Your search keyword '"Albinism, Ocular genetics"' showing total 184 results

1. Clinical and mutational characteristics of oculocutaneous albinism type 7.

Author

Kruijt CC, de Wit GC, van Minderhout HM, Schalij-Delfos NE, and van Genderen MM

Subjects

Humans, Retina, Mutation, Vision Disorders, Albinism, Ocular diagnosis, Albinism, Ocular genetics, Albinism, Oculocutaneous diagnosis, Albinism, Oculocutaneous genetics, Nystagmus, Pathologic, Hypopigmentation

Abstract

The purpose of this paper is to expand on the phenotype of oculocutaneous albinism type 7 (OCA7). We described three patients with OCA7: two from a consanguineous family of Kurdish origin and one patient of Dutch origin. We compared them with all patients described to date in the literature. All newly described patients had severely reduced visual acuity (VA), nystagmus, hypopigmentation of the fundus, severe foveal hypoplasia, and chiasmal misrouting. None had iris translucency. All patients had normal pigmentation of skin and hair. We found one novel mutation in the Dutch patient: c.565G > A; p.(Gly189Ser). We compared our patients to the 15 described in the literature to date. All 18 patients had substantially pigmented skin and hair, very poor VA (0.4-1.3 logMAR), nystagmus, (mild) ocular hypopigmentation, foveal hypoplasia, and misrouting. Although pigmentation levels were mildly affected in OCA7, patients had a severe ocular phenotype with VA at the poorer end of the albinism spectrum, severe foveal hypoplasia, and chiasmal misrouting. OCA7 patients had a phenotype restricted to the eyes, and similar to that of X-linked ocular albinism. We therefore propose to rename the disorder in ocular albinism type 2. Unfolding the role of LRMDA in OCA7, may bring us a step closer in identifying the responsible factors for the co-occurrence of foveal hypoplasia and misrouting., (© 2024. The Author(s).)

Published

2024

2. Case series: Fundus autofluorescence abnormalities in a family of ocular albinism carriers.

Author

Gleason S and Bass SJ

Subjects

Humans, Retina, Fundus Oculi, Electroretinography, Tomography, Optical Coherence, Fluorescein Angiography, Albinism, Ocular diagnosis, Albinism, Ocular genetics

Abstract

Significance: Carriers of ocular albinism demonstrate signs of retinal mosaicism with unique features on fundus autofluorescence testing, which differentiate this condition from other x-linked retinal disorders in carrier patients. Distinctive findings include a mud-splattered fundus with peripheral hyperpigmented streaks, which correlate with areas of hyperautofluorescence and hypoautofluorescence., Purpose: This is the first reported case series of a family that demonstrates diagnostic retinal and fundus autofluorescence abnormalities related to retinal mosaicism in three sisters who were unaware they were carriers of ocular albinism type 1. Multimodal imaging, electrodiagnostic testing, and genetic testing can be used to confirm the diagnosis and differentiate this clinical presentation from other sight-threatening hereditary retinal diseases., Case Reports: Three sisters, aged 21, 17, and 13 years, were referred to determine the cause of abnormal retinal pigmentation. All presented with normal vision, and anterior segment examination was unremarkable without iris transillumination. They denied family history of ocular disease. Fundus examination of all three sisters revealed a mud-splattered pattern of pigmentation in the posterior pole and radial pigmentary streaks. Fundus autofluorescence showed a pattern of hyperautofluorescence and hypoautofluorescence corresponding to this pigmentary pattern. Spectral domain optical coherence tomography, electro-oculogram, and electroretinogram were normal in all three sisters. Genetic testing of their father, who was unaware of any disorder, tested positive for ocular albinism., Conclusions: Ocular albinism carriers have abnormal retinal pigmentation in a characteristic pattern. Fundus autofluorescence shows a correlative pattern that can confirm carrier status of ocular albinism in individuals unaware of their status and rule out other retinal degenerations., Competing Interests: Conflict of Interest Disclosure: None of the authors have reported a financial conflict of interest., (Copyright © 2024 American Academy of Optometry.)

Published

2024

3. Novel Variants of HPS6 Cause Suspected Ocular Albinism: A Report of 2 Cases and the Profile of HPS6 Variants.

Author

Zhou B, Yang J, Bai Y, Li Y, Chen S, Chen X, Zhang N, Cao Z, Zhu Y, and Xu Y

Subjects

Humans, Retrospective Studies, Phenotype, Proteins genetics, Mutation, Pedigree, Intracellular Signaling Peptides and Proteins genetics, Albinism, Ocular diagnosis, Albinism, Ocular genetics, Hermanski-Pudlak Syndrome diagnosis, Hermanski-Pudlak Syndrome genetics

Abstract

Introduction: Hermansky-Pudlak syndrome (HPS) is a rare autosomal-recessive disease characterized by ocular albinism (OA) or oculocutaneous albinism (OCA), platelet dysfunction, and other symptoms. This study aimed to analyze the molecular defect in two Chinese families with suspected OA, as well as to investigate the profile of HPS6 variants and their genotype-phenotype correlations., Methods: Seven members from two families were recruited and underwent clinical ophthalmologic examinations. The genomic DNA was extracted from peripheral blood leukocytes. Whole-exome sequencing was performed on the proband of family JX. The single coding exon of HPS6 was directly Sanger sequenced based on PCR amplification in all available family members. An additional 46 probands from families or sporadic cases with the pathogenic variants of HPS6 reported in the literature were reviewed., Results: We identified two different compound heterozygous truncating variants of HPS6 in probands with suspected OA from two independent families. The proband of family JX had c.1674dup and c.503-504del variants, and the other proband from family CZ had a nonsense variant of c.1114C>T and a frameshift variant of c.1556del. Among them, c.1674dup and c.1556del variants in HPS6 have not been reported previously. Therefore, our patients were diagnosed as HPS6 disease by molecular diagnostics. In the retrospective cohort of HPS6 patients, we delineated the profile of HPS6 variants and revealed a significant overlap between CpG islands and the variants of HPS6, suggesting a potential link between DNA methylation and HPS6 variants. We also observed a spatial aggregation of the variants in 3D structure of HPS6 protein, implying the possible functional significance of these structural regions. In addition, we did not find any significant genotype-phenotype correlation of HPS6, and neither did we observe a correlation between the truncation length of the HPS6 protein and the phenotype of HPS6 disease., Conclusion: Our research expands the spectrum of HPS6 variants, providing a comprehensive delineation of their profile and systematically investigating genotype-phenotype correlations in HPS6. These findings could offer potentially valuable clues for investigating the molecular mechanism underlying HPS6 pathogenesis, as well as aiding the clinical diagnosis of HPS6 patients and improving disease prognosis., (© 2023 The Author(s). Published by S. Karger AG, Basel.)

Published

2024

4. GPR143 mutations in an X-linked infantile nystagmus syndrome cohort in Southeast China.

Author

Xu J, Zheng Y, Cheng L, Sun H, Yu X, Gu F, and Song E

Subjects

Humans, Albinism, Ocular genetics, Albinism, Ocular diagnosis, Iris, Mutation genetics, Pedigree, Eye Proteins genetics, Genetic Diseases, X-Linked, Membrane Glycoproteins genetics, Nystagmus, Congenital genetics, Nystagmus, Congenital diagnosis

Abstract

Purpose: Infantile nystagmus syndrome (INS), or congenital nystagmus (CN), refers to a group of ocular motor disorders characterized by rapid to-and-fro oscillations of the eyes. GPR143 is the causative gene of ocular albinism type 1 (OA1), which is a special type of INS that manifests as reduced vision, nystagmus, and iris and fundus hypopigmentation. Here, we explored the genetic spectrum of INS and the genotype-phenotype correlation., Methods: A total of 98 families with INS from Southeast China were recruited for this study. A sample from each participant was subjected to PCR-based DNA direct sequencing of GPR143 . Varied bioinformatics analysis was subsequently used in a mutation assessment. All participants received detailed ophthalmic examinations., Results: Genetic analysis identified 11 GPR143 mutations in 11.2% (11/98) of the X-linked INS families. These included seven novel mutations (c.899 C>T, c.886-2 A>G, c.1A>G, c.633_643del CCTGTTCCAAA, c.162_198delCGCGGGCCCCGGGTCCCCCGCGACGTCCCCGCCGGCC, c.628C>A, and c.178_179insGGGTCCC) and four known mutations. Patients who carried a GPR143 mutation were found to present a typical or atypical phenotype of OA1. All patients with GPR143 mutations manifested foveal hypoplasia; thus, about 45.8% (11/24) of the families with total X-linked INS exhibited foveal hypoplasia., Conclusions: We discovered seven novel mutations and four previously reported mutations of GPR143 in a cohort of families with X-linked INS and enlarged the Chinese genetic spectrum of INS. These findings offer new insights for developing genetic screening strategies and shed light on the importance of conducting genetic analysis in confirming the clinical diagnosis in unresolved patients and atypical phenotypes., (Copyright © 2023 Molecular Vision.)

Published

2023

5. Determining a Worldwide Prevalence of Oculocutaneous Albinism: A Systematic Review.

Author

Kromberg JGR, Flynn KA, and Kerr RA

Subjects

Humans, Mutation, Prevalence, Phenotype, Albinism, Oculocutaneous epidemiology, Albinism, Oculocutaneous diagnosis, Albinism, Ocular epidemiology, Albinism, Ocular genetics

Abstract

Purpose: The aim of this systematic review was to investigate the available data on the epidemiology of oculocutaneous albinism (OCA) around the world, and to determine whether a generalizable, worldwide prevalence figure could be proposed., Methods: Extensive literature search strategies were conducted, interrogating PubMed, Scopus, and Web of Science, to locate relevant literature. Ultimately 34 studies reporting original data were included for analysis., Results: Findings showed that most data were outdated, and only 6 of 34 articles (18%) were published after 2010. There were few good studies with sound methodology and large, clearly defined population samples. Only a small proportion of countries worldwide (26/193 [13%]) have produced prevalence figures for OCA. By continent, African studies were disproportionately represented (15/34 [44%]). The highest prevalence rates (range, 1 in 22 to 1 in 1300; mean, 1 in 464) were reported in population isolates. The mean prevalence from four African countries was 1 in 4264 (range, 1 in 1755 to 1 in 7900). Prevalence for three countries in Europe (mean, 1 in 12,000; range, 1 in 10,000 to 1 in 15,000) may be underestimated, as the phenotype, in fair-skinned populations, may be missed or misdiagnosed as ocular albinism or isolated visual impairment. Population rates may vary depending on local cultural factors (e.g., consanguineous matings) and may change over time., Conclusions: The prevalence of OCA varies widely between continents and population groups, and it is often influenced by local factors. It was not possible, therefore, to determine a single, generalizable worldwide prevalence rate for OCA, although continental rates for Africa and Europe are useful.

