Development of a Chromatic Pupillography Protocol for the First Gene Therapy Trial in Patients With <i>CNGA3</i>-Linked Achromatopsia

Lisowska, Jolanta; Lisowski, Łukasz; Kelbsch, Carina; Maeda, Fumiatsu; Richter, Paul; Kohl, Susanne; Zobor, Ditta; Straßer, Torsten; Stingl, Krunoslav; Zrenner, Eberhart; Peters, Tobias; Wilhelm, Helmut; Fischer, Manuel; Wilhelm, Barbara

doi:10.1167/iovs.16-20505

Cited by 30 publications

(24 citation statements)

References 38 publications

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“…For a reliable interpretation of the data and to facilitate replication of findings, the absolute pupil baseline diameter before the stimulation should be reported. This metric varies widely across participants with a characteristic decreasing pupil size with age (2) and hints for smaller pupil sizes in specific retinal diseases, e.g., in CNGA3-linked Achromatopsia (35). Further analyses should usually be based on relative values as pupillary responses are dependent on the initial baseline diameter, which should be obtained during a sufficiently long recording period to ensure a steady and reliable estimate.…”

Section: Part: General Standards For Pupillographymentioning

confidence: 99%

“…There are examples of chromatic pupillometry methodologies that provide initial efforts to separate rod and cone function through the careful control of the wavelength, irradiance, size and duration of the test stimuli; the degree of separation of rod and cone (and melanopsin) function that these conditions provide is still to be determined. At light levels below cone threshold, short wavelength lights are presented in the dark to bias the response to rods, with the PIPR amplitudes minimized under such conditions (9, 11, 35). To ensure maximal rod sensitivity, the pre-stimulus dark adaptation time should be at least 30 min (91); although this is not practical for all clinical protocols, shorter periods will influence the relative rod and cone sensitivity to the test stimuli.…”

Section: The Afferent Pupillary Pathway Authors: Carina Kelbsch Amentioning

confidence: 99%

“…On the other hand, there are pupillographic clinical studies in humans in order to better understand the pupil circuitry [e.g., (17, 18)] and the pathomechanism and remaining retinal functionality of certain diseases, e.g., glaucoma (19–23), Retinitis pigmentosa (9, 24–27), age-related macular degeneration (28–30), diabetes (31–33) or hereditary optic neuropathy (34). Furthermore, pupillography comes into use in clinical observational and therapy studies like gene therapy of hereditary retinal degenerations (35), studies on attention-modulation (36), in chronobiology [(37–39), for a review see (40)] and in psychopathology, psychiatric disorders and neurodegenerative conditions (41–45). Additionally, pupillography is indispensable in sleepiness-related research and the pupillographic sleepiness test (PST) has been developed into an objective measures of day time sleepiness (46, 47).…”

Section: Introductionmentioning

confidence: 99%

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Standards in Pupillography

et al. 2019

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The number of research groups studying the pupil is increasing, as is the number of publications. Consequently, new standards in pupillography are needed to formalize the methodology including recording conditions, stimulus characteristics, as well as suitable parameters of evaluation. Since the description of intrinsically photosensitive retinal ganglion cells (ipRGCs) there has been an increased interest and broader application of pupillography in ophthalmology as well as other fields including psychology and chronobiology. Color pupillography plays an important role not only in research but also in clinical observational and therapy studies like gene therapy of hereditary retinal degenerations and psychopathology. Stimuli can vary in size, brightness, duration, and wavelength. Stimulus paradigms determine whether rhodopsin-driven rod responses, opsin-driven cone responses, or melanopsin-driven ipRGC responses are primarily elicited. Background illumination, adaptation state, and instruction for the participants will furthermore influence the results. This standard recommends a minimum set of variables to be used for pupillography and specified in the publication methodologies. Initiated at the 32nd International Pupil Colloquium 2017 in Morges, Switzerland, the aim of this manuscript is to outline standards in pupillography based on current knowledge and experience of pupil experts in order to achieve greater comparability of pupillographic studies. Such standards will particularly facilitate the proper application of pupillography by researchers new to the field. First we describe general standards, followed by specific suggestions concerning the demands of different targets of pupil research: the afferent and efferent reflex arc, pharmacology, psychology, sleepiness-related research and animal studies.

