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9. Deep learning‐accelerated image reconstruction in MRI of the orbit to shorten acquisition time and enhance image quality.

Author

Estler, Arne, Zerweck, Leonie, Brunnée, Merle, Estler, Bent, Richter, Vivien, Örgel, Anja, Bürkle, Eva, Becker, Hannes, Hurth, Helene, Stahl, Stéphane, Konrad, Eva‐Maria, Kelbsch, Carina, Ernemann, Ulrike, Hauser, Till‐Karsten, and Gohla, Georg

Subjects
DEEP learning, IMAGE reconstruction, MAGNETIC resonance imaging, DIFFUSION magnetic resonance imaging, CONTRAST-enhanced magnetic resonance imaging, ORBITAL diseases, LIKERT scale, DIAGNOSTIC imaging
Abstract

Background and Purpose: This study explores the use of deep learning (DL) techniques in MRI of the orbit to enhance imaging. Standard protocols, although detailed, have lengthy acquisition times. We investigate DL‐based methods for T2‐weighted and T1‐weighted, fat‐saturated, contrast‐enhanced turbo spin echo (TSE) sequences, aiming to improve image quality, reduce acquisition time, minimize artifacts, and enhance diagnostic confidence in orbital imaging. Methods: In a 3‐Tesla MRI study of 50 patients evaluating orbital diseases from March to July 2023, conventional (TSES) and DL TSE sequences (TSEDL) were used. Two neuroradiologists independently assessed the image datasets for image quality, diagnostic confidence, noise levels, artifacts, and image sharpness using a randomized and blinded 4‐point Likert scale. Results: TSEDL significantly reduced image noise and artifacts, enhanced image sharpness, and decreased scan time, outperforming TSES (p <.05). TSEDL showed superior overall image quality and diagnostic confidence, with relevant findings effectively detected in both DL‐based and conventional images. In 94% of cases, readers preferred accelerated imaging. Conclusion: The study proved that using DL for MRI image reconstruction in orbital scans significantly cut acquisition time by 69%. This approach also enhanced image quality, reduced image noise, sharpened images, and boosted diagnostic confidence. [ABSTRACT FROM AUTHOR]

Published
2024
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14. Diagnostic genome sequencing improves diagnostic yield: a prospective single- centre study in 1000 patients with inherited eye diseases.

Author

Weisschuh, Nicole, Mazzola, Pascale, Zuleger, Theresia, Schaeferhoff, Karin, Kühlewein, Laura, Kortüm, Friederike, Witt, Dennis, Liebmann, Alexandra, Falb, Ruth, Pohl, Lisa, Reith, Milda, Stühn, Lara G., Bertrand, Miriam, Müller, Amelie, Casadei, Nicolas, Kelemen, Olga, Kelbsch, Carina, Kernstock, Christoph, Richter, Paul, and Sadler, Francoise

Abstract

Purpose Genome sequencing (GS) is expected to reduce the diagnostic gap in rare disease genetics. We aimed to evaluate a scalable framework for genome-based analyses 'beyond the exome' in regular care of patients with inherited retinal degeneration (IRD) or inherited optic neuropathy (ION). Methods PCR-free short-read GS was performed on 1000 consecutive probands with IRD/ION in routine diagnostics. Complementary whole-blood RNA-sequencing (RNA-seq) was done in a subset of 74 patients. An open-source bioinformatics analysis pipeline was optimised for structural variant (SV) calling and combined RNA/DNA variation interpretation. Results A definite genetic diagnosis was established in 57.4% of cases. For another 16.7%, variants of uncertain significance were identified in known IRD/ION genes, while the underlying genetic cause remained unresolved in 25.9%. SVs or alterations in non-coding genomic regions made up for 12.7% of the observed variants. The RNA-seq studies supported the classification of two unclear variants. Conclusion GS is feasible in clinical practice and reliably identifies causal variants in a substantial proportion of individuals. GS extends the diagnostic yield to rare non-coding variants and enables precise determination of SVs. The added diagnostic value of RNA-seq is limited by low expression levels of the major IRD disease genes in blood. [ABSTRACT FROM AUTHOR]

Published
2024
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16. Influence of Patient Age and Presence of Optic Disc Drusen on Fluctuations in Retinal Nerve Fiber Layer Thickness.

Author

Tonagel, Felix, Wilhelm, Helmut, Stock, Lydia, and Kelbsch, Carina

Abstract

Background: It is generally believed that optic disc drusen (ODD) change only over long periods of time. Because, in our experience, this does not apply to younger patients, we investigated the natural course of changes of the peripapillary retinal nerve fiber layer (RNFL) in patients with ODD. Methods: In this retrospective study, 40 eyes with and 40 eyes without ODD were examined, both cohorts were equally subdivided into younger subjects (20 years or younger) and older subjects (21 years or older). Three optical coherence tomography (OCT) scans of the peripapillary RNFL that had an interval of at least 1 month were required for each patient to be included in this study. The largest difference in total RNFL thickness (delta RNFL-t) and in RNFL thickness of the most differing sector (delta RNFL max) measured by OCT was compared. Results: The differences in total RNFL thickness and in the most differing RNFL sector in the group of patients with ODD younger than 21 years were significantly larger than in each of the other 3 groups (P = 0.0001). The other 3 groups did not differ significantly. Conclusions: Patients with ODD younger than 21 years have distinct variations in peripapillary RNFL thickness without evidence of increased intracranial pressure. In the absence of further pathological findings or neurological symptoms, an observational approach seems adequate in these patients. [ABSTRACT FROM AUTHOR]

Published
2023
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20. PandAcuity in paediatrics: a novel clinical measure of visual function based on the panda illusion.

