SPOT: Scotoma Perimetry Oculomotor Training

Sponsor

University of Alabama at Birmingham (Other)

Overall Status

Recruiting

CT.gov ID

NCT05456581

Collaborator

University of California, Riverside (Other)

Enrollment

Location

Arms

Anticipated Duration (Months)

1.1

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The proposed research is relevant to public health because a greater understanding of plasticity after central vision loss can inform new therapies for treating low vision and has potential to benefit millions of individuals suffering from low vision. The treatment of low vision is particularly relevant to the mission of the NEI to support research on visual disorders, mechanisms of visual function and preservation of sight.

Declines in vision are particularly common in older adults and thus increasing our understanding of how to cre- ate effective means of improving vision is also highly relevant to the mission of the NIA to support research on aging and the health and well-being of older people.

Condition or Disease	Intervention/Treatment	Phase
Macular Degeneration Central Visual Impairment	Behavioral: 'Scotoma awareness' Training Behavioral: Control Training	N/A

Detailed Description

This proposal tests a novel 'scotoma awareness' approach to aid those with Macular Degeneration (MD). MD is the leading cause of central vision loss worldwide. MD patients spontaneously develop oculomotor strategies to overcome loss of central vision, such as developing a new peripheral fixation spot to replace the fovea (preferred retinal locus, or PRL). However, development of a PRL and the rate of success in developing one vary greatly, meaning some patients live years without making effective use of their spared vision. Recent, studies in Vision Science show that training healthy participants with gaze-contingent displays, obstructing central vision ('simulated scotoma'), leads to development of PRLs at a faster time scale than found for MD patients. Additionally, oculomotor metrics developed in our lab, are effective in characterizing individual eye movement patterns in simulated scotoma participants. The ability to describe differences in compensatory strategies in MD represents a crucial step towards individualized rehabilitative strategies, which could be further improved by accelerating PRL development. However, it is unclear whether these results can be reproduced in those with MD. It has been suggested that the visible, sharp-edged occluder in the gaze- contingent displays increases scotoma awareness, thus accelerating PRL development. Many MD patients are unaware of the location of their scotoma, with some persisting to use their damaged fovea as a fixation spot. No study to date has translated the use of a simulated scotoma to promote rapid PRL development in MD patients. As a first step towards addressing individual differences in patients and examine whether Vision Science paradigms can be used as a rehabilitative tool in MD, we propose two Aims: In Aim 1 we will use a set of oculomotor metrics to characterize individual profiles of compensation. In Aim 2 we will test the effectiveness of the visible, simulated scotoma as a technique to promote the rapid development of a PRL. Patients will undergo a 'scotoma awareness' training, in which a simulated scotoma, individually tailored for each patient, will be used to help them visualize their region of vision loss. Patients will be tested on the same metrics from Aim 1 and a battery of visual and cognitive assessments before and after the 'scotoma awareness' (or control) sessions. This will enable quantification of the effect of scotoma awareness both in terms of visual abilities and oculomotor strategies, and test the hypothesis that awareness of the location and extent of retinal damage promotes fast PRL development. While challenging, the use of eye tracking techniques in patients could be highly rewarding if this scotoma awareness procedure proves to be effective. A null result would be equally informative, suggesting fundamental differences between physiological and simulated scotomas, thus providing a limit in the use of simulations of retinal damage as a framework for the study of retinal pathologies such as MD. This will provide a unique data set to help those developing interventions for central vision loss understand how approaches to visual rehabilitation, and individual differences, give rise to training outcomes.

Study Design

Study Type:

Interventional

Anticipated Enrollment :

16 participants

Allocation:

Randomized

Intervention Model:

Parallel Assignment

Masking:

Single (Outcomes Assessor)

Primary Purpose:

Basic Science

Official Title:

New Methods to Quantify and Train Eye Movement Strategies in Macular Degeneration

Anticipated Study Start Date :

Sep 1, 2022

Anticipated Primary Completion Date :

Sep 1, 2023

Anticipated Study Completion Date :

Nov 1, 2023

Arms and Interventions

Arm	Intervention/Treatment
Experimental: Condition 1 - 'Scotoma awareness' Training Participants will be asked to report the emotion of an emoji face ('happy' vs 'sad') that could appear anywhere on screen. For the entire duration of the training, an explicit, sharp outlined occluder surrounding the participant's true retinal scotoma will be rendered on screen. This occluder will be generated through a gaze-contingent display. The size and the contrast of the target will change adaptively in response to the patient's performance.	Behavioral: 'Scotoma awareness' Training In the 'scotoma awareness' training, patients will perform visual search and orientation discrimination tasks while an opaque occluder, custom-tailored to overlap each patient's retinal scotoma, is constantly presented on the computer screen.
Experimental: Condition 2 - Control Training In the control condition, participants will perform the same task as the scotoma awareness training, without the artificial visible scotoma.	Behavioral: Control Training The task will be performed in the control group without the visible scotoma.

