Your search keyword '"Zein, Wadih"' showing total 16 results

1. Joubert Syndrome: Ophthalmological Findings in Correlation with Genotype and Hepatorenal Disease in 99 Patients Prospectively Evaluated at a Single Center.

Author

Brooks, Brian P., Zein, Wadih M., Thompson, Amy H., Mokhtarzadeh, Maryam, Doherty, Daniel A., Parisi, Melissa, Glass, Ian A., Malicdan, May C., Vilboux, Thierry, Vemulapalli, Meghana, Mullikin, James C., Gahl, William A., and Gunay-Aygun, Meral

Subjects

*JOUBERT syndrome, *HEPATORENAL syndrome, *CEREBELLUM diseases, *EYE abnormalities, *OPHTHALMOLOGY

Abstract

Purpose Joubert syndrome (JS) is caused by mutations in >34 genes that encode proteins involved with primary (nonmotile) cilia and the cilium basal body. This study describes the varying ocular phenotypes in JS patients, with correlation to systemic findings and genotype. Design Patients were systematically and prospectively examined at the National Institutes of Health (NIH) Clinical Center in the setting of a dedicated natural history clinical trial. Participants Ninety-nine patients with JS examined at a single center. Methods All patients underwent genotyping for JS, followed by complete age-appropriate ophthalmic examinations at the NIH Clinical Center, including visual acuity (VA), fixation behavior, lid position, motility assessment, slit-lamp biomicroscopy, dilated fundus examination with an indirect ophthalmoscope, and retinoscopy. Color and fundus autofluorescence imaging, Optos wide-field photography (Dunfermline, Scotland, UK), and electroretinography (ERG) were performed when possible. Main Outcome Measures The VA (with longitudinal follow-up where possible), ptosis, extraocular muscle function, retinal and optic nerve status, and retinal function as measured by ERG. Results Among patients with JS with quantifiable VA (68/99), values ranged from 0 logarithm of the minimum angle of resolution (logMAR) (Snellen 20/20) to 1.5 logMAR (Snellen 20/632). Strabismus (71/98), nystagmus (66/99), oculomotor apraxia (60/77), ptosis (30/98), coloboma (28/99), retinal degeneration (20/83), and optic nerve atrophy (8/86) were identified. Conclusions We recommend regular monitoring for ophthalmological manifestations of JS beginning soon after birth or diagnosis. We demonstrate delayed visual development and note that the amblyogenic time frame may last significantly longer in JS than is typical. In general, patients with coloboma were less likely to display retinal degeneration, and those with retinal degeneration did not have coloboma. Severe retinal degeneration that is early and aggressive is seen in disease caused by specific genes, such as CEP290 - and AHI1 -associated JS. Retinal degeneration in INPP5E-, MKS1-, and NPHP1- associated JS was generally milder. Finally, ptosis surgery can be helpful in a subset of patients with JS; decisions as to timing and benefit/risk ratio need to be made on an individual basis according to expert consultation. [ABSTRACT FROM AUTHOR]

Published

2018

2. Brittle hair, developmental delay, neurologic abnormalities, and photosensitivity in a 4-year-old girl.

Author

Zhou, Xiaolong, Khan, Sikandar G., Tamura, Deborah, Patronas, Nicholas J., Zein, Wadih M., Brooks, Brian P., Kraemer, Kenneth H., and DiGiovanna, John J.

Published

2010

3. AAPOS Genetic Eye Disease Committee Workshop—hiding in plain sight: genetic disorders in routine pediatric practice.

Author

Dumitrescu, Alina V., Utz, Virginia Miraldi, Whitman, Mary C., Alcorn, Deborah, Couser, Natario L., Khan, Arif O., Levin, Alex V., Lloyd, I. Christopher, Schmitt, Melanie A., Zein, Wadih M., Nagiel, Aaron, Haider, Kathryn M., Doyle, Jefferson J., Zeid, Janice Lasky, and Drack, Arlene V.