Author

Kelbsch, Carina, Spieth, Bettina, Zrenner, Eberhart, Besch, Dorothea, and Straßer, Torsten

Abstract

Background/aims To evaluate the PandAcuity test for visual function testing in a paediatric cohort and to examine its agreement with conventional visual acuity (VA) testing. Methods PandAcuity scores were determined in 152 children (77 males) aged between 3 and 15 years after VA testing (LEATM-test, E-chart, Landolt-C-rings or numbers). The PandAcuity test consisted of illusions made up from silhouettes of animals 'hidden' within zig-zag-patterns of decreasing spatial frequencies. Correlation analyses between PandAcuity score and VA were performed. Results 150 children completed the test in at least one eye, 148 in both eyes. The PandAcuity test demonstrated good test-retest reliability (intraclass correlation coefficient=0.89) between two runs. VA and PandAcuity score showed a medium to large correlation (Spearman's ρ=0.52, p<0.0001). 93% of the children's visual impairment was classified in the same range by both test types. Receiver operating characteristic analysis of predicted visual impairment showed an excellent agreement with the classification based on VA testing (AUC=0.84). Conclusion The PandAcuity test is rapid, simple and well accepted, rendering it a suitable supplement for the clinical assessment of VA in children. Because of its counterintuitive application (a higher number of correctly identified images means worse VA), it can be used to cross-validate conventional acuity tests to assure children's compliance. [ABSTRACT FROM AUTHOR]

Published
2023
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21. Spatial and temporal resolution of the photoreceptors rescue dynamics after treatment with voretigene neparvovec.

Author

Stingl, Krunoslav, Kempf, Melanie, Bartz-Schmidt, Karl U., Dimopoulos, Spyridon, Reichel, Felix, Jung, Ronja, Kelbsch, Carina, Kohl, Susanne, Kortüm, Friederike Charlotte, Nasser, Fadi, Peters, Tobias, Wilhelm, Barbara, Wissinger, Bernd, Wozar, Fabian, Zrenner, Eberhart, Fischer, M. Dominik, and Stingl, Katarina

Abstract

Background Voretigene neparvovec is a gene therapeutic agent for treatment of retinal dystrophies caused by bi-allelic RPE65 mutations. In this study, we report on a novel and objective evaluation of a retinotopic photoreceptor rescue. Methods Seven eyes of five patients (14, 21, 23, 24, 36 years, 1 male, 4 females) with bi-allelic RPE65 mutations have been treated with voretigene neparvovec. The clinical examinations included visual acuity testing, dark-adapted full-field stimulus threshold (FST), dark-adapted chromatic perimeter (DAC) with a 30-degree grid, and a 30 degrees grid scotopic and photopic chromatic pupil campimetry (CPC). All evaluations and spectral domain optical coherence tomography were performed at baseline, 1 month and 3 months. Results All except the oldest patient had a measurable improvement of the rod function assessed via FST, DAC or scotopic CPC at 1 month. The visual acuity improved slightly or remained stable in all eyes. A cone function improvement as measured by photopic CPC was observed in three eyes. The gain of the dark-adapted threshold with blue FST and the DAC stimuli (cyan) average correlated strongly with age (R2>0.7). The pupil response improvement in the scotopic CPC correlated with the baseline local retinal volume (R2=0.5). Conclusions The presented protocols allow evaluating the individual spatial and temporal effects of gene therapy effects. Additionally, we explored parameters that correlated with the success of the therapy. CPC and DAC present new and fast ways to assess functional changes in retinotopic maps of rod and cone function, measuring complementary aspects of retinal function. [ABSTRACT FROM AUTHOR]

Published
2022
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22. Clinical Protocols for the Evaluation of Rod Function.

Author

Stingl, Krunoslav, Stingl, Katarina, Nowomiejska, Katarzyna, Kuehlewein, Laura, Kohl, Susanne, Kempf, Melanie, Strasser, Torsten, Jung, Ronja, Wilhelm, Barbara, Peters, Tobias, Kelbsch, Carina, Bartz-Schmidt, Karl Ulrich, Langrova, Hana, and Zrenner, Eberhart

Subjects
MEDICAL protocols, SPATIAL resolution, VISUAL fields, PERIMETRY, INTRACLASS correlation
Abstract

This work presents a quick clinical protocol for dark-adapted chromatic (DAC) perimetry as well as a novel clinical tool, scotopic chromatic pupil campimetry (CPC). The goal of the study was to explore the applicability of these methods in a clinical setting, their test-retest repeatability, and the congruence of the results. Local rod sensitivity was assessed at 36 locations within 30° eccentricity of the visual field in 15 healthy subjects (mean age 43 ± 16 years; 7 females and 8 males) with DAC perimetry (red and cyan stimuli) and CPC 2 times in repeated measurements. The duration of individual measurements was 370 ± 5 s for CPC and 366 ± 62 s for DAC perimetry. The intraclass correlation (ICC) coefficient was 0.53 for DAC perimetry cyan stimuli, 0.67 for red stimuli, and 0.93 for CPC. However, the spatial resolution of CPC was substantially smaller than in DAC perimetry. We did not find a correlation of DAC perimetry and CPC measurements on the global or the local level. In comparison to DAC perimetry, CPC shows a superior intervisit repeatability in detecting functional changes in the rod population in an objective way with lower spatial resolution. Our results also indicate that these 2 methods measure the rod function in different ways and could thus constitute complementary scotopic functional diagnostics. [ABSTRACT FROM AUTHOR]

Published
2021
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23. Mutation spectrum of the OPA1 gene in a large cohort of patients with suspected dominant optic atrophy: Identification and classification of 48 novel variants.