Published

2023

6. Comments on: Choroidal and retinal thickness variations in ocular albinism.

Author

Gioia M, La Marca A, De Luca M, and De Bernardo M

Subjects

Humans, Retina, Visual Acuity, Choroid, Tomography, Optical Coherence, Albinism, Ocular diagnosis, Albinism, Ocular genetics

Abstract

Competing Interests: None

Published

2023

7. Response to comments on: Choroidal and retinal thickness variations in ocular albinism.

Author

Venkatesh R, Agrawal S, Reddy NG, Sridharan A, Ong J, Yadav NK, and Chhablani J

Subjects

Humans, Retina, Visual Acuity, Choroid, Albinism, Ocular diagnosis, Albinism, Ocular genetics

Abstract

Competing Interests: None

Published

2023

8. Ocular findings and a comparative study of hair, skin and iris color in Chinese patients with albinism.

Author

Arcot Sadagopan K, Teng CH, Hui G, and Lin DL

Subjects

Humans, East Asian People, Prospective Studies, Hair, Iris, Hermanski-Pudlak Syndrome diagnosis, Hermanski-Pudlak Syndrome genetics, Albinism, Oculocutaneous diagnosis, Albinism, Oculocutaneous genetics, Albinism, Albinism, Ocular diagnosis, Albinism, Ocular genetics

Abstract

Background: Oculocutaneous albinism (OCA) could be either non-syndromic or syndromic. There are significant challenges in clinically recognizing and differentiating Hermansky-Pudlak syndrome (HPS) from non-syndromic OCA., Materials and Methods: In a prospective consecutive case series, 63 patients (less than 18 years old) with a molecular genetic diagnosis of albinism (except OCA1A ), Ocular albinism (OA) and Hermansky-Pudlak syndrome seen over a 3-year period were evaluated and analyzed. Hair colour, iris colour was graded, compared and correlated with the degree of fundus pigmentation and foveal development., Results: A total of 63 patients were evaluated. Forty-five patients had non-syndromic OCA (11 OCA1B, 24 OCA2, 9 OCA4, and 1 OCA6), 5 patients had OA and 13 patients had HPS. All 3 BLOC-related HPS categories were seen (1 with BLOC1, 7 with BLOC-2 and 5 with BLOC-3 related HPS). All patients with OA were hyperopic, had darker fundus pigmentation, but had poor foveal development. All HPS patients had lighter fundus pigmentation. The degree of fundus pigmentation correlated positively with the iris pigmentation and also with the foveal development only in OCA2., Conclusions: Careful observation of the phenotype by comparison of the skin, hair, iris colour, with the degree of fundus pigmentation and foveal development may help clinically differentiate HPS from OCA patients of Chinese ethnicity even in the absence of any bleeding tendency.

Published

2023

9. Diagnostic Yield of Genetic Testing for Ocular and Oculocutaneous Albinism in a Diverse United States Pediatric Population.

Author

Chan KS, Bohnsack BL, Ing A, Drackley A, Castelluccio V, Zhang KX, Ralay-Ranaivo H, and Rossen JL

Subjects

Child, Humans, Retrospective Studies, Mutation, Membrane Transport Proteins genetics, Genetic Testing, Albinism, Ocular genetics, Hermanski-Pudlak Syndrome genetics

Abstract

The diagnostic yield of genetic testing for ocular/oculocutaneous albinism (OA/OCA) in a diverse pediatric population in the United States (U.S.) is unclear. Phenotypes of 53 patients who presented between 2006-2022 with OA/OCA were retrospectively correlated with genetic testing results. Genetic diagnostic yield was defined as detection of pathogenic/likely pathogenic variant(s) matching the anticipated inheritance for that gene-disease relationship. Variant reclassifications of those with variants of uncertain significance (VUS) and without positive diagnostic yield were completed. Overall initial genetic diagnostic yield of OA/OCA was 66%. There was no significant difference ( p = 0.59) between race and ethnicities (Black (78%), White (59%), Hispanic/Latino (64%)); however, the diagnostic yield of OA (33%) was significantly lower ( p = 0.007) than OCA (76%). Causative variants in OCA2 (28%) and TYR (20%) were most common. Further, Hermansky-Pudlak syndrome variants were identified in 9% of patients. Re-classification of VUS in non-diagnostic cases resulted in genetic diagnoses for 29% of individuals and increased overall diagnostic yield to 70% of all subjects. There is a high diagnostic yield of genetic testing of patients overall with OA/OCA in a diverse U.S. based pediatric population. Presence or absence of cutaneous involvement of albinism significantly affects genetic diagnostic yield.

Published

2023

10. Foveal hypoplasia in parents of patients with albinism.

Author

Lejoyeux R, Alonso AS, Lafolie J, Michaud V, Lasseaux E, Vasseur V, Derrien S, Robert MP, Le Mer Y, Tadayoni R, Arveiler B, and Mauget-Faÿsse M

Subjects

Humans, Fovea Centralis abnormalities, Retina, Vision Disorders diagnosis, Tomography, Optical Coherence methods, Albinism genetics, Albinism, Oculocutaneous diagnosis, Albinism, Oculocutaneous genetics, Albinism, Ocular diagnosis, Albinism, Ocular genetics

Abstract

Background: Albinism is a group of genetic disorders characterized by general skin and retinal hypopigmentation. It is in most cases an autosomal recessive condition. Foveal hypoplasia (FH) is one of the main criteria for the diagnosis of albinism. The aim of this study was to analyze the macular profile of the parents of patients with albinism., Methods: This study included a case series of 27 patients with albinism seen in Rothschild Foundation between April 2017 and February 2020. Spectral-domain optical coherence tomography (SD-OCT) and OCT angiography (OCT-A) were performed in every patient when possible and in every available parents. FH was graded according to Thomas' classification based on OCT. Next generation sequencing-based gene panel testing was performed in parents and children when a FH was detected on OCT in a parent., Results: Twenty-seven patients with albinism were examined. Nine parents had FH based on the OCT B-scan (33%). In parents without FH based on the SD-OCT B-scan (67%), OCT-A showed a reduced avascular zone in the deep vascular plexus in 4 parents. Six parents carried variants that could explain their phenotype, including TYR R402Q hypomorphic alleles., Conclusion: This study showed the presence of FH in parents of patients with albinism, and aimed to genetically explain this phenotype.

Published

2022

11. Macular Findings in Carriers of Ocular Albinism With a Novel GPR143 Mutation.

Author

Nanda T, Coombs A, Shi A, and Baumal CR

Subjects

Eye Proteins genetics, Female, Humans, Membrane Glycoproteins genetics, Mutation, Albinism, Ocular diagnosis, Albinism, Ocular genetics

Abstract

This case series details macular findings in three female siblings who were found to be carriers of a previously unreported splice mutation in GPR143 (X-linked ocular albinism [OA1]). Presumed lyonization is responsible for both the subtle and varied findings in OA1 carriers, even among siblings, and especially in patients with darker skin pigmentation. In this series, we used green-light autofluorescence to reveal subtle subfoveal involvement and used optical coherence tomography angiography to uncover previously unreported narrowing of the foveal avascular zone, consistent with foveal hypoplasia. [ Ophthalmic Surg Lasers Imaging Retina 2022;53:460-463.] .

Published

2022

12. CRISPR-AsCas12a Efficiently Corrects a GPR143 Intronic Mutation in Induced Pluripotent Stem Cells from an Ocular Albinism Patient.

Author

Torriano S, Baulier E, Garcia Diaz A, Corneo B, and Farber DB

Subjects

CRISPR-Cas Systems genetics, Eye Proteins genetics, Eye Proteins metabolism, Gene Editing, Humans, Membrane Glycoproteins genetics, Membrane Glycoproteins metabolism, Mutation, Albinism, Ocular genetics, Albinism, Ocular metabolism, Albinism, Ocular pathology, Induced Pluripotent Stem Cells metabolism

Abstract

Mutations in the GPR143 gene cause X-linked ocular albinism type 1 (OA1), a disease that severely impairs vision. We recently generated induced pluripotent stem cells (iPSCs) from skin fibroblasts of an OA1 patient carrying a point mutation in intron 7 of GPR143 . This mutation activates a new splice site causing the incorporation of a pseudoexon. In this study, we present a high-performance CRISPR-Cas ribonucleoprotein strategy to permanently correct the GPR143 mutation in these patient-derived iPSCs. Interestingly, the two single-guide RNAs available for SpCas9 did not allow the cleavage of the target region. In contrast, the cleavage achieved with the CRISPR-AsCas12a system promoted homology-directed repair at a high rate. The CRISPR-AsCas12a-mediated correction did not alter iPSC pluripotency or genetic stability, nor did it result in off-target events. Moreover, we highlight that the disruption of the pathological splice site caused by CRISPR-AsCas12a-mediated insertions/deletions also rescued the normal splicing of GPR143 and its expression level.

