Visual outcome of treating proliferative sickle cell retinopathy in 108 eyes

Author:

Okonkwo Ogugua Ndubuisi123ORCID,Hassan Adekunle Olubola123,Oyekunle Idris2,Akanbi Toyin3,Agweye Chineze4

Affiliation:

1. Department of Ophthalmology, Eye Foundation Retina Institute, Lagos, Nigeria

2. Department of Ophthalmology, Eye Foundation Hospital, Lagos, Nigeria

3. Department of Ophthalmology, Eye Foundation Hospital, Abuja, Nigeria

4. Ophthalmology Department, University of Calabar Teaching Hospital, Cross River, Nigeria

Abstract

Aim To report treatment methods and visual outcome of treating proliferative sickle cell retinopathy (PSCR). Design Retrospective interventional. Methods Review of PSCR eyes treated between 2017 to 2022. Patient demographics, fundus findings at presentation, genotype, PSCR stage, treatment used, and visual outcome were assessed. Results 108 eyes of 88 consecutive patients were studied. Male: Female 48:40. Mean age: 38.91 (SD:12.52) years. Genotype: sickle cell haemoglobin C (SC) 83 eyes (76.9%), sickle cell haemoglobin S (SS) 19 eyes (17.6%), and sickle cell trait (AS) 6 eyes (5.5%). PSCR stages: 3: 15 eyes (11.0%), 4: 74 eyes (67.0%), and 5: 19 eyes (22.0%). Treatment methods: Intravitreal Injection (IVI) of anti-vascular endothelial growth factor (VEGF) only (27 eyes,25%), scatter retinal laser photocoagulation (SRLP) only (7 eyes, 6.5%), Vitrectomy + SRLP (29 eyes, 26.9%), IVI + SRLP (25 eyes, 23.1%), and Vitrectomy + IVI + SRLP (20 eyes, 18.5%). The treatment used correlated with PSCR stage (p = 0.000). IVI only was mostly used to treat stage 4 (81.4%), and SRLP only was used for stages 3 (42.9%) and 5 (57.1%). IVI + SRLP treated eyes had the best pre- and post-treatment vision. Vitrectomy + SRLP treated eyes had the most improved vision. SRLP only had least visual improvement. Fundus findings correlated with visual outcome (p = 0.003); but stage of PSCR, genotype and treatment used had no correlation (P > 0.05). Conclusion Several options effectively treat PSCR. Visual outcome improved or remained same in 90.7% of treated eyes. Randomized controlled trials will determine the optimum treatment for each distinct presentation of PSCR. Treatment guidelines and a disease classification system of prognostic value are unmet needs.

Publisher

SAGE Publications

Subject

Ophthalmology,General Medicine

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