Author

Weisschuh, Nicole, Schimpf-Linzenbold, Simone, Mazzola, Pascale, Kieninger, Sinja, Xiao, Ting, Kellner, Ulrich, Neuhann, Teresa, Kelbsch, Carina, Tonagel, Felix, Wilhelm, Helmut, Kohl, Susanne, and Wissinger, Bernd

Subjects
RNA splicing, GENETIC variation, HIGH performance liquid chromatography, GENETIC testing, ATROPHY
Abstract

Autosomal dominant optic atrophy is one of the most common inherited optic neuropathies. This disease is genetically heterogeneous, but most cases are due to pathogenic variants in the OPA1 gene: depending on the population studied, 32–90% of cases harbor pathogenic variants in this gene. The aim of this study was to provide a comprehensive overview of the entire spectrum of likely pathogenic variants in the OPA1 gene in a large cohort of patients. Over a period of 20 years, 755 unrelated probands with a diagnosis of bilateral optic atrophy were referred to our laboratory for molecular genetic investigation. Genetic testing of the OPA1 gene was initially performed by a combined analysis using either single-strand conformation polymorphism or denaturing high performance liquid chromatography followed by Sanger sequencing to validate aberrant bands or melting profiles. The presence of copy number variations was assessed using multiplex ligation-dependent probe amplification. Since 2012, genetic testing was based on next-generation sequencing platforms. Genetic screening of the OPA1 gene revealed putatively pathogenic variants in 278 unrelated probands which represent 36.8% of the entire cohort. A total of 156 unique variants were identified, 78% of which can be considered null alleles. Variant c.2708_2711del/p.(V903Gfs*3) was found to constitute 14% of all disease-causing alleles. Special emphasis was placed on the validation of splice variants either by analyzing cDNA derived from patients´ blood samples or by heterologous splice assays using minigenes. Splicing analysis revealed different aberrant splicing events, including exon skipping, activation of exonic or intronic cryptic splice sites, and the inclusion of pseudoexons. Forty-eight variants that we identified were novel. Nine of them were classified as pathogenic, 34 as likely pathogenic and five as variant of uncertain significance. Our study adds a significant number of novel variants to the mutation spectrum of the OPA1 gene and will thereby facilitate genetic diagnostics of patients with suspected dominant optic atrophy. [ABSTRACT FROM AUTHOR]

Published
2021
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24. Räumliche und zeitliche Auflösung der Wiederherstellungsdynamik der Photorezeptoren nach Behandlung mit Voretigen Neparvovec.

Author

Stingl, Krunoslav, Kempf, Melanie, Bartz-Schmidt, Karl U., Dimopoulos, Spyridon, Reichel, Felix, Jung, Ronja, Kelbsch, Carina, Kohl, Susanne, Körtum, Friederike Charlotte, Nasser, Fadi, Peters, Tobias, Wilhelm, Barbara, Wissinger, Bernd, Wozar, Fabian, Zrenner, Eberhart, Fischer, M. Dominik, and Stingl, Katarina

Published
2021
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30. Standards in Pupillography.

Author

Kelbsch, Carina, Strasser, Torsten, Chen, Yanjun, Feigl, Beatrix, Gamlin, Paul D., Kardon, Randy, Peters, Tobias, Roecklein, Kathryn A., Steinhauer, Stuart R., Szabadi, Elemer, Zele, Andrew J., Wilhelm, Helmut, and Wilhelm, Barbara J.

Subjects
RETINAL ganglion cells, RETINAL degeneration, GENE therapy
Abstract

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. [ABSTRACT FROM AUTHOR]

Published
2019
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32. Phosphene perception and pupillary responses to sinusoidal electrostimulation - For an objective measurement of retinal function.

Author

Kelbsch, Carina, Jalligampala, Archana, Strasser, Torsten, Richter, Paul, Stingl, Katarina, Braun, Christoph, Rathbun, Daniel L., Zrenner, Eberhart, Wilhelm, Helmut, Wilhelm, Barbara, Peters, Tobias, and Stingl, Krunoslav

Subjects
*PHOSPHENES, *RETINA, *PHOTORECEPTORS, *RETINAL ganglion cells, *BIPOLAR cells
Abstract

Abstract The purpose was to evaluate retinal function by measuring pupillary responses to sinusoidal transcorneal electrostimulation in healthy young human subjects. This work also translates data from analogous in vitro experiments and connects it to the pupillary responses obtained in human experiments. 14 healthy human subjects participated (4 males, 10 females); for the in vitro experiments, two male healthy mouse retinas (adult wild-type C57B/6J) were used. Pupillary responses to sinusoidal transcorneal electrostimulation of varying stimulus carrier frequencies (10, 20 Hz; envelope frequency constantly kept at 1.2 Hz) and intensities (10, 20, 50 μA) were recorded and compared with those obtained with light stimulation (1.2 Hz sinusoidal blue, red light). A strong correlation between the sinusoidal stimulation (electrical as well as light) and the pupillary sinusoidal response was found. The difference between the lag of electrical and light stimulation allowed the estimation of an intensity threshold for pupillary responses to transcorneal electrostimulation (mean ± SD: 30 ± 10 μA (10 Hz); 38 ± 10 μA (20 Hz)). A comparison between the results of the two stimulation frequencies showed a not statistically significant smaller lag for 10 Hz (10 Hz: 633 ± 90 ms; 20 Hz: 725 ± 178 ms; 50 μA intensity). Analogous in vitro experiments on murine retinas indicated a selective stimulation of photoreceptors and bipolar cells (lower frequencies) and retinal ganglion cells (higher frequencies) and lower stimulation thresholds for the retinal network with sinusoidal compared to pulsatile stimulation – emphasizing that sinusoidal waveforms are well-suited to our purposes. We demonstrate that pupillary responses to sinusoidal transcorneal electrostimulation are measurable as an objective marker in healthy young subjects, even at very low stimulus intensities. By using this unique approach, we unveil the potential for an estimation of the individual intensity threshold and a selective activation of different retinal cell types in humans by varying the stimulation frequency. This technique may have broad clinical utility as well as specific relevance in the monitoring of patients with hereditary retinal disorders, especially as implemented in study protocols for novel therapies, e.g. retinal prostheses or gene therapies. Highlights • Functional evaluation of the retina in humans based on pupillary responses. • New paradigm for transcorneal sinusoidal electrical stimulation. • Method for an easy estimation of individual thresholds for pupillary responses. • Possibility for a selective activation of different retinal cell types. • Verification of sinusoidal stimulation in animal in vitro model. [ABSTRACT FROM AUTHOR]

Published
2018
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34. Analysis of retinal function using chromatic pupillography in retinitis pigmentosa and the relationship to electrically evoked phosphene thresholds.

