Your search keyword '"Lies H. Hoefsloot"' showing total 146 results

1. What proportion of couples with a history of recurrent pregnancy loss and with a balanced rearrangement in one parent can potentially be identified through cell-free DNA genotyping?

Author

Laura J. C. M. van Zutven, Jona Mijalkovic, Monique van Veghel-Plandsoen, Margaret Goense, Marike Polak, Maarten F. C. M. Knapen, Sabina de Weerd, Marieke Joosten, Karin E. M. Diderich, Lies H. Hoefsloot, Diane Van Opstal, and Malgorzata I. Srebniak

Subjects

Recurrent pregnancy loss, NIPT, Karyotyping, Balanced translocation, cfDNA, Genetics, QH426-470

Abstract

Abstract Background Balanced chromosome aberrations are reported in about 1:30 couples with recurrent pregnancy loss (RPL). Karyotyping of both parents is necessary to identify these aberrations. Genome-wide non-invasive prenatal testing (NIPT) in case of recurrent pregnancy loss could be a more efficient way to identify couples at increased risk for carrying a balanced chromosome rearrangement. The aim of this study was to evaluate whether the potential fetal imbalances caused by parental balanced aberrations detected in our center are large enough to be detectable by genome-wide non-invasive prenatal testing (NIPT). Material and methods From January 1970 until May 2020 our laboratory received 30,863 unique requests for karyotyping due to RPL. We have identified 16,045 couples and evaluated all abnormal cytogenetic results to assess the minimal size of the involved chromosomal segments in potential unbalanced products of the rearrangements. Results In the presented cohort we detected 277 aberrant balanced translocations/inversions in females and 185 in males amongst 16,045 couples with RPL, which can be translated to a risk of 1:35 (2.9%, 95% CI 2.6–3.2%). Our study showed that the vast majority (98.7%, 95% CI 97.1–99.5%) of these balanced aberrations will potentially cause a fetal imbalance > 10 Mb, which is detectable with genome-wide NIPT if it was performed during one of the miscarriages. Conclusions Our study suggests that genome-wide NIPT is able to reveal most unbalanced products of balanced chromosomal rearrangements carried by couples with RPL and therefore can potentially identify balanced chromosomal aberration carriers. Moreover, our data suggest that these couples can be offered NIPT in case they decline invasive testing in future pregnancies.

Published

2023

2. Identification of Rare Variants Involved in High Myopia Unraveled by Whole Genome Sequencing

Author

Annechien E.G. Haarman, MD, Caroline C.W. Klaver, MD, PhD, Milly S. Tedja, MD, Susanne Roosing, PhD, Galuh Astuti, MSc, Christian Gilissen, PhD, Lies H. Hoefsloot, MD, PhD, Marianne van Tienhoven, BSc, Tom Brands, Ing, Frank J. Magielsen, Ing, Bert H.J.F.M.M. Eussen, Ing, Annelies de Klein, PhD, Erwin Brosens, PhD, and Virginie J.M. Verhoeven, MD, PhD

Subjects

Blindness, Complex genetics, Genetic risk score, Mendelian diseases, Ophthalmology, RE1-994

Abstract

Purpose: Myopia (nearsightedness) is a condition in which a refractive error (RE) affects vision. Although common variants explain part of the genetic predisposition (18%), most of the estimated 70% heritability is missing. Here, we investigate the contribution of rare genetic variation because this might explain more of the missing heritability in the more severe forms of myopia. In particular, high myopia can lead to blindness and has a tremendous impact on a patient and at the societal level. The exact molecular mechanisms behind this condition are not yet completely unraveled, but whole genome sequencing (WGS) studies have the potential to identify novel (rare) disease genes, explaining the high heritability. Design: Cross-sectional study performed in the Netherlands. Participants: We investigated 159 European patients with high myopia (RE > −10 diopters). Methods: We performed WGS using a stepwise filtering approach and burden analysis. The contribution of common variants was calculated as a genetic risk score (GRS). Main Outcome Measures: Rare variant burden, GRS. Results: In 25% (n = 40) of these patients, there was a high (> 75th percentile) contribution of common predisposing variants; that is, these participants had higher GRSs. In 7 of the remaining 119 patients (6%), deleterious variants in genes associated with known (ocular) disorders, such as retinal dystrophy disease (prominin 1 [PROM1]) or ocular development (ATP binding cassette subfamily B member 6 [ABCB6], TGFB induced factor homeobox 1 [TGIF1]), were identified. Furthermore, without using a gene panel, we identified a high burden of rare variants in 8 novel genes associated with myopia. The genes heparan sulfate 6-O-sulfotransferase 1 (HS6ST1) (proportion in study population vs. the Genome Aggregation Database (GnomAD) 0.14 vs. 0.03, P = 4.22E-17), RNA binding motif protein 20 (RBM20) (0.15 vs. 0.06, P = 4.98E-05), and MAP7 domain containing 1 (MAP7D1) (0.19 vs. 0.06, P = 1.16E-10) were involved in the Wnt signaling cascade, melatonin degradation, and ocular development and showed most biologically plausible associations. Conclusions: We found different contributions of common and rare variants in low and high grade myopia. Using WGS, we identified some interesting candidate genes that could explain the high myopia phenotype in some patients. Financial Disclosure(s): The author(s) have no proprietary or commercial interest in any materials discussed in this article.

