Stem Cell Research (May 2017)

Patient-specific induced pluripotent stem cells to evaluate the pathophysiology of TRNT1-associated Retinitis pigmentosa

  • Tasneem P. Sharma,
  • Luke A. Wiley,
  • S. Scott Whitmore,
  • Kristin R. Anfinson,
  • Cathryn M. Cranston,
  • Douglas J. Oppedal,
  • Heather T. Daggett,
  • Robert F. Mullins,
  • Budd A. Tucker,
  • Edwin M. Stone

DOI
https://doi.org/10.1016/j.scr.2017.03.005
Journal volume & issue
Vol. 21, no. C
pp. 58 – 70

Abstract

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Retinitis pigmentosa (RP) is a heterogeneous group of monogenic disorders characterized by progressive death of the light-sensing photoreceptor cells of the outer neural retina. We recently identified novel hypomorphic mutations in the tRNA Nucleotidyl Transferase, CCA-Adding 1 (TRNT1) gene that cause early-onset RP. To model this disease in vitro, we generated patient-specific iPSCs and iPSC-derived retinal organoids from dermal fibroblasts of patients with molecularly confirmed TRNT1-associated RP. Pluripotency was confirmed using rt-PCR, immunocytochemistry, and a TaqMan Scorecard Assay. Mutations in TRNT1 caused reduced levels of full-length TRNT1 protein and expression of a truncated smaller protein in both patient-specific iPSCs and iPSC-derived retinal organoids. Patient-specific iPSCs and iPSC-derived retinal organoids exhibited a deficit in autophagy, as evidenced by aberrant accumulation of LC3-II and elevated levels of oxidative stress. Autologous stem cell-based disease modeling will provide a platform for testing multiple avenues of treatment in patients suffering from TRNT1-associated RP.

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