Author

Kelbsch, Carina, Maeda, Fumiatsu, Lisowska, Jolanta, Lisowski, Lukasz, Strasser, Torsten, Stingl, Krunoslav, Wilhelm, Barbara, Wilhelm, Helmut, and Peters, Tobias

Subjects
*RETINITIS pigmentosa, *RETINA physiology, *PHOSPHENES, *PUPIL (Eye), *DIAGNOSIS, *PATIENTS
Abstract

Purpose To analyse pupil responses to specific chromatic stimuli in patients with advanced retinitis pigmentosa ( RP) to ascertain whether chromatic pupillography can be used as an objective marker for residual retinal function. To examine correlations between parameters of the pupil response and the perception threshold of electrically evoked phosphenes. Methods Chromatic pupillography was performed in 40 patients with advanced RP (visual acuity < 0.02 or visual field ≤5°, non-recordable ERGs) and 40 age-matched healthy subjects. Pupil responses to full-field red (605 nm) and blue (420 nm) stimuli of 28 lx corneal illumination were recorded and analysed for two stimulus durations (1 and 4 seconds). The perception threshold of phosphenes to transcorneal electrostimulation was ascertained and correlated to the pupil responses and visual acuity. Results Patients with RP showed significantly reduced pupil responses to red and blue stimuli compared with the controls. With red stimuli, pupillary escape could be observed; blue stimuli resulted in a well-preserved postillumination pupil response. Phosphene thresholds were significantly increased in patients with RP and correlated with the parameters of the pupil response if all subjects were considered. Within the RP group alone, this relationship was less pronounced and statistically not significant. Conclusions Chromatic pupillography demonstrated a significant decrease in outer retinal photoreceptor responses but a persisting and disinhibited intrinsic photosensitive retinal ganglion cell function in advanced RP. These phenomena may be useful as an objective marker for the efficacy of any interventional treatment for hereditary retinal diseases as well as for the selection of suitable patients for an electronic retinal implant. [ABSTRACT FROM AUTHOR]

Published
2017
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35. Unilateral ocular malingering – a new test for the assessment of visual acuity.

Author

Tonagel, Felix, Kelbsch, Carina, and Kernstock, Christoph

Subjects
*VISUAL acuity, *MALINGERING, *BINOCULAR vision, *EYE examination
Abstract

The article offers information on the Unilateral ocular malingering is a phenomenon that every ophthalmologist encounters regularly in his clinical practice. It mentions the lack of multiple charts with different letter sizes makes it impossible to determine the genuine visual acuity; and also mentions the downside of test setting is the possible discovery of the separation of the stimuli of both eyes via closing one eye during the test.

Published
2019
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36. Cell-specific electrical stimulation of human retinal neurons assessed by pupillary response dynamics in vivo.

Author

Jung, Ronja, Kelbsch, Carina, Wilhelm, Helmut, Wilhelm, Barbara, Strasser, Torsten, Peters, Tobias, Kempf, Melanie, Kortüm, Friederike, Pohl, Lisa, Stingl, Krunoslav, and Stingl, Katarina

Subjects
*PUPILLARY reflex, *ELECTRIC stimulation, *RETINITIS pigmentosa, *RETINAL diseases, *NEURONS
Abstract

Studies on the electrical excitability of retinal neurons show that photoreceptors and other cell types can be selectively activated by distinct stimulation frequencies in vitro. Yet, this principle still needs to be validated in humans in vivo. As a first step, this study explored the frequency preferences of human rods by means of transcorneal electrostimulation (TES), using the electrically-elicited pupillary responses (EEPRs) as an objective readout. The stimulation paradigm contained a 1.2 Hz sinusoidal envelope, which was superimposed on variable carrier frequencies (4–30 Hz). These currents were delivered to one of the participant's eyes via a corneal electrode and consensual pupillary reactions were recorded from the contralateral eye. The responsiveness of the retina at each frequency was assessed based on the EEPR dynamics. Differences between healthy participants and patients with retinitis pigmentosa were evaluated to identify the preferred frequency range of rods. The responsiveness of healthy individuals revealed a clear peak around 6–8 Hz. In contrast, the pupillary responses of patients were significantly reduced in the lower frequency range. These findings suggest that the responses in this frequency bin were selectively mediated by rods. This work provides evidence that different retinal cell types can be selectively activated via TES in vivo, and that this effect can be captured noninvasively using EEPRs. This knowledge may be exploited for the diagnostics and therapy of retinal diseases, e.g., to design cell-specific functional tests for the degenerating retina, or to optimize stimulation paradigms which are currently used by retinal prostheses. • Sinusoidal currents of 4–30 Hz were applied to volunteers via corneal electrodes. • Pupillary responses served as an objective readout for the retinal responsiveness. • Healthy participants displayed elevated responsiveness in the 6–10 Hz range. • Patients with Retinitis Pigmentosa showed reduced responses in the 6–10 Hz range. • The difference suggests that rods are tuned to low-frequency stimulation. [ABSTRACT FROM AUTHOR]

Published
2022
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37. Influencing Factors on Pupillary Light Responses as a Biomarker for Local Retinal Function in a Large Normative Cohort.