Arm

Intervention/Treatment

Experimental: Condition 1 - 'Scotoma awareness' Training

Participants will be asked to report the emotion of an emoji face ('happy' vs 'sad') that could appear anywhere on screen. For the entire duration of the training, an explicit, sharp outlined occluder surrounding the participant's true retinal scotoma will be rendered on screen. This occluder will be generated through a gaze-contingent display. The size and the contrast of the target will change adaptively in response to the patient's performance.

Behavioral: 'Scotoma awareness' Training

In the 'scotoma awareness' training, patients will perform visual search and orientation discrimination tasks while an opaque occluder, custom-tailored to overlap each patient's retinal scotoma, is constantly presented on the computer screen.

Experimental: Condition 2 - Control Training

In the control condition, participants will perform the same task as the scotoma awareness training, without the artificial visible scotoma.

Behavioral: Control Training

The task will be performed in the control group without the visible scotoma.

Outcome Measures

Primary Outcome Measures

Change from Baseline Visual Acuity after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
Score measured on EDTRS chart
Change from Baseline Fixation stability after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
Dispersion of fixation locations averaged across trials for the PRL (expressed as the Bivariate contour ellipse area (BCEA) of the dispersion).
Change from Baseline Saccadic re-referencing after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
Proportion of trials with first fixation using PRL (expressed as a % of the total number of trials).

Secondary Outcome Measures

Change from Baseline First saccade landing dispersion after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
The dispersion of the end point of the first saccade (expressed as the BCEA of the dispersion).
Change from Baseline Latency of target acquisition after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
The mean time until target is visible outside scotoma (expressed in seconds).
Change from Baseline Saccadic precision after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
The dispersion of the end point of the saccade that puts the target outside scotoma (expressed as the BCEA of the dispersion).
Change from Baseline Percentage of trials that are useful after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
How often participants place the target outside of the scotoma (% of dots in Saccadic precision relative to total trials).
Change from Baseline Minimal print size from MNREAD task after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
For the MNREAD test we will primarily rely upon minimal print size (a secondary measure of acuity)
Change from Baseline time-to-complete Trailmaking B subtest after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
We will look at time-to-complete the Trail Making B subtest, measured in seconds
Change from Baseline Contrast Sensitivity after completion of Training at approximately 6 weeks and 14 weeks [Baseline, after training completion, training is complete 6 weeks from baseline on average, and at follow up, 14 weeks from baseline on average]
Measured via Robson-Pelli charts

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years to 89 Years

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion Criteria:

Severely impaired vision in both eyes (20/100 or worse)
Diagnosis of Macular Degeneration
Light sensitivity in the macular retina that is at least 10 dB units worse than in peripheral regions, as demonstrated by a scanning laser ophthalmoscope (SLO, MAIA)
Medical record review indicates this disease severity level has been present for at least 2 years.

Exclusion Criteria:

Inability to sit still in eye tracker for extended periods
Inability to visualize iris on video eye tracker
Bilateral retinal scotomas larger than 20° diameter

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	UAB	Birmingham	Alabama	United States	35294

Sponsors and Collaborators

University of Alabama at Birmingham
University of California, Riverside

Investigators

None specified.

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.

Responsible Party:

Kristina M Visscher, Associate Professor, University of Alabama at Birmingham

ClinicalTrials.gov Identifier:

NCT05456581

Other Study ID Numbers:

300006197 (R21)

First Posted:

Jul 13, 2022

Last Update Posted:

Jul 13, 2022

Last Verified:

Jul 1, 2022

Individual Participant Data (IPD) Sharing Statement:

Yes

Plan to Share IPD:

Yes

Studies a U.S. FDA-regulated Drug Product:

Studies a U.S. FDA-regulated Device Product:

Keywords provided by Kristina M Visscher, Associate Professor, University of Alabama at Birmingham

plasticity

central vision loss

Additional relevant MeSH terms:

Vision Disorders

Vision, Low

Macular Degeneration

Study Results

No Results Posted as of Jul 13, 2022