Microperimetry as a diagnostic tool for the detection of early, subclinical retinal damage and visual impairment in multiple sclerosis

Approval for this cross-sectional study was obtained from the Institutional Review Board at the University of Missouri – Kansas City. MS subjects were recruited from neurology and neuro-ophthalmology clinics and an advertisement in the Multiple Sclerosis Society Quarterly newsletter. Age, race, and gender-matched controls were recruited from clinics and flyers. Informed consent for participation was obtained from all subjects.

All testing was performed at the University of Missouri – Kansas City School of Medicine clinical sites in Kansas City, Missouri, USA. Inclusion criteria included age ≥ 18 years, BCVA by Early Treatment Diabetic Retinopathy Study (ETDRS) chart of > 20/25 in the study eye, and intraocular pressure < 21 mmHg. MS patients were required to have been diagnosed by the McDonald criteria [27]. Exclusion criteria included a history of optic neuritis in either eye (verified by medical records, history of suggestive symptoms, or clinical exam showing features of possible optic neuritis), current use of steroids for acute exacerbations, any media opacity affecting retinal sensitivity or preventing capture of good quality scans, diabetes mellitus type 1, uncontrolled diabetes mellitus type II, uncontrolled hypertension, other systemic or neurodegenerative diseases examiner believed may have affected retinal sensitivity or impacted optical coherence tomography (OCT) imaging, evidence of retinopathy or macular pathology, abnormal optic nerve head appearance, any eye that could not be adequately tracked by MP in order to complete the exam, and any eye that could not be adequately scanned to provide sufficient image signal for accurate measurement.

The expected mean for control subjects was determined from a normative database of 19 healthy subjects 40–49 years of age (18.2 ± 1.1 dB) [23]. Since MP has not been measured in MS patients in peer-reviewed studies, the expected mean for MS patients was conservatively predicted at 17.2 ± 1.1 dB. Power was set at 0.80 and α at 0.05. Sample size was calculated at 20 per group using a Cohen’s d of 0.91 [28].

Patients were consecutively enrolled. Informed consent was obtained from all patients involved in the study. Visual acuity assessment was measured via high-contrast ETDRS and low-contrast Sloan 2.5% charts. Color vision was assessed using Hardy-Rand-Rittler plates. Applanation was performed using Goldmann tonometry. These measures were collected in all MS patients.

Pupil dilation was obtained using 1% tropicamide and 2.5% phenylephrine drops prior to fundus examination. Macular sensitivity and macular thickness were assessed in all subjects. MP was performed with Optos spectral-domain optical coherence tomography [SD-OCT]/ SLO with add-on Microperimetry module (SLO/SD-OCT microperimeter; Dunfermline, Scotland, UK). Macular sensitivity was recorded at 28 points organized into 3 circles (Polar 3 pattern) using the Optos Microperimetry software. The points were arranged into a central circle with 4 points within 4 degrees from the foveal center, a middle circle with 12 points within 8 degrees, and an outer circle with 12 points within 12 degrees. The target size was 108 μm (Goldman III) and the stimulus duration was 200 milliseconds with a 2 s interval between stimulus presentations. Threshold sensitivity was established at each point using a 4-dB to 2-dB staircase strategy and sensitivity was expressed on a scale of 0 to 20 dB. Fundus localization was automatically tracked by SLO based on retinal vessel alignment.

Measurements of retinal microarchitecture were determined with the Cirrus HD-OCT spectral-domain OCT (Carl Zeiss Meditec, Dublin, CA). Retinal nerve fiber layer (RNFL) thickness and optic nerve head analyses were determined by scanning the optic disc while macular thickness was determined by obtaining a scan centered on the fovea. Retinal thickness was defined in this study as the distance between the RNFL and the retinal pigment epithelial layer. Each scan was manually examined for accuracy of automated layer designation and was repeated as necessary. Retinal thickness was calculated using the ETDRS grid. The grid has a central circle that measures 1 mm in diameter and is centered on the fovea with concentric inner and outer circles that measure 3 mm and 6 mm in diameter, respectively. Central macular thickness was defined as the average thickness within the central circle while average macular thickness was defined as the average thickness within the entire grid. Average macular thickness as measured by Optos SLO/SD-OCT was used to measure agreement with average macular thickness as assessed by Cirrus HD-OCT. All other correlations were obtained using macular thickness as measured by Cirrus HD-OCT.

Patient data was de-identified prior to analysis. Pearson correlation coefficients were measured using bivariate correlations. A Bland-Altman analysis was used to determine the degree of agreement between average macular thickness measured with Optos SLO/SD-OCT and Cirrus HD-OCT. Sample means, mean differences, and 95% confidence intervals were obtained using independent sample t-tests. Hypothesis tests were 2-sided. Repeated measurements were statistically managed by averaging values from both eyes and nonparametric tests (Mann-Whitney U and Spearman’s correlation) were used to confirm statistical significance and degree of correlation. Receiver-operating-characteristic (ROC) curves were calculated by splitting MS patients into two categorical groups of decreased or normal macular thickness based on previously-established normative average and central macular thickness values [29]. Subjects with below-average values were classified as diseased while subjects with above-average values were classified as without disease. The areas under the ROC curves (AUCs) were calculated and compared with the AUC under the reference line. Analyses were performed with Microsoft Excel Version 16.32 (Microsoft Systems, Redmond, WA) and IBM SPSS Statistics Version 25 (IBM Corp., Armonk, NY).