Published

2023

3. Novel GAA Variants and Mosaicism in Pompe Disease Identified by Extended Analyses of Patients with an Incomplete DNA Diagnosis

Author

Stijn L.M. in ’t Groen, Douglas O.S. de Faria, Alessandro Iuliano, Johanna M.P. van den Hout, Hannie Douben, Trijnie Dijkhuizen, David Cassiman, Peter Witters, Miguel-Ángel Barba Romero, Annelies de Klein, Galhana M. Somers-Bolman, Jasper J. Saris, Lies H. Hoefsloot, Ans T. van der Ploeg, Atze J. Bergsma, and W.W.M. Pim Pijnappel

Subjects

glycogen storage disease type II, Pompe disease, diagnostics, mosaicism, segmental uniparental isodisomy, Genetics, QH426-470, Cytology, QH573-671

Abstract

Pompe disease is a metabolic disorder caused by a deficiency of the glycogen-hydrolyzing lysosomal enzyme acid α-glucosidase (GAA), which leads to progressive muscle wasting. This autosomal-recessive disorder is the result of disease-associated variants located in the GAA gene. In the present study, we performed extended molecular diagnostic analysis to identify novel disease-associated variants in six suspected Pompe patients from four different families for which conventional diagnostic assays were insufficient. Additional assays, such as a generic-splicing assay, minigene analysis, SNP array analysis, and targeted Sanger sequencing, allowed the identification of an exonic deletion, a promoter deletion, and a novel splicing variant located in the 5′ UTR. Furthermore, we describe the diagnostic process for an infantile patient with an atypical phenotype, consisting of left ventricular hypertrophy but no signs of muscle weakness or motor problems. This led to the identification of a genetic mosaicism for a very severe GAA variant caused by a segmental uniparental isodisomy (UPD). With this study, we aim to emphasize the need for additional analyses to detect new disease-associated GAA variants and non-Mendelian genotypes in Pompe disease where conventional DNA diagnostic assays are insufficient.

Published

2020

4. Social and medical need for whole genome high resolution NIPT

Author

Malgorzata I. Srebniak, Maarten F. C. M. Knapen, Lutgarde C. P. Govaerts, Marike Polak, Marieke Joosten, Karin E. M. Diderich, Laura J. C. M. van Zutven, Krista A. K. E. Prinsen, Sam Riedijk, Attie T. J. I. Go, Robert‐Jan H. Galjaard, Lies H. Hoefsloot, and Diane Van Opstal

Subjects

diagnostic yield, microarray, NIPT, patients preferences, prenatal diagnosis, Genetics, QH426-470

Abstract

Abstract Background Two technological innovations in the last decade significantly influenced the diagnostic yield of prenatal cytogenetic testing: genomic microarray allowing high resolution analysis and noninvasive prenatal testing (NIPT) focusing on aneuploidy. To anticipate future trends in prenatal screening and diagnosis, we evaluated the number of invasive tests in our center and the number of aberrant cases diagnosed in the last decade. Methods We retrospectively analyzed fetal chromosomal aberrations diagnosed in 2009–2018 in 8,608 pregnancies without ultrasound anomalies. Results The introduction of NIPT as the first‐tier test led to a substantial decrease in the number of invasive tests and a substantially increased diagnostic yield of aneuploidies in the first trimester. However, we have also noted a decreased detection of submicroscopic aberrations, since the number of invasive tests substantially decreased. We have observed that pregnant women were interested in broader scope of prenatal screening and diagnosis than detection of common trisomies. Conclusion Since the frequency of syndromic disorders caused by microdeletions/microduplications is substantial and current routine NIPT and ultrasound investigations are not able to detect them, we suggest that a noninvasive test with resolution comparable to microarrays should be developed, which will also meet patient's needs.

Published

2020

5. Web-accessible application for identifying pathogenic transcripts with RNA-seq: Increased sensitivity in diagnosis of neurodevelopmental disorders

Author

Jordy Dekker, Rachel Schot, Michiel Bongaerts, Walter G. de Valk, Monique M. van Veghel-Plandsoen, Kathryn Monfils, Hannie Douben, Peter Elfferich, Esmee Kasteleijn, Leontine M.A. van Unen, Geert Geeven, Jasper J. Saris, Yvette van Ierland, Frans W. Verheijen, Marianne L.T. van der Sterre, Farah Sadeghi Niaraki, Daphne J. Smits, Hidde H. Huidekoper, Monique Williams, Martina Wilke, Virginie J.M. Verhoeven, Marieke Joosten, Anneke J.A. Kievit, Ingrid M.B.H. van de Laar, Lies H. Hoefsloot, Marianne Hoogeveen-Westerveld, Mark Nellist, Grazia M.S. Mancini, Tjakko J. van Ham, Clinical Genetics, Erasmus MC other, Pediatrics, and Emergency Medicine

Subjects

Genetics, Genetics (clinical)

Abstract

For neurodevelopmental disorders (NDDs), a molecular diagnosis is key for management, predicting outcome, and counseling. Often, routine DNA-based tests fail to establish a genetic diagnosis in NDDs. Transcriptome analysis (RNA sequencing [RNA-seq]) promises to improve the diagnostic yield but has not been applied to NDDs in routine diagnostics. Here, we explored the diagnostic potential of RNA-seq in 96 individuals including 67 undiagnosed subjects with NDDs. We performed RNA-seq on single individuals' cultured skin fibroblasts, with and without cycloheximide treatment, and used modified OUTRIDER Z scores to detect gene expression outliers and mis-splicing by exonic and intronic outliers. Analysis was performed by a user-friendly web application, and candidate pathogenic transcriptional events were confirmed by secondary assays. We identified intragenic deletions, monoallelic expression, and pseudoexonic insertions but also synonymous and non-synonymous variants with deleterious effects on transcription, increasing the diagnostic yield for NDDs by 13%. We found that cycloheximide treatment and exonic/intronic Z score analysis increased detection and resolution of aberrant splicing. Importantly, in one individual mis-splicing was found in a candidate gene nearly matching the individual's specific phenotype. However, pathogenic splicing occurred in another neuronal-expressed gene and provided a molecular diagnosis, stressing the need to customize RNA-seq. Lastly, our web browser application allowed custom analysis settings that facilitate diagnostic application and ranked pathogenic transcripts as top candidates. Our results demonstrate that RNA-seq is a complementary method in the genomic diagnosis of NDDs and, by providing accessible analysis with improved sensitivity, our transcriptome analysis approach facilitates wider implementation of RNA-seq in routine genome diagnostics.

