TRANSPLANTATION OF SUBRETINAL STEM CELL–DERIVED RETINAL PIGMENT EPITHELIUM FOR STARGARDT DISEASE

视网膜色素上皮 超声乳化术 医学 眼科 视网膜 视网膜 干细胞 移植 玻璃体切除术 视力 视网膜脱离 外科 生物 遗传学 神经科学
作者
Rodrigo Brant,Fernando H. Lojudice,Lucas Zago Ribeiro,Natasha Ferreira Santos da Cruz,Murilo Ubukata Polizelli,Priscila Cardoso Cristovam,Francesco Innocenti,Lisângela Morimoto,Octaviano Magalhães,Juliana Maria Ferraz Sallum,Fernando M. Penha,Mari Cleide Sogayar,Rubens Belfort,Maurício Maia
出处
期刊:Retina-the Journal of Retinal and Vitreous Diseases [Ovid Technologies (Wolters Kluwer)]
卷期号:43 (2): 263-274 被引量:22
标识
DOI:10.1097/iae.0000000000003655
摘要

To assess the safety of injecting human embryonic stem cell retinal pigment epithelial cell dose to treat Stargardt disease.In this prospective, Phase I clinical trial, human embryonic stem cell retinal pigment epithelial cells in suspension were injected into the subretinal space in eyes with the worse best-corrected visual acuity (BCVA). After vitrectomy/posterior hyaloid removal, a partial retinal detachment was created and the human embryonic stem cell retinal pigment epithelial cells were administered. Phacoemulsification with intraocular lens implantation was performed in eyes with lens opacity. All procedures were optical coherence tomography-guided. The 12-month follow-up included retinal imaging, optical coherence tomography, visual field/electrophysiologic testing, and systemic evaluation. The main outcome was the absence of ocular/systemic inflammation or rejection, tumor formation, or toxicity during follow-up.The mean baseline BCVAs in the phacoemulsification and no phacoemulsification groups were similar (1.950 ± 0.446 and 1.575 ± 0.303, respectively). One year postoperatively, treated eyes showed a nonsignificant increase in BCVA. No adverse effects occurred during follow-up. Intraoperative optical coherence tomography was important for guiding all procedures.This surgical procedure was feasible and safe without cellular migration, rejection, inflammation, or development of ocular or systemic tumors during follow-up.
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