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Full-Field Pupillary Light Responses, Luminance Thresholds, and Light Discomfort Thresholds in CEP290 Leber Congenital Amaurosis Patients.

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posted on 2016-06-14, 00:00 authored by FT Collison, JC Park, GA Fishman, JJ McAnany, EM Stone
PURPOSE: To investigate visual function in patients with CEP290 Leber congenital amaurosis (LCA-CEP290), using three full-field tests that can be performed by patients with poor fixation. METHODS: Six patients (age range, 9-39 years) with LCA-CEP290 participated in the study. Stimuli for all three tests (full-field stimulus test [FST], pupillometry, and light discomfort threshold [LDT] testing) were generated by the Diagnosys ColorDome ganzfeld, by using achromatic stimuli as well as long- and short-wavelength stimuli to target rod and cone photoreceptors with all three tests and, in the latter two tests, melanopsin photoreceptors. RESULTS: Dark-adapted FST thresholds in LCA-CEP290 patients were cone mediated and elevated between 4.8 and 6.2 log units above the normal achromatic threshold. The FST threshold was not measurable in one patient. The rod-mediated transient pupillary light reflex (PLR) was absent in all but the youngest patient, where unreliable responses precluded PLR quantification. Cone-mediated transient PLRs were subnormal in five patients, and absent in another. Sustained melanopsin-mediated PLRs were measurable in all patients. Full-field LDT thresholds were elevated compared to normal controls, and were lower for short-wavelengh than for long-wavelength stimuli. CONCLUSIONS: The FST thresholds and transient PLRs were cone mediated in our cohort LCA-CEP290 patients. Rod-mediated PLRs were undetectable, whereas melanopsin-mediated sustained responses were detected in all patients, suggesting a relative preservation of inner-retina function. The LDT elevations for the patients are somewhat paradoxical, given their subjective perception of photoaversion. Relative aversion to short-wavelength light suggests influence from melanopsin on LDTs in these patients.

Funding

Supported by The Grousbeck Family Foundation, Boston, Massachusetts (EMS and GAF); The Pangere Family Foundation, Gary, Indiana (GAF); National Institutes of Health Research Grants EY019510 (JJM) and EY001792 (University of Illinois at Chicago core grant) and an unrestricted departmental grant from Research to Prevent Blindness

History

Publisher Statement

This is a copy of an article published in Investigative Ophthalmology & Visual Science. © 2015 Association for Research in Vision and Ophthalmology Inc.

Publisher

Association for Research in Vision and Ophthalmology

Language

  • en_US

issn

0146-0404

Issue date

2015-11-01

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