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1. Variants in PAX6, PITX3 and HSF4 causing autosomal dominant congenital cataracts

Author

Berry, Vanita, Ionides, Alex, Pontikos, Nikolas, Moore, Anthony T, Quinlan, Roy A, and Michaelides, Michel

Subjects
Genetics, Congenital Structural Anomalies, Pediatric, Human Genome, Eye Disease and Disorders of Vision, 2.1 Biological and endogenous factors, Aetiology, Cataract, Heat Shock Transcription Factors, Homeodomain Proteins, Humans, Mutation, PAX6 Transcription Factor, Pedigree, Transcription Factors, Clinical Sciences, Immunology, Opthalmology and Optometry, Ophthalmology & Optometry
Abstract

BackgroundLens development is orchestrated by transcription factors. Disease-causing variants in transcription factors and their developmental target genes are associated with congenital cataracts and other eye anomalies.MethodsUsing whole exome sequencing, we identified disease-causing variants in two large British families and one isolated case with autosomal dominant congenital cataract. Bioinformatics analysis confirmed these disease-causing mutations as rare or novel variants, with a moderate to damaging pathogenicity score, with testing for segregation within the families using direct Sanger sequencing.ResultsFamily A had a missense variant (c.184 G>A; p.V62M) in PAX6 and affected individuals presented with nuclear cataract. Family B had a frameshift variant (c.470-477dup; p.A160R*) in PITX3 that was also associated with nuclear cataract. A recurrent missense variant in HSF4 (c.341 T>C; p.L114P) was associated with congenital cataract in a single isolated case.ConclusionsWe have therefore identified novel variants in PAX6 and PITX3 that cause autosomal dominant congenital cataract.

Published
2022

2. The genetic landscape of crystallins in congenital cataract

Author

Berry, Vanita, Ionides, Alex, Pontikos, Nikolas, Georgiou, Michalis, Yu, Jing, Ocaka, Louise A, Moore, Anthony T, Quinlan, Roy A, and Michaelides, Michel

Subjects
Biological Sciences, Bioinformatics and Computational Biology, Biomedical and Clinical Sciences, Genetics, Ophthalmology and Optometry, Aging, Pediatric, Clinical Research, Congenital Structural Anomalies, Eye Disease and Disorders of Vision, 2.1 Biological and endogenous factors, Aetiology, Cataract, Crystallins, DNA Mutational Analysis, Humans, Lens, Crystalline, Mutation, Missense, Pedigree, Autosomal dominant congenital cataract, Next generation sequencing, Other Medical and Health Sciences, Genetics & Heredity, Clinical sciences
Abstract

BackgroundThe crystalline lens is mainly composed of a large family of soluble proteins called the crystallins, which are responsible for its development, growth, transparency and refractive index. Disease-causing sequence variants in the crystallins are responsible for nearly 50% of all non-syndromic inherited congenital cataracts, as well as causing cataract associated with other diseases, including myopathies. To date, more than 300 crystallin sequence variants causing cataract have been identified.MethodsHere we aimed to identify the genetic basis of disease in five multi-generation British families and five sporadic cases with autosomal dominant congenital cataract using whole exome sequencing, with identified variants validated using Sanger sequencing. Following bioinformatics analysis, rare or novel variants with a moderate to damaging pathogenicity score, were filtered out and tested for segregation within the families.ResultsWe have identified 10 different heterozygous crystallin variants. Five recurrent variants were found: family-A, with a missense variant (c.145C>T; p.R49C) in CRYAA associated with nuclear cataract; family-B, with a deletion in CRYBA1 (c.272delGAG; p.G91del) associated with nuclear cataract; and family-C, with a truncating variant in CRYGD (c.470G>A; W157*) causing a lamellar phenotype; individuals I and J had variants in CRYGC (c.13A>C; T5P) and in CRYGD (c.418C>T; R140*) causing unspecified congenital cataract and nuclear cataract, respectively. Five novel disease-causing variants were also identified: family D harboured a variant in CRYGC (c.179delG; R60Qfs*) responsible for a nuclear phenotype; family E, harboured a variant in CRYBB1 (c.656G>A; W219*) associated with lamellar cataract; individual F had a variant in CRYGD (c.392G>A; W131*) associated with nuclear cataract; and individuals G and H had variants in CRYAA (c.454delGCC; A152del) and in CRYBB1 (c.618C>A; Y206*) respectively, associated with unspecified congenital cataract. All novel variants were predicted to be pathogenic and to be moderately or highly damaging.ConclusionsWe report five novel variants and five known variants. Some are rare variants that have been reported previously in small ethnic groups but here we extend this to the wider population and record a broader phenotypic spectrum for these variants.

Published
2020

3. Whole Exome Sequencing Reveals Novel and Recurrent Disease-Causing Variants in Lens Specific Gap Junctional Protein Encoding Genes Causing Congenital Cataract.

