Exploring the relationship between 24‐2 visual field and widefield optical coherence tomography data across healthy, glaucoma suspect and glaucoma eyes

Author:

Tong Janelle123ORCID,Phu Jack12345ORCID,Alonso‐Caneiro David67,Kugelman Jason7,Khuu Sieu2,Agar Ashish8,Coroneo Minas8,Kalloniatis Michael23ORCID

Affiliation:

1. Centre for Eye Health University of New South Wales Sydney New South Wales Australia

2. School of Optometry and Vision Science University of New South Wales Sydney New South Wales Australia

3. School of Medicine (Optometry) Deakin University Waurn Ponds Victoria Australia

4. Faculty of Medicine University of Sydney Sydney New South Wales Australia

5. Concord Clinical School Concord Repatriation General Hospital Sydney New South Wales Australia

6. School of Science, Technology and Engineering University of Sunshine Coast Sunshine Coast Queensland Australia

7. Contact Lens and Visual Optics Laboratory, Centre for Vision and Eye Research, School of Optometry and Vision Science Queensland University of Technology Kelvin Grove Queensland Australia

8. Department of Ophthalmology University of New South Wales at Prince of Wales Hospital Sydney New South Wales Australia

Abstract

AbstractPurposeTo utilise ganglion cell‐inner plexiform layer (GCIPL) measurements acquired using widefield optical coherence tomography (OCT) scans spanning 55° × 45° to explore the link between co‐localised structural parameters and clinical visual field (VF) data.MethodsWidefield OCT scans acquired from 311 healthy, 268 glaucoma suspect and 269 glaucoma eyes were segmented to generate GCIPL thickness measurements. Estimated ganglion cell (GC) counts, calculated from GCIPL measurements, were plotted against 24‐2 SITA Faster visual field (VF) thresholds, and regression models were computed with data categorised by diagnosis and VF status. Classification of locations as VF defective or non‐defective using GCIPL parameters computed across eccentricity‐ and hemifield‐dependent clusters was assessed by analysing areas under receiver operating characteristic curves (AUROCCs). Sensitivities and specificities were calculated per diagnostic category.ResultsSegmented linear regression models between GC counts and VF thresholds demonstrated higher variability in VF defective locations relative to non‐defective locations (mean absolute error 6.10–9.93 dB and 1.43–1.91 dB, respectively). AUROCCs from cluster‐wide GCIPL parameters were similar across methods centrally (p = 0.06–0.84) but significantly greater peripherally, especially when considering classification of more central locations (p < 0.0001). Across diagnoses, cluster‐wide GCIPL parameters demonstrated variable sensitivities and specificities (0.36–0.93 and 0.65–0.98, respectively), with the highest specificities observed across healthy eyes (0.73–0.98).ConclusionsQuantitative prediction of VF thresholds from widefield OCT is affected by high variability at VF defective locations. Prediction of VF status based on cluster‐wide GCIPL parameters from widefield OCT could become useful to aid clinical decision‐making in appropriately targeting VF assessments.

Funder

National Health and Medical Research Council

Publisher

Wiley

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