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A versatile laser-induced porcine model of outer retinal and choroidal degeneration for preclinical testing
Francesca Barone, Juan Amaral, Irina Bunea, Mitra Farnoodian, Rohan Gupta, Rishabh Gupta, Dara Baker, M. Joseph Phillips, Richard J. Blanch, Arvydas Maminishkis, David M. Gamm, Kapil Bharti
Francesca Barone, Juan Amaral, Irina Bunea, Mitra Farnoodian, Rohan Gupta, Rishabh Gupta, Dara Baker, M. Joseph Phillips, Richard J. Blanch, Arvydas Maminishkis, David M. Gamm, Kapil Bharti
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Resource and Technical Advance Ophthalmology Stem cells

A versatile laser-induced porcine model of outer retinal and choroidal degeneration for preclinical testing

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Abstract

Over 30 million people worldwide suffer from untreatable vision loss and blindness associated with childhood-onset and age-related eye diseases caused by photoreceptor (PR), retinal pigment epithelium (RPE), and choriocapillaris (CC) degeneration. Recent work suggests that RPE-based cell therapy may slow down vision loss in late stages of age-related macular degeneration (AMD), a polygenic disease induced by RPE atrophy. However, accelerated development of effective cell therapies is hampered by the lack of large-animal models that allow testing safety and efficacy of clinical doses covering the human macula (20 mm2). We developed a versatile pig model to mimic different types and stages of retinal degeneration. Using an adjustable power micropulse laser, we generated varying degrees of RPE, PR, and CC damage and confirmed the damage by longitudinal analysis of clinically relevant outcomes, including analyses by adaptive optics and optical coherence tomography/angiography, along with automated image analysis. By imparting a tunable yet targeted damage to the porcine CC and visual streak — with a structure similar to the human macula — this model is optimal for testing cell and gene therapies for outer retinal diseases including AMD, retinitis pigmentosa, Stargardt, and choroideremia. The amenability of this model to clinically relevant imaging outcomes will facilitate faster translation to patients.

Authors

Francesca Barone, Juan Amaral, Irina Bunea, Mitra Farnoodian, Rohan Gupta, Rishabh Gupta, Dara Baker, M. Joseph Phillips, Richard J. Blanch, Arvydas Maminishkis, David M. Gamm, Kapil Bharti

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Figure 3

OCTA segmentation of choriocapillaris.

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OCTA segmentation of choriocapillaris.
(A–C) Simultaneous evaluation of ...
(A–C) Simultaneous evaluation of 2 weeks 1% DC laser lesion (A) by ICGA (B) and OCTA (C). (D and E) Serial OCTA scans are projected as pseudo-color yellow signal; blue arrowhead shows margin of choriocapillaris as a continuous yellow signal. (E) OCTA signal was segmented into the retinal capillaries, choriocapillaris (CC), and choroid vasculature (red dotted lines); IZ/RPE layer was used as a landmark to define retinal from CC vasculature. (F–K) The choriocapillaris signal was represented in C-scan (en face) OCTA images of 1% duty cycle laser lesion (F–H) and 1.5% duty cycle laser lesion (I–K) shown at 2-, 6-, and 12 weeks past the laser lesion. (L) The graph depicts the pixel gray value changes in percent in CC density from baseline to 12 weeks as seen in en face images. Box and whiskers represent minimum to maximum, 25th and 75th percentile, median, and single values. Data were analyzed with mixed-effect model (REML) and Bonferroni multiple-comparison test. n = 13, 7, 4, 4, 4, 4 eyes for 1% DC at baseline, 2 weeks, 4 weeks, 6 weeks, 8 weeks, and 12 weeks, respectively; n = 13, 10, 10, 4, 4, 4 for 1.5% DC at baseline, 2 weeks, 4 weeks, 8 weeks, and 12 weeks, respectively. P values are reported as *P < 0.05; **P < 0.005; ***P < 0.0005; ****P < 0.0001. Scale bars: 500 μm

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