Published

2023

6. AMFR dysfunction causes autosomal recessive spastic paraplegia in human that is amenable to statin treatment in a preclinical model

Author

Ruizhi Deng, Eva Medico-Salsench, Anita Nikoncuk, Reshmi Ramakrishnan, Kristina Lanko, Nikolas A. Kühn, Herma C. van der Linde, Sarah Lor-Zade, Fatimah Albuainain, Yuwei Shi, Soheil Yousefi, Ivan Capo, Evita Medici van den Herik, Marjon van Slegtenhorst, Rick van Minkelen, Geert Geeven, Monique T. Mulder, George J. G. Ruijter, Dieter Lütjohann, Edwin H. Jacobs, Henry Houlden, Alistair T. Pagnamenta, Kay Metcalfe, Adam Jackson, Siddharth Banka, Lenika De Simone, Abigail Schwaede, Nancy Kuntz, Timothy Blake Palculict, Safdar Abbas, Muhammad Umair, Mohammed AlMuhaizea, Dilek Colak, Hanan AlQudairy, Maysoon Alsagob, Catarina Pereira, Roberta Trunzo, Vasiliki Karageorgou, Aida M. Bertoli-Avella, Peter Bauer, Arjan Bouman, Lies H. Hoefsloot, Tjakko J. van Ham, Mahmoud Issa, Maha S. Zaki, Joseph G. Gleeson, Rob Willemsen, Namik Kaya, Stefan T. Arold, Reza Maroofian, Leslie E. Sanderson, Tahsin Stefan Barakat, Clinical Genetics, Neurology, and Internal Medicine

Subjects

Cellular and Molecular Neuroscience, AMFR, Zebrafish disease modeling, Neurology, Whole genome sequencing, Precision medicine, Genetics, Hereditary spastic paraplegia, Cholesterol metabolism, Statin, Neurology (clinical), Pathology and Forensic Medicine

Abstract

Hereditary spastic paraplegias (HSP) are rare, inherited neurodegenerative or neurodevelopmental disorders that mainly present with lower limb spasticity and muscle weakness due to motor neuron dysfunction. Whole genome sequencing identified bi-allelic truncating variants in AMFR, encoding a RING-H2 finger E3 ubiquitin ligase anchored at the membrane of the endoplasmic reticulum (ER), in two previously genetically unexplained HSP-affected siblings. Subsequently, international collaboration recognized additional HSP-affected individuals with similar bi-allelic truncating AMFR variants, resulting in a cohort of 20 individuals from 8 unrelated, consanguineous families. Variants segregated with a phenotype of mainly pure but also complex HSP consisting of global developmental delay, mild intellectual disability, motor dysfunction, and progressive spasticity. Patient-derived fibroblasts, neural stem cells (NSCs), and in vivo zebrafish modeling were used to investigate pathomechanisms, including initial preclinical therapy assessment. The absence of AMFR disturbs lipid homeostasis, causing lipid droplet accumulation in NSCs and patient-derived fibroblasts which is rescued upon AMFR re-expression. Electron microscopy indicates ER morphology alterations in the absence of AMFR. Similar findings are seen in amfra-/- zebrafish larvae, in addition to altered touch-evoked escape response and defects in motor neuron branching, phenocopying the HSP observed in patients. Interestingly, administration of FDA-approved statins improves touch-evoked escape response and motor neuron branching defects in amfra-/- zebrafish larvae, suggesting potential therapeutic implications. Our genetic and functional studies identify bi-allelic truncating variants in AMFR as a cause of a novel autosomal recessive HSP by altering lipid metabolism, which may potentially be therapeutically modulated using precision medicine with statins.

Published

2023

7. Early onset X-linked female limited high myopia in three multigenerational families caused by novel mutations in the ARR3 gene

Author

Ralph Mazijk, Annechien E.G. Haarman, Lies H. Hoefsloot, Jan R. Polling, Marianne Tienhoven, Caroline C.W. Klaver, Virginie J.M. Verhoeven, Sjoukje E. Loudon, Alberta A.H.J. Thiadens, Anneke J.A. Kievit, Clinical Genetics, Ophthalmology, and Epidemiology

Subjects

genetic structures, Arrestins, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], eye diseases, Pedigree, Cohort Studies, Genes, X-Linked, Mutation, Exome Sequencing, Genetics, Myopia, Humans, Female, Genetics (clinical)

Abstract

Contains fulltext : 249568.pdf (Publisher’s version ) (Open Access) This study describes the clinical spectrum and genetic background of high myopia caused by mutations in the ARR3 gene. We performed an observational case series of three multigenerational families with high myopia (SER≤-6D), from the departments of Clinical Genetics and Ophthalmology of a tertiary Dutch hospital. Whole-exome sequencing (WES) with a vision-related gene panel was performed, followed by a full open exome sequencing. We identified three Caucasian families with high myopia caused by three different pathogenic variants in the ARR3 gene (c.214C>T, p.Arg72*; c.767+1G>A; p.?; c.848delG, p.(Gly283fs)). Myopia was characterized by a high severity (

Published

2022

8. High-yield identification of pathogenic NF1 variants by skin fibroblast transcriptome screening after apparently normal diagnostic DNA testing

Author

Hannie C. W. Douben, Mark Nellist, Leontine van Unen, Peter Elfferich, Esmee Kasteleijn, Marianne Hoogeveen‐Westerveld, Jesse Louwen, Monique van Veghel‐Plandsoen, Walter de Valk, Jasper J. Saris, Femke Hendriks, Esther Korpershoek, Lies H. Hoefsloot, Margreethe van Vliet, Yolande van Bever, Ingrid van de Laar, Emmelien Aten, Augusta M. A. Lachmeijer, Walter Taal, Lisa van den Bersselaar, Juliette Schuurmans, Rianne Oostenbrink, Rick van Minkelen, Yvette van Ierland, Tjakko J. van Ham, Clinical Genetics, Erasmus MC other, Pathology, Neurology, and Pediatrics

Subjects

Neurofibromatosis 1, Neurofibromin 1, RNA Splicing, RNA-sequencing, DNA, Fibroblasts, mRNA splicing, neurofibromatosis type 1, molecular diagnostics, noncoding variants, Mutation, Genetics, Humans, Genetics (clinical), exon skipping