Author

Berry, Vanita, Ionides, Alex, Pontikos, Nikolas, Moghul, Ismail, Moore, Anthony T, Quinlan, Roy A, and Michaelides, Michel

Subjects
Lens, Crystalline, Animals, Vertebrates, Cataract, Connexins, Pedigree, Sequence Alignment, Amino Acid Sequence, Base Sequence, Protein Conformation, Sequence Homology, Amino Acid, Genes, Dominant, Phenotype, Mutation, Missense, Models, Molecular, Female, Male, Genetic Variation, High-Throughput Nucleotide Sequencing, Exome, United Kingdom, Whole Exome Sequencing, GJA3, GJA8, autosomal dominant congenital cataract, whole exome sequencing, Genetics
Abstract

Pediatric cataract is clinically and genetically heterogeneous and is the most common cause of childhood blindness worldwide. In this study, we aimed to identify disease-causing variants in three large British families and one isolated case with autosomal dominant congenital cataract, using whole exome sequencing. We identified four different heterozygous variants, three in the large families and one in the isolated case. Family A, with a novel missense variant (c.178G>C, p.Gly60Arg) in GJA8 with lamellar cataract; family B, with a recurrent variant in GJA8 (c.262C>T, p.Pro88Ser) associated with nuclear cataract; and family C, with a novel variant in GJA3 (c.771dupC, p.Ser258GlnfsTer68) causing a lamellar phenotype. Individual D had a novel variant in GJA3 (c.82G>T, p.Val28Leu) associated with congenital cataract. Each sequence variant was found to co-segregate with disease. Here, we report three novel and one recurrent disease-causing sequence variant in the gap junctional protein encoding genes causing autosomal dominant congenital cataract. Our study further extends the mutation spectrum of these genes and further facilitates clinical diagnosis. A recurrent p.P88S variant in GJA8 causing isolated nuclear cataract provides evidence of further phenotypic heterogeneity associated with this variant.

Published
2020

4. A novel frameshift variant in BCOR causes congenital nuclear cataract.

Author

Berry, Vanita, Ponnekanti, Manav B., Pontikos, Nikolas, Quinlan, Roy A., and Michaelides, Michel

Subjects
*ACUTE myeloid leukemia, *GENETIC variation, *DEGENERATION (Pathology), *CATARACT, *PHENOTYPES
Abstract

Background: BCL6 co-repressor (BCOR) gene variants are involved in oculofaciocardiodental (OFCD) syndrome, acute myeloid leukaemia, renal tumours, and photoreceptor degenerative diseases. Here, we describe a British family with a pathogenic heterozygous variant in the BCOR gene causing congenital nuclear cataract. Methods: Whole-exome sequencing was conducted on an individual affected by X-linked dominant congenital cataract in a three-generation family to establish the underlying genetic basis. Bioinformatics analysis confirmed the variants with damaging pathogenicity scores. Results: A novel likely pathogenic frameshift variant BCOR NM_001123385.1: c.3621del; p.Lys1207AsnfsTer31, was identified and found to co-segregate with the disease in this family. Conclusions: This is apparently the first report of a variant in BCOR causing X-linked dominant congenital cataract which is potentially isolated or presenting with a remarkably mild systemic phenotype. Our findings extend the genetic basis for congenital cataract and add to the phenotypic spectrum of BCOR variants. [ABSTRACT FROM AUTHOR]

Published
2024
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5. Dysfunctional LAT2 Amino Acid Transporter Is Associated With Cataract in Mouse and Humans

Author

Knöpfel, Emilia Boiadjieva, Vilches, Clara, Camargo, Simone MR, Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L, Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shomi S, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T, Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, and Kloeckener-Gruissem, Barbara

Subjects
Biomedical and Clinical Sciences, Ophthalmology and Optometry, Eye Disease and Disorders of Vision, Aging, Congenital Structural Anomalies, Pediatric, Genetics, 2.1 Biological and endogenous factors, Aetiology, amino acid transporters LAT2 and TAT1, gene expression, cataract, ocular tissues, mouse model, patient screen, Physiology, Medical Physiology, Psychology, Biochemistry and cell biology, Medical physiology
Abstract

Cataract, the loss of ocular lens transparency, accounts for ∼50% of worldwide blindness and has been associated with water and solute transport dysfunction across lens cellular barriers. We show that neutral amino acid antiporter LAT2 (Slc7a8) and uniporter TAT1 (Slc16a10) are expressed on mouse ciliary epithelium and LAT2 also in lens epithelium. Correspondingly, deletion of LAT2 induced a dramatic decrease in lens essential amino acid levels that was modulated by TAT1 defect. Interestingly, the absence of LAT2 led to increased incidence of cataract in mice, in particular in older females, and a synergistic effect was observed with simultaneous lack of TAT1. Screening SLC7A8 in patients diagnosed with congenital or age-related cataract yielded one homozygous single nucleotide deletion segregating in a family with congenital cataract. Expressed in HeLa cells, this LAT2 mutation did not support amino acid uptake. Heterozygous LAT2 variants were also found in patients with cataract some of which showed a reduced transport function when expressed in HeLa cells. Whether heterozygous LAT2 variants may contribute to the pathology of cataract needs to be further investigated. Overall, our results suggest that defects of amino acid transporter LAT2 are implicated in cataract formation, a situation that may be aggravated by TAT1 defects.

