Reflexive Eye Closure in Response to Cone and Melanopsin Stimulation: A Study of Implicit Measures of Light Sensitivity in Migraine.

Eric A Kaiser, Harrison McAdams, Aleksandra Igdalova, Edda B Haggerty, Brett L Cucchiara, David H Brainard, Geoffrey K Aguirre
Author Information
  1. Eric A Kaiser: From the Departments of Neurology (E.A.K., A.I., E.B.H., B.L.C., G.K.A.) and Neuroscience (H.M.), Perelman School of Medicine, and Department of Psychology (D.H.B.), University of Pennsylvania, Philadelphia. aguirreg@upenn.edu. ORCID
  2. Harrison McAdams: From the Departments of Neurology (E.A.K., A.I., E.B.H., B.L.C., G.K.A.) and Neuroscience (H.M.), Perelman School of Medicine, and Department of Psychology (D.H.B.), University of Pennsylvania, Philadelphia.
  3. Aleksandra Igdalova: From the Departments of Neurology (E.A.K., A.I., E.B.H., B.L.C., G.K.A.) and Neuroscience (H.M.), Perelman School of Medicine, and Department of Psychology (D.H.B.), University of Pennsylvania, Philadelphia.
  4. Edda B Haggerty: From the Departments of Neurology (E.A.K., A.I., E.B.H., B.L.C., G.K.A.) and Neuroscience (H.M.), Perelman School of Medicine, and Department of Psychology (D.H.B.), University of Pennsylvania, Philadelphia.
  5. Brett L Cucchiara: From the Departments of Neurology (E.A.K., A.I., E.B.H., B.L.C., G.K.A.) and Neuroscience (H.M.), Perelman School of Medicine, and Department of Psychology (D.H.B.), University of Pennsylvania, Philadelphia.
  6. David H Brainard: From the Departments of Neurology (E.A.K., A.I., E.B.H., B.L.C., G.K.A.) and Neuroscience (H.M.), Perelman School of Medicine, and Department of Psychology (D.H.B.), University of Pennsylvania, Philadelphia.
  7. Geoffrey K Aguirre: From the Departments of Neurology (E.A.K., A.I., E.B.H., B.L.C., G.K.A.) and Neuroscience (H.M.), Perelman School of Medicine, and Department of Psychology (D.H.B.), University of Pennsylvania, Philadelphia.

Abstract

BACKGROUND AND OBJECTIVES: To quantify interictal photophobia in migraine with and without aura using reflexive eye closure as an implicit measure of light sensitivity and to assess the contribution of melanopsin and cone signals to these responses.
METHODS: Participants were screened to meet criteria for 1 of 3 groups: headache-free (HF) controls, migraine without aura (MO), and migraine with visual aura (MA). MO and MA participants were included if they endorsed ictal and interictal photophobia. Exclusion criteria included impaired vision, inability to collect usable pupillometry, and history of either head trauma or seizure. Participants viewed light pulses that selectively targeted melanopsin, the cones, or their combination during recording of orbicularis oculi EMG (OO-EMG) and blinking activity.
RESULTS: We studied 20 participants in each group. MA and MO groups reported increased visual discomfort to light stimuli (discomfort rating, 400% contrast, MA: 4.84 [95% confidence interval 0.33, 9.35]; MO: 5.23 [0.96, 9.50]) as compared to HF controls (2.71 [0, 6.47]). Time course analysis of OO-EMG and blinking activity demonstrated that reflexive eye closure was tightly coupled to the light pulses. The MA group had greater OO-EMG and blinking activity in response to these stimuli (EMG activity, 400% contrast: 42.9%Δ [28.4, 57.4]; blink activity, 400% contrast: 11.2% [8.8, 13.6]) as compared to the MO (EMG activity, 400% contrast: 9.9%Δ [5.8, 14.0]; blink activity, 400% contrast: 4.7% [3.5, 5.9]) and HF control (EMG activity, 400% contrast: 13.2%Δ [7.1, 19.3]; blink activity, 400% contrast: 4.5% [3.1, 5.9]) groups.
DISCUSSION: Our findings suggest that the intrinsically photosensitive retinal ganglion cells (ipRGCs), which integrate melanopsin and cone signals, provide the afferent input for light-induced reflexive eye closure in a photophobic state. Moreover, we find a dissociation between implicit and explicit measures of interictal photophobia depending on a history of visual aura in migraine. This implies distinct pathophysiology in forms of migraine, interacting with separate neural pathways by which the amplification of ipRGC signals elicits implicit and explicit signs of visual discomfort.

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Grants

  1. P30 EY001583/NEI NIH HHS
  2. R01 EY024681/NEI NIH HHS
  3. T32 AG000255/NIA NIH HHS
  4. R25 NS065745/NINDS NIH HHS

MeSH Term

Adult
Blinking
Electromyography
Female
Humans
Male
Migraine Disorders
Photic Stimulation
Photophobia
Reflex, Abnormal
Retinal Cone Photoreceptor Cells
Retinal Ganglion Cells
Rod Opsins

Chemicals

Rod Opsins
melanopsin

Word Cloud

Created with Highcharts 10.0.0activity400%contrast:migraineauralightMOvisualMAEMG45interictalphotophobiareflexiveeyeclosureimplicitmelanopsinsignals1HFOO-EMGblinkingdiscomfort9blinkwithoutconeParticipantscriteriacontrolsparticipantsincludedhistorypulsesgroupgroupsstimuli[0compared9%Δ813[39]explicitBACKGROUNDANDOBJECTIVES:quantifyusingmeasuresensitivityassesscontributionresponsesMETHODS:screenedmeet3groups:headache-freeendorsedictalExclusionimpairedvisioninabilitycollectusablepupillometryeitherheadtraumaseizureviewedselectivelytargetedconescombinationrecordingorbicularisoculiRESULTS:studied20reportedincreasedratingcontrastMA:84[95%confidenceinterval03335]MO:239650]271647]Timecourseanalysisdemonstratedtightlycoupledgreaterresponse42[28574]112%[86][5140]7%control2%Δ[7193]5%DISCUSSION:findingssuggestintrinsicallyphotosensitiveretinalganglioncellsipRGCsintegrateprovideafferentinputlight-inducedphotophobicstateMoreoverfinddissociationmeasuresdependingimpliesdistinctpathophysiologyformsinteractingseparateneuralpathwaysamplificationipRGCelicitssignsReflexiveEyeClosureResponseConeMelanopsinStimulation:StudyImplicitMeasuresLightSensitivityMigraine

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