Abstract

Neurofibromatosis type 1 (NF1) is caused by inactivating mutations in NF1. Due to the size, complexity, and high mutation rate at the NF1 locus, the identification of causative variants can be challenging. To obtain a molecular diagnosis in 15 individuals meeting diagnostic criteria for NF1, we performed transcriptome analysis (RNA-seq) on RNA obtained from cultured skin fibroblasts. In each case, routine molecular DNA diagnostics had failed to identify a disease-causing variant in NF1. A pathogenic variant or abnormal mRNA splicing was identified in 13 cases: 6 deep intronic variants and 2 transposon insertions causing noncanonical splicing, 3 postzygotic changes, 1 branch point mutation and, in 1 case, abnormal splicing for which the responsible DNA change remains to be identified. These findings helped resolve the molecular findings for an additional 17 individuals in multiple families with NF1, demonstrating the utility of skin-fibroblast-based transcriptome analysis for molecular diagnostics. RNA-seq improves mutation detection in NF1 and provides a powerful complementary approach to DNA-based methods. Importantly, our approach is applicable to other genetic disorders, particularly those caused by a wide variety of variants in a limited number of genes and specifically for individuals in whom routine molecular DNA diagnostics did not identify the causative variant.

Published

2022

9. The potential diagnostic yield of whole exome sequencing in pregnancies complicated by fetal ultrasound anomalies

Author

Grazia M.S. Mancini, Kathleen Romijn, Alice S. Brooks, Hennie T. Brüggenwirth, Marjon van Slegtenhorst, Ingrid M.B.H. van de Laar, Lutgarde C.P. Govaerts, Joan N.R. Kromosoeto, Malgorzata I. Srebniak, Robert-Jan H. Galjaard, Marike Polak, Diane Van Opstal, Attie T.J.I. Go, Yolande van Bever, Lies H. Hoefsloot, Marieke Joosten, Martina Wilke, Maarten F. C. M. Knapen, Karin E. M. Diderich, Clinical Genetics, Research Methods and Techniques, and Obstetrics & Gynecology

Subjects

Adult, medicine.medical_specialty, Microarray, Genetic counseling, Chromosome Disorders, Prenatal diagnosis, Ultrasonography, Prenatal, whole exome sequencing, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, Exome Sequencing, ultrasound anomalies, medicine, Humans, Abnormalities, Multiple, Genetic Testing, Original Research Article, fetal anomalies, 030212 general & internal medicine, Exome, Exome sequencing, Retrospective Studies, prenatal whole exome sequencing testing, Fetus, 030219 obstetrics & reproductive medicine, Obstetrics, business.industry, Genetic disorder, Obstetrics and Gynecology, Retrospective cohort study, General Medicine, medicine.disease, Fetal Diseases, diagnostic yield, Female, business

Abstract

IntroductionThe aim of this retrospective cohort study was to determine the potential diagnostic yield of prenatal whole exome sequencing in fetuses with structural anomalies on expert ultrasound scans and normal chromosomal microarray results.Material and methodsIn the period 2013-2016, 391 pregnant women with fetal ultrasound anomalies who received normal chromosomal microarray results, were referred for additional genetic counseling and opted for additional molecular testing pre- and/or postnatally. Most of the couples received only a targeted molecular test and in 159 cases (40.7%) whole exome sequencing (broad gene panels or open exome) was performed. The results of these molecular tests were evaluated retrospectively, regardless of the time of the genetic diagnosis (prenatal or postnatal).ResultsIn 76 of 391 fetuses (19.4%, 95% CI 15.8%-23.6%) molecular testing provided a genetic diagnosis with identification of (likely) pathogenic variants. In the majority of cases (91.1%, 73/76) the (likely) pathogenic variant would be detected by prenatal whole exome sequencing analysis.ConclusionsOur retrospective cohort study shows that prenatal whole exome sequencing, if offered by a clinical geneticist, in addition to chromosomal microarray, would notably increase the diagnostic yield in fetuses with ultrasound anomalies and would allow early diagnosis of a genetic disorder irrespective of the (incomplete) fetal phenotype.

Published

2021

10. RNA-sequencing improves diagnosis for neurodevelopmental disorders by identifying pathogenic non-coding variants and reinterpretation of coding variants

Author

Jordy Dekker, Rachel Schot, Michiel Bongaerts, Walter G. de Valk, Monique M. van Veghel-Plandsoen, Kathryn Monfils, Hannie Douben, Peter Elfferich, Esmee Kasteleijn, Leontine M.A. van Unen, Geert Geeven, Jasper J. Saris, Yvette van Ierland, Frans W. Verheijen, Marianne L.T. van der Sterre, Farah Sadeghi Niaraki, Hidde H. Huidekoper, Monique Williams, Martina Wilke, Virginie J.M. Verhoeven, Marieke Joosten, Anneke J.A. Kievit, Ingrid M.B.H. van de Laar, Lies H. Hoefsloot, Marianne Hoogeveen-Westerveld, Mark Nellist, Grazia M.S. Mancini, and Tjakko J. van Ham

Abstract

BackgroundFor neurodevelopmental disorders (NDD), a molecular diagnosis is key for predicting outcome, treatment and genetic counseling. Currently, in about half of NDD cases, routine DNA-based testing fails to establish a genetic diagnosis. Transcriptome analysis (RNA-seq) improves the diagnostic yield for some groups of diseases, but has not been applied to NDD in a routine diagnostic setting.MethodsHere, we explored the diagnostic potential of RNA-seq in a cohort of 96 individuals including 67 undiagnosed NDD subjects. We created a user-friendly web-application to analyze RNA-seq data from single individuals’ cultured skin fibroblasts for genic, exonic and intronic expression outliers, based on modified OUTRIDER Z-scores. Candidate pathogenic events were complemented/matched with genomic data and, if required, confirmed with additional functional assays.ResultsWe identified pathogenic small genomic deletions, mono-allelic expression, aberrant splicing events, deep intronic variants resulting in pseudo-exon insertion, but also synonymous and nonsynonymous variants with deleterious effects on transcription. This approach increased the diagnostic yield for NDD by 12%. Diagnostic pitfalls during transcriptome analysis include detection of splice abnormalities in putative disease genes caused by benign polymorphisms and/or absence of expression of the responsible gene in the tissue of choice. This was misleading in one case and could have led to the wrong diagnosis in the absence of appropriate phenotyping.ConclusionsNonetheless, our results demonstrate the utility of RNA-seq in molecular diagnostics and stress the importance of multidisciplinary team consultation. In particular, the approach is useful for the identification and interpretation of unexpected pathogenic changes in mRNA processing and expression in NDD.

