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Hyperspectral Drusen Classification

O

Optina Diagnostics

Status

Completed

Conditions

Dry Age Related Macular Degeneration

Treatments

Device: Mydriatic Hyperspectral retinal Camera, (MHRC) and Optical coherence tomography (OCT)

Study type

Observational

Funder types

Industry

Identifiers

NCT06860555
22-003

Details and patient eligibility

About

This observational, cross-sectional study is designed to explore the feasibility to extract spatial-spectral features from hyperspectral retinal images captured with Optina Diagnostics' MHRC that are characteristic to the different types of drusenoid deposits associated with dry age-related macular degeneration.

Full description

In this observational, cross-sectional, prospective study, participants with dry AMD in at least one eye will undergo a hyperspectral retinal imaging session with the Optina Diagnostics' MHRC in addition to retinal imaging with OCT, used as the gold standard method to identify and classify the drusenoid deposits.

Eligible participants visiting the eye clinic for AMD with dry AMD in at least one eye will be invited to participate in the study. Subjects who sign an informed consent to participate in the study will have their eyes evaluated to confirm that at least one eye is meeting all of the inclusion criteria, and none of the exclusion criteria. The dry AMD status and stage as well as information about eye diseases and conditions will be documented for both eyes. If eligible (no ocular exclusion criteria present in at least one eye), subjects will undergo OCT imaging of the macular region. If the OCT imaging session is successful (as described in the OCT imaging procedure below), the participants will then undergo hyperspectral retinal imaging with the Optina Diagnostics MHRC.

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Enrollment

112 patients

Sex

All

Ages

50+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

  • To be eligible for participation, volunteers must conform to all of the following inclusion criteria:

    • Male and female adults aged 50 years and older (inclusive).

    • Dry AMD in at least one eye, with at least one type of the following retinal drusenoid deposits: reticular pseudodrusen, soft drusen, hard drusen.

      ○ The presence of multiple small drusen (< 63µm) or intermediate drusen (≥63µm and ≥125µm) is sufficient to qualify for this study (Coleman, 2008).

    • Ability and willingness to give informed consent.

Exclusion criteria

Individuals that meet any of the following exclusionary criteria cannot be enrolled:

  • Any ophthalmologic condition that would prevent obtaining retinal imaging and/or could interfere with the analysis of the MHRC images and OCT images, including:

    • Pupil dilation contraindicated (due to a pathology or with 3 quadrants with Van Herick of 0 or 1 without iridotomy)
    • Inadequate pupil dilatation (< 6mm diameter) preventing uniform illumination of the retina with the MHRC
    • Dry AMD presenting only with pigmentary changes or geographic atrophy (no drusenoid deposits)
    • Presence of geographic atrophy in a cumulative area of >0.5 disc area
    • Presence of neovascular AMD, defined as the presence of at least 1 of the following 4 characteristics: serous sensory retinal detachment, RPE detachment, subretinal hemorrhage, or subretinal fibrous tissue; or history of photocoagulation for choroidal new vessels (AREDS, 2005)
    • Signs of vascular occlusion or retinopathy (microaneurysm, exudate, hemorrhage or edema) within a diameter of 10 mm from the mid-point between the optic nerve head and the macula (i.e. the area of interest for the MHRC imaging)
    • Macular dystrophy
    • Nuclear sclerosis > 2 (LOCS II four-point grading system) or presence of central cortical or central posterior subcapsular cataract
    • Deficient visual fixation (inability to fixate for at least 2 s)
    • Refractive error outside the range of -15 D to +15 D
    • Corneal or media opacities (e.g. Weiss ring) affecting retinal imaging on a cumulative area > 1 disc area within a diameter of 10 mm from the mid-point between the optic nerve head and the macula (i.e. the area of interest for the MHRC imaging)
    • Scar, atrophy, naevus, tumor, epiretinal membrane or retinal pucker with a cumulative area > 1 disc area within a diameter of 10 mm from the mid-point between the optic nerve head and the macula (i.e. the area of interest for the MHRC imaging).
    • Papilledema

  • Inability to obtain an OCT image centered on the macular region of satisfactory quality for analysis of the drusenoid deposits (as indicated by the OCT's software quality indicator)

  • Inability of obtaining at least 3 images of satisfactory quality with the MHRC per the Optina Diagnostics quality index software.

Trial design

112 participants in 1 patient group

Participants with dry AMD
Description:
Participants with dry AMD in at least one eye will undergo a hyperspectral retinal imaging session with Optina Diagnostics' MHRC in addition to retinal imaging with OCT, used as the gold standard method to identify and classify the drusenoid deposits.
Treatment:
Device: Mydriatic Hyperspectral retinal Camera, (MHRC) and Optical coherence tomography (OCT)

Trial contacts and locations

1

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Data sourced from clinicaltrials.gov

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