Published

2022

13. Genotypic and Phenotypic Spectrum of Foveal Hypoplasia: A Multicenter Study.

Author

Kuht HJ, Maconachie GDE, Han J, Kessel L, van Genderen MM, McLean RJ, Hisaund M, Tu Z, Hertle RW, Gronskov K, Bai D, Wei A, Li W, Jiao Y, Smirnov V, Choi JH, Tobin MD, Sheth V, Purohit R, Dawar B, Girach A, Strul S, May L, Chen FK, Heath Jeffery RC, Aamir A, Sano R, Jin J, Brooks BP, Kohl S, Arveiler B, Montoliu L, Engle EC, Proudlock FA, Nishad G, Pani P, Varma G, Gottlob I, and Thomas MG

Subjects

Cytoskeletal Proteins, Fovea Centralis abnormalities, Humans, Membrane Proteins, Vision Disorders diagnosis, Albinism, Albinism, Ocular diagnosis, Albinism, Ocular genetics, Albinism, Oculocutaneous diagnosis, Albinism, Oculocutaneous genetics, Color Vision Defects diagnosis, Color Vision Defects genetics

Abstract

Purpose: To characterize the genotypic and phenotypic spectrum of foveal hypoplasia (FH)., Design: Multicenter, observational study., Participants: A total of 907 patients with a confirmed molecular diagnosis of albinism, PAX6, SLC38A8, FRMD7, AHR, or achromatopsia from 12 centers in 9 countries (n = 523) or extracted from publicly available datasets from previously reported literature (n = 384)., Methods: Individuals with a confirmed molecular diagnosis and availability of foveal OCT scans were identified from 12 centers or from the literature between January 2011 and March 2021. A genetic diagnosis was confirmed by sequence analysis. Grading of FH was derived from OCT scans., Main Outcome Measures: Grade of FH, presence or absence of photoreceptor specialization (PRS+ vs. PRS-), molecular diagnosis, and visual acuity (VA)., Results: The most common genetic etiology for typical FH in our cohort was albinism (67.5%), followed by PAX6 (21.8%), SLC38A8 (6.8%), and FRMD7 (3.5%) variants. AHR variants were rare (0.4%). Atypical FH was seen in 67.4% of achromatopsia cases. Atypical FH in achromatopsia had significantly worse VA than typical FH (P < 0.0001). There was a significant difference in the spectrum of FH grades based on the molecular diagnosis (chi-square = 60.4, P < 0.0001). All SLC38A8 cases were PRS- (P = 0.003), whereas all FRMD7 cases were PRS+ (P < 0.0001). Analysis of albinism subtypes revealed a significant difference in the grade of FH (chi-square = 31.4, P < 0.0001) and VA (P = 0.0003) between oculocutaneous albinism (OCA) compared with ocular albinism (OA) and Hermansky-Pudlak syndrome (HPS). Ocular albinism and HPS demonstrated higher grades of FH and worse VA than OCA. There was a significant difference (P < 0.0001) in VA between FRMD7 variants compared with other diagnoses associated with FH., Conclusions: We characterized the phenotypic and genotypic spectrum of FH. Atypical FH is associated with a worse prognosis than all other forms of FH. In typical FH, our data suggest that arrested retinal development occurs earlier in SLC38A8, OA, HPS, and AHR variants and later in FRMD7 variants. The defined time period of foveal developmental arrest for OCA and PAX6 variants seems to demonstrate more variability. Our findings provide mechanistic insight into disorders associated with FH and have significant prognostic and diagnostic value., (Copyright © 2022 American Academy of Ophthalmology. Published by Elsevier Inc. All rights reserved.)

Published

2022

14. Neurodevelopmental Profile in Children Affected by Ocular Albinism.

Author

Galli J, Loi E, Morandi A, Scaglioni V, Rossi A, Molinaro A, Pasini N, Semeraro F, Ruberto G, and Fazzi E

Subjects

Child, Preschool, Evoked Potentials, Visual, Eye Proteins genetics, Humans, Membrane Glycoproteins genetics, Retrospective Studies, Albinism, Ocular genetics

Abstract

Aim: The aim of this study was to detail the neurodevelopmental profile of subjects affected by ocular albinism (OA) and to collect data on GPR143 gene analysis., Design: The design of the study involves a retrospective longitudinal observational case series., Methods: We collected data on the neurodevelopmental profile of 13 children affected by OA from clinical annual assessments conducted for a period of 6 years after the first evaluation. We described visual profile, neuromotor development and neurological examination, cognitive profile, communication and language skills and behavioral characteristics. The GPR143 gene analysis was performed as well., Results: Children presented a variable combination of ocular and oculomotor disorders unchanged during the follow-up, a deficit in visual acuity and in contrast sensitivity that progressively improved. Abnormalities in pattern visual evoked potential were found. No deficits were detected at neurological examination and neuromotor development except for a mild impairment in hand-eye coordination observed in five cases. A language delay was observed in five cases, two of whom had also a developmental quotient delay at 2 years evolving to a borderline/deficit cognitive level at preschool age, difficulties in adaptive behavior and autistic-like features were found. Mutations in the GPR143 gene were identified in the two patients who presented the most severe clinical phenotype., Conclusion: Children with OA may share, in addition to a variable combination of ocular signs and symptoms, a neurodevelopment impairment regarding mostly the cognitive, communicative, and social area, especially those with GPR143 mutation., Competing Interests: None declared., (Thieme. All rights reserved.)

Published

2022

15. Strikingly High Myopia in Aland Island Eye Disease.

Author

Lai WC, Etter J, and Schechet SA

Subjects

Albinism, Ocular genetics, Calcium Channels, L-Type genetics, Cataract diagnosis, Genetic Diseases, X-Linked genetics, Genetic Testing, Humans, Male, Middle Aged, Mutation, Nystagmus, Pathologic diagnosis, Visual Acuity physiology, Vitreous Body pathology, Albinism, Ocular diagnosis, Genetic Diseases, X-Linked diagnosis, Myopia, Degenerative diagnosis

Published

2022

16. GPR143 genotypic and ocular phenotypic characterisation in a Chinese cohort with ocular albinism.

Author

Zhong J, You B, Xu K, Zhang X, Xie Y, and Li Y

Subjects

Adolescent, Adult, Albinism, Ocular diagnosis, Albinism, Ocular physiopathology, Albinism, Oculocutaneous, Child, Child, Preschool, China epidemiology, Cross-Sectional Studies, Electroretinography, Female, Genetic Association Studies, High-Throughput Nucleotide Sequencing, Humans, Infant, Male, Middle Aged, Nystagmus, Congenital diagnosis, Nystagmus, Congenital genetics, Nystagmus, Congenital physiopathology, Pedigree, Retina physiology, Retrospective Studies, Slit Lamp Microscopy, Tomography, Optical Coherence, Visual Acuity physiology, Albinism, Ocular genetics, Asian People genetics, Eye Proteins genetics, Membrane Glycoproteins genetics, Mutation genetics

Abstract

Purpose: Ocular albinism type I (OA1) is caused by mutations in the GPR143 gene. The purpose of this study was to describe the clinical and genetic findings in 13 patients from 12 unrelated Chinese pedigrees with a pathogenic variant of the GPR143 gene., Methods: Most patients underwent clinical examination, including best-corrected visual acuity (BCVA), slit-lamp biomicroscopy, fundus examination, spectral domain optical coherence tomography, and full-field electroretinograms (ERG). A combination of molecular screening procedures, consisting of Sanger-DNA sequencing of GPR143 and targeted next-generation sequencing, was performed to identify each mutation. In silico programs were utilized to evaluate the pathogenicity of all the variants., Results: The 13 patients (mean age 21.75 ± 16.63 years, range 1-54 years) all presented with congenital nystagmus, different extents of visual impairment, and severe foveal hypoplasia. Their BCVA was between 0.05 and 0.3 (decimal notation). The patients and obligate carriers exhibited different extents of mild depigmentation of the iris and fundus. We detected 11 distinct mutations in this patient cohort, including 7 novel mutations. Most (82%) were null mutations and included frameshift indel, nonsense, splicing effect, and large genomic DNA deletions, while missense mutations only accounted for 18%., Conclusions: Patients with GPR143 mutations all have congenital nystagmus, visual impairment, and foveal hypoplasia, whereas hypopigmentation in their iris and fundus is mild. They exhibit no evident genotype-phenotype correlations. GPR143 mutation screening is very important for establishing a precise diagnosis and for providing genetic counseling for patients and their families.

Published

2021

17. Clinical utility gene card for oculocutaneous (OCA) and ocular albinism (OA)-an update.

Author

Aamir A, Kuht HJ, Grønskov K, Brooks BP, and Thomas MG

Subjects

Albinism, Ocular diagnosis, Albinism, Oculocutaneous diagnosis, Genetic Heterogeneity, Genetic Loci, Genetic Testing standards, Humans, Mutation, Sensitivity and Specificity, Albinism, Ocular genetics, Albinism, Oculocutaneous genetics, Genetic Testing methods

Published

2021

18. Genotype-phenotype associations in Danish patients with ocular and oculocutaneous albinism.

Author

Kessel L, Kjer B, Lei U, Duno M, and Grønskov K

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Albinism, Ocular diagnosis, Albinism, Oculocutaneous diagnosis, Child, Child, Preschool, Denmark, Eye Proteins genetics, Female, Genetic Association Studies, High-Throughput Nucleotide Sequencing, Humans, Male, Membrane Glycoproteins genetics, Membrane Transport Proteins genetics, Middle Aged, Monophenol Monooxygenase genetics, Mutation, Albinism, Ocular genetics, Albinism, Oculocutaneous genetics

Abstract

Background: The study aimed to describe genotype-phenotype associations in patients with oculocutaneous and ocular-only albinism and to evaluate a set of diagnostic criteria proposed recently by Kruijt et al., Materials and Methods: Genotype-phenotype associations in patients with a clinical diagnosis of albinism were studied based on imaging of hair and ocular features (nystagmus, iris color and translucency, fundus pigmentation and foveal development) and self-evaluated skin type. Patients were sub-grouped based on genetic findings., Results: Patients with biallelic variants in TYR (n = 29), OCA2 (n = 22), other albinism genes (n = 13) or monoallelic variants in GPR143 (n = 13) were included as were 15 patients with a pure clinical diagnosis but no genetic findings. In descending order the most common findings were: foveal hypoplasia (any hypoplasia 95.2%, severe 88.0%), nystagmus (93.5%), iris translucency (any translucency 80.2%, moderate to severe 31.5%), misrouting on VEP (80.0%): fundus hypopigmentation (any hypopigmentation: 75.8%, severe 30.1%), fair skin type (73.8%), blue irides (62.0%), blonde hair (57.5%), and unpigmented eye lashes (39.1%). There were no phenotypic differences between the different genetic subgroups of albinism but patients with a pathogenic haplotype in TYR in combination with a classic variant had less iris translucency than patients with two classic variants in TYR ., Conclusions: Ocular developmental features were the most common findings whereas phenotypic features related to pigmentation were less common findings but there were no genotype-phenotype correlations. All patients with a genetically confirmed diagnosis of albinism fulfilled the diagnostic criteria by Kruijt irrespective of genetic subtype.