Published
2019

6. Whole-genome sequencing reveals a recurrent missense mutation in the Connexin 46 (GJA3) gene causing autosomal-dominant lamellar cataract

Author

Berry, Vanita, Ionides, Alexander CW, Pontikos, Nikolas, Moghul, Ismail, Moore, Anthony T, Cheetham, Michael E, and Michaelides, Michel

Subjects
Biomedical and Clinical Sciences, Ophthalmology and Optometry, Genetics, Biotechnology, Aging, Eye Disease and Disorders of Vision, Human Genome, Pediatric, 2.1 Biological and endogenous factors, Aetiology, Cataract, Child, Connexins, DNA, DNA Mutational Analysis, Female, Genetic Linkage, Genome-Wide Association Study, Haplotypes, Heterozygote, Humans, Lens, Crystalline, Male, Mutation, Missense, Pedigree, Phenotype, Polymerase Chain Reaction, Recurrence, Clinical Sciences, Immunology, Opthalmology and Optometry, Ophthalmology & Optometry, Ophthalmology and optometry
Abstract

PurposeCongenital cataract, opacification of the ocular lens, is clinically and genetically a heterogeneous childhood disease. In this study we aimed to identify the underlying genetic cause of isolated autosomal-dominant lamellar cataract in a multi-generation English family.MethodsWhole-genome sequencing (WGS) was undertaken in two affected subjects and one unaffected individual. Segregation analysis was performed and a known cataract-causing mutation was identified. Segregation was further validated by sanger sequencing in the entire pedigree.ResultsA heterozygous mutation c.7 G > T; p.D3Y was identified in an NH2-terminal region of the gap junction protein GJA3 and found to co-segregate with disease.ConclusionWe have identified a recurrent mutation in GJA3 in a large British pedigree causing the novel phenotype of autosomal-dominant congenital lamellar cataract. Previously, p.D3Y was found in a Hispanic family causing pulverulent cataract. WGS proved an efficient method to find the underlying molecular cause in this large family, which could not be mapped due to uninformative markers.

Published
2018

7. Wolfram gene (WFS1) mutation causes autosomal dominant congenital nuclear cataract in humans

Author

Berry, Vanita, Gregory-Evans, Cheryl, Emmett, Warren, Waseem, Naushin, Raby, Jacob, Prescott, DeQuincy, Moore, Anthony T, and Bhattacharya, Shomi S

Subjects
Pediatric, Clinical Research, Eye Disease and Disorders of Vision, Biotechnology, Genetics, Human Genome, Base Sequence, Cataract, Exons, Female, Genes, Dominant, Genetic Linkage, Genetic Predisposition to Disease, Genotype, Humans, Introns, Male, Membrane Proteins, Molecular Sequence Data, Mutation, Missense, Pedigree, Polymorphism, Single Nucleotide, Clinical Sciences, Genetics & Heredity
Abstract

Congenital cataracts are an important cause of bilateral visual impairment in infants. Through genome-wide linkage analysis in a four-generation family of Irish descent, the disease-associated gene causing autosomal-dominant congenital nuclear cataract was mapped to chromosome 4p16.1. The maximum logarithm of odds (LOD) score was 2.62 at a recombination fraction θ=0, obtained for marker D4S432 physically close to the Wolfram gene (WFS1). By sequencing the coding regions and intron-exon boundaries of WFS1, we identified a DNA substitution (c.1385A-to-G) in exon 8, causing a missense mutation at codon 462 (E462G) of the Wolframin protein. This is the first report of a mutation in this gene causing an isolated nuclear congenital cataract. These findings suggest that the membrane trafficking protein Wolframin may be important for supporting the developing lens.

Published
2013

8. A novel 1-bp deletion in PITX3 causing congenital posterior polar cataract.

Author

Berry, Vanita, Francis, Peter J, Prescott, Quincy, Waseem, Naushin H, Moore, Anthony T, and Bhattacharya, Shomi S

Subjects
Biomedical and Clinical Sciences, Ophthalmology and Optometry, Human Genome, Genetics, Clinical Research, Biotechnology, Cataract, Chromosomes, Human, Pair 10, Cytosine, Exons, Gene Deletion, Genes, Dominant, Genetic Linkage, Genetic Markers, Haplotypes, Homeodomain Proteins, Humans, Lod Score, Pedigree, Transcription Factors, Opthalmology and Optometry, Ophthalmology & Optometry, Ophthalmology and optometry
Abstract

PurposeCataracts are the most common cause of blindness worldwide. Inherited cataract is a clinically and genetically heterogeneous disease. Here we report a novel mutation in the paired-like homeodomain 3 (PITX3) gene segregating in a four generation English family with an isolated autosomal dominant posterior polar cataract.MethodsA genome-wide linkage was performed by means of single nucleotide polymorphism (SNP) and microsatellite markers. Linkage analyses were performed with the GeneHunter and MLINK programs. Direct sequencing of PCR products was performed to detect mutation in the gene, using the BigDye version 3.1 and analyzed using Sequence analysis version 5.2.ResultsGenome-wide linkage analysis with SNP markers, identified a disease-haplotype interval on chromosome 10q. Two point positive logarithm of odds (LOD) scores was obtained with markers D10S205 (Z=3.10 at θ=0.00), flanked by markers D10S1709 and D10S543, which harbors the homeobox gene PITX3. Sequence analysis of PITX3 revealed a 1-bp deletion that cosegregated with all the affected members of this family which resulted in a frameshift in codon 181 and likely to produce an aberrant protein consisting of 127 additional residues.ConclusionsThe 542delC is a novel mutation in PITX3 causing an isolated posterior polar cataract.

