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Modeling Retinal Degeneration Using Patient-Specific Induced Pluripotent Stem Cells

Figure 1

iPS cells derived from RP patients.

Mutations identified in patients K21 (RP1) (A), K11 and K10 (RP9) (B), P101 (PRPH2) (C), and P59 (RHO) (D). Patient-derived fibroblast cells (E) were reprogrammed into iPS cells (F). The iPS cells expressed SSEA-4 (G) and Nanog (H). A teratoma formation test confirmed iPS cells' ability to generate all three germ layers: endoderm (I), mesoderm (J) and ectoderm (K). Karyotype analysis (I). Scale bars, 50 µm.

Figure 1

doi: https://doi.org/10.1371/journal.pone.0017084.g001