Author

Jendritza R, Stingl K, Strasser T, Jung R, Tonagel F, Richter P, Sonntag A, Peters T, Wilhelm H, Wilhelm B, and Kelbsch C

Subjects
Humans, Middle Aged, Female, Male, Adult, Aged, Young Adult, Adolescent, Biomarkers, Photic Stimulation, Retina physiology, Retina diagnostic imaging, Healthy Volunteers, Light, Reference Values, Tomography, Optical Coherence methods, Pupil physiology, Reflex, Pupillary physiology
Abstract

Purpose: Investigating influencing factors on the pupillary light response (PLR) as a biomarker for local retinal function by providing epidemiological data of a large normative collective and to establish a normative database for the evaluation of chromatic pupil campimetry (CPC)., Methods: Demographic and ophthalmologic characteristics were captured and PLR parameters of 150 healthy participants (94 women) aged 18 to 79 years (median = 46 years) were measured with L-cone- and rod-favoring CPC protocols. Linear-mixed effects models were performed to determine factors influencing the PLR and optical coherence tomography (OCT) data were correlated with the pupillary function volume., Results: Relative maximal constriction amplitude (relMCA) and latency under L-cone- and rod-favoring stimulation were statistically significantly affected by the stimulus eccentricity (P < 0.0001, respectively). Iris color and gender did not affect relMCA or latency significantly; visual hemifield, season, and daytime showed only minor influence under few stimulus conditions. Age had a statistically significant effect on latency under rod-specific stimulation with a latency prolongation ≥60 years. Under photopic and scotopic conditions, baseline pupil diameter declined significantly with increasing age (P < 0.0001, respectively). Pupillary function volume and OCT data were not correlated relevantly., Conclusions: Stimulus eccentricity had the most relevant impact on relMCA and latency of the PLR during L-cone- and rod-favoring stimulation. Latency is prolonged ≥60 years under scotopic conditions. Considering the large study collective, a representative normative database for relMCA and latency as valid readout parameters for L-cone- and rod-favoring stimulation could be established. This further validates the usability of the PLR in CPC as a biomarker for local retinal function.

Published
2024
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38. Rod and Cone Function Measured Objectively by Chromatic Pupil Campimetry Show a Different Preservation Between Distinct Genotypes in Retinitis Pigmentosa.

Author

Kelbsch C, Kempf M, Jung R, Kortüm F, Reith M, Kuehlewein L, Kohl S, Strasser T, Peters T, Wilhelm H, Wilhelm B, Stingl K, and Stingl K

Subjects
Humans, Male, Pupil, Retinal Cone Photoreceptor Cells physiology, Genotype, Electroretinography methods, Eye Proteins genetics, Cyclic Nucleotide Phosphodiesterases, Type 6 genetics, Visual Field Tests, Retinitis Pigmentosa diagnosis, Retinitis Pigmentosa genetics
Abstract

Purpose: Verifying whether specific genotypes causing retinitis pigmentosa (RP) show differences in the preservation of rod and cone function measured by chromatic pupil campimetry (CPC)., Methods: Sixty-three RP eyes (37 male, 14-58 years) were measured using CPC with specific photopic and scotopic protocols, and the relative maximal constriction amplitudes and latencies to constriction onset were analyzed per genotype (RP due to variants in EYS, n = 14; PDE6A, n = 10; RPE65, n = 15; USH2A, n = 10; and RPGR, n = 14). Correlation analyses between the pupillary responses were performed with age, full-field stimulus threshold (FST), and optical coherence tomography (OCT) for cones and rods, respectively, to the genotype., Results: Pupillary responses were most severely reduced in RPE65-RP. Patients with disease-associated variants in EYS and USH2A were accompanied with better-preserved rod function compared with the other subgroups, reaching statistical significance between EYS and RPE65. Cone function was statistically significantly correlated with age in USH2A-RP with an annual decline of 2.4%. Correlations of pupillary responses were found with FST but barely with the ellipsoid zone area in OCT. Latency was significantly more prolonged in RPE65-RP compared with the other genotypes for cones., Conclusions: Rod and cone function measured objectively by CPC showed a different preservation between genotypes in RP. However, heterogeneity inside the same genotype was present. CPC data correlated with FST, but structural OCT parameters seem to be limited indicators for photoreceptor function in RP. Prolonged time dynamics for cones in RPE65 mutations suggest an impact on cone processing and might provide additional information in the evaluation of therapy effects.

Published
2023
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39. [Optical coherence tomography in the differential diagnostics of important neuro-ophthalmological disease patterns].

Author

Schultheiss M, Wenzel DA, Spitzer MS, Poli S, Wilhelm H, Tonagel F, and Kelbsch C

Subjects
Humans, Tomography, Optical Coherence methods, Optic Disk Drusen, Optic Neuritis diagnosis, Optic Neuropathy, Ischemic, Papilledema diagnosis
Abstract

There are many disease patterns that are treated jointly by neurologists and ophthalmologists, for which optical coherence tomography (OCT) is of important differential diagnostic significance. In this context neurologists are mainly confronted by two patient collectives: patients with an acute ischemic event, who present with an acute but painless monocular visual deterioration (for central retinal artery occlusion) or with a monocular visual field defect (for arterial branch occlusion or anterior ischemic optic neuropathy). The second collective is patients without ophthalmological symptoms but with conspicuous optic nerve findings (papilledema or optic disc drusen). In this overview article both patient collectives are considered separately. In addition, the most important OCT findings for optic neuritis are presented. Before the disease patterns are described in detail, the normal OCT findings and the diagnostic possibilities of OCT are explained., (© 2022. The Author(s), under exclusive licence to Springer Medizin Verlag GmbH, ein Teil von Springer Nature.)

Published
2022
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40. Evaluation of Local Rod and Cone Function in Stargardt Disease.