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Section: Part: General Standards For Pupillographymentioning

confidence: 99%

Section: The Afferent Pupillary Pathway Authors: Carina Kelbsch Amentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Standards in Pupillography

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“…Indeed, these and subsequent studies showed that the PLR for chromatic light may potentially be used for diagnosis and monitoring disease progression as well as determination of treatment efficacy and safety in retinal and optic nerve diseases. 5,[7][8][9][10][13][14][15][16] Recently, Park et al 17 characterized the PLR mediated by the different photoreceptor classes when using smaller stimulus sizes presented in the center of the visual field (VF) over a large range of light intensities. Chibel et al 18 provided evidence that the function of rods and cones at different locations in the central (16.28) VF can be assessed using smaller (Goldmann size III, 0.438) red and blue light stimuli at 1000 and 200 cd/m 2 , respectively, under mesopic (0.05 cd/m 2 uniform white light) adaptation.…”

mentioning

confidence: 99%

Effect of Stimulus Intensity and Visual Field Location on Rod- and Cone-Mediated Pupil Response to Focal Light Stimuli

Yahia

Hamburg

Sher

et al. 2018

Invest. Ophthalmol. Vis. Sci.

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Citation: Haj Yahia S, Hamburg A, Sher I, et al. Effect of stimulus intensity and visual field location on rod-and conemediated pupil response to focal light stimuli. Invest Ophthalmol Vis Sci. 2018;59:6027-6035. https://doi.org/ 10.1167/iovs.18-23767 PURPOSE.To assess the effect of stimulus intensity on rod-and cone-mediated pupil light reflex (PLR) to small stimuli presented at central and peripheral visual field (VF) locations.METHODS. The PLR to small (0.438) chromatic stimuli was tested in the right eye of healthy subjects. Blue (485 6 20 nm) and red (625 6 15 nm) stimuli were presented at incremental light intensities (0.5-3.75 log cd/m 2 ) at peripheral (21.218) and central (4.248) VF locations using a chromatic pupilloperimeter under mesopic or blue light adaptation conditions. The percentage of pupil contraction (PPC), maximal pupil contraction velocity (MCV), latency of MCV (LMCV) and the ratio of central to peripheral responses for PPC (Q PPC value) were determined.RESULTS. Under mesopic light adaptation conditions, the mean PPC recorded in response to red stimuli was lower than blue stimuli in all VF locations and light intensities, and the Q PPC values were higher in response to red compared with blue light stimuli across the light intensity range tested. With blue background light, the pupil responses for red and blue light stimuli were approximately the same in the peripheral VF. LMCV was nearly constant in all VF locations for blue and red stimuli, respectively.CONCLUSIONS. The chromatic pupilloperimeter enables the assessment of rod-and conecontribution to the PLR in different VF locations. The optimal light intensities determined here for the assessment of focal activation of the two photoreceptor systems may be used for clinical evaluation of photoreceptor health.

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“…Stimulus projection was achieved with a time-triggered Espion Ganzfeld ColorDome Stimulator (Espion E 2 ; Diagnosys LLC, Lowell, MA, USA). Based on the protocols described by Park et al, 23 Kardon et al, 24 Kawasaki et al, 25 and Lisowska et al, 26 blue and red stimuli were displayed with a duration of 1 second under darkand light-adapted conditions. All preterm-born and term-born children were tested with a protocol containing three repeats of fixed illuminances (0.01 cd/m 2 blue stimuli at a wavelength of 460 nm and 100 cd/m 2 red stimuli at a wavelength of 640 nm).…”

Section: Optical Coherence Tomography and Layer Segmentationmentioning

confidence: 99%