Published
2011

9. Focus on molecular mechanisms underlying cataract development: Several hundred genes are associated with congenital forms

Author

Berry, Vanita, Quinlan, Roy A., and Michaelides, Michel

Subjects
Blindness -- Genetic aspects, Vision disorders in children -- Genetic aspects, Genetic disorders -- Genetic aspects, Genes -- Analysis -- Genetic aspects, Developing countries -- Analysis, Cataract -- Genetic aspects, Health
Abstract

Cataracts are the most common cause of blindness worldwide (1) and a very significant cause of visual impairment in infants and children. Congenital cataracts are seen in 10 to 60 [...]

Published
2021

18. Connexin46 mutations in autosomal dominant congenital cataract

Author

Mackay, Donna, Ionides, Alexander, Kibar, Zoha, Rouleau, Guy, Berry, Vanita, Moore, Anthony, Shiels, Alan, and Bhattacharya, Shomi

Subjects
Genetic disorders -- Research, Chromosome mapping -- Usage, Birth defects -- Research, Cataract -- Genetic aspects, Biological sciences
Abstract

Loci for autosomal dominant zonular pulverulent cataract have been mapped to chromosomes 1q (CZP1) and 13q (CZP3), and for the latter genetic refinement has been achieved. Underlying mutations have been identified in the gene for gap junction protein alpha-3 (GJA3) (ital) or connexin46 (Cx46). GJA3 (ital) has been shown to be the sixth member of the connexin gene family implicated in human disease. The importance of gap-junction communication in development of transparent eye lenses is substantiated.

Published
1999

19. Pathogenic variants in the CYP21A2 gene cause isolated autosomal dominant congenital posterior polar cataracts.

Author

Berry, Vanita, Pontikos, Nikolas, Ionides, Alex, Kalitzeos, Angelos, Quinlan, Roy A., and Michaelides, Michel

Subjects
*ADRENOGENITAL syndrome, *GENETIC variation, *CATARACT, *CRYSTALLINE lens, *VISION disorders, *MISSENSE mutation, *ADRENAL glands
Abstract

Congenital cataracts are the most common cause of visual impairment worldwide. Inherited cataract is a clinically and genetically heterogeneous disease. Here we report disease-causing variants in a novel gene, CYP21A2, causing autosomal dominant posterior polar cataract. Variants in this gene are known to cause autosomal recessive congenital adrenal hyperplasia (CAH). Using whole-exome sequencing (WES), we have identified disease-causing sequence variants in two families of British and Irish origin, and in two isolated cases of Asian-Indian and British origin. Bioinformatics analysis confirmed these variants as rare with damaging pathogenicity scores. Segregation was tested within the families using direct Sanger sequencing. A nonsense variant NM_000500.9 c.955 C > T; p.Q319* was identified in CYP21A2 in two families with posterior polar cataract and in an isolated case with unspecified congenital cataract phenotype. This is the same variant previously linked to CAH and identified as Q318* in the literature. We have also identified a rare missense variant NM_000500.9 c.770 T > C; p.M257T in an isolated case with unspecified congenital cataract phenotype. This is the first report of separate sequence variants in CYP21A2 associated with congenital cataract. Our findings extend the genetic basis for congenital cataract and add to the phenotypic spectrum of CYP21A2 variants and particularly the CAH associated Q318* variant. CYP21A2 has a significant role in mineralo- and gluco-corticoid biosynthesis. These findings suggest that CYP21A2 may be important for extra-adrenal biosynthesis of aldosterone and cortisol in the eye lens. [ABSTRACT FROM AUTHOR]

Published
2022
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20. Variants in PAX6, PITX3and HSF4causing autosomal dominant congenital cataracts

Author

Berry, Vanita, Ionides, Alex, Pontikos, Nikolas, Moore, Anthony T., Quinlan, Roy A., and Michaelides, Michel

Abstract

Background: Lens development is orchestrated by transcription factors. Disease-causing variants in transcription factors and their developmental target genes are associated with congenital cataracts and other eye anomalies. Methods: Using whole exome sequencing, we identified disease-causing variants in two large British families and one isolated case with autosomal dominant congenital cataract. Bioinformatics analysis confirmed these disease-causing mutations as rare or novel variants, with a moderate to damaging pathogenicity score, with testing for segregation within the families using direct Sanger sequencing. Results: Family A had a missense variant (c.184 G>A; p.V62M) in PAX6and affected individuals presented with nuclear cataract. Family B had a frameshift variant (c.470–477dup; p.A160R*) in PITX3that was also associated with nuclear cataract. A recurrent missense variant in HSF4(c.341 T>C; p.L114P) was associated with congenital cataract in a single isolated case. Conclusions: We have therefore identified novel variants in PAX6and PITX3that cause autosomal dominant congenital cataract.