Published

2021

19. Prospective Study of the Phenotypic and Mutational Spectrum of Ocular Albinism and Oculocutaneous Albinism.

Author

Chan HW, Schiff ER, Tailor VK, Malka S, Neveu MM, Theodorou M, and Moosajee M

Subjects

Adolescent, Adult, Albinism, Ocular genetics, Albinism, Oculocutaneous genetics, Child, Child, Preschool, Diagnosis, Differential, Female, Humans, Infant, Male, Pedigree, Phenotype, Prospective Studies, Whole Genome Sequencing methods, Young Adult, Albinism, Ocular diagnosis, Albinism, Oculocutaneous diagnosis, Genetic Testing methods, Mutation

Abstract

Albinism encompasses a group of hereditary disorders characterized by reduced or absent ocular pigment and variable skin and/or hair involvement, with syndromic forms such as Hermansky-Pudlak syndrome and Chédiak-Higashi syndrome. Autosomal recessive oculocutaneous albinism (OCA) is phenotypically and genetically heterogenous (associated with seven genes). X-linked ocular albinism (OA) is associated with only one gene, GPR143 . We report the clinical and genetic outcomes of 44 patients, from 40 unrelated families of diverse ethnicities, with query albinism presenting to the ocular genetics service at Moorfields Eye Hospital NHS Foundation Trust between November 2017 and October 2019. Thirty-six were children (≤ 16 years) with a median age of 31 months (range 2-186), and eight adults with a median age of 33 years (range 17-39); 52.3% ( n = 23) were male. Genetic testing using whole genome sequencing (WGS, n = 9) or a targeted gene panel ( n = 31) gave an overall diagnostic rate of 42.5% (44.4% (4/9) with WGS and 41.9% (13/31) with panel testing). Seventeen families had confirmed mutations in TYR ( n = 9), OCA2 , ( n = 4), HPS1 ( n = 1), HPS3 ( n = 1), HPS6 ( n = 1), and GPR143 ( n = 1). Molecular diagnosis of albinism remains challenging due to factors such as missing heritability. Differential diagnoses must include SLC38A8 -associated foveal hypoplasia and syndromic forms of albinism.

Published

2021

20. A Novel Splice-Site Variant in CACNA1F Causes a Phenotype Synonymous with Åland Island Eye Disease and Incomplete Congenital Stationary Night Blindness.

Author

Mahmood U, Méjécase C, Ali SMA, Moosajee M, and Kozak I

Subjects

Adolescent, Alleles, DNA Mutational Analysis, Electroretinography, Genetic Association Studies methods, Genetic Predisposition to Disease, Genetic Testing, Genotype, Humans, Male, Optical Imaging, Pedigree, Tomography, Optical Coherence, Albinism, Ocular diagnosis, Albinism, Ocular genetics, Calcium Channels, L-Type genetics, Eye Diseases, Hereditary diagnosis, Eye Diseases, Hereditary genetics, Genetic Diseases, X-Linked diagnosis, Genetic Diseases, X-Linked genetics, Mutation, Myopia diagnosis, Myopia genetics, Night Blindness diagnosis, Night Blindness genetics, Phenotype, RNA Splice Sites

Abstract

Background: CACNA1F -related disorders encompass progressive and non-progressive disorders, including Åland island eye disease and incomplete congenital stationary night blindness. These two X-linked disorders are characterized by nystagmus, color vision defect, myopia, and electroretinography (ERG) abnormalities. Ocular hypopigmentation and iris transillumination are reported only in patients with Åland island eye disease. Around 260 variants were reported to be associated with these two non-progressive disorders, with 19 specific to Åland island eye disease and 14 associated with both Åland island eye disease and incomplete congenital stationary night blindness. CACNA1F variants spread on the gene and further analysis are needed to reveal phenotype-genotype correlation., Case Report: A complete ocular exam and genetic testing were performed on a 13-year-old boy. A novel splice-site variant, c.4294-11C>G in intron 36 in CACNA1F , was identified at hemizygous state in the patient and at heterozygous state in his asymptomatic mother and explained the phenotype synonymous with Åland island eye disease and incomplete congenital stationary night blindness observed in the patient., Conclusion: We present a novel variant in the CACNA1F gene causing phenotypic and electrophysiologic findings indistinguishable from those of AIED/CSNB2A disease. This finding further expands the mutational spectrum and our knowledge of CACNA1F -related disease.

Published

2021

21. Comprehensive Geno- and Phenotyping in a Complex Pedigree Including Four Different Inherited Retinal Dystrophies.

Author

Birtel J, Gliem M, Hess K, Birtel TH, Holz FG, Zechner U, Bolz HJ, and Herrmann P

Subjects

Adolescent, Albinism, Ocular genetics, Child, Cone-Rod Dystrophies genetics, Eye Diseases, Hereditary genetics, Female, Fluorescein Angiography, Genetic Diseases, X-Linked genetics, Genetic Testing, High-Throughput Nucleotide Sequencing, Humans, Male, Middle Aged, Mutation, Myopia genetics, Night Blindness genetics, Parents, Pedigree, Phenotype, Polymorphism, Single Nucleotide, Sequence Analysis, DNA, ATP-Binding Cassette Transporters genetics, Albinism, Ocular diagnosis, Calcium Channels, L-Type genetics, Cone-Rod Dystrophies diagnosis, Eye Diseases, Hereditary diagnosis, Genetic Diseases, X-Linked diagnosis, Microphthalmia-Associated Transcription Factor genetics, Myopia diagnosis, Night Blindness diagnosis

Abstract

Inherited retinal dystrophies (IRDs) are characterized by high clinical and genetic heterogeneity. A precise characterization is desirable for diagnosis and has impact on prognosis, patient counseling, and potential therapeutic options. Here, we demonstrate the effectiveness of the combination of in-depth retinal phenotyping and molecular genetic testing in complex pedigrees with different IRDs. Four affected Caucasians and two unaffected relatives were characterized including multimodal retinal imaging, functional testing, and targeted next-generation sequencing. A considerable intrafamilial phenotypic and genotypic heterogeneity was identified. While the parents of the index family presented with rod-cone dystrophy and ABCA4 -related retinopathy, their two sons revealed characteristics in the spectrum of incomplete congenital stationary night blindness and ocular albinism, respectively. Molecular testing revealed previously described variants in RHO , ABCA4 , and MITF as well as a novel variant in CACNA1F . Identified variants were verified by intrafamilial co-segregation, bioinformatic annotations, and in silico analysis. The coexistence of four independent IRDs caused by distinct mutations and inheritance modes in one pedigree is demonstrated. These findings highlight the complexity of IRDs and underscore the need for the combination of extensive molecular genetic testing and clinical characterization. In addition, a novel variant in the CACNA1F gene is reported associated with incomplete congenital stationary night blindness., Competing Interests: M.G. is employee and equity owner of F. Hoffmann-La Roche Ltd., Basel, Switzerland. The other authors report no conflict of interest.

Published

2020

22. A novel GPR143 mutation in a Chinese family with X‑linked ocular albinism type 1.

Author

Gao X, Liu T, Cheng X, Dai A, Liu W, Li R, and Zhang M

Subjects

Adolescent, Adult, Aged, Albinism, Ocular metabolism, Albinism, Ocular pathology, China, Eye Proteins metabolism, Female, Humans, Male, Membrane Glycoproteins metabolism, Middle Aged, Albinism, Ocular genetics, Asian People, Eye Proteins genetics, Family, Membrane Glycoproteins genetics, Mutation

Abstract

Ocular albinism type 1 (OA1) is a genetic disorder characterized by reduced eye pigmentation and nystagmus, which is often accompanied by decreased visual acuity, strabismus and other symptoms, whereas skin and hair color remain normal. The present study aimed to assess the clinical features and perform genotype analysis of a family with OA1, and to determine the disease‑causing mutation. A total of 18 family members (nine affected patients and nine normal subjects) from Hainan, China, were recruited to the present study in December 2017. A detailed clinical ophthalmic examination was performed for all participants, including a visual acuity test, anterior segment slit lamp examination, eye fundus examination and optical coherence tomography. Mutations in the G protein‑coupled receptor 143 (GPR143) gene were determined by DNA sequencing assays and polymerase chain reaction assays for deletions; all exon coding sequences, exons at the 5'‑ and 3'‑ends, and non‑coding region sequences of intron splicing were assessed. Within the family, nine male patients exhibited disease occurrence at the age of 0‑6 months. All patients presented with different degrees of iris depigmentation, horizontal jerk nystagmus, foveal hypoplasia and reduced visual acuity. The fundus of only one patient exhibited choroid coloboma; in the remaining patients, their fundi exhibited different degrees of irregular retinal depigmentation. The mutation c.360+5G>T in the GPR143 gene was identified in this family. In conclusion, the present study identified the splicing mutation c.360+5G>T in the GPR143 gene in a Chinese family with OA1 and successfully identified the site. To the best of our knowledge, there have been no previous reports regarding this mutation in any major genome databases; therefore, this outcome may enrich the mutation spectrum of the GPR143 gene.

Published

2020

23. X-linked ocular albinism: mapping and cloning the gene.

Author

MacDonald IM

Subjects

Albinism, Ocular history, Canada, Genetic Diseases, X-Linked history, History, 19th Century, History, 20th Century, Humans, Albinism, Ocular genetics, Chromosome Mapping, Chromosomes, Human, X genetics, Cloning, Molecular, Genetic Diseases, X-Linked genetics

Published

2019

24. Evaluation of the iris thickness changes for the Chinese families with GPR143 gene mutations.

Author

Jiang J, Yang L, Li H, Huang L, and Li N

Subjects

Adolescent, Adult, Albinism, Ocular metabolism, Albinism, Ocular pathology, Child, China, DNA Mutational Analysis, Eye Proteins metabolism, Female, Humans, Male, Membrane Glycoproteins metabolism, Middle Aged, Pedigree, Pigment Epithelium of Eye pathology, Tomography, Optical Coherence, Young Adult, Albinism, Ocular genetics, Eye Proteins genetics, Iris pathology, Membrane Glycoproteins genetics, Mutation, Pigment Epithelium of Eye metabolism

Abstract

Purpose: Pathogenic variants of the G-protein coupled receptor 143 (GPR143) gene may result in Ocular albinism type I (OA1). In this study, we describe the clinical features and investigate the GPR143 gene mutations in six Chinese families with OA1 and evaluate the thickness changes of iris for the affected males and female carriers., Methods: Families were ascertained, and patients underwent complete ophthalmologic examinations, including the best corrected visual acuity (BCVA), anterior segment of the eyes, vitreous and fundus changes. Spectral domain optical coherence tomography (SD-OCT) was used to measure the full iris thickness, the stroma/anterior border (SAB) layer, and the posterior epithelial layer (PEL) at the pupillary and ciliary regions. DNA was extracted from the peripheral blood vessels after confirmed consent information. GPR143 gene was directly sequenced by the Sanger method., Results: The affected males had variable reduced visual acuity, nystagmus and macular hypoplasia. Four novel frameshift mutations and two previously reported missense/nonsense mutations in the GPR143 gene were detected in these families. The thickness of the iris was significantly reduced at the ciliary region in the affected males, compared with that in the normal controls and the female carriers., Conclusions: Pathogenic variants in the GPR143 gene may disturb the normal melanogenesis in the pigmented tissues of the eye, result in macular hypoplasia, and alter the thickness of the iris., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

25. Ocular albinism with mutation in GPR143: Findings in wide-field autofluorescence and optical coherence tomography.

Author

Montoya Delgado MJ, Astiazarán MC, Casanova Imken F, Ramírez Estudillo A, and Hernández Vázquez Á