Subjects

GENETIC disorders, EYE diseases, WORKS councils

Published

2021

4. Phenotypic and genetic differences of autosomal recessive bestrophinopathy and Best vitelliform macular dystrophy.

Author

Pfister, Tyler, Zein, Wadih, Sen, Hatice, Maldonado, Ramiro, Huryn, Laryssa, Cukras, Cathy, and Hufnagel, Robert

Subjects

PHENOTYPES, DYSTROPHY, RECESSIVE genes

Published

2021

5. AAPOS Genetic Eye Disease Committee workshop: does this patient have a genetic eye disease? should I refer?

Author

Drack, Arlene V., Alcorn, Deborah M., Costakos, Deborah M., Levin, Alex V., Lloyd, I. Christopher, Miraldi Utz, Virginia A., Schmitt, Melanie A., Heon, Elise, Whitman, Mary, Zein, Wadih, and Dumitrescu, Alina

Subjects

EYE diseases, GENETIC disorders, WORKS councils, CONGENITAL glaucoma

Abstract

AAPOS Genetic Eye Disease Committee workshop: does this patient have a genetic eye disease? (1) Clinicians will develop a systematic approach to identify patients with genetic eye disorders. In a rapidly changing field, this case-based workshop will provide up-to-date algorithms to confidently provide the best care for patients with genetic eye disorders. [Extracted from the article]

Published

2019

6. Multimodal imaging including optical coherence tomography in pediatric RP2 patients.

Author

Hufnagel, Robert B., Zein, Wadih M., Huryn, Laryssa A., Turriff, Amy, Blain, Delphine, and Brooks, Brian P.

Published

2018

7. What's new and important in pediatric ophthalmology and strabismus in 2017.

Author

Bacal, Darron A., Rutar, Tina, Adamopoulou, Chryssa, Reznick, Leah, Herlihy, Erin, Motley, Walker, Capo, Hilda, McCourt, Emily, Zein, Wadih, Rotberg, Leemor, and Gianfermi, Elena

Published

2017

8. Ophthalmic Manifestations of ROSAH (Retinal Dystrophy, Optic Nerve Edema, Splenomegaly, Anhidrosis, and Headache) Syndrome, an Inherited NF κB–Mediated Autoinflammatory Disease with Retinal Dystrophy.

Author

Huryn, Laryssa A., Kozycki, Christina Torres, Serpen, Jasmine Y., Zein, Wadih M., Ullah, Ehsan, Iannaccone, Alessandro, Williams, Lloyd B., Sobrin, Lucia, Brooks, Brian P., Sen, H. Nida, Hufnagel, Robert B., Kastner, Daniel L., and Kodati, Shilpa

Subjects

*RETINAL degeneration, *OPTIC nerve, *RETINAL diseases, *MYELOFIBROSIS, *AUTOINFLAMMATORY diseases, *IRIDOCYCLITIS, *FLUORESCENCE angiography