Published
2022
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21. A missense mutation in the human connexin50 gene (GJA8 (ital)) underlies autosomal dominant 'zonular pulverulent' cataract, on chromosome 1q

Author

Shiels, alan, Mackay, Donna, Ionides, Alexander, Berry, Vanita, Moore, Anthony, and Chattacharya, Shomi

Subjects
Genetic disorders -- Research, Chromosome mapping -- Usage, Cataract -- Genetic aspects, Biological sciences
Abstract

A missense mutation in the human connexin50 gene (GJA8(ital)) on chromosome 1q brings on autosomal dominant 'zonular pulverulent' cataract. Genetic refinement of the CZP1 (ital) locus has been undertaken successfully. LInkage analysis was undertaken using microsatellite markers on two distantly related branches of the original eight-generation Ev. pedigree. Evidence now exists for the genetic defect thought to underlie the first inherited disease to be linked to a human autosome.

Published
1998

26. Dysfunctional LAT2 Amino Acid Transporter Is Associated With Cataract in Mouse and Humans

Author

Knöpfel, Emilia Boiadjieva, primary, Vilches, Clara, additional, Camargo, Simone M. R., additional, Errasti-Murugarren, Ekaitz, additional, Stäubli, Andrina, additional, Mayayo, Clara, additional, Munier, Francis L., additional, Miroshnikova, Nataliya, additional, Poncet, Nadège, additional, Junza, Alexandra, additional, Bhattacharya, Shomi S., additional, Prat, Esther, additional, Berry, Vanita, additional, Berger, Wolfgang, additional, Heon, Elise, additional, Moore, Anthony T., additional, Yanes, Óscar, additional, Nunes, Virginia, additional, Palacín, Manuel, additional, Verrey, Francois, additional, and Kloeckener-Gruissem, Barbara, additional

Published
2019
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27. Dysfunctional LAT2 Amino Acid Transporter Is Associated With Cataract in Mouse and Humans

Author

Boiadjieva Knöpfel, Emilia, Vilches, Clara, Camargo, Simone M R, Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L, Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shomi S, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T, Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, Kloeckener-Gruissem, Barbara, Boiadjieva Knöpfel, Emilia, Vilches, Clara, Camargo, Simone M R, Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L, Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shomi S, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T, Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, and Kloeckener-Gruissem, Barbara

Abstract

Cataract, the loss of ocular lens transparency, accounts for ∼50% of worldwide blindness and has been associated with water and solute transport dysfunction across lens cellular barriers. We show that neutral amino acid antiporter LAT2 ) and uniporter TAT1 () are expressed on mouse ciliary epithelium and LAT2 also in lens epithelium. Correspondingly, deletion of LAT2 induced a dramatic decrease in lens essential amino acid levels that was modulated by TAT1 defect. Interestingly, the absence of LAT2 led to increased incidence of cataract in mice, in particular in older females, and a synergistic effect was observed with simultaneous lack of TAT1. Screening in patients diagnosed with congenital or age-related cataract yielded one homozygous single nucleotide deletion segregating in a family with congenital cataract. Expressed in HeLa cells, this LAT2 mutation did not support amino acid uptake. Heterozygous LAT2 variants were also found in patients with cataract some of which showed a reduced transport function when expressed in HeLa cells. Whether heterozygous LAT2 variants may contribute to the pathology of cataract needs to be further investigated. Overall, our results suggest that defects of amino acid transporter LAT2 are implicated in cataract formation, a situation that may be aggravated by TAT1 defects.

Published
2019

28. Dysfunctional LAT2 amino acid transporter is associated with cataract in mouse and humans

Author

Hartmann Müller Foundation for Medical Research, Novartis Foundation for Sustainable Development, Swiss National Science Foundation, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Instituto de Salud Carlos III, Generalitat de Catalunya, Centro de Investigación Biomédica en Red Enfermedades Raras (España), Wellcome Trust, National Institute for Health Research (UK), Knöpfel, Emilia Boiadjieva, Vilches, Clara, Camargo, Simone M. R., Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L., Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shom Shanker, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T., Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, Kloeckener-Gruissem, Barbara, Hartmann Müller Foundation for Medical Research, Novartis Foundation for Sustainable Development, Swiss National Science Foundation, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Instituto de Salud Carlos III, Generalitat de Catalunya, Centro de Investigación Biomédica en Red Enfermedades Raras (España), Wellcome Trust, National Institute for Health Research (UK), Knöpfel, Emilia Boiadjieva, Vilches, Clara, Camargo, Simone M. R., Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L., Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shom Shanker, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T., Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, and Kloeckener-Gruissem, Barbara