Author

Stingl K, Hoyng C, Kempf M, Kohl S, Jung R, Righetti G, Kühlewein L, Pohl L, Kortüm F, Kelbsch C, Wilhelm B, Peters T, and Stingl K

Subjects
ATP-Binding Cassette Transporters genetics, Adult, Electroretinography, Female, Humans, Male, Middle Aged, Retina, Visual Fields, Retinal Cone Photoreceptor Cells physiology, Stargardt Disease, Visual Field Tests
Abstract

Purpose: In this study, chromatic pupil campimetry (CPC) was used to map local functional degenerative changes of cones and rods in Stargardt disease (STGD1)., Methods: 19 patients (age 36 ± 8 years; 12 males) with genetically confirmed ABCA4 mutations and a clinical diagnosis of STGD1 and 12 age-matched controls (age 37 ± 11 years; 2 males) underwent scotopic (rod-favoring) and photopic (cone-favoring) CPC. CPC evaluates the local retinal function in the central 30° visual field via analysis of the pupil constriction to local stimuli in a gaze-corrected manner., Results: Scotopic CPC revealed that the rod function of patients with STGD1 inside the 30° visual field was not impaired when compared with age-matched controls. However, a statistically significant faster pupil response onset time (∼ 40 ms) was observed in the measured area. Photopic CPC showed a significant reduction of the central cone function up to 6°, with a minor, non-significant reduction beyond this eccentricity. The time dynamic of the pupillary response in photopic CPC did not reveal differences between STGD1 and controls., Conclusions: The functional analysis of the macular region in STGD1 disease indicates reduced central cone function, corresponding to photoreceptor degeneration. In contrast, the rod function in the central area was not affected. Nevertheless, some alteration of the time dynamics in the rod system was observed indicating a complex effect of cone degeneration on the functional performance of the rod system. Our results should be considered when interpreting safety and efficacy in interventional trials of STGD1.

Published
2022
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41. Chromatic Pupil Campimetry Reveals Functional Defects in Exudative Age-Related Macular Degeneration with Differences Related to Disease Activity.

Author

Kelbsch C, Lange J, Wilhelm H, Wilhelm B, Peters T, Kempf M, Kuehlewein L, and Stingl K

Subjects
Aged, Female, Humans, Pupil, Visual Acuity, Visual Fields, Macular Degeneration diagnostic imaging, Visual Field Tests
Abstract

Purpose: The purpose of this study was to use chromatic pupil campimetry (CPC) for an objective evaluation of local retinal function in exudative age-related macular degeneration (AMD) and to assess disease activity., Methods: Gaze-controlled CPC was performed in 19 subjects with optical coherence tomography-confirmed exudative AMD (75 ± 4 years; 11 women) and the results compared with those of an age-matched control group (n = 11; 72 ± 6 years; 8 women). Local retinal function was evaluated by measuring pupil responses to 3° red stimuli (60 cd/m 2 , 1 second) at 41 positions covering 30° of the central visual field on a dim blue background (test duration 6 minutes). Primary outcome parameters were relative maximal pupil constriction amplitude (% from baseline) and latency to constriction onset., Results: Pupil constriction amplitudes were significantly reduced in the macular region, and especially in the fovea in AMD (16% ± 4.7%; mean ± standard deviation), compared with the control group (24% ± 6%; P = 0.00036). Receiver operating characteristic values were 0.84 for the constriction amplitude in the fovea, and 0.9 for the steepness angle between periphery and center. Mean latency to constriction onset in the fovea in AMD was significantly longer (333 ± 53 ms; normals 273 ± 59 ms, P = 0.0072), and particularly in the active compared with the inactive status of exudative AMD ( P = 0.01)., Conclusions: CPC detected functional changes in exudative AMD with high sensitivity. Time dynamics of active exudative AMD differed from disease inactivity., Translational Relevance: With the combination of short recording time, objectiveness of the measurement and gaze-correction for fixation problems, this method presents a suitable complement to the currently used clinical functional tests of the macula., Competing Interests: Disclosure: C. Kelbsch, None; J. Lange, None; H. Wilhelm, None; B. Wilhelm, None; T. Peters, None; M. Kempf, None; L. Kuehlewein, None; K. Stingl, None, (Copyright 2020 The Authors.)

Published
2020
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42. Chromatic Full-Field Stimulus Threshold and Pupillography as Functional Markers for Late-Stage, Early-Onset Retinitis Pigmentosa Caused by CRB1 Mutations.

Author

Stingl KT, Kuehlewein L, Weisschuh N, Biskup S, Cremers FPM, Khan MI, Kelbsch C, Peters T, Ueffing M, Wilhelm B, Zrenner E, and Stingl K

Abstract

Purpose: Mutations in the CRB1 gene cause early-onset retinal degeneration (EORD). Clinical disease progression markers, such as visual fields or electrophysiology, are not reliably measurable in most patients to follow the retinal function in patients with CRB1 -mutations., Methods: Ten patients (five females, five males; age 22-56 years) with EORD caused by CRB1 mutations were examined in a cross-sectional manner using best corrected visual acuity (BCVA), perimetry, full-field and multifocal electroretinography, full-field stimulus threshold (FST), and pupillography to red and blue light. Disease duration was defined as the difference between the age at the first symptoms to the age at examination in years., Results: BCVA was quantifiable in six patients and ranged from light perception to 20/50. The visual field was measurable only in three patients who had the shortest disease duration. Full-field and multifocal electroretinography were not measurable in any patient. FST to blue and red light were measurable in all patients except the one with the longest disease duration; the thresholds ranged from -16.7 to 1.5 dB for red light and from -40.2 to 2.5 dB for blue light (0 dB = 0.01 cd.s/m 2 ) and showed correlations with disease duration ( r = 0.87 for blue, r = 0.65 for red, r = 0.8 for blue-red difference). The maximal relative pupil constriction amplitude (MRA) showed low or no correlations with disease duration ( r = -0.55 for blue, r = -0.3 for red light); the blue-red difference in the post-illumination pupil responses (PIPR) showed no correlation with disease duration ( r = -0.05). Compared to healthy eyes, the MRA to red and blue light was significantly decreased ( P < 0.001) and the blue-red PIPR difference was significantly increased ( P = 0.003)., Conclusions: FST features a valid clinical marker in late-stage early-onset retinitis pigmentosa caused by CRB1 mutations correlating with disease duration. This indicates the potential as a progression marker of disease. The pupil responses to full-field chromatic stimuli show significant differences from the normal population: the remaining responses, although reduced, indicate a partially preserved inner retinal function despite severe photoreceptor dysfunction., Translational Relevance: The functional measurements presented in this study present a valid clinical progression marker in late-stage early onset retinitis pigmentosa caused by biallelic CRB1 mutations. Additionally, they can be used as outcome measures for safety and efficacy in clinical therapy trials., (Copyright 2019 The Authors.)

