Your search keyword '"Balikova, Irina"' showing total 6 results

1. Two siblings with Heimler syndrome caused by PEX1 variants: follow-up of ophthalmologic findings.

Author

Herijgers D, Denayer E, Balikova I, Witters P, Jacob J, and Casteels I

Subjects

Amelogenesis Imperfecta diagnostic imaging, Amelogenesis Imperfecta physiopathology, Child, Cone-Rod Dystrophies diagnostic imaging, Cone-Rod Dystrophies physiopathology, Electroretinography, Female, Follow-Up Studies, Hearing Loss, Sensorineural diagnostic imaging, Hearing Loss, Sensorineural physiopathology, Humans, Macular Edema diagnostic imaging, Macular Edema physiopathology, Male, Nails, Malformed diagnostic imaging, Nails, Malformed physiopathology, Pedigree, Retina physiopathology, Retrospective Studies, Siblings, Slit Lamp Microscopy, Tomography, Optical Coherence, Tonometry, Ocular, Visual Acuity physiology, ATPases Associated with Diverse Cellular Activities genetics, Amelogenesis Imperfecta genetics, Cone-Rod Dystrophies genetics, Hearing Loss, Sensorineural genetics, Macular Edema genetics, Membrane Proteins genetics, Mutation, Nails, Malformed genetics

Abstract

Background: Heimler syndrome (OMIM number #234580 and #616617) is a rare condition comprising sensorineural hearing loss (SNHL), nail abnormalities and amelogenesis imperfecta. In addition, patients with this syndrome can have retinal dystrophies. Heimler syndrome is caused by bi-allelic pathogenic variants in the PEX1 or PEX6 gene. Only few patients with this syndrome have been reported. We hereby describe two siblings with genetically confirmed Heimler syndrome and provide imaging of the ocular phenotype., Materials and Methods: The medical records of the siblings were reviewed retrospectively., Results: Both brother and sister were diagnosed with SNHL and amelogenesis imperfecta of the permanent teeth; one of the affected siblings also had nail abnormalities. Both patients presented to the ophthalmology department with suboptimal visual acuity, fundus abnormalities and intraretinal cystoid spaces. Full-field electroretinogram revealed a cone-rod dysfunction. A genetic analysis revealed a homozygous likely pathogenic variant c.3077 T > C (p.Leu1026Pro) in the PEX1 gene in both siblings. The parents are heterozygous carriers of the variant., Conclusion: We recommend performing regular ophthalmic examination in patients with Heimler syndrome since the ophthalmic manifestations can manifest later in life. Our patients presented with cone-rod dystrophy and intraretinal cystoid spaces. Review of the literature shows that the ocular phenotype can be very variable in patients with Heimler syndrome.

Published

2021

2. Three cases of molecularly confirmed Knobloch syndrome.

Author

Balikova I, Sanak NS, Fanny D, Smits G, Soblet J, de Baere E, and Cordonnier M

Subjects

Adolescent, Child, Preschool, Encephalocele genetics, Female, Humans, Male, Middle Aged, Prognosis, Retinal Degeneration genetics, Retinal Detachment genetics, Retinal Detachment pathology, Collagen Type XVIII genetics, Encephalocele pathology, Mutation, Retinal Degeneration pathology, Retinal Detachment congenital

Abstract

Background: Knobloch syndrome (OMIM 267750) is a rare autosomal recessive disorder due to genetic defects in the COL18A1 gene. The triad of high myopia, occipital defect, vitreoretinal degeneration has been described as pathognomonic for this condition. Patients with Knobloch syndrome have also extraocular problems as brain and kidney malformations. High genetic and phenotypic variation has been reported in the affected patients. Materials and Methods: Here we provide detailed clinical description of 3 individuals with Knobloch syndrome. Ocular examination and fundus imaging have been performed. Detailed information about systemic conditions has been provided. Results: Mutations in COL18A1 were identified in all three patients. Patient 1 had congenital hip dislocation and patient 2 had renal atrophy, cardiac insufficiency and difficult skin healing. Conclusions: With this report we add to the clinical and genetic knowledge of this rare condition.

Published

2020

3. The majority of autosomal recessive nanophthalmos and posterior microphthalmia can be attributed to biallelic sequence and structural variants in MFRP and PRSS56.