Published

2022

11. Novel GAA Variants and Mosaicism in Pompe Disease Identified by Extended Analyses of Patients with an Incomplete DNA Diagnosis

Author

Alessandro Iuliano, Johanna M. P. Van den Hout, Stijn L.M. in 't Groen, Lies H. Hoefsloot, W.W.M. Pim Pijnappel, David Cassiman, Hannie Douben, Ans T. van der Ploeg, Atze J. Bergsma, Jasper J. Saris, Galhana M. Somers-Bolman, Miguel-Ángel Barba Romero, Douglas O. S. de Faria, Peter Witters, T. Dijkhuizen, Annelies de Klein, Pediatrics, Clinical Genetics, and Internal Medicine

Subjects

0301 basic medicine, lcsh:QH426-470, UNIPARENTAL DISOMY, THERAPY, EXON INCLUSION, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Genotype, Glycogen storage disease type II, Genetics, medicine, diagnostics, lcsh:QH573-671, Molecular Biology, Gene, Sanger sequencing, COMPLEX, business.industry, lcsh:Cytology, DELETION, Metabolic disorder, Pompe disease, medicine.disease, ALPHA-GLUCOSIDASE, segmental uniparental isodisomy, Uniparental disomy, lcsh:Genetics, 030104 developmental biology, mosaicism, Uniparental Isodisomy, glycogen storage disease type II, 030220 oncology & carcinogenesis, HUMAN GENE MUTATION, symbols, Molecular Medicine, business, Minigene

Abstract

Pompe disease is a metabolic disorder caused by a deficiency of the glycogen-hydrolyzing lysosomal enzyme acid α-glucosidase (GAA), which leads to progressive muscle wasting. This autosomal-recessive disorder is the result of disease-associated variants located in the GAA gene. In the present study, we performed extended molecular diagnostic analysis to identify novel disease-associated variants in six suspected Pompe patients from four different families for which conventional diagnostic assays were insufficient. Additional assays, such as a generic-splicing assay, minigene analysis, SNP array analysis, and targeted Sanger sequencing, allowed the identification of an exonic deletion, a promoter deletion, and a novel splicing variant located in the 5' UTR. Furthermore, we describe the diagnostic process for an infantile patient with an atypical phenotype, consisting of left ventricular hypertrophy but no signs of muscle weakness or motor problems. This led to the identification of a genetic mosaicism for a very severe GAA variant caused by a segmental uniparental isodisomy (UPD). With this study, we aim to emphasize the need for additional analyses to detect new disease-associated GAA variants and non-Mendelian genotypes in Pompe disease where conventional DNA diagnostic assays are insufficient. ispartof: MOLECULAR THERAPY-METHODS & CLINICAL DEVELOPMENT vol:17 pages:337-348 ispartof: location:United States status: published

Published

2020

12. Noninvasive prenatal testing as compared to chorionic villus sampling is more sensitive for the detection of confined placental mosaicism involving the cytotrophoblast

Author

Geerke M. Eggenhuizen, Karin E. M. Diderich, Nicole van Koetsveld, Attie T.J.I. Go, Malgorzata I. Srebniak, Femke A. T. de Vries, Wai Yee Cheung, Diane Van Opstal, Lutgarde C.P. Govaerts, Walter G. de Valk, Robert-Jan H. Galjaard, Stefanie van Veen, Lies H. Hoefsloot, Maarten F. C. M. Knapen, Marieke Joosten, Marjan Boter, Fernanda Sarquis Jehee, Iris H.I.M. Hollink, Clinical Genetics, and Obstetrics & Gynecology

Subjects

Pathology, medicine.medical_specialty, Cytotrophoblast, medicine.diagnostic_test, business.industry, Obstetrics and Gynecology, Chorionic villus sampling, General Medicine, Research Letters, medicine.anatomical_structure, medicine, Research Letter, Confined placental mosaicism, business, Genetics (clinical)

Published

2020

13. Prenatal ultrasound finding of atypical genitalia: Counseling, genetic testing and outcomes

Author

Yolande van Bever, Irene A. L. Groenenberg, Maarten F. C. M. Knapen, Arianne B. Dessens, Sabine E. Hannema, Katja P. Wolffenbuttel, Karin E. M. Diderich, Lies H. Hoefsloot, Malgorzata I. Srebniak, Hennie T. Bruggenwirth, Pediatrics, Amsterdam Gastroenterology Endocrinology Metabolism, Amsterdam Reproduction & Development (AR&D), Clinical Genetics, Obstetrics & Gynecology, Child and Adolescent Psychiatry / Psychology, Urology, and Amsterdam Reproduction & Development

Subjects

Obstetrics and Gynecology, Genetics (clinical)

Abstract

Objective To report uptake of genetic counseling (GC) and prenatal genetic testing after the finding of atypical genitalia on prenatal ultrasound (US) and the clinical and genetic findings of these pregnancies. Methods A retrospective cohort study (2017-2019) of atypical fetal genitalia in a large expert center for disorders/differences of sex development. We describe counseling aspects, invasive prenatal testing, genetic and clinical outcome of fetuses apparently without [group 1, n = 22 (38%)] or with [group 2, n = 36 (62%)] additional anomalies on US. Results In group 1, 86% of parents opted for GC versus 72% in group 2, and respectively 58% and 15% of these parents refrained from invasive testing. Atypical genitalia were postnatally confirmed in 91% (group 1) and 64% (group 2), indicating a high rate of false positive US diagnosis of ambiguous genitalia. Four genetic diagnoses were established in group 1 (18%) and 10 in group 2 (28%). The total genetic diagnostic yield was 24%. No terminations of pregnancy occurred in group 1. Conclusions For optimal care, referral for an expert fetal US scan, GC and invasive diagnostics including broad testing should be offered after prenatal detection of isolated atypical genitalia.