Published
2019
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43. Objective Measurement of Local Rod and Cone Function Using Gaze-Controlled Chromatic Pupil Campimetry in Healthy Subjects.

Author

Kelbsch C, Stingl K, Kempf M, Strasser T, Jung R, Kuehlewein L, Wilhelm H, Peters T, Wilhelm B, and Stingl K

Abstract

Purpose: We introduce a new approach for functional mapping of rod and cone activity by measuring pupillary responses to local stimulation via gaze-controlled chromatic pupil campimetry (CPC)., Methods: Pupillary constriction amplitude and latency to constriction onset to local photopic and scotopic light stimuli at different locations within the 30° central visual field were analyzed in 14 healthy subjects (4 males, 34 ± 11 years, mean ± standard deviation [SD]). All subjects were measured twice for evaluating the test-retest variability and reproducibility of the method., Results: For the cone-favoring protocol (ConeProt), the relative maximal constriction amplitude was most pronounced in the center (26.8% ± 6.3%) with a hill-shaped decrease from the fovea to the periphery. For the rod-favoring protocol (RodProt), it was smaller (center, 13.5% ± 4.5%) with a profile lacking the central peak. Mean latency to constriction onset was faster for cones (277 ± 25 ms) than for rods (372 ± 13 ms). Mean intraclass correlation at the different stimulus locations was 0.84 ± 0.08 for RodProt and 0.75 ± 0.11 for ConeProt; mean coefficients of repeatability value of all stimulus locations was 5.9% ± 1.2% and 8.6% ± 1.7%, respectively., Conclusions: CPC provides an objective evaluation of local rod and cone function within the central 30° visual field. It shows a photoreceptor-specific profile in healthy subjects. Due to its easy, noncontact, gaze-controlled character, it is a clinically applicable method and may fill the gap of functional diagnostics of rods and cones of the human retina., Translational Relevance: Chromatic pupil campimetry provides information about the local rod and cone function of the human retina with distinct pattern of distributions in an objective manner., (Copyright 2019 The Authors.)

Published
2019
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44. [Visual Acuity and Visual Field in Optic Disc Drusen].

Author

Kelbsch C, Sonntag A, Wilhelm H, and Tonagel F

Subjects
Adolescent, Aged, Humans, Visual Field Tests, Optic Disk, Optic Disk Drusen complications, Visual Acuity, Visual Fields
Abstract

Background: It has been assumed that visual field defects in optic disc drusen slowly increase with age or occur during adolescence and do not change substantially in later years. In our study, we aimed to validate these assumptions., Material and Methods: 255 consecutive cases with optic disc drusen were identified from the patient records of the University Eye Hospital Tübingen; the diagnosis was verified and visual fields were quantified as long as available and of sufficient quality. Additionally, visual acuity was evaluated., Results: In 104 cases, quantifiable visual fields of sufficient quality for both eyes were available. In general, few patients with marked visual field defects could be detected. Only three patients showed visual field defects of ≥ 50% in both eyes. Both eyes were usually involved to approximately the same extent. Older age was correlated with more visual field defects. Only one patient remained below visual acuity of 0.3 in both eyes., Discussion: By means of our patient base, a continuous slight decline in the visual field with age can be assumed. Marked visual field defects were rare. The same was true for visual acuity, which showed some mild decline above the age of 60 years., Competing Interests: Die Autoren geben an, dass kein Interessenkonflikt besteht., (Georg Thieme Verlag KG Stuttgart · New York.)

Published
2019
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45. [Optic Disc Drusen].

Author

Tonagel F, Kernstock C, Wilhelm H, and Kelbsch C

Subjects
Humans, Ophthalmoscopy, Tomography, Optical Coherence, Glaucoma, Optic Disk, Optic Disk Drusen
Abstract

With a prevalence of about 2%, drusen papillae are a very frequent papilla anomaly. The pathological mechanism of their origin is unclear. If the ophthalmoscopic image is not unambiguous, it may be helpful to examine relatives, as the heredity exhibits irregular dominance. Calcium deposits are common and can be detected by sonography. Glands can also be detected by OCT in section and by autofluorescence. Precise funduscopy and documentation of the findings and follow-up are very important. There is no therapy for drusen papillae. The internal ocular pressure must be regularly controlled, as glaucoma cannot be identified from the papilla findings. The risk is increased of anterior ischaemia of the optical nerve., Competing Interests: Die Autoren geben an, dass kein Interessenkonflikt besteht., (Georg Thieme Verlag KG Stuttgart · New York.)

Published
2019
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46. [Pupil disorders].

Author

Wermund T, Wilhelm H, and Kelbsch C

Subjects
Humans, Pupil, Reflex, Pupillary, Eye Diseases, Pupil Disorders diagnosis, Pupil Disorders therapy
Abstract

The evaluation of pupillary function is a keystone in the neuro-ophthalmic assessment of patients. The diagnosis of an afferent or efferent pupillary disorder is crucial in the acquisition of a broad range of diseases of the brain or the peripheral nervous system. This "update" of pupillary disorders covers a major part of clinical conditions eye doctors have to expect in their daily practice. The significance of pupillary evaluation, however, extends far beyond the area of ophthalmology., Competing Interests: Die Autoren geben an, dass kein Interessenkonflikt besteht., (Georg Thieme Verlag KG Stuttgart · New York.)

Published
2019
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47. Pupillographic campimetry: an objective method to measure the visual field.