Abstract

We aimed to characterize the ocular phenotype of patients with ROSAH (retinal dystrophy, optic nerve edema, splenomegaly, anhidrosis, and headache) syndrome and their response to therapy. Single-center observational case study. Eleven patients with a diagnosis of ROSAH syndrome and mutation in ALPK1 were included. Patients with molecularly confirmed ROSAH syndrome underwent ophthalmic evaluation, including visual acuity testing, slit-lamp and dilated examinations, color fundus and autofluorescence imaging, fluorescein angiography, OCT, and electrophysiologic testing. Visual acuity, electrophysiology, fluorescein angiography, and OCT findings. Eleven individuals (6 female and 5 male patients) from 7 families ranging in age from 7.3 to 60.2 years at the time of the initial evaluation were included in this study. Seven patients were followed up for a mean of 2.6 years (range, 0.33–5.0 years). Best-corrected visual acuity at baseline ranged from 20/16 to no light perception. Variable signs or sequelae of intraocular inflammation were observed in 9 patients, including keratic precipitates, band keratopathy, trace to 2+ anterior chamber cells, cystoid macular edema, and retinal vasculitis on fluorescein angiography. Ten patients were observed to show optic disc elevation and demonstrated peripapillary thickening on OCT. Seven patients showed retinal degeneration consistent with a cone–rod dystrophy, with atrophy tending to involve the posterior pole and extending peripherally. One patient with normal electroretinography findings and visual evoked potential was found to have decreased Arden ratio on electro-oculography. Leveraging insights from the largest single-center ROSAH cohort described to date, this study identified 3 main factors as contributing to changes in visual function of patients with ROSAH syndrome: optic nerve involvement; intraocular inflammation, including cystoid macular edema; and retinal degeneration. More work is needed to determine how to arrest the progressive vision loss associated with ROSAH syndrome. Proprietary or commercial disclosure may be found after the references. [ABSTRACT FROM AUTHOR]

Published

2023

9. Oral cysteamine bitartrate and N-acetylcysteine for patients with infantile neuronal ceroid lipofuscinosis: a pilot study.

Author

Levin, Sondra W., Baker, Eva H., Zein, Wadih M., Zhongjian Zhang, Quezado, Zenaide M. N., Ning Miao, Gropman, Andrea, Griffin, Kurt J., Bianconi, Simona, Chandra, Goutam, Khan, Omar I., Caruso, Rafael C., Aiyi Liu, and Mukherjee, Anil B.

Subjects

*HEALTH outcome assessment, *NEURODEGENERATION, *THERAPEUTICS, *LYSOSOMAL storage diseases, *NEURONAL ceroid-lipofuscinosis, *GENETIC mutation, *CHROMOSOME abnormalities, *CYSTEAMINE, *ACETYLCYSTEINE

Abstract

Background: Infantile neuronal ceroid lipofuscinosis is a devastating neurodegenerative lysosomal storage disease caused by mutations in the gene (CLN1 or PPT1) encoding palmitoyl-protein thioesterase-1 (PPT1). We have previously reported that phosphocysteamine and N-acetylcysteine mediate ceroid depletion in cultured cells from patients with this disease. We aimed to assess whether combination of oral cysteamine bitartrate and N-acetylcysteine is beneficial for patients with neuronal ceroid lipofuscinosis. Methods: Children between 6 months and 3 years of age with infantile neuronal ceroid lipofuscinosis with any two of the seven most lethal PPT1 mutations were eligible for inclusion in this pilot study. All patients were recruited from physician referrals. Patients received oral cysteamine bitartrate (60 mg/kg per day) and N-acetylcysteine (60 mg/kg per day) and were assessed every 6-12 months until they had an isoelectric electroencephalogram (EEG, attesting to a vegetative state) or were too ill to travel. Patients were also assessed by electroretinography, brain MRI and magnetic resonance spectroscopy (MRS), and electron microscopic analyses of leukocytes for granular osmiophilic deposits (GRODs). Children also underwent physical and neurodevelopmental assessments on the Denver scale. Outcomes were compared with the reported natural history of infantile neuronal ceroid lipofuscinosis and that of affected older siblings. This trial is registered with ClinicalTrials.gov, number NCT00028262. Findings: Between March 14, 2001, and June 30, 2012, we recruited ten children with infantile neuronal ceroid lipofuscinosis; one child was lost to follow-up after the first visit and nine patients (five girls and four boys) were followed up for 8 to 75 months. MRI showed abnormalities similar to those in previous reports; brain volume and N-acetyl aspartic acid (NAA) decreased steadily, but no published quantitative MRI or MRS studies were available for comparison. None of the children acquired new developmental skills, and their retinal function decreased progressively. Average time to isoelectric EEG (52 months, SD 13) was longer than reported previously (36 months). At the first follow-up visit, peripheral leukocytes in all nine patients showed virtually complete depletion of GRODs. Parents and physicians reported less irritability, improved alertness, or both in seven patients. No treatment-related adverse events occurred apart from mild gastrointestinal discomfort in two patients, which disappeared when liquid cysteamine bitartrate was replaced with capsules. Interpretation: Our findings suggest that combination therapy with cysteamine bitartrate and N-acetylcysteine is associated with delay of isoelectric EEG, depletion of GRODs, and subjective benefits as reported by parents and physicians. Our systematic and quantitative report of the natural history of patients with infantile neuronal ceroid lipofuscinosis provides a guide for future assessment of experimental therapies. Funding: National Institutes of Health. [ABSTRACT FROM AUTHOR]