Published

2022

14. Whole exome sequencing of known eye genes reveals genetic causes for high myopia

Author

Annechien E G Haarman, Alberta A H J Thiadens, Marianne van Tienhoven, Sjoukje E Loudon, J E M M Annelies de Klein, Erwin Brosens, Jan Roelof Polling, Vyne van der Schoot, Arjan Bouman, Anneke J A Kievit, Lies H Hoefsloot, Caroline C W Klaver, Virginie J M Verhoeven, Ophthalmology, Epidemiology, and Clinical Genetics

Subjects

Adult, Retinal Dystrophies, Exome Sequencing, Genetics, Myopia, Humans, General Medicine, Child, Eye, Eye Proteins, Molecular Biology, Genetics (clinical), Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12]

Abstract

Contains fulltext : 282474.pdf (Publisher’s version ) (Open Access) High myopia [refractive error ≤ -6 diopters (D)] is a heterogeneous condition, and without clear accompanying features, it can be difficult to pinpoint a genetic cause. This observational study aimed to evaluate the utility of whole exome sequencing (WES) using an eye disorder gene panel in European patients with high myopia. Patients with high myopia were recruited by ophthalmologists and clinical geneticists. Clinical features were categorized into isolated high myopia, high myopia with other ocular involvement or with systemic involvement. WES was performed and an eye disorder gene panel of ~500 genes was evaluated. Hundred and thirteen patients with high myopia [mean (SD) refractive error - 11.8D (5.2)] were included. Of these, 53% were children younger than 12 years of age (53%), 13.3% were aged 12-18 years and 34% were adults (aged > 18 years). Twenty-three out of 113 patients (20%) received a genetic diagnosis of which 11 patients displayed additional ocular or systemic involvement. Pathogenic variants were identified in retinal dystrophy genes (e.g. GUCY2D and CACNA1F), connective tissue disease genes (e.g. COL18A1 and COL2A1), non-syndromic high myopia genes (ARR3), ocular development genes (e.g. PAX6) and other genes (ASPH and CNNM4). In 20% of our high myopic study population, WES using an eye gene panel enabled us to diagnose the genetic cause for this disorder. Eye genes known to cause retinal dystrophy, developmental or syndromic disorders can cause high myopia without apparent clinical features of other pathology.

Published

2022

15. Placental studies elucidate discrepancies between NIPT showing a structural chromosome aberration and a differently abnormal fetal karyotype

Author

Diane Van Opstal, Dimitri N.M. Papatsonis, Joke Polak, Lies H. Hoefsloot, Malgorzata I. Srebniak, Karin E. M. Diderich, Krista A. K. E. Prinsen, Marjan Boter, Stefanie van Veen, Nicole van Koetsveld, Marieke Joosten, Lutgarde C.P. Govaerts, Attie T.J.I. Go, Clinical Genetics, and Obstetrics & Gynecology

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Noninvasive Prenatal Testing, Placenta, Karyotype, 030105 genetics & heredity, Biology, Chromosome aberration, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Gene duplication, medicine, Humans, Genetics (clinical), Chromosome Aberrations, 030219 obstetrics & reproductive medicine, Cytotrophoblast, Obstetrics and Gynecology, Chromosome, Original Articles, medicine.anatomical_structure, Uniparental Isodisomy, Chorionic villi, Original Article, Female, SNP array

Abstract

Objective Placental cytogenetic studies may reveal the origin of discordant noninvasive prenatal testing (NIPT). We performed placental studies to elucidate discordances between NIPT showing a structural chromosome aberration and the fetus having a different chromosome aberration in three cases. Method Diagnostic testing with genomic SNP microarray was performed in three cases with NIPT showing a duplication on 4q (case 1), a terminal deletion of 13q (case 2), and a terminal deletion of 15q (case 3). Placental studies involved SNP array analysis of cytotrophoblast and mesenchymal core of chorionic villi of four placental quadrants. Clinical follow‐up was performed as well. Results Amniotic fluid revealed a different structural chromosome aberration than predicted by NIPT: a terminal 2q deletion (case 1), a segmental uniparental isodisomy of 13q (case 2), and a terminal duplication of 15q and of 13q (case 3). Placental studies revealed the aberration detected with NIPT in the cytotrophoblast, whereas the fetal karyotype was confirmed in the placental mesenchymal core. Conclusion Our study shows that targeted cytogenetic investigations for confirmation of NIPT showing a microscopically visible structural chromosome aberration should be avoided, since another aberration, even a submicroscopic one or one involving another chromosome, may be present in the fetus.

Published

2019

16. Holoprosencephaly, orofacial cleft, and frontonaso‐orbital encephaloceles: Genetic evaluation of a possible new syndrome

Author

Fernanda Sarquis Jehee, Madelief Overes, Siulan Vendramini-Pittoli, Cristiano Tonello, Rejane A.C. Monteiro, Roseli Maria Zechi-Ceide, Juliana F. Mazzeu, Roza Ali-Amin, Nancy Mizue Kokitsu-Nakata, Antonio Richieri-Costa, Rosana Maria Candido-Souza, Lies H. Hoefsloot, Marjon van Slegtenhorst, Mariana Lacerda de Freitas, and Clinical Genetics

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, ANORMALIDADES CRANIOFACIAIS, Oral cleft, business.industry, 030105 genetics & heredity, Semilobar holoprosencephaly, medicine.disease, Encephalocele, 03 medical and health sciences, 030104 developmental biology, Holoprosencephaly, Bilateral cleft lip, Genetics, medicine, Craniofacial, Agenesis of the corpus callosum, business, Genetics (clinical), Exome sequencing

