Your search keyword '"Huryn, Laryssa"' showing total 4 results

1. Ocular findings in Jansen metaphyseal chondrodysplasia.

Author

Obiezu, Fiona, Magone De Quadros Costa, M Teresa, Huryn, Laryssa A, Pan, Kristen, Almpani, Konstantinia, Ninan, Anisha, Roszko, Kelly L, Weinstein, Lee S, Gafni, Rachel I, Ferreira, Carlos R, Lee, Janice, Collins, Michael T, and Jha, Smita

Subjects

COLOR blindness, SCOTOMA, OPTICAL coherence tomography, BONE growth, NEURONS, VISUAL fields, RETINAL ganglion cells

Abstract

Jansen metaphyseal chondrodysplasia (JMC) is an ultra-rare disorder caused by germline heterozygous PTHR1 variants resulting in constitutive activation of parathyroid hormone type 1 receptor. A description of ocular manifestations of the disease is lacking. Six patients with JMC underwent a detailed ophthalmic evaluation, spectral-domain optical coherence tomography (OCT), visual field testing, and craniofacial CT scans. Five of 6 patients had good visual acuity. All patients had widely spaced eyes; 5/6 had downslanted palpebral fissures. One patient had proptosis, and another had bilateral ptosis. Two patients had incomplete closure of the eyelids (lagophthalmos), one had a history of progressive right facial nerve palsy with profuse epiphora, while the second had advanced optic nerve atrophy with corresponding retinal nerve fiber layer (RNFL) thinning on OCT and significant bilateral optic canal narrowing on CT scan. Additionally, this patient also had central visual field defects and abnormal color vision. A third patient had normal visual acuity, subtle temporal pallor of the optic nerve head, normal average RNFL, but decreased temporal RNFL and retinal ganglion cell layer analysis (GCA) on OCT. GCA was decreased in 4/6 patients indicating a subclinical optic nerve atrophic process. None of the patients had glaucoma or high myopia. These data represent the first comprehensive report of ophthalmic findings in JMC. Patients with JMC have significant eye findings associated with optic canal narrowing due to extensive skull base dysplastic bone overgrowth that appear to be more prevalent and pronounced with age. Progressive optic neuropathy from optic canal narrowing may be a feature of JMC, and OCT GCA can serve as a useful biomarker for progression in the setting of optic canal narrowing. We suggest that patients with JMC should undergo regular ophthalmic examination including color vision, OCT, visual field testing, orbital, and craniofacial imaging. Lay Summary: Jansen metaphyseal chondrodysplasia (JMC) is an ultra-rare disorder caused by overactivity of the parathyroid hormone type 1 receptor, a receptor that is important for regulating bone development. Some patients report eye problems, but these have not been well-described. We therefore performed extensive eye examinations in 6 individuals with JMC. One had progressive right-sided facial paralysis associated with eye-tearing and dryness. A second individual had decreased central vision. Using optical coherence tomography (OCT), a method which takes detailed pictures of the retina, we found thinning of the retina's nerve layers (RNFL). Computed tomography (CT) of the skull showed narrowing of the bony canal through which the optic nerve passes. A third individual had normal vision but RNFL thinning just on the sides. Analysis of ganglion cells, the nerve cells carrying signals from the retina to the brain, showed localized deterioration of the optic nerve; skull CT also revealed optic canal narrowing. These findings suggest that JMC is associated with progressive damage to the optic nerve. Thus, patients with JMC would benefit from regular eye exams including OCT and visual field testing, in addition to routine imaging. Graphical Abstract [ABSTRACT FROM AUTHOR]

Published

2024

2. Clinical Phenotypes of CDHR1 -Associated Retinal Dystrophies.

Author

Malechka, Volha V., Cukras, Catherine A., Chew, Emily Y., Sergeev, Yuri V., Blain, Delphine, Jeffrey, Brett G., Ullah, Ehsan, Hufnagel, Robert B., Brooks, Brian P., Huryn, Laryssa A., and Zein, Wadih M.

Subjects

DYSTROPHY, RETINAL degeneration, OPTICAL coherence tomography, MACULAR degeneration, PHENOTYPES, COLOR photography

Abstract

The retinal dystrophy phenotype associated with CDHR1 retinopathy is clinically heterogenous. In this study, we describe the clinical and molecular findings of a retinal dystrophy cohort (10 patients) attributed to autosomal recessive CDHR1 and report novel variants in populations not previously identified with CDHR1-related retinopathy. Seven patients had evaluations covering at least a three-year period. The mean age of individuals at first symptoms was 36 ± 8.5 years (range 5–45 years). Visual acuity at the last visit ranged from 20/20 to 20/2000 (mean LogMAR 0.8 or 20/125). Three clinical subgroups were identified: rod–cone dystrophy (RCD), cone–rod dystrophy (CRD), and maculopathy. Extinguished scotopic electroretinography responses were noted in the RCD patients. Macular involvement was noted in all patients and documented on color fundus photography, fundus autofluorescence, and optical coherence tomography. Notable asymmetry of the degree of macular atrophy was present in two patients. The possible association between CDHR1 variants and clinical findings was predicted using molecular modeling. [ABSTRACT FROM AUTHOR]