Abstract

Cataract, the loss of ocular lens transparency, accounts for ~50% of worldwide blindness and has been associated with water and solute transport dysfunction across lens cellular barriers. We show that neutral amino acid antiporter LAT2 (Slc7a8) and uniporter TAT1 (Slc16a10) are expressed on mouse ciliary epithelium and LAT2 also in lens epithelium. Correspondingly, deletion of LAT2 induced a dramatic decrease in lens essential amino acid levels that was modulated by TAT1 defect. Interestingly, the absence of LAT2 led to increased incidence of cataract in mice, in particular in older females, and a synergistic effect was observed with simultaneous lack of TAT1. Screening SLC7A8 in patients diagnosed with congenital or age-related cataract yielded one homozygous single nucleotide deletion segregating in a family with congenital cataract. Expressed in HeLa cells, this LAT2 mutation did not support amino acid uptake. Heterozygous LAT2 variants were also found in patients with cataract some of which showed a reduced transport function when expressed in HeLa cells. Whether heterozygous LAT2 variants may contribute to the pathology of cataract needs to be further investigated. Overall, our results suggest that defects of amino acid transporter LAT2 are implicated in cataract formation, a situation that may be aggravated by TAT1 defects.

Published
2019

30. Understanding the molecular mechanisms underlying cataracts: Several hundred genes have been found to be associated with congenital forms.

Author

Berry, Vanita, Quinlan, Roy A., and Michaelides, Michel

Subjects
GENES, CATARACT, BONE morphogenetic proteins, MEMBRANE proteins, AQUAPORINS, GONADAL dysgenesis
Abstract

12 (1B) Slit-lamp presentation of examples of inherited cataract phenotypes: (A) nuclear cataract, (B) posterior polar cataract, (C) cortical cataract and (D) pulverulent cataract. 46,47 Lens regeneration from endogenous stem cells has been developed to treat cataract: cataract lenses have been removed from mammals and human infants while preserving the lens capsule and LECs. A C B D Figure 1A: Cataract Phenotypes 33% 31% 9% 7% 6% 5% 3% 2% Figure 1B: Inherited Cataract Phenotypes (FIGURE 1A) Frequency of cataract phenotypes seen in families. After the lens vesicle has closed (weeks 4-5; Carnegie stage 15), secondary fibre cells add to the growing lens as the IN SHORT A greater understanding of lens embryology and the phenotype/genotype correlation of cataracts should help guide future therapeutic approaches. [Extracted from the article]

Published
2021

31. A novel missense mutation in LIM2 causing isolated autosomal dominant congenital cataract.

Author

Berry, Vanita, Pontikos, Nikolas, Dudakova, Lubica, Moore, Anthony T., Quinlan, Roy, Liskova, Petra, and Michaelides, Michel

Subjects
*MISSENSE mutation, *CATARACT, *GENETIC disorders, *MEMBRANE proteins, *BLINDNESS
Abstract

Background: Congenital cataract is the most common cause of blindness in the world. Congenital cataracts are clinically and genetically heterogeneous and are mostly inherited in an autosomal dominant fashion. We identified the genetic cause of isolated autosomal dominant cataract in a four-generation British family and a Czech family. Methods: Whole exome sequencing (WES) was performed on one affected member in the British family and two affected members in the Czech family. Results: A novel missense variant c.388C > T; p.(R130C) was identified in the Lens integral membrane protein (LIM2) and found to co-segregate with disease in both families. Conclusions: Here we report the first autosomal dominant congenital cataract variant p.(R130C) in LIM2, causing a non-syndromic pulverulent and nuclear phenotype in European families. [ABSTRACT FROM AUTHOR]

Published
2020
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34. A recurrent splice-site mutation in EPHA2 causing congenital posterior nuclear cataract.

Author

Berry, Vanita, Pontikos, Nikolas, Albarca-Aguilera, Monica, Plagnol, Vincent, Massouras, Andreas, Prescott, DeQuincy, Moore, Anthony T., Arno, Gavin, Cheetham, Michael E., and Michaelides, Michel

Subjects
*CATARACT, *BLINDNESS in children, *NUCLEOTIDE sequencing, *HAPLOTYPES, *DNA mutational analysis, *GENETICS
Abstract

Intoduction: Inherited cataract, opacification of the lens, is the most common worldwide cause of blindness in children. We aimed to identify the genetic cause of autosomal dominant (AD) posterior nuclear cataract in a four generation British family. Methods: Whole genome sequence (WGS) was performed on two affected and one unaffected individual of the family and further validated by direct sequencing. Haplotype analysis was performed via genotying. Results: A splice-site mutation c.2826-9G>A in the geneEPHA2, encoding EPH receptor A2 was identified and found to co-segregate with disease. Conclusions: We have identified a recurrent splice-site mutation c.2826-9G>A inEPHA2causing isolated posterior nuclear cataract, providing evidence of further phenotypic heterogeneity associated with this variant. [ABSTRACT FROM AUTHOR]

Published
2018
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35. Whole-genome sequencing reveals a recurrent missense mutation in the Connexin 46 (GJA3)gene causing autosomal-dominant lamellar cataract

Author

Berry, Vanita, Ionides, Alexander, Pontikos, Nikolas, Moghul, Ismail, Moore, Anthony, Cheetham, Michael, and Michaelides, Michel