Subjects

Albinism, Ocular diagnostic imaging, Child, Humans, Male, Optical Imaging, Tomography, Optical Coherence, Albinism, Ocular genetics, Eye Proteins genetics, Membrane Glycoproteins genetics, Mutation

Abstract

A 12 year-old boy who consulted due to nystagmus and low vision from birth. His mother also consulted for low vision of the right eye since she was a child, which worsened recently. The physical examination revealed no alterations in skin and hair pigmentation. In the examination of the anterior segment of the child, areas of slight circumferential hypopigmentation were observed in the iris in both eyes. The fundus examination revealed a choroidal fundus due to the absence of melanin in the retinal pigment epithelium. In the autofluorescence, an absence of physiological macular hypo-autofluorescence was observed and, in optical coherence tomography, foveal hypoplasia was observed in both eyes. In the ocular fundus examination of the mother, slight macular pigmentary changes were observed in the right eye, with hyperpigmented radiated spots in the retinal periphery of both eyes, which were hypo-autofluorescent in the wide-field autofluorescence. In the optical coherence tomography of the right eye, a cavitation of the outer retinal layers was observed in the fovea. The genetic study by nucleotide sequencing was performed on the mother and the child. In the mutation found in the GPR143 gene, the son was hemizygous and the mother was heterozygous. X-linked ocular albinism was diagnosed and the genetic counselling was carried out. Ocular albinism linked to X is the most frequent genetic variant of this disease. Peripheral pigment alterations in heterozygous mothers have been previously described in the literature, but there are no reports of cavitations in the external retinal layers using optical coherence tomography., (Copyright © 2019 Sociedad Española de Oftalmología. Publicado por Elsevier España, S.L.U. All rights reserved.)

Published

2019

26. Conversations with Ray Guillery on albinism: linking Siamese cat visual pathway connectivity to mouse retinal development.

Author

Mason C and Guillery R

Subjects

Animals, Cats, History, 20th Century, History, 21st Century, Mice, Monophenol Monooxygenase genetics, Retina metabolism, Retina physiology, Albinism, Ocular genetics, Genetics history, Neurosciences history, Retina growth & development, Visual Pathways physiology

Abstract

In albinism of all species, perturbed melanin biosynthesis in the eye leads to foveal hypoplasia, retinal ganglion cell misrouting, and, consequently, altered binocular vision. Here, written before he died, Ray Guillery chronicles his discovery of the aberrant circuitry from eye to brain in the Siamese cat. Ray's characterization of visual pathway anomalies in this temperature sensitive mutation of tyrosinase and thus melanin synthesis in domestic cats opened the exploration of albinism and simultaneously, a genetic approach to the organization of neural circuitry. I follow this account with a remembrance of Ray's influence on my work. Beginning with my postdoc research with Ray on the cat visual pathway, through my own work on the mechanisms of retinal axon guidance in the developing mouse, Ray and I had a continuous and rich dialogue about the albino visual pathway. I will present the questions Ray posed and clues we have to date on the still-elusive link between eye pigment and the proper balance of ipsilateral and contralateral retinal ganglion cell projections to the brain., (© 2019 Federation of European Neuroscience Societies and John Wiley & Sons Ltd.)

Published

2019

27. Clinical and molecular findings of FRMD7 related congenital nystagmus as adifferential diagnosis of ocular albinism.

Author

Michaud V, Defoort-Dhellemmes S, Drumare I, Pennamen P, Plaisant C, Lasseaux E, and Arveiler B

Subjects

Albinism, Ocular diagnosis, Child, Diagnosis, Differential, Female, High-Throughput Nucleotide Sequencing, Humans, Infant, Male, Nystagmus, Congenital diagnosis, Pedigree, Slit Lamp Microscopy, Tomography, Optical Coherence, Albinism, Ocular genetics, Cytoskeletal Proteins genetics, Genetic Diseases, X-Linked genetics, Membrane Proteins genetics, Mutation, Missense, Nystagmus, Congenital genetics, X Chromosome Inactivation genetics

Abstract

Background: Congenital nystagmus is one of the most common neuro-ophthalmological disorders. X chromosome-linked forms are associated with pathogenic variants of the GPR143 and FRMD7 genes., Materials and Methods: Patients' DNA was analyzed using a next-generation sequencing (NGS) panel of genes involved in albinism and related pathologies (TYR, OCA2, TYRP1, SLC45A2, SLC24A5, C10ORF11, GPR143, SLC38A8, HPS 1 to 10, LYST, MITF, FRMD7) Results: We report a 4 generation family with 5 affected members initially referred for molecular diagnosis of ocular albinism. A missense variant of FRMD7 was found in 3 affected cases and one female carrier. We show that the disease in the affected girl is due to skewed inactivation of the X chromosome., Conclusions: By compiling all the published cases we discuss the variable penetrance among females due to different types of mutation and to X-inactivation.

Published

2019

28. A pathogenic haplotype, common in Europeans, causes autosomal recessive albinism and uncovers missing heritability in OCA1.

Author

Grønskov K, Jespersgaard C, Bruun GH, Harris P, Brøndum-Nielsen K, Andresen BS, and Rosenberg T

Subjects

Europe, Female, Humans, Male, Pedigree, Polymorphism, Single Nucleotide, Albinism, Ocular genetics, Haplotypes

Abstract

Oculocutaneous albinism (OCA) is a genetically heterogeneous disorder. Six genes are associated with autosomal recessive OCA (TYR, OCA2, TYRP1, SLC45A2, SLC24A5 and LRMDA), and one gene, GPR143, is associated with X-linked ocular albinism (OA). Molecular genetic analysis provides a genetic diagnosis in approximately 60% of individuals with clinical OA/OCA. A considerably number of the remaining 40% are heterozygous for a causative sequence variation in TYR. To identify missing causative sequence variants in these, we used a NGS based approach, genotyping and segregation analysis. We report two putative pathogenic haplotypes which only differ by two extremely rare SNVs, indicating that the haplotypes have a common derivation. Both haplotypes segregate consistent with an autosomal recessive inheritance pattern and include the allele p.S192Y-p.R402Q. An explanation for the pathogenicity of the haplotypes could be the combination of p.S192Y and p.R402Q. Homozygosity for the pathogenic haplotypes causes a partial albinism phenotype. In our cohort, 15% of affected individuals had a molecular genetic diagnosis involving the pathogenic haplotype. Consequently, the prevalence of albinism seems to be substantially underestimated, and children with unexplained bilateral subnormal vision and/or nystagmus should be analysed clinically and molecularly for albinism.

Published

2019

29. Pigmentation and vision: Is GPR143 in control?

Author

McKay BS

Subjects

Albinism, Ocular genetics, Albinism, Ocular pathology, Eye Proteins genetics, Humans, Melanins biosynthesis, Melanins genetics, Melanins metabolism, Membrane Glycoproteins genetics, Mutation, Pigmentation genetics, Retina metabolism, Albinism, Ocular metabolism, Eye Proteins metabolism, Membrane Glycoproteins metabolism, Pigmentation physiology, Retinal Pigment Epithelium metabolism

Abstract

Albinism, typically characterized by decreased melanin synthesis, is associated with significant visual deficits owing to developmental changes during neurosensory retina development. All albinism is caused by genetic mutations in a group of diverse genes including enzymes, transporters, G-protein coupled receptor. Interestingly, these genes are not expressed in the neurosensory retina. Further, regardless of cause of albinism, all forms of albinism have the same retinal pathology, the extent of which is variable. In this review, we explore the possibility that this similarity in retinal phenotype is because all forms of albinism funnel through the same final common pathway. There are currently seven known genes linked to the seven forms of ocular cutaneous albinism. These types of albinism are the most common, and result in changes to all pigmented tissues (hair, skin, eyes). We will discuss the incidence and mechanism, where known, to develop a picture as to how the mutations cause albinism. Next, we will examine the one form of albinism which causes tissue-specific pathology, ocular albinism, where the eye exhibits the retinal albinism phenotype despite near normal melanin synthesis. We will discuss a potential way to treat the disease and restore normal retinal development. Finally, we will briefly discuss the possibility that this same pathway may intersect with the most common cause of permanent vision loss in the elderly., (© 2018 Wiley Periodicals, Inc.)

Published

2019

30. Identification of a novel GPR143 mutation in X-linked ocular albinism with marked intrafamilial phenotypic variability.

Author

Jung JH, Oh EH, Shin JH, Kim HS, Choi SY, Choi KD, Lee C, and Choi JH

Subjects

Base Sequence, Eye Proteins chemistry, Family Health, Female, Humans, Male, Membrane Glycoproteins chemistry, Pedigree, Phenotype, Exome Sequencing methods, Albinism, Ocular genetics, Eye Proteins genetics, Genetic Diseases, X-Linked genetics, Membrane Glycoproteins genetics, Mutation

Abstract

Ocular albinism type 1 (OA1) is an X-linked inherited disease characterized by impaired visual acuity, congenital nystagmus, foveal hypoplasia, hypopigmentation of iris and fundus. It is caused by mutations in the G protein-coupled receptor143 ( GPR143 ) gene. The genetic characteristics of OA1 have not been well defined in Asians. In this study, six members from three consecutive generations of a Korean family with OA1 were enrolled. We performed whole-exome sequencing followed by validation and segregation analysis. Two affected patients underwent detailed ophthalmic examinations and eye movement recordings. Of the two affected males, the proband had all classical phenotypes of OA1, but the other showed isolated foveal hypoplasia without nystagmus. We identified a hemizygous missense (c.623C > A, p.Ala208Glu) mutation of GPR143 in affected males. This mutation was also present as heterozygous in two obligate female carriers, and was not found in unaffected members. Our data expands thespectrum of phenotypes and genotype in GPR143 in Asians, and highlights the phenotypic heterogeneity in OA1.