Published

2022

3. Persistent Dark Cones in Oligocone Trichromacy Revealed by Multimodal Adaptive Optics Ophthalmoscopy.

Author

Li, Joanne, Liu, Tao, Flynn, Oliver J., Turriff, Amy, Liu, Zhuolin, Ullah, Ehsan, Liu, Jianfei, Dubra, Alfredo, Johnson, Mary A., Brooks, Brian P., Hufnagel, Robert B., Hammer, Daniel X., Huryn, Laryssa A., Jeffrey, Brett G., and Tam, Johnny

Subjects

ADAPTIVE optics, OPHTHALMOSCOPY, CONES, COLOR vision, OPTICAL coherence tomography

Abstract

Dark cone photoreceptors, defined as those with diminished or absent reflectivity when observed with adaptive optics (AO) ophthalmoscopy, are increasingly reported in retinal disorders. However, their structural and functional impact remain unclear. Here, we report a 3-year longitudinal study on a patient with oligocone trichromacy (OT) who presented with persistent, widespread dark cones within and near the macula. Diminished electroretinogram (ERG) cone but normal ERG rod responses together with normal color vision confirmed the OT diagnosis. In addition, the patient had normal to near normal visual acuity and retinal sensitivity. Occasional dark gaps in the photoreceptor layer were observed on optical coherence tomography, in agreement with reflectance AO scanning light ophthalmoscopy, which revealed that over 50% of the cones in the fovea were dark, increasing to 74% at 10° eccentricity. In addition, the cone density was 78% lower than normal histologic value at the fovea, and 20–40% lower at eccentricities of 5–15°. Interestingly, color vision testing was near normal at locations where cones were predominantly dark. These findings illustrate how a retina with predominant dark cones that persist over at least 3 years can support near normal central retinal function. Furthermore, this study adds to the growing evidence that cones can continue to survive under non-ideal conditions. [ABSTRACT FROM AUTHOR]

Published

2021

4. Clinical Features of Optic Disc Drusen in an Ophthalmic Genetics Cohort.

Author

Serpen, Jasmine Y., Prasov, Lev, Zein, Wadih M., Cukras, Catherine A., Cunningham, Denise, Murphy, Elizabeth C., Turriff, Amy, Brooks, Brian P., and Huryn, Laryssa A.

Subjects

EYE abnormalities, OPTIC nerve, OPTIC nerve diseases, USHER'S syndrome, VISION disorders, GENETIC testing, OPTICAL coherence tomography, ODDS ratio

Abstract

Background/Aims. Optic disc drusen (ODD) are calcified deposits of proteinaceous material in the optic disc, and their burden in ocular conditions is unknown. As ODD can be associated with visual field defects further compromising already degenerating visual function in patients with retinal degenerations, it is important to further our knowledge of ODD in inherited eye disease. The present study aims to evaluate prevalence, demographic features, and optic disc parameters of eyes with superficial ODD in inherited eye conditions. Materials and Methods. Electronic medical records of patients evaluated in the Ophthalmic Genetics clinic at the National Eye Institute (NEI) between 2008 and 2018 were searched for a superficial ODD diagnosis. Color fundus and autofluorescence images were reviewed to confirm ODD, supplemented with optical coherence tomography (OCT) in uncertain cases when available. Demographic information, examination, and genetic testing were reviewed. Disc areas and disc-to-macula distance to disc diameter ratios (DM : DD) were calculated. Results. Fifty six of 6207 patients had photographically confirmed ODD (0.9%). Drusen were predominantly bilateral (66%), with a female (62%) and Caucasian (73%) predilection. ODD prevalence in our cohort of patients with inherited retinal degenerations was 2.5%, and ODD were more prevalent in the rod-cone dystrophy subgroup at 2.95% (OR = 3.3 [2.1–5.3], P < 0.001) compared to the ophthalmic genetics cohort. Usher patients were more likely to have ODD (10/132, 7.6%, OR = 9.0 [4.3–17.7], P < 0.001) and had significantly smaller discs compared to the rest of our ODD cohort (disc area: P = 0.001 , DM : DD: P = 0.03). Discussion. While an association between ODD and retinitis pigmentosa has been reported, this study surveys a large cohort of patients with inherited eye conditions and finds the prevalence of superficial ODD is lower than that in the literature. Some subpopulations, such as rod-cone dystrophy and Usher syndrome, had a higher prevalence than the cohort as a whole. [ABSTRACT FROM AUTHOR]

Published

2020