Published

2014

10. DICER1 Syndrome: Characterization of the Ocular Phenotype in a Family-Based Cohort Study.

Author

Huryn, Laryssa A., Turriff, Amy, Harney, Laura A., Carr, Ann Garrity, Chevez-Barrios, Patricia, Gombos, Dan S., Ram, Radha, Hufnagel, Robert B., Hill, D. Ashley, Zein, Wadih M., Schultz, Kris Ann P., Bishop, Rachel, and Stewart, Douglas R.

Subjects

*NATIONAL competency-based educational tests, *GENETIC testing, *INTRACRANIAL pressure, *PROLIFERATIVE vitreoretinopathy, *VISUAL fields, *BIOFLUORESCENCE

Abstract

Purpose To characterize the ocular phenotype of DICER1 syndrome. Design Prospective, single-center, case-control study. Participants One hundred three patients with an identified germline pathogenic DICER1 variant (DICER1 carriers) and 69 family control participants underwent clinical and ophthalmic examination at the National Institutes of Health between 2011 and 2016. Methods All participants were evaluated with a comprehensive ophthalmic examination, including best-corrected visual acuity, slit-lamp biomicroscopy, and a dilated fundus examination. A subset of patients returned for a more detailed evaluation including spectral-domain OCT, color fundus photography, fundus autofluorescence imaging, visual field testing, full-field electroretinography, and genetic testing for inherited retinal degenerative diseases. Main Outcome Measures Visual acuity and examination findings. Results Most DICER1 carriers (97%) maintained a visual acuity of 20/40 or better in both eyes. Twenty-three DICER1 carriers (22%) showed ocular abnormalities compared with 4 family controls (6%; P = 0.005). These abnormalities included retinal pigment abnormalities (n = 6 [5.8%]), increased cup-to-disc ratio (n = 5 [4.9%]), optic nerve abnormalities (n = 2 [1.9%]), epiretinal membrane (n = 2 [1.9%]), and drusen (n = 2 [1.9%]). Overall, we observed a significant difference (P = 0.03) in the rate of retinal abnormalities in DICER1 carriers (n = 11 [11%]) versus controls (n = 1 [1.5%]). One patient demonstrated an unexpected diagnosis of retinitis pigmentosa with a novel variant of unknown significance in PRPF31 , and 1 showed optic nerve elevation in the setting of increased intracranial pressure (ICP) of unclear cause. Three patients (3%) demonstrated DICER1 -related ciliary body medulloepithelioma (CBME), 2 of which were identified during routine examination, a higher rate than that reported previously. Conclusions Ophthalmologists should be aware of the ophthalmic manifestations of DICER1 syndrome, and individuals and families should be counseled on the potential signs and symptoms. We recommend that children with a germline pathogenic variant in DICER1 , especially those younger than 10 years, undergo annual dilated ophthalmic examination, looking for evidence of CBME, signs of increased ICP, and perhaps changes in the retinal pigment epithelium. [ABSTRACT FROM AUTHOR]

Published

2019

11. Ocular and Systemic Findings in Adults with Uveal Coloboma.

Author

Daich Varela, Malena, Huryn, Laryssa A., Hufnagel, Robert B., Zein, Wadih M., Blain, Delphine, and Brooks, Brian P.