Published

2018

31. Generation of a human Ocular Albinism type 1 iPSC line, SEIi001-A, with a mutation in GPR143.

Author

Baulier E, Garcia Diaz A, Corneo B, and Farber DB

Subjects

Adult, Humans, Male, Mutation, Albinism, Ocular genetics, Eye Proteins genetics, Induced Pluripotent Stem Cells metabolism, Membrane Glycoproteins genetics

Abstract

Ocular albinism type 1 is a genetic eye disease caused by mutations in the GPR143 gene. Little is known about the molecular pathways involved in this disease and no therapeutic candidate has been identified as yet. Here we report the generation of an iPSC line from the skin fibroblasts of a patient with a mutation in the GPR143 gene using Sendai Virus vectors. This new iPSC line will allow a better understanding of the Ocular Albinism type 1 disease and to screen for potential therapeutic candidates., (Copyright © 2018 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2018

32. Ocular albinism with infertility and late-onset sensorineural hearing loss.

Author

Fabian-Jessing BK, Vestergaard EM, Plomp AS, Bergen AA, Dreschler WA, Duno M, Winiarska BS, Neumann L, Gaihede M, Vorum H, and Petersen MB

Subjects

Adult, Aged, Albinism, Ocular complications, Albinism, Ocular genetics, Female, Gene Deletion, Genetic Diseases, X-Linked complications, Genetic Diseases, X-Linked genetics, Genetic Diseases, X-Linked pathology, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural genetics, Humans, Infertility complications, Infertility genetics, Male, Middle Aged, Pedigree, Albinism, Ocular pathology, Eye Proteins genetics, Hearing Loss, Sensorineural pathology, Infertility pathology, Membrane Glycoproteins genetics, Membrane Proteins genetics, Mutation, Transducin genetics

Abstract

Ocular albinism type 1 (OA1) is caused by mutations in the GPR143 gene located at Xp22.2. The manifestations, which are due to hypopigmentation, are confined to the eyes and optic pathway. OA1 associated with late-onset sensorineural hearing loss was previously reported in a single family and hypothesized to be caused by a contiguous gene deletion syndrome involving GPR143 and the adjacent gene, TBL1X. Here, we report on a family with OA1, infertility, late-onset sensorineural hearing loss, and a small interstitial Xp microdeletion including the GPR143, TBL1X, and SHROOM2 genes. In addition, we re-examined a patient previously described with OA1, infertility and a similar Xp deletion with audiologic follow-up showing a late-onset sensorineural hearing loss. Our results raise an intriguing question about the possibility for TBL1X (absence) involvement in this type of hearing loss. However, our study cannot claim a causative relationship and more convincing evidence is needed before the hypothesis can be accepted that TBL1X could be involved in late-onset sensorineural hearing loss and that ocular albinism with late-onset sensorineural hearing loss can present itself as a contiguous gene deletion/microdeletion syndrome. The finding of infertility in all affected male patients demonstrates that this deletion, including the SHROOM2 gene, may be a potentially causative X-linked genetic factor of male infertility., (© 2018 Wiley Periodicals, Inc.)

Published

2018

33. Mutations in GPR143/OA1 and ABCA4 Inform Interpretations of Short-Wavelength and Near-Infrared Fundus Autofluorescence.

Author

Paavo M, Zhao J, Kim HJ, Lee W, Zernant J, Cai C, Allikmets R, Tsang SH, and Sparrow JR

Subjects

Adolescent, Adult, Albinism, Ocular metabolism, Animals, Child, Female, Fluorescein Angiography, Humans, Infrared Rays, Macular Degeneration congenital, Macular Degeneration genetics, Macular Degeneration metabolism, Male, Mice, Mice, Inbred C57BL, Middle Aged, Ophthalmoscopy, Radio Waves, Retinal Pigment Epithelium metabolism, Retrospective Studies, Stargardt Disease, Tomography, Optical Coherence, Young Adult, ATP-Binding Cassette Transporters genetics, Albinism, Ocular genetics, Eye Proteins genetics, Lipofuscin metabolism, Melanins metabolism, Membrane Glycoproteins genetics, Mutation, Optical Imaging

Abstract

Purpose: We sought to advance interpretations and quantification of short-wavelength fundus autofluorescence (SW-AF) emitted from bisretinoid lipofuscin and near-infrared autofluoresence (NIR-AF) originating from melanin., Methods: Carriers of mutations in X-linked GPR143/OA1, a common form of ocular albinism; patients with confirmed mutations in ABCA4 conferring increased SW-AF; and subjects with healthy eyes were studied. SW-AF (488 nm excitation, 500-680 nm emission) and NIR-AF (excitation 787 nm, emission >830 nm) images were acquired with a confocal scanning laser ophthalmoscope. SW-AF images were analyzed for quantitative autofluoresence (qAF). Analogous methods of image acquisition and analysis were performed in albino and pigmented Abca4-/- mice and wild-type mice., Results: Quantitation of SW-AF (qAF), construction of qAF color-coded maps, and examination of NIR-AF images from GPR143/OA1 carriers revealed mosaics in which patches of fundus exhibiting NIR-AF signal had qAF levels within normal limits whereas the hypopigmented areas in the NIR-AF image corresponded to foci of elevated qAF. qAF also was increased in albino versus pigmented mice. Although melanin contributes to fundus infrared reflectance, the latter appeared to be uniform in en face reflectance images of GPR143/OA1-carriers. In patients diagnosed with ABCA4-associated disease, NIR-AF increased in tandem with increased qAF originating in bisretinoid lipofuscin. Similarly in Abca4-/- mice having increased SW-AF, NIR-AF was more pronounced than in wild-type mice., Conclusions: These studies corroborate RPE melanin as the major source of NIR-AF but also indicate that bisretinoid lipofuscin, when present at sufficient concentrations, contributes to the NIR-AF signal. Ocular melanin attenuates the SW-AF signal.

Published

2018

34. Mud-splattered fundus.

Author

Welch RJ, Li X, and Shields CL

Subjects

Albinism, Ocular diagnosis, Albinism, Ocular genetics, Chromosomes, Human, Pair 13 genetics, Eye Proteins genetics, Female, Fluorescein Angiography, Germ-Line Mutation, Humans, Infant, Membrane Glycoproteins genetics, Retinal Detachment diagnosis, Retinal Neoplasms diagnosis, Retinal Neoplasms genetics, Retinoblastoma diagnosis, Retinoblastoma genetics, Retinoblastoma Binding Proteins genetics, Ubiquitin-Protein Ligases genetics, Albinism, Ocular complications, Fundus Oculi, Retinal Neoplasms complications, Retinoblastoma complications

Abstract

Competing Interests: There are no conflicts of interest

Published

2018

35. DETAILED RETINAL IMAGING IN CARRIERS OF OCULAR ALBINISM.

Author

Khan KN, Lord EC, Arno G, Islam F, Carss KJ, Raymond F, Toomes C, Ali M, Inglehearn CF, Webster AR, Moore AT, Poulter JA, and Michaelides M

Subjects

Adult, Albinism, Ocular genetics, Eye Proteins genetics, Female, Heterozygote, Humans, Macula Lutea pathology, Membrane Glycoproteins genetics, Middle Aged, Prospective Studies, Retinal Pigment Epithelium pathology, Albinism, Ocular pathology, Retina pathology

Abstract

Background: Albinism refers to a group of disorders primarily characterized by hypopigmentation. Affected individuals usually manifest both ocular and cutaneous features of the disease, but occasionally hair and skin pigmentation may appear normal. This is the case in ocular albinism, an X chromosome linked disorder resulting from mutation of GPR143. Female carriers may be recognized by a "mud-splatter" appearance in the peripheral retina. The macula is thought to be normal, however., Methods: Obligate female carriers of pathogenic GPR143 alleles were recruited. Molecular confirmation of disease was performed only for atypical cases. Detailed retinal imaging was performed (colour fundus photography, optical coherence tomography, fundus autofluorescence., Results: Eight individuals were ascertained. A novel GPR143 mutation was identified in one family (p.Gln328Ter). Foveal fundus autofluorescence was subjectively reduced in 6/6 patients imaged. A "tapetal-like" pattern of autofluorescence was visible at the macula in 3/6. Persistence of the inner retinal layers at the fovea was observed in 6/8 females., Conclusion: Female carriers of ocular albinism may manifest signs of retinal pigment epithelium mosaicism at the macula and the peripheral fundus. A tapetal-like reflex on fundus autofluorescence may be considered the macular correlate of "mud-splatter."

Published

2018

36. [Oculocutaneous and ocular albinism].

Author

Kubasch AS and Meurer M

Subjects

Albinism, Ocular classification, Albinism, Ocular genetics, Albinism, Ocular therapy, Albinism, Oculocutaneous classification, Albinism, Oculocutaneous genetics, Albinism, Oculocutaneous therapy, Chromosome Aberrations, DNA Mutational Analysis, Diagnosis, Differential, Early Diagnosis, Early Medical Intervention, Genes, Recessive genetics, Genes, X-Linked, Humans, Interdisciplinary Communication, Intersectoral Collaboration, Melanins biosynthesis, Monophenol Monooxygenase genetics, Albinism, Ocular diagnosis, Albinism, Oculocutaneous diagnosis

Abstract

Albinism can be divided into oculocutaneous albinism (OCA) and ocular albinism (OA). In the differential diagnostics these can be distinguished from rarer syndromes with partial albinism, which are frequently associated with susceptibility to infections and neurological symptoms. The OCA is an autosomal recessive inherited disease of melanin biosynthesis, which leads to complete or partial loss of melanin in the skin, hair follicles and eyes. Of the seven currently known subtypes (OCA 1-7), four are well-characterized (OCA 1-4). These are based on gene mutations, which code for tyrosinase, a key enzyme in melanin synthesis and for further proteins. These play an important role in the catalytic activity of tyrosinase and the structure and function of melanosomes. In the presence of these subtypes, the clinical symptoms and the course of the disease show a pronounced variability, especially in the type and extent of pigmentation of the skin and hair as well as the severity of eye involvement, which makes the phenotypic classification difficult. Treatment priorities are a consistent protection from UV light for prophylaxis against skin cancer and regular preventive investigations. The ocular alterations typical for albinism necessitate timely diagnostics and care by institutions specialized in ophthalmology. Novel strategies for systemic treatment of subtypes of albinism are in preclinical testing. The OA without skin involvement shows X‑linked inheritance, is much rarer and is characterized by reduced pigmentation of the retina and iris, nystagmus and macular hypoplasia, sometimes with substantial loss of visual acuity. The typical ocular symptoms of OA can be manifested to a varying extent in all forms of OCA.

Published

2017

37. Identification of a functionally significant tri-allelic genotype in the Tyrosinase gene (TYR) causing hypomorphic oculocutaneous albinism (OCA1B).