Abstract

Congenital cataract, opacification of the ocular lens, is clinically and genetically a heterogeneous childhood disease. In this study we aimed to identify the underlying genetic cause of isolated autosomal-dominant lamellar cataract in a multi-generation English family. Whole-genome sequencing (WGS) was undertaken in two affected subjects and one unaffected individual. Segregation analysis was performed and a known cataract-causing mutation was identified. Segregation was further validated by sanger sequencing in the entire pedigree. A heterozygous mutation c.7 G > T; p.D3Y was identified in an NH2-terminal region of the gap junction protein GJA3 and found to co-segregate with disease. We have identified a recurrent mutation in GJA3 in a large British pedigree causing the novel phenotype of autosomal-dominant congenital lamellar cataract. Previously, p.D3Y was found in a Hispanic family causing pulverulent cataract. WGS proved an efficient method to find the underlying molecular cause in this large family, which could not be mapped due to uninformative markers.

Published
2018
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38. Alpha-B Crystallin Gene (CRYAB) Mutation Causes Dominant Congenital Posterior Polar Cataract in Humans

Author

Berry, Vanita, Bhattacharya, Shom Shanker, Quinlan, Roy A., Berry, Vanita, Bhattacharya, Shom Shanker, and Quinlan, Roy A.

Abstract

Congenital cataracts are an important cause of bilateral visual impairment in infants. In a four-generation family of English descent, we mapped dominant congenital posterior polar cataract to chromosome 11q22-q22.3. The maximum LOD score, 3.92 at recombination fraction 0, was obtained for marker D11S898, near the gene that encodes crystallin alpha-B protein (CRYAB). By sequencing the coding regions of CRYAB, we found in exon 3 a deletion mutation, 450delA, that is associated with cataract in this family. The mutation resulted in a frameshift in codon 150 and produced an aberrant protein consisting of 184 residues. This is the first report of a mutation, in this gene, resulting in isolated congenital cataract.

Published
2001

39. Congenital progressive polymorphic cataract caused by a mutation in the major intrinsic protein of the lens, MIP (AQP0)

Author

Wellcome Trust, Francis, Peter J., Berry, Vanita, Bhattacharya, Shom Shanker, Moore, Anthony T., Wellcome Trust, Francis, Peter J., Berry, Vanita, Bhattacharya, Shom Shanker, and Moore, Anthony T.

Abstract

BACKGROUND: Congenital cataract, when inherited as an isolated abnormality, is phenotypically and genetically heterogeneous. Although there is no agreed nomenclature for the patterns of cataract observed, a recent study identified eight readily identifiable phenotypes. METHODS: The Moorfields Eye Hospital genetic eye clinic database was used to identify a four generation family with isolated autosomal dominant congenital cataracts. All individuals (affected and unaffected) underwent a full ophthalmic assessment. RESULTS: The results of the molecular linkage study identifying a missense mutation in the gene encoding the major intrinsic protein of the lens (MIP) have been published elsewhere. Affected individuals had bilateral discrete progressive punctate lens opacities limited to mid and peripheral lamellae with additional asymmetric polar opacification. One young female had predominantly cortical cataract and another had serpiginous nuclear opacities. CONCLUSIONS: This phenotype has not been recorded in human families before and has been termed polymorphic. The pattern of opacification appears to reflect the distribution of MIP in the lens. Furthermore, this is the first clear evidence of allelic heterogeneity in this condition following the identification of a family with lamellar cataracts who have a different mutation within the MIP gene.

Published
2000

40. Connexin46 Mutations in Autosomal Dominant Congenital Cataract

Author

Wellcome Trust, National Institutes of Health (US), Medical Council of Canada, Moorfields Eye Hospital (UK), Mackay, Donna, Ionides, Alexander, Kibar, Zoha, Rouleau, Guy, Berry, Vanita, Moore, Anthony T., Shiels, Alan, Bhattacharya, Shom Shanker, Wellcome Trust, National Institutes of Health (US), Medical Council of Canada, Moorfields Eye Hospital (UK), Mackay, Donna, Ionides, Alexander, Kibar, Zoha, Rouleau, Guy, Berry, Vanita, Moore, Anthony T., Shiels, Alan, and Bhattacharya, Shom Shanker

Abstract

Loci for autosomal dominant "zonular pulverulent" cataract have been mapped to chromosomes 1q (CZP1) and 13q (CZP3). Here we report genetic refinement of the CZP3 locus and identify underlying mutations in the gene for gap-junction protein alpha-3 (GJA3), or connexin46 (Cx46). Linkage analysis gave a significantly positive two-point LOD score (Z) at marker D13S175 (maximum Z [Zmax]=>7.0; maximum recombination frequency [thetamax] =0). Haplotyping indicated that CZP3 probably lies in the genetic interval D13S1236-D13S175-D13S1316-cen-13pter, close to GJA3. Sequencing of a genomic clone isolated from the CZP3 candidate region identified an open reading frame coding for a protein of 435 amino acids (47,435 D) that shared approximately 88% homology with rat Cx46. Mutation analysis of GJA3 in two families with CZP3 detected distinct sequence changes that were not present in a panel of 105 normal, unrelated individuals. In family B, an A-->G transition resulted in an asparagine-to-serine substitution at codon 63 (N63S) and introduced a novel MwoI restriction site. In family E, insertion of a C at nucleotide 1137 (1137insC) introduced a novel BstXI site, causing a frameshift at codon 380. Restriction analysis confirmed that the novel MwoI and BstXI sites cosegregated with the disease in families B and E, respectively. This study identifies GJA3 as the sixth member of the connexin gene family to be implicated in human disease, and it highlights the physiological importance of gap-junction communication in the development of a transparent eye lens.