Subjects

*CORNEAL dystrophies, *ADULTS, *STRABISMUS

Published

2020

12. Lines of Blaschko and Choroideremia

Author

MacDonald, Ian M., Sui, Ruifang, and Zein, Wadih

Published

2009

13. Ophthalmic Manifestations and Long-Term Visual Outcomes in Patients with Cobalamin C Deficiency.

Author

Brooks, Brian P., Thompson, Amy H., Sloan, Jennifer L., Manoli, Irini, Carrillo-Carrasco, Nuria, Zein, Wadih M., and Venditti, Charles P.

Subjects

*VITAMIN B12 deficiency, *ELECTRORETINOGRAPHY, *OPTICAL coherence tomography, *RETROSPECTIVE studies, *SCIENTIFIC observation, *HEALTH outcome assessment, *DIAGNOSIS

Abstract

Purpose To explore the ocular manifestations of cobalamin C ( cblC ) deficiency, an inborn error of intracellular vitamin B12 metabolism. Design Retrospective, observational case series. Participants Twenty-five cblC patients underwent clinical and ophthalmic examination at the National Institutes of Health between August 2004 and September 2012. Patient ages ranged from 2 to 27 years at last ophthalmic visit, and follow-up ranged from 0 to 83 months (median, 37 months; range, 13–83 months) over a total of 69 visits. Methods Best-corrected visual acuity, slit-lamp biomicroscopy, dilated fundus examination, wide-field photography, fundus autofluorescence imaging, sedated electroretinography, optical coherence tomography, genetics and metabolite assessment. Main Outcome Measures Visual acuity and presence and degree of retinal degeneration and optic nerve pallor. Results Nystagmus (64%), strabismus (52%), macular degeneration (72%), optic nerve pallor (68%), and vascular changes (64%) were present. c.271dupA (p.R91KfsX14) homozygous patients (n = 14) showed early and extensive macular degeneration. Electroretinography showed that scotopic and photopic responses were reduced and delayed, but were preserved remarkably in some patients despite severe degeneration. Optical coherence tomography images through the central macular lesion of a patient with severe retinal degeneration showed extreme thinning, some preservation of retinal lamination, and nearly complete loss of the outer nuclear layer. Despite hyperhomocysteinemia, no patients exhibited lens dislocation. Conclusions This longitudinal study reports ocular outcomes in the largest group of patients with cblC deficiency systematically examined at a single center over an extended period. Differences in progression and severity of macular degeneration, optic nerve pallor, and vascular attenuation between homozygous c.271dupA (p.R91KfsX14) patients and compound heterozygotes were noted. The pace and chronicity of ophthalmic manifestations lacked strict correlation to metabolic status as measured during visits. Prenatal or early treatment, or both, may have mitigated ocular disease, leading to better functional acuity, but patients still progressed to severe macular degeneration. The effects of prenatal or early treatment, or both, in siblings; the manifestation of severe disease in infancy; the presence of comorbid developmental abnormalities; and the possible laminar structural defect noted in many patients are findings showing that cblC deficiency displays a developmental as well as a degenerative ocular phenotype. [ABSTRACT FROM AUTHOR]

Published

2016

14. Systemic Diagnostic Testing in Patients With Apparently Isolated Uveal Coloboma.

Author

HUYNH, NANCY, BLAIN, DELPHINE, GLASER, TANYA, DOSS, E. LAUREN, ZEIN, WADIH M., LANG, DAVID M., BAKER, EVA H., HILL, SUVIMOL, BREWER, CARMEN C., KOPP, JEFFREY B., BARDAKJIAN, TANYA M., MAUMENEE, IRENE H., BATEMAN, BRONWYN J., and BROOKS, BRIAN P.