Author

Stingl K, Peters T, Strasser T, Kelbsch C, Richter P, Wilhelm H, and Wilhelm B

Subjects
Diagnostic Techniques, Ophthalmological, Humans, Pupil physiology, Vision Disorders physiopathology, Visual Field Tests
Abstract

Pupillographic campimetry allows measuring the visual field objectively by analyzing the pupil response to perimetric stimuli. One of the drawbacks of this technique, similar to static perimetry, is the need of reliable fixation of the subject. By using stimulus sizes comparable to static perimetry and applying gaze tracking, we enable a retinotopic visual field examination regardless of fixation problems and with an increased stability and improved spatial resolution. Here, we present the results of applying the method in eight normal sighted subjects as well as in three patients suffering from diseases usually diagnosed by perimetry. The results in normal sighted subjects show a reduction in the amplitude of the pupil response with increasing eccentricity as expected. We also demonstrate that gaze-controlled campimetry is able to detect organic visual field defects objectively in a patient group and classify the visual field defects without an organic background. Moreover, we show that our method is able to evaluate the visual field sensitivity loss beyond classical perimetry in patients with late-stage retinitis pigmentosa. Thus, gaze-controlled pupil campimetry can be used in addition to classical perimetry, allowing for an objective monitoring of disease progression, rendering it as a biomarker for novel treatments.

Published
2018
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48. [Acute Diplopia: Differential Diagnosis and Treatment Options].

Author

Kelbsch C, Besch D, and Wilhelm H

Subjects
Acute Disease, Brain Diseases diagnosis, Brain Diseases physiopathology, Brain Diseases therapy, Diagnosis, Differential, Diplopia physiopathology, Diplopia therapy, Eye Diseases diagnosis, Eye Diseases physiopathology, Eye Diseases therapy, Humans, Optic Nerve Diseases diagnosis, Optic Nerve Diseases physiopathology, Optic Nerve Diseases therapy, Optical Devices, Orbital Diseases diagnosis, Orbital Diseases physiopathology, Orbital Diseases therapy, Diplopia diagnosis, Diplopia etiology
Abstract

Acute diplopia can be caused by harmless disorders of the optical system, but also by dangerous intracranial or intraorbital processes that lead to movement disorders of the eyes. It may therefore be difficult to decide whether further diagnostic evaluation is necessary. This article presents a short, structural overview of the most important differential diagnoses of acute diplopia and the treatment options., Competing Interests: Interessenkonflikt: Die Autoren geben an, dass kein Interessenkonflikt besteht., (Georg Thieme Verlag KG Stuttgart · New York.)

Published
2017
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49. Pupil response components: attention-light interaction in patients with Parinaud's syndrome.

Author

Binda P, Straßer T, Stingl K, Richter P, Peters T, Wilhelm H, Wilhelm B, and Kelbsch C

Subjects
Adult, Attention, Female, Fixation, Ocular, Humans, Light, Male, Middle Aged, Ocular Motility Disorders diagnosis, Ocular Motility Disorders physiopathology, Ocular Motility Disorders therapy, Pupil physiology, Reflex, Pupillary radiation effects
Abstract

Covertly shifting attention to a brighter or darker image (without moving one's eyes) is sufficient to evoke pupillary constriction or dilation, respectively. One possibility is that this attentional modulation involves the pupillary light response pathway, which pivots around the olivary pretectal nucleus. We investigate this possibility by studying patients with Parinaud's syndrome, where the normal pupillary light response is strongly impaired due to lesions in the pretectal area. Four patients and nine control participants covertly attended (while maintaining fixation at the center of a monitor screen) to one of two disks located in the left and right periphery: one brighter, the other darker than the background. Patients and control subjects behaved alike, showing smaller pupils when attending to the brighter stimulus (despite no eye movements); consistent results were obtained with a dynamic version of the stimulus. We interpret this as proof of principle that attention to bright or dark stimuli can dynamically modulate pupil size in patients with Parinaud's syndrome, suggesting that attention acts independently of the pretectal circuit for the pupillary light response and indicating that several components of the pupillary response can be isolated - including one related to the focus of covert attention.

Published
2017
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50. Development of a Chromatic Pupillography Protocol for the First Gene Therapy Trial in Patients With CNGA3-Linked Achromatopsia.

Author

Lisowska J, Lisowski L, Kelbsch C, Maeda F, Richter P, Kohl S, Zobor D, Strasser T, Stingl K, Zrenner E, Peters T, Wilhelm H, Fischer MD, and Wilhelm B

Subjects
Adult, Case-Control Studies, Clinical Protocols, Color Vision Defects physiopathology, Dark Adaptation physiology, Female, Humans, Light, Male, Middle Aged, Photic Stimulation methods, Young Adult, Color Vision Defects therapy, Diagnostic Techniques, Ophthalmological, Genetic Therapy, Reflex, Pupillary physiology
Abstract

Purpose: To establish a feasible and sensitive pupillographic protocol to assess outer and inner retinal function for the first gene therapy trial in achromatopsia patients (ACHM) with mutations in CNGA3., Methods: Twenty-seven CNGA3-ACHM patients and 22 age-matched control subjects were tested using chromatic pupillography. Three different protocols were established to assess the pupillary light reflex parameters and to create the final protocol. In the individual protocols, various stimulus parameters (i.e., intensity, duration, wavelength, adaptation states) were applied to evaluate the impact of these stimuli on the pupillary response in untreated ACHM patients., Results: In the light-adapted conditions, CNGA3-ACHM patients showed significantly reduced maximal amplitudes compared with the control group when using a 1-second high intensity (28-lux corneal illumination) blue or red stimulus (P < 0.005). In the dark-adapted conditions, CNGA3-ACHM patients unexpectedly revealed significantly increased maximal amplitudes when stimulating with red (1 second) or blue (4 ms and 1 second) stimuli of low intensity (0.01-lux corneal illumination; P < 0.05). Pupil responses of CNGA3-ACHM patients after high intensity (28 lux) red and blue 1-second stimuli were within the normal range., Conclusions: Chromatic pupillography demonstrated significant reduced pupil responses to stimuli addressing primarily cone function, an increased sensitivity to rod-favoring stimuli and evidence for disinhibition of intrinsically photosensitive retinal ganglion cells in CNGA3-ACHM patients. A final protocol was established based on these findings. These conclusions may be useful for the objective assessment of efficacy gained by gene therapy or other innovative interventions in this hereditary retinal disorder.

Published
2017
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