Abstract

Here we report on a Brazilian child who presented semilobar holoprosencephaly, frontonasal encephaloceles and bilateral cleft lip and palate. Malformations also included agenesis of the corpus callosum, abnormal cortical gyres, dilation of the aqueduct, bilateral endolymphatic sac, bilateral cystic cocci-vestibular malformation, and a cribriform defect. The 3D TC craniofacial images showed abnormal frontonasal transition region, with a bone bifurcation, and partial agenesis of nasal bone. The trunk and upper and lower limbs were normal. To our knowledge, this rare association of holoprocensephaly with frontonaso-orbital encephaloceles without limb anomalies has never been reported before. Karyotype was normal. SNP-array showed no copy-number alterations but revealed 25% of regions of homozygosity (ROH) with normal copy number, indicating a high coefficient of inbreeding, which significantly increases the risk for an autosomal recessive disorder. Whole exome sequencing analysis did not reveal any pathogenic or likely pathogenic variants. We discuss the possible influence of two variants of uncertain significance found within the patient's ROHs. First, a missense p.(Gly394Ser) in PCSK9, a gene involved in the regulation of plasma low-density lipoprotein cholesterol. Second, an inframe duplication p.(Ala75_Ala81dup) in SP8, a zinc-finger transcription factor that regulates signaling centers during craniofacial development. Further studies and/or the identification of other patients with a similar phenotype will help elucidate the genetic etiology of this complex case.

Published

2019

17. Segmental and total uniparental isodisomy (UPiD) as a disease mechanism in autosomal recessive lysosomal disorders

Author

Clara Sá Miranda, Lies H. Hoefsloot, Karin Naess, Galhana M. Somers-Bolman, Ineke Labrijn-Marks, Irene Mavridou, Trijnie Dijkhuizen, Jasper J. Saris, Marianne Hoogeveen-Westerveld, Ans T. van der Ploeg, Frans W. Verheijen, Olga Amaral, Sirpa Ala-Mello, Hannerieke J. M. P. van den Hout, Dicky J. Halley, Helen Michelakakis, Stijn L.M. in 't Groen, W.W.M. Pim Pijnappel, Marloes Benjamins, M. A. Kroos, Department of Medical and Clinical Genetics, Medicum, Helsinki University Hospital Area, Clinical Genetics, and Pediatrics

Subjects

Male, Genetic testing, Mucopolysaccharidosis I, Genotype, Medicine, DISOMY, HOMOZYGOSITY, Child, 10. No inequality, Genetics (clinical), Genetics, 0303 health sciences, Disease genetics, Glycogen Storage Disease Type II, Medical genetics, 030305 genetics & heredity, 1184 Genetics, developmental biology, physiology, Uniparental disomy, 3. Good health, SNP genotyping, Chromosome 17 (human), Child, Preschool, Female, Adolescent, Genetic Diagnosis, Genética Humana, MOSAICISM, Polymorphism, Single Nucleotide, PATIENT, Article, 03 medical and health sciences, Mucopolysaccharidosis type I, Humans, SNP, CYSTIC-FIBROSIS, business.industry, DELETION, Laboratory techniques and procedures, Infant, Human Genetics, Uniparental Disomy, medicine.disease, GENE, Human genetics, Doenças Genéticas, Uniparental Isodisomy, Lysiosomal Diseases, 1182 Biochemistry, cell and molecular biology, 3111 Biomedicine, business

Abstract

Collaboration from previous work institution. Free PMC article: https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/30737479/ Analyses in our diagnostic DNA laboratory include genes involved in autosomal recessive (AR) lysosomal storage disorders such as glycogenosis type II (Pompe disease) and mucopolysaccharidosis type I (MPSI, Hurler disease). We encountered 4 cases with apparent homozygosity for a disease-causing sequence variant that could be traced to one parent only. In addition, in a young child with cardiomyopathy, in the absence of other symptoms, a diagnosis of Pompe disease was considered. Remarkably, he presented with different enzymatic and genotypic features between leukocytes and skin fibroblasts. All cases were examined with microsatellite markers and SNP genotyping arrays. We identified one case of total uniparental disomy (UPD) of chromosome 17 leading to Pompe disease and three cases of segmental uniparental isodisomy (UPiD) causing Hurler-(4p) or Pompe disease (17q). One Pompe patient with unusual combinations of features was shown to have a mosaic segmental UPiD of chromosome 17q. The chromosome 17 UPD cases amount to 11% of our diagnostic cohort of homozygous Pompe patients (plus one case of pseudoheterozygosity) where segregation analysis was possible. We conclude that inclusion of parental DNA is mandatory for reliable DNA diagnostics. Mild or unusual phenotypes of AR diseases should alert physicians to the possibility of mosaic segmental UPiD. SNP genotyping arrays are used in diagnostic workup of patients with developmental delay. Our results show that even small Regions of Homozygosity that include telomeric areas are worth reporting, regardless of the imprinting status of the chromosome, as they might indicate segmental UPiD. info:eu-repo/semantics/publishedVersion

Published

2019

18. Unexpected finding of uniparental disomy mosaicism in term placentas: Is it a common feature in trisomic placentas?

Author

Diane Van Opstal, Jasper J. Saris, Malgorzata I. Srebniak, Maarten F. C. M. Knapen, Robert-Jan H. Galjaard, Femke A. T. de Vries, Dimitri N.M. Papatsonis, Stefanie van Veen, Joke Polak, Lies H. Hoefsloot, Karin E. M. Diderich, Attie T.J.I. Go, Robert van de Helm, Marjan Boter, Marieke Joosten, Lutgarde C.P. Govaerts, Anneke Dijkman, Wai Yee Cheung, Clinical Genetics, Emergency Medicine, and Obstetrics & Gynecology

Subjects

0301 basic medicine, Placenta Diseases, Zygote, Placenta, Trisomy, 030105 genetics & heredity, Trisomy 22, Polymorphism, Single Nucleotide, Andrology, 03 medical and health sciences, Pregnancy, Prenatal Diagnosis, medicine, Humans, Genetic Testing, Confined placental mosaicism, Genetics (clinical), medicine.diagnostic_test, business.industry, Mosaicism, Obstetrics and Gynecology, Karyotype, Original Articles, Uniparental Disomy, medicine.disease, Amniotic Fluid, Uniparental disomy, medicine.anatomical_structure, Karyotyping, embryonic structures, Amniocentesis, Chorionic villi, Original Article, Female, business