Author

Norman CS, O'Gorman L, Gibson J, Pengelly RJ, Baralle D, Ratnayaka JA, Griffiths H, Rose-Zerilli M, Ranger M, Bunyan D, Lee H, Page R, Newall T, Shawkat F, Mattocks C, Ward D, Ennis S, and Self JE

Subjects

Albinism, Ocular diagnosis, Albinism, Oculocutaneous diagnosis, Electroretinography, Evoked Potentials, Visual, Female, Humans, Male, Pedigree, Phenotype, Tomography, Optical Coherence, Albinism, Ocular genetics, Albinism, Oculocutaneous genetics, Alleles, Genetic Association Studies, Genetic Predisposition to Disease, Genotype, Monophenol Monooxygenase genetics

Abstract

Oculocutaneous albinism (OCA) and ocular albinism (OA) are inherited disorders of melanin biosynthesis, resulting in loss of pigment and severe visual deficits. OCA encompasses a range of subtypes with overlapping, often hypomorphic phenotypes. OCA1 is the most common cause of albinism in European populations and is inherited through autosomal recessive mutations in the Tyrosinase (TYR) gene. However, there is a high level of reported missing heritability, where only a single heterozygous mutation is found in TYR. This is also the case for other OCA subtypes including OCA2 caused by mutations in the OCA2 gene. Here we have interrogated the genetic cause of albinism in a well phenotyped, hypomorphic albinism population by sequencing a broad gene panel and performing segregation studies on phenotyped family members. Of eighteen probands we can confidently diagnose three with OA and OCA2, and one with a PAX6 mutation. Of six probands with only a single heterozygous mutation in TYR, all were found to have the two common variants S192Y and R402Q. Our results suggest that a combination of R402Q and S192Y with a deleterious mutation in a 'tri-allelic genotype' can account for missing heritability in some hypomorphic OCA1 albinism phenotypes.

Published

2017

38. Identification of Novel G Protein-Coupled Receptor 143 Ligands as Pharmacologic Tools for Investigating X-Linked Ocular Albinism.

Author

De Filippo E, Manga P, and Schiedel AC

Subjects

Albinism, Ocular drug therapy, Albinism, Ocular metabolism, Cells, Cultured, DNA Mutational Analysis, Ethacridine pharmacology, Exons, Eye Proteins antagonists & inhibitors, Eye Proteins metabolism, Genetic Diseases, X-Linked diet therapy, Genetic Diseases, X-Linked metabolism, Humans, Ligands, Membrane Glycoproteins antagonists & inhibitors, Membrane Glycoproteins metabolism, Niclosamide pharmacology, Pedigree, Pimozide pharmacology, Albinism, Ocular genetics, Eye Proteins genetics, Genetic Diseases, X-Linked genetics, Membrane Glycoproteins genetics, Mutation, RNA genetics

Abstract

Purpose: GPR143 regulates melanosome biogenesis and organelle size in pigment cells. The mechanisms underlying receptor function remain unclear. G protein-coupled receptors (GPCRs) are excellent pharmacologic targets; thus, we developed and applied a screening approach to identify potential GPR143 ligands and chemical modulators., Methods: GPR143 interacts with β-arrestin; we therefore established a β-arrestin recruitment assay to screen for compounds that modulate activity. Because GPR143 is localized intracellularly, screening with the wild-type receptor would be restricted to agents absorbed by the cell. For the screen we used a mutant receptor, which shows similar basal activity as the wild type but traffics to the plasma membrane. We tested two compound libraries and investigated validated hits for their effects on melanocyte pigmentation., Results: GPR143, which showed high constitutive activity in the β-arrestin assay, was inhibited by several compounds. The three validated inhibitors (pimozide, niclosamide, and ethacridine lactate) were assessed for impact on melanocytes. Pigmentation and expression of tyrosinase, a key melanogenic enzyme, were reduced by all compounds. Because GPR143 appears to be constitutively active, these compounds may turn off its activity., Conclusions: X-linked ocular albinism type I, characterized by developmental eye defects, results from GPR143 mutations. Identifying pharmacologic agents that modulate GPR143 activity will contribute significantly to our understanding of its function and provide novel tools with which to study GPCRs in melanocytes and retinal pigment epithelium. Pimozide, one of three GPR143 inhibitors identified in this study, maybe be a good lead structure for development of more potent compounds and provide a platform for design of novel therapeutic agents.

Published

2017

39. GPR143 mutations in Chinese patients with ocular albinism type 1.

Author

Jia X, Yuan J, Jia X, Ling S, Li S, and Guo X

Subjects

Albinism, Ocular diagnosis, Albinism, Ocular pathology, China, DNA Mutational Analysis, Exons, Female, Humans, Introns, Male, Nystagmus, Congenital diagnosis, Nystagmus, Congenital genetics, Nystagmus, Congenital pathology, Polymorphism, Genetic, Albinism, Ocular genetics, Eye Proteins genetics, Membrane Glycoproteins genetics, Mutation

Abstract

The aim of the present study was to evaluate mutations of the G protein-coupled receptor 143 (GPR143) gene for ocular albinism type 1 (OA1) in Chinese patients. For the current study, 8 patients with OA1 were selected from the database of ocular genetic diseases. Genomic DNA of OA1 was prepared from venous leukocytes collected from the patients. Cycle sequencing was used to analyze the exons and adjacent introns of GPR143. The variation detected was analyzed by bidirectional DNA sequencing and further evaluated in 96 controls using heteroduplex‑single strand conformational polymorphism analysis. Additionally, slit lamp photography of anterior segment, fundus photography and optical coherence tomography (OCT) were performed to identify the clinical features of OA1. In five patients with OA1, 5 GPR143 gene mutations were identified and four of them there were novel mutations. The screening rate is 62.5%, including c.333G>A (p.W111X), c.353G>A (p.G118E) (known mutation), C.658+2T>G (splice mutation), c.215&#95;216insCGCTGC (p.71‑72insAA) and c.17T>C (p. L6P). These mutations were absent in the 96 normal controls. Only one patient with OA1 in the present study was female. Patients with OA1 often have congenital nystagmus, refractive error, severe decline of visual acuity (from 0.1 to 0.4) and foveal hypoplasia. Different degrees of pigment loss were evident in the patients' iris and retina, whereas macular structure was not identified in the OCT examination. The findings of the present study expanded the gene mutation spectrum of GPR143 and investigated the clinical phenotype of patients with OA1 in the Chinese population. Additional evidence for clinical diagnosis was provided along with differential diagnosis and genetic counseling.

Published

2017

40. [Identification of a novel GPR143 mutation in a Chinese family affected with X-linked ocular albinism].

Author

Zhao Q, Guan M, Wang L, Liao Y, Li-Ling J, and Wan H

Subjects

Adult, Asian People genetics, Base Sequence, Female, Humans, Infant, Male, Molecular Sequence Data, Mutation, Albinism, Ocular genetics, Eye Proteins genetics, Genetic Diseases, X-Linked genetics, Membrane Glycoproteins genetics

Abstract

Objective: To detect mutation of GPR143 gene in a Chinese patient affected with ocular albinism., Methods: Peripheral blood samples were collected from the proband and his parents. The coding regions of the GPR143 gene were subjected to PCR amplification and Sanger sequencing., Results: A previously unreported mutation (c.758T>A) was found in exon 6 of the GPR143 gene in the proband and his mother. The same mutation was not found in his father. As predicted, the mutation has resulted in a stop codon, causing premature termination of protein translation., Conclusion: A novel mutation of the GPR143 gene related to X-linked ocular albinism has been identified.

Published

2017

41. Molecular genetic and clinical evaluation of three Chinese families with X-linked ocular albinism.

Author

Zou X, Li H, Yang L, Sun Z, Yuan Z, Li H, and Sui R

Subjects

Asian People, DNA Mutational Analysis, Humans, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Sequence Analysis, DNA, Albinism, Ocular genetics, Albinism, Ocular pathology, Eye Proteins genetics, Family Health, Membrane Glycoproteins genetics

Abstract

X-linked ocular albinism (OA1) is an X-linked inherited disease characterized by hypopigmentation of the fundus and nystagmus. Our study performed mutation analysis of the G protein-coupled receptor 143 gene (GPR143) and assessed the clinical characteristics of OA1 in three Chinese families. Three novel mutations, c.333&#95;360+14del42insCTT, c.276G>A (p.W92X), and c.793C>T (p.R265X), were identified in GPR143 by PCR followed by Sanger sequencing in these families. All affected individuals presented with nystagmus, photophobia, poor visual acuity, foveal hypoplasia and varying degrees of hypopigmentation of the fundus. The fundus of female carriers showed pigmented streaks alternating with hypopigmented streaks. These results allowed us to expand the spectrum of mutations in GPR143 and phenotypes associated with ocular albinism.

Published

2017

42. GNAI3: Another Candidate Gene to Screen in Persons with Ocular Albinism.

Author

Young A, Dandekar U, Pan C, Sader A, Zheng JJ, Lewis RA, and Farber DB

Subjects

3' Untranslated Regions genetics, 5' Untranslated Regions genetics, Albinism, Ocular diagnosis, Base Pairing genetics, Base Sequence, Exons genetics, GTP-Binding Protein alpha Subunits, Gi-Go chemistry, Genetic Loci, Heterozygote, Homozygote, Humans, Introns genetics, Models, Molecular, Mutation genetics, Polymorphism, Single Nucleotide genetics, Reproducibility of Results, Sequence Analysis, DNA, Albinism, Ocular genetics, GTP-Binding Protein alpha Subunits, Gi-Go genetics, Genetic Association Studies, Genetic Predisposition to Disease

Abstract

Ocular albinism type 1 (OA), caused by mutations in the OA1 gene, encodes a G-protein coupled receptor, OA1, localized in melanosomal membranes of the retinal pigment epithelium (RPE). This disorder is characterized by both RPE macro-melanosomes and abnormal decussation of ganglion cell axons at the brain's optic chiasm. We demonstrated previously that Oa1 specifically activates Gαi3, which also signals in the Oa1 transduction pathway that regulates melanosomal biogenesis. In this study, we screened the human Gαi3 gene, GNAI3, in DNA samples from 26 patients who had all clinical characteristics of OA but in whom a specific mutation in the OA1 gene had not been found, and in 6 normal control individuals. Using the Agilent HaloPlex Target Enrichment System and next-generation sequencing (NGS) on the Illumina MiSeq platform, we identified 518 variants after rigorous filtering. Many of these variants were corroborated by Sanger sequencing. Overall, 98.8% coverage of the GNAI3 gene was obtained by the HaloPlex amplicons. Of all variants, 6 non-synonymous and 3 synonymous were in exons, 41 in a non-coding exon embedded in the 3' untranslated region (UTR), 6 in the 5' UTR, and 462 in introns. These variants included novel SNVs, insertions, deletions, and a frameshift mutation. All were found in at least one patient but none in control samples. Using computational methods, we modeled the GNAI3 protein and its non-synonymous exonic mutations and determined that several of these may be the cause of disease in the patients studied. Thus, we have identified GNAI3 as a second gene possibly responsible for X-linked ocular albinism., Competing Interests: The authors have declared that no competing interests exist.

