Abstract

The 2-year ophthalmic sequelae of Ebola virus disease (EVD) in survivors of the 2013 to 2016 epidemic is unknown and may have public health implications for future outbreaks. To assess the potential for uveitis recurrence, the behavior of dark without pressure, and visual outcomes in a cohort of Sierra Leonean survivors of EVD 2 years following the 2013 to 2016 Ebola epidemic. Prospective, 1-year observational cohort study performed between 2016 and 2017 at 34 Military Hospital, Freetown, Sierra Leone. Participants included survivors of EVD who reported ocular symptoms since Ebola treatment unit discharge and were participants of a previous case-control study. Participants were invited for ophthalmic reexamination and finger-prick blood sampling for immunoglobulin G (IgG) to Toxoplasma gondii and HIV. Ebola virus disease. Primary outcome measure: comparative ultra-widefield retinal imaging. Secondary outcome measures: visual acuity and detection of IgG to T gondii and HIV. Of 57 survivors of EVD who underwent repeated ophthalmic evaluation, 37 were women (64.9%). Mean (SD) age was 31.9 (11.1) years. Median interval between first and last examination was 370 days (interquartile range [IQR], 365-397.5 days), and median time from discharge to last examination was 779 days (IQR, 732-821 days). Fifteen eyes of 10 survivors (17.5%) had retinal lesions secondary to EVD. No new EVD-associated retinal lesions were observed. Two survivors (3.5%) developed new posterior uveitis resembling toxoplasmosis chorioretinitis and 41 (73%) were seropositive for T gondii IgG. Areas of dark without pressure were observed either confined to the perimeter of Ebola retinal lesions (n = 7) and non-Ebola lesions (n = 2), involving extensive retinal areas adjacent to Ebola retinal lesions (n = 4) and non-Ebola lesions (n = 2) or in isolation (n = 6). Both expansion and regression of areas of dark without pressure were observed over the study period. Best eye-presenting visual acuity had mild or no visual impairment in 55 survivors (96.4%) 2 years following discharge. Vision was maintained in survivors of EVD 2 years following discharge. Evolving regions of dark without pressure may be associated with EVD retinal lesions and might suggest the presence of an ongoing intraretinal stimulus, which may be associated with infective etiology. Treatment strategies should account for the possibility of toxoplasmosis chorioretinitis recurrence within survivors of EVD.

Highlights

  • Two survivors (3.5%) developed new posterior uveitis resembling toxoplasmosis chorioretinitis and 41 (73%) were seropositive for T gondii immunoglobulin G (IgG)

  • Evolving regions of dark without pressure may be associated with Ebola virus disease (EVD) retinal lesions and might suggest the presence of an ongoing intraretinal stimulus, which may be associated with infective etiology

  • Treatment strategies should account for the possibility of toxoplasmosis chorioretinitis recurrence within survivors of EVD

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Summary

Methods

Study Design and Population A prospective, controlled study of survivors of EVD who had attended the EVD survivors clinic at 34 Military Hospital in Freetown, Sierra Leone, or other medical facilities in the region and reported ophthalmic symptoms since discharge was conducted in 2016.5 All participants of this study who attended between January 22, 2016, and April 26, 2016, were contacted by telephone and invited to attend the ophthalmology clinic for review 1 year following their baseline examination. The study was approved by the Sierra Leone Ethics and Scientific Review Committee and followed the tenets set forth by the World Medical Association Declaration of Helsinki, seventh revision (2013). Survivors were invited to participate in English or Krio, as preferred, with local ophthalmic nurses acting as inter-

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