Published
1999

41. Connexin 50 mutation in a family with congenital 'zonular nuclear' pulverulent cataract of Pakistani origin

Author

Wellcome Trust, Berry, Vanita, Mackay, Donna, Khaliq, Shagufta, Francis, Peter J., Hameed, Abdul, Anwar, Khalid, Mehdi, S. Qasim, Newbold, Richard J., Ionides, Alexander, Shiels, Alan, Moore, Anthony T., Bhattacharya, Shom Shanker, Wellcome Trust, Berry, Vanita, Mackay, Donna, Khaliq, Shagufta, Francis, Peter J., Hameed, Abdul, Anwar, Khalid, Mehdi, S. Qasim, Newbold, Richard J., Ionides, Alexander, Shiels, Alan, Moore, Anthony T., and Bhattacharya, Shom Shanker

Abstract

Inherited cataract is a clinically and genetically heterogeneous disease that most often presents as a congenital autosomal dominant trait. Here we report linkage of a three-generation family of Pakistani origin with autosomal dominant cataract "zonular nuclear" pulverulent type (CZNP) on chromosome 1q21.1. Genome wide-linkage analysis excluded all the known cataract loci except on chromosome 1q. Significantly positive 2-point lod score values (Z=3.01 at theta=0) were obtained for markers D1S305 and D1S2721, which are known to flank the gene for connexin 50 (Cx50) or gap junction protein alpha-8 (Gja8). Previously a mutation in this gene has been reported in a British family with zonular pulverulent cataract (CZP). Here we describe a second mutation (E48K) in connexin 50 that confirms the involvement of this gene in cataractogenesis.

Published
1999

42. Anterior polar cataract: clinical spectrum and genetic linkage in a single family

Author

Ionides, Alexander, Berry, Vanita, Mackay, Donna, Shiels, Alan, Bhattacharya, Shom Shanker, Moore, Anthony T., Ionides, Alexander, Berry, Vanita, Mackay, Donna, Shiels, Alan, Bhattacharya, Shom Shanker, and Moore, Anthony T.

Abstract

Anterior polar cataract can occur as a sporadic finding, in association with other ocular abnormalities or as an inherited, autosomal dominant disorder. We have demonstrated linkage in a family with autosomal dominant anterior polar cataract to the short arm of chromosome 17, locating the gene to the region 17p12-13. All affected members of this large family had an opacity at the anterior pole of the lens that varied only in size and the effect on visual acuity. Anterior polar cataract is thought to have a minimal effect on visual acuity although in the affected members of this family there was a high incidence of unilateral amblyopia.

Published
1998

43. A locus for autosomal dominant posterior polar cataract on chromosome 1p

Author

Wellcome Trust, Moorfields Eye Hospital (UK), Ionides, Alexander, Berry, Vanita, Mackay, Donna, Moore, Anthony T., Bhattacharya, Shom Shanker, Shiels, Alan, Wellcome Trust, Moorfields Eye Hospital (UK), Ionides, Alexander, Berry, Vanita, Mackay, Donna, Moore, Anthony T., Bhattacharya, Shom Shanker, and Shiels, Alan

Abstract

Autosomal dominant congenital cataract is a clinically and genetically heterogeneous lens disease. Here we report the linkage of a locus for autosomal dominant posterior polar cataract (CPP) to the distal short arm of chromosome 1. To map the CPP locus we performed molecular genetic linkage analysis using microsatellite markers in a three-generation pedigree. After exclusion of 13 known loci and candidate lens genes for autosomal dominant cataract, we obtained significantly positive LOD scores for markers D1S508 (Z = 3.14, theta = 0) and D1S468 (Z = 2.71, theta = 0). Multipoint analysis gave a maximum LOD score of 3.48 (theta = 0.07) between markers D1S508 and D1S468. From haplotype data, however, CPP probably lies in the telomeric interval D1S2845-1pter, which includes the locus for the clinically distinct Volkman congenital cataract (CCV). This study provides the first evidence for genetic heterogeneity of autosomal dominant posterior polar cataract for which a locus had been linked previously to chromosome 16q.

Published
1997

44. Reply to Veromann

Author

Berry, Vanita, primary, Francis, Peter, additional, Reddy, M. Ashwin, additional, Collyer, Dean, additional, Vithana, Eranga, additional, MacKay, Ian, additional, Dawson, Gary, additional, Carey, Alisoun H., additional, Moore, Anthony, additional, Bhattacharya, Shomi S., additional, and Quinlan, Roy A., additional

Published
2002
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