Published

2016

43. Novel HPS6 mutations identified by whole-exome sequencing in two Japanese sisters with suspected ocular albinism.

Author

Miyamichi D, Asahina M, Nakajima J, Sato M, Hosono K, Nomura T, Negishi T, Miyake N, Hotta Y, Ogata T, and Matsumoto N

Subjects

Alleles, Child, Preschool, Exome, Female, Fluorescein Angiography, Genes, Recessive, Genotype, High-Throughput Nucleotide Sequencing, Humans, Japan, Pedigree, Phenotype, Tomography, Optical Coherence, Albinism, Ocular diagnosis, Albinism, Ocular genetics, Intracellular Signaling Peptides and Proteins genetics, Mutation, Siblings

Abstract

Hermansky-Pudlak syndrome (HPS) is an autosomal recessive disorder characterized by oculocutaneous albinism, platelet dysfunction and ceroid deposition. We report suspected ocular albinism in two Japanese sisters, caused by mutations in the HPS6 (Hermansky-Pudlak syndrome 6) gene. Trio-based whole-exome sequencing (WES) identified novel compound heterozygous mutations in HPS6 (c.1898delC: mother origin and c.2038C>T: father origin) in the two sisters. To date, 10 associated mutations have been detected in HPS6. Although we detected no general manifestations, including platelet dysfunction, in the sisters, even in long-term follow-up, we established a diagnosis of HPS type 6 based on the HPS6 mutations and absence of dense bodies in the platelets, indicating that WES can identify cases of HPS type 6. To the best of our knowledge, this is the first report of HPS6 mutations in Japanese patients.

Published

2016

44. Simultaneous Expression of ABCA4 and GPR143 Mutations: A Complex Phenotypic Manifestation.

Author

Lee W, Schuerch K, Xie Y, Zernant J, Tsang SH, Sparrow JR, and Allikmets R

Subjects

Adolescent, Adult, Albinism, Ocular genetics, Electroretinography, Female, Fluorescein Angiography, Humans, Macular Degeneration genetics, Macular Degeneration metabolism, Macular Degeneration pathology, Male, Microscopy, Confocal, Phenotype, Retina pathology, Retina physiopathology, Sequence Analysis, DNA, Stargardt Disease, ATP-Binding Cassette Transporters genetics, Albinism, Ocular metabolism, Eye Proteins genetics, Macular Degeneration congenital, Membrane Glycoproteins genetics, Mutation

Abstract

Purpose: To describe the complex, overlapping phenotype expressed in a two generation family harboring pathogenic mutations in the ABCA4 and GPR143 genes., Methods: Clinical evaluation of a two generation family included quantitative autofluorescence imaging (qAF, 488-nm excitation) using a modified confocal scanning laser ophthalmoscope equipped with an internal fluorescent reference to account for varying laser power detector sensitivity, spectral-domain optical coherence tomography, and full-field ERG testing. Complete sequencing of the ABCA4 and GPR143 genes was carried out in each individual., Results: Affected individuals presented with bull's eye lesions and qAF levels above the 95% confidence interval for healthy eyes; full-field ERG revealed no generalized rod dysfunction but mild implicit time delays in cone responses. Complete sequencing of the ABCA4 gene revealed two disease-causing mutations, p.L541P and p.G1961E; and mutational phase was confirmed in each unaffected parent. Further examination in the affected patients revealed a peripheral "mud-splattered" pattern of hypopigmented RPE after which sequencing of GPR143 revealed a novel missense variant, p.Y157C. The GPR143 variant segregated from the father who did not exhibit any indications of retinal disease with the exception of an abnormal near-infrared autofluorescence (NIR-AF) signal distribution in the macula., Conclusions: An individual carrying both ABCA4 and GPR143 disease-causing mutations can express a complex, overlapping phenotype associated with both Stargardt disease and X-linked ocular albinism (OA1). The absence of OA1-related disease changes (with the exception of NIR-AF changes associated with melanin distribution) in the father may be indicative of mild expressivity or variable gene penetrance.

Published

2016

45. A novel mutation, c.494C>A (p.Ala165Asp), in the GPR143 gene causes a mild phenotype in a Chinese X-linked ocular albinism patient.

Author

Pan Q, Yi C, Xu T, Liu J, Jing X, Hu B, and Wang Y

Subjects

Adult, Albinism, Ocular diagnosis, Albinism, Ocular ethnology, Asian People genetics, China epidemiology, DNA Mutational Analysis, Female, Genetic Diseases, X-Linked diagnosis, Genetic Diseases, X-Linked ethnology, Humans, Infant, Male, Pedigree, Phenotype, Polymerase Chain Reaction, Albinism, Ocular genetics, Eye Proteins genetics, Genetic Diseases, X-Linked genetics, Membrane Glycoproteins genetics, Mutation, Missense

Published

2016

46. Homozygosity mapping in albinism patients using a novel panel of 13 STR markers inside the nonsyndromic OCA genes: introducing 5 novel mutations.

Author

Khordadpoor-Deilamani F, Akbari MT, Karimipoor M, and Javadi GR

Subjects

Alleles, Consanguinity, DNA Mutational Analysis, Exons, Female, Heterozygote, Humans, Introns, Male, Pedigree, Albinism, Ocular diagnosis, Albinism, Ocular genetics, Chromosome Mapping, DNA, Satellite, Genetic Association Studies, Genetic Markers, Homozygote, Mutation

Abstract

Albinism is a heterogeneous genetic disorder of melanin synthesis that results in hypopigmented hair, skin and eyes. It is associated with decreased visual acuity, nystagmus, strabismus and photophobia. Six genes are known to be involved in nonsyndromic oculocutaneous albinism (OCA). In this study, we aimed to find the disease causing mutations in albinism patients using homozygosity mapping. Twenty three unrelated patients with nonsyndromic OCA or autosomal recessive ocular albinism were recruited in this study. All of the patients' parents had consanguineous marriage and all were screened for TYR mutations previously. At first, we performed homozygosity mapping using fluorescently labeled primers to amplify a novel panel of 13 STR markers inside the OCA genes and then the screened loci in each family were studied using PCR and cycle sequencing methods. We found five mutations including three mutations in OCA2, one mutation in SLC45A2 and one mutation in C10ORF11 genes, all of which were novel. In cases where the disease causing mutations are identical by descent due to a common ancestor, these STR markers can enable us to screen for the responsible genes.

Published

2016

47. [Albinism and the Range of Fundus Hypopigmentation, Macular Hypoplasia, and Nystagmus].

Author

Preising MN and Lorenz B

Subjects

Genetic Predisposition to Disease genetics, Humans, Mutation genetics, Albinism, Ocular genetics, Eye Proteins genetics, Macula Lutea abnormalities, Nystagmus, Congenital genetics, Retinal Diseases genetics

Abstract

From the ophthalmological view, albinism is a disorder of reduced pigmentation of the retinal and irdial pigment epithelium and the iris and choroid stroma. The reduced pigmentation is accompanied by morphological changes in the retina and the optic nerve. The functional relationship of these morphological changes is not yet well understood. This review summarises the genetic causes of reduced pigment synthesis and impaired pigment distribution, and discusses the variability of expression of albinism symptoms, in the light of other disorders affecting retinal development., (Georg Thieme Verlag KG Stuttgart · New York.)

Published

2016

48. Illusions of Certainty.

Author

Keirns CC

Subjects

Albinism, Ocular genetics, Humans, Infant, Male, Sequence Analysis, DNA, Uncertainty, Albinism, Ocular diagnosis, Genetic Testing ethics

Published

2015

49. Sequence analysis of tyrosinase gene in ocular and oculocutaneous albinism patients: introducing three novel mutations.

Author

Khordadpoor-Deilamani F, Akbari MT, Karimipoor M, and Javadi G

Subjects

Albinism, Oculocutaneous classification, Consanguinity, DNA Mutational Analysis, Female, Genes, Recessive, Humans, Male, Pedigree, Albinism, Ocular enzymology, Albinism, Ocular genetics, Albinism, Oculocutaneous enzymology, Albinism, Oculocutaneous genetics, Monophenol Monooxygenase genetics, Mutation

Abstract

Purpose: Albinism is a heterogeneous genetic disorder of melanin synthesis that results in hypopigmented eyes (in patients with ocular albinism) or hair, skin, and eyes (in individuals with oculocutaneous albinism). It is associated with decreased visual acuity, nystagmus, strabismus, and photophobia. The tyrosinase gene is known to be involved in both oculocutaneous albinism and autosomal recessive ocular albinism. In this study, we aimed to screen the mutations in the TYR gene in the nonsyndromic OCA and autosomal recessive ocular albinism patients from Iran., Methods: The tyrosinase gene was examined in 23 unrelated patients with autosomal recessive ocular albinism or nonsyndromic OCA using DNA sequencing and bioinformatics analysis., Results: TYR gene mutations were identified in 14 (app. 60%) albinism patients., Conclusions: We found 10 mutations, 3 of which were novel. No mutation was found in our ocular albinism patients, but one of them was heterozygous for the p.R402Q polymorphism.

Published

2015

50. Deep intronic GPR143 mutation in a Japanese family with ocular albinism.

Author

Naruto T, Okamoto N, Masuda K, Endo T, Hatsukawa Y, Kohmoto T, and Imoto I

Subjects

Albinism, Ocular diagnosis, Asian People genetics, Base Sequence, Child, Exome genetics, High-Throughput Nucleotide Sequencing, Humans, Infant, Introns genetics, Japan, Male, Mutation genetics, Sequence Analysis, DNA, Albinism, Ocular genetics, Codon, Nonsense genetics, Eye Proteins genetics, Membrane Glycoproteins genetics, Nystagmus, Congenital genetics

Abstract

Deep intronic mutations are often ignored as possible causes of human disease. Using whole-exome sequencing, we analysed genomic DNAs of a Japanese family with two male siblings affected by ocular albinism and congenital nystagmus. Although mutations or copy number alterations of coding regions were not identified in candidate genes, the novel intronic mutation c.659-131 T > G within GPR143 intron 5 was identified as hemizygous in affected siblings and as heterozygous in the unaffected mother. This mutation was predicted to create a cryptic splice donor site within intron 5 and activate a cryptic acceptor site at 41nt upstream, causing the insertion into the coding sequence of an out-of-frame 41-bp pseudoexon with a premature stop codon in the aberrant transcript, which was confirmed by minigene experiments. This result expands the mutational spectrum of GPR143 and suggests the utility of next-generation sequencing integrated with in silico and experimental analyses for improving the molecular diagnosis of this disease.

Published

2015