Abstract

Objective Non‐invasive prenatal testing (NIPT) detects placental chromosome aberrations. When amniocentesis reveals a normal karyotype, confined placental mosaicism (CPM) may be assumed. In order to confirm this, placental cytogenetic studies were performed. Method NIPT was conducted in the course of the Dutch TRIDENT study. Placentas of 10 cases with NIPT results indicating an autosomal trisomy and showing a normal (N = 9) or low mosaic karyotype (N = 1) in amniotic fluid (AF) were investigated. The cytotrophoblast as well as the mesenchymal core of two to four placental chorionic villi biopsies were studied with single nucleotide polymorphism (SNP) array. Clinical outcome data were collected. Results In 10/10 cases, CPM was proven. In 3/10 cases trisomy/uniparental disomy (UPD)/biparental disomy (BPD) mosaicism was discovered. In 2/3 cases, all three cell lines were present in the placenta, whereas BPD was found in AF. In 1/3 cases trisomy 22/UPD22 was present in AF while trisomy 22/BPD22 mosaicism was found in the placenta. Five of 10 pregnancies were affected with pre‐eclampsia, low birth weight, preterm delivery, and/or congenital malformations. Conclusion The presence of trisomy/UPD/BPD mosaicism in 3/10 cases that we investigated proves that trisomic zygote rescue may involve multiple rescue events during early embryogenesis. UPD mosaicism, when present in crucial fetal tissues, may explain the abnormal phenotype in undiagnosed cases., What's already known about this topic? Trisomic zygote rescue is the main mechanism for uniparental disomy (UPD) formation.Confined placental mosaicism (CPM) is the major source of discordant NIPT results.CPM is associated with a risk for adverse pregnancy outcome. What does this study add? Trisomic zygote rescue may involve multiple rescue events based on the co‐occurrence of a trisomy‐, UPD‐, and BPD‐cell line in half of the rescued cases as revealed by placental studies.

Published

2018

19. Social and medical need for whole genome high resolution NIPT

Author

Marike Polak, Marieke Joosten, Maarten F. C. M. Knapen, Robert-Jan H. Galjaard, Laura J. C. M. van Zutven, Attie T.J.I. Go, Karin E. M. Diderich, Krista A. K. E. Prinsen, Diane Van Opstal, Lutgarde C.P. Govaerts, Lies H. Hoefsloot, Malgorzata I. Srebniak, Sam Riedijk, Clinical Genetics, Obstetrics & Gynecology, Research Methods and Techniques, and Erasmus MC other

Subjects

0301 basic medicine, medicine.medical_specialty, Microarray, lcsh:QH426-470, Noninvasive Prenatal Testing, Aneuploidy, High resolution, Prenatal diagnosis, 030105 genetics & heredity, Sensitivity and Specificity, 03 medical and health sciences, patients preferences, Pregnancy, Genetics, medicine, Humans, Molecular Biology, Genetics (clinical), High resolution analysis, Chromosome Aberrations, Genome, prenatal diagnosis, business.industry, Obstetrics, Original Articles, medicine.disease, First trimester, lcsh:Genetics, 030104 developmental biology, Prenatal screening, Attitude, diagnostic yield, Female, Original Article, Pregnant Women, business, microarray, Needs Assessment, NIPT

Abstract

Background Two technological innovations in the last decade significantly influenced the diagnostic yield of prenatal cytogenetic testing: genomic microarray allowing high resolution analysis and noninvasive prenatal testing (NIPT) focusing on aneuploidy. To anticipate future trends in prenatal screening and diagnosis, we evaluated the number of invasive tests in our center and the number of aberrant cases diagnosed in the last decade. Methods We retrospectively analyzed fetal chromosomal aberrations diagnosed in 2009–2018 in 8,608 pregnancies without ultrasound anomalies. Results The introduction of NIPT as the first‐tier test led to a substantial decrease in the number of invasive tests and a substantially increased diagnostic yield of aneuploidies in the first trimester. However, we have also noted a decreased detection of submicroscopic aberrations, since the number of invasive tests substantially decreased. We have observed that pregnant women were interested in broader scope of prenatal screening and diagnosis than detection of common trisomies. Conclusion Since the frequency of syndromic disorders caused by microdeletions/microduplications is substantial and current routine NIPT and ultrasound investigations are not able to detect them, we suggest that a noninvasive test with resolution comparable to microarrays should be developed, which will also meet patient's needs., The frequency of syndromic disorders caused by microdeletions/microduplications is substantial and because current prenatal screening protocols with noninvasive prenatal testing (NIPT) focusing on aneuploidies and ultrasound investigations are not able to detect them, we suggest to develop the genotype‐first approach through higher resolution NIPT, which will also meet patient's needs.

Published

2019

20. Genotype–Phenotype Relationship in Inherited Disorders of Hearing Impairment

Author

Lies H. Hoefsloot and Anne-Françoise Roux

Subjects

Genetics, Massive parallel sequencing, Usher syndrome, medicine, Audiogram, Biology, medicine.disease, Exome sequencing, Heimler syndrome, Genotype phenotype

Published

2017

21. The diagnostic yield of whole-exome sequencing targeting a gene panel for hearing impairment in The Netherlands

Author

Ilse Feenstra, Marieke F. van Dooren, Marie José H. Van Den Boogaard, Rolph Pfundt, Stefan H. Lelieveld, Celia Zazo Seco, Henricus P. M. Kunst, Ilse J. de Wijs, Christian Gilissen, Saskia M. Maas, Arjan C. Houweling, Saskia Tamminga, Astrid S Plomp, Steven Castelein, Helger G. Yntema, Margit Schraders, Els K. Vanhoutte, Ronald J.C. Admiraal, Sarina G. Kant, Suzanna G.M. Frints, Hans Scheffer, Christa M. De Geus, Pia A. M. de Koning Gans, Jiddeke M. van de Kamp, