicity was identified. Delivery of the CHM cDNA to affected cells restores REP1 enzymatic activity and also restores proper protein trafficking. The gene transfer is efficient and the preliminary safety data are encouraging. These studies pave the way for a human clinical trial of gene therapy for CHM.