Subjects

*COLOBOMA, *UVEAL diseases, *CROSS-sectional method, *HEALTH outcome assessment, *ECHOCARDIOGRAPHY, *AUDIOLOGY, *DIAGNOSIS

Abstract

PURPOSE: To investigate the frequency and types of systemic findings in patients with apparently isolated uveal coloboma. DESIGN: Cross-sectional observational study. METHODS: SETTING: Single-center ophthalmic genetics clinic. STUDY POPULATION: Ninety-nine patients with uveal coloboma seen at theNationalEye Institute. OBSERVATIONAL PROCEDURE: Results of audiology testing, echocardiogram, brain magnetic resonance imaging, renal ultrasound, and total spine radiographs. MAIN OUTCOME MEASURE: Prevalence of abnormal findings on systemic testing. RESULTS: Uveal coloboma affected only the anterior segment in 8 patients, only the posterior segment in 23 patients, and both anterior and posterior segments in 68 patients. Best-corrected visual acuity (BCVA) of eyes with coloboma was ≥20/40 in 45% of eyes; 23% of eyes had BCVA of ≤20/400. The majority of patients (74%) had good vision (>20/60) in at least 1 eye. Ten of the 19 patients (53%) who underwent echocardiography had abnormalities, with ventral septal defects being the most prevalent. Abnormal findings were observed in 5 of 72 patients (7%) who had a renal ultrasound and in 5 of 29 patients (17%) who underwent a brain MRI. Audiology testing revealed abnormalities in 13 of 75 patients (17%), and spine radiographs showed anomalies in 10 of 77 patients (13%). Most findings required no acute intervention. CONCLUSIONS: Although some patients with coloboma had evidence of extraocular abnormalities, the majority of findings on routine clinical examination did not require acute intervention, but some warranted follow-up. Results from the systemic evaluation of patients with coloboma should be interpreted with caution and in view of their clinical context. [ABSTRACT FROM AUTHOR]

Published

2013

15. Ocular Manifestations of Xeroderma Pigmentosum: Long-Term Follow-up Highlights the Role of DNA Repair in Protection from Sun Damage.

Author

Brooks, Brian P., Thompson, Amy H., Bishop, Rachel J., Clayton, Janine A., Chan, Chi-Chao, Tsilou, Ekaterini T., Zein, Wadih M., Tamura, Deborah, Khan, Sikandar G., Ueda, Takahiro, Boyle, Jennifer, Oh, Kyu-Seon, Imoto, Kyoko, Inui, Hiroki, Moriwaki, Shin-lchi, Emmert, Steffen, Ilif, Nicholas T., Bradford, Porcia, DiGiovanna, John J., and Kraemer, Kenneth H.

Subjects

*XERODERMA pigmentosum, *DNA repair, *OCULAR manifestations of general diseases, *FOLLOW-up studies (Medicine), *INFLAMMATION, *GENETIC mutation, *COCKAYNE syndrome