Author

Almoallem B, Arno G, De Zaeytijd J, Verdin H, Balikova I, Casteels I, de Ravel T, Hull S, Suzani M, Destrée A, Peng M, Williams D, Ainsworth JR, Webster AR, Leroy BP, Moore AT, and De Baere E

Subjects

Adolescent, Adult, Aged, Child, Child, Preschool, Cohort Studies, Family, Female, Heterozygote, Humans, Male, Middle Aged, Whole Genome Sequencing, Alleles, DNA Copy Number Variations, Membrane Proteins genetics, Microphthalmos genetics, Mutation, Serine Proteases genetics

Abstract

This study aimed to genetically and clinically characterize a unique cohort of 25 individuals from 21 unrelated families with autosomal recessive nanophthalmos (NNO) and posterior microphthalmia (MCOP) from different ethnicities. An ophthalmological assessment in all families was followed by targeted MFRP and PRSS56 testing in 20 families and whole-genome sequencing in one family. Three families underwent homozygosity mapping using SNP arrays. Eight distinct MFRP mutations were found in 10/21 families (47.6%), five of which are novel including a deletion spanning the 5' untranslated region and the first coding part of exon 1. Most cases harbored homozygous mutations (8/10), while a compound heterozygous and a monoallelic genotype were identified in the remaining ones (2/10). Six distinct PRSS56 mutations were found in 9/21 (42.9%) families, three of which are novel. Similarly, homozygous mutations were found in all but one, leaving 2/21 families (9.5%) without a molecular diagnosis. Clinically, all patients had reduced visual acuity, hyperopia, short axial length and crowded optic discs. Retinitis pigmentosa was observed in 5/10 (50%) of the MFRP group, papillomacular folds in 12/19 (63.2%) of MCOP and in 3/6 (50%) of NNO cases. A considerable phenotypic variability was observed, with no clear genotype-phenotype correlations. Overall, our study represents the largest NNO and MCOP cohort reported to date and provides a genetic diagnosis in 19/21 families (90.5%), including the first MFRP genomic rearrangement, offering opportunities for gene-based therapies in MFRP-associated disease. Finally, our study underscores the importance of sequence and copy number analysis of the MFRP and PRSS56 genes in MCOP and NNO.

Published

2020

4. Where are the missing gene defects in inherited retinal disorders? Intronic and synonymous variants contribute at least to 4% of CACNA1F-mediated inherited retinal disorders.

Author

Zeitz C, Michiels C, Neuillé M, Friedburg C, Condroyer C, Boyard F, Antonio A, Bouzidi N, Milicevic D, Veaux R, Tourville A, Zoumba A, Seneina I, Foussard M, Andrieu C, N Preising M, Blanchard S, Saraiva JP, Mesrob L, Le Floch E, Jubin C, Meyer V, Blanché H, Boland A, Deleuze JF, Sharon D, Drumare I, Defoort-Dhellemmes S, De Baere E, Leroy BP, Zanlonghi X, Casteels I, de Ravel TJ, Balikova I, Koenekoop RK, Laffargue F, McLean R, Gottlob I, Bonneau D, Schorderet DF, L Munier F, McKibbin M, Prescott K, Pelletier V, Dollfus H, Perdomo-Trujillo Y, Faure C, Reiff C, Wissinger B, Meunier I, Kohl S, Banin E, Zrenner E, Jurklies B, Lorenz B, Sahel JA, and Audo I

Subjects

Genetic Predisposition to Disease, Hemizygote, Humans, Introns, Male, Pedigree, RNA Splicing, Silent Mutation, Calcium Channels, L-Type genetics, Eye Diseases, Hereditary genetics, Genetic Diseases, X-Linked genetics, Mutation, Myopia genetics, Night Blindness genetics, Sequence Analysis, DNA methods

Abstract

Inherited retinal disorders (IRD) represent clinically and genetically heterogeneous diseases. To date, pathogenic variants have been identified in ~260 genes. Albeit that many genes are implicated in IRD, for 30-50% of the cases, the gene defect is unknown. These cases may be explained by novel gene defects, by overlooked structural variants, by variants in intronic, promoter or more distant regulatory regions, and represent synonymous variants of known genes contributing to the dysfunction of the respective proteins. Patients with one subgroup of IRD, namely incomplete congenital stationary night blindness (icCSNB), show a very specific phenotype. The major cause of this condition is the presence of a hemizygous pathogenic variant in CACNA1F. A comprehensive study applying direct Sanger sequencing of the gene-coding regions, exome and genome sequencing applied to a large cohort of patients with a clinical diagnosis of icCSNB revealed indeed that seven of the 189 CACNA1F-related cases have intronic and synonymous disease-causing variants leading to missplicing as validated by minigene approaches. These findings highlight that gene-locus sequencing may be a very efficient method in detecting disease-causing variants in clinically well-characterized patients with a diagnosis of IRD, like icCSNB., (© 2019 Wiley Periodicals, Inc.)

Published

2019

5. Ocular manifestations of microcephaly with or without chorioretinopathy, lymphedema or intellectual disability (MCLID) syndrome associated with mutations in KIF11.

Author

Balikova I, Robson AG, Holder GE, Ostergaard P, Mansour S, and Moore AT

Subjects

Child, Child, Preschool, Electroretinography, Facies, Female, Humans, Lymphedema genetics, Male, Microcephaly genetics, Optical Imaging, Phenotype, Retinal Diseases genetics, Retinal Dysplasia genetics, Tomography, Optical Coherence, Visual Acuity, Kinesins genetics, Lymphedema diagnosis, Microcephaly diagnosis, Mutation, Retinal Diseases diagnosis, Retinal Dysplasia diagnosis

Abstract

Purpose: Microcephaly with or without chorioretinopathy, lymphedema or intellectual disability (MCLID) is an autosomal dominant condition. Mutations in KIF11 have been found to be causative in approximately 75% of cases. This study describes the ocular phenotype in patients with confirmed KIF11 mutations., Methods: Standard ophthalmic examination and investigation including visual acuity, refraction and fundus examination was carried out in all patients. Fundus autofluorescence imaging (FAF) was performed in three patients, and four patients underwent spectral domain optical coherence tomography (OCT). Flash electroretinography (ERG) was performed in seven patients, and five underwent additional pattern electroretinography (PERG)., Results: The patients ranged in age from 2 to 10 years. Most presented with visual acuity loss. Fundus examination revealed lacunae of chorioretinal atrophy. Pigmentary macular changes and optic disc pallor were present in three of seven patients. Fundus autofluorescence demonstrated hypoautofluorescence at the macula in two of three patients. The lacunae of chorioretinal atrophy were hypoautofluorescent. The OCT showed atrophic maculae in three of four patients. Follow-up in one patient showed no deterioration of the vision over a 9-year period. The lesions appear not to be progressive on the follow-up imaging. Electrophysiology showed generalized rod and cone dysfunction and severe macular dysfunction. Inner retinal dysfunction was evident in three of seven patients., Conclusions: Patients with KIF11 mutations show a specific ocular phenotype with variable expressivity and intrafamilial variability. Macular atrophy and dysfunction have not been consistently documented before. The fundus lesions appear non-progressive. The findings assist in providing an accurate diagnosis and thus improving the management and follow-up of patients with this syndrome., (© 2015 Acta Ophthalmologica Scandinavica Foundation. Published by John Wiley & Sons Ltd.)

Published

2016

6. No evidence of locus heterogeneity in familial microcephaly with or without chorioretinopathy, lymphedema, or mental retardation syndrome.

Author

Schlögel, Matthieu J., Mendola, Antonella, Fastré, Elodie, Vasudevan, Pradeep, Devriendt, Koen, de Ravel, Thomy J. L., Van Esch, Hilde, Casteels, Ingele, Arroyo Carrera, Ignacio, Cristofoli, Francesca, Fieggen, Karen, Jones, Katheryn, Lipson, Mark, Balikova, Irina, Singer, Ami, Soller, Maria, Villanueva, María Mercedes, Revencu, Nicole, Boon, Laurence M., and Brouillard, Pascal

Subjects

MICROCEPHALY, LYMPHEDEMA, INTELLECTUAL disabilities, KINESIN, PATIENTS, GERM cells

Abstract

Background: Microcephaly with or without chorioretinopathy, lymphedema, or mental retardation syndrome (MCLMR) is a rare autosomal dominant disorder with variable expressivity. It is characterized by mild-to-severe microcephaly, often associated with intellectual disability, ocular defects and lymphedema. It can be sporadic or inherited. Eighty-seven patients have been described to carry a mutation in, which encodes a homotetrameric KIF11 motor kinesin, EG5. Methods: We tested 23 unreported MCLMR index patients for . We also reviewed the clinical phenotypes of KIF11 all our patients as well as of those described in previously published studies. Results: We identified 14 mutations, 12 of which are novel. We detected mutations in 12 affected individuals, from 6 out of 6 familial cases, and in 8 out of 17 sporadic patients. Phenotypic evaluation of patients (our 26 + 61 earlier published = 87) revealed microcephaly in 91%, eye anomalies in 72%, intellectual disability in 67% and lymphedema in 47% of the patients. Unaffected carriers were rare (4 out of 87: 5%). Family history is not a requisite for diagnosis; 31% (16 out of 52) were cases. de novo Conclusions: All inherited cases, and 50% of sporadic cases of MCLMR are due to germline mutations. It is KIF11 possible that mosaic mutations cause the remainder of sporadic cases, which the methods employed here KIF11 were not designed to detect. On the other hand, some of them might have another mimicking disorder and genetic defect, as microcephaly is highly heterogeneous. In aggregate, mutations likely cause the majority, if KIF11 not all, of MCLMR. [ABSTRACT FROM AUTHOR]

Published

2015