Abstract

Objective: Xeroderma pigmentosum (XP) is a rare autosomal recessive disease caused by mutations in DNA repair genes. Clinical manifestations of XP include mild to extreme sensitivity to ultraviolet radiation resulting in inflammation and neoplasia in sun-exposed areas of the skin, mucous membranes, and ocular surfaces. This report describes the ocular manifestations of XP in patients systematically evaluated in the Clinical Center at the National Institutes of Health. Design: Retrospective observational case series. Participants: Eighty-seven participants, aged 1.3 to 63.4 years, referred to the National Eye Institute (NEI) for examination from 1964 to 2011. Eighty-three patients had XP, 3 patients had XP/Cockayne syndrome complex, and 1 patient had XP/trichothiodystrophy complex. Methods: Complete age- and developmental stage-appropriate ophthalmic examination. Main Outcome Measures: Visual acuity; eyelid, ocular surface, and lens pathology; tear film and tear production measures; and cytologic analysis of conjunctival surface swabs. Results: Of the 87 patients, 91 % had at least 1 ocular abnormality. The most common abnormalities were conjunctivitis (51 %), corneal neovascularization (44%), dry eye (38%), corneal scarring (26%), ectropion (25%), blepharitis (23%), conjunctival melanosis (20%), and cataracts (14%). Thirteen percent of patients had some degree of visual axis impingement, and 5% of patients had no light perception in 1 or both eyes. Ocular surface cancer or a history of ocular surface cancer was present in 10% of patients. Patients with an acute sunburning skin phenotype were less likely to develop conjunctival melanosis and ectropion but more likely to develop neoplastic ocular surface lesions than nonburning patients. Some patients also showed signs of limbal stem cell deficiency. Conclusions: Our longitudinal study reports the ocular status of the largest group of patients with XP systematically examined at 1 facility over an extended period of time. Structural eyelid abnormalities, neoplasms of the ocular surface and eyelids, tear film and tear production abnormalities, ocular surface disease and inflammation, and corneal abnormalities were present in this population. Burning and nonburning patients with XP exhibit different rates of important ophthalmologic findings, including neoplasia. In addition, ophthalmic char-acteristics can help refine diagnoses in the case of XP complex phenotypes. DNA repair plays a major role in protection of the eye from sunlight-induced damage. [ABSTRACT FROM AUTHOR]

Published

2013

16. Ocular Manifestations of Trichothiodystrophy

Author

Brooks, Brian P., Thompson, Amy H., Clayton, Janine A., Chan, Chi-Chao, Tamura, Deborah, Zein, Wadih M., Blain, Delphine, Hadsall, Casey, Rowan, John, Bowles, Kristen E., Khan, Sikandar G., Ueda, Takahiro, Boyle, Jennifer, Oh, Kyu-Seon, DiGiovanna, John J., and Kraemer, Kenneth H.

Subjects

*OCULAR manifestations of general diseases, *DNA repair, *GENETIC disorders, *XERODERMA pigmentosum, *EYE movements, *CORNEA diseases

Abstract

Objective: Trichothiodystrophy (TTD) is a rare, autosomal recessive disorder characterized by sulfur-deficient brittle hair and multisystem abnormalities. Many TTD patients have a defect in known DNA repair genes. This report systematically evaluates the ocular manifestations of the largest-to-date cohort of TTD patients and xeroderma pigmentosum (XP)/TTD patients. Design: Case series. Participants: Thirty-two participants, ages 1 to 30 years, referred to the National Eye Institute for examination from 2001 to 2010; 25 had TTD and 7 had XP/TTD. Methods: Complete, age- and developmental stage-appropriate ophthalmic examination. Main Outcome Measures: Visual acuity (VA), best-corrected VA, ocular motility, state of the ocular surface and corneal endothelial cell density, corneal diameter, and lens assessment. Results: Developmental abnormalities included microcornea (44% TTD), microphthalmia (8% TTD, 14% XP/TTD), nystagmus (40% TTD), and infantile cataracts (56% TTD, 86% XP/TTD). Corrective lenses were required by 65% of the participants, and decreased best-corrected VA was present in 28% of TTD patients and 71% of XP/TTD patients. Degenerative changes included dry eye (32% TTD, 57% XP/TTD) and ocular surface disease identified by ocular surface staining with fluorescein (32% TTD) that usually are exhibited by much older patients in the general population. The 2 oldest TTD patients exhibited clinical signs of retinal/macular degeneration. Four XP/TTD patients presented with corneal neovascularization. Conclusions: These TTD and XP/TTD study participants had a wide variety of ocular findings including refractive error, infantile cataracts, microcornea, nystagmus, and dry eye/ocular surface disease. Although many of these can be ascribed to abnormal development—likely owing to abnormalities in basal transcription of critical genes—patients may also have a degenerative course. Financial Disclosure(s): Proprietary or commercial disclosures may be found after the references. [Copyright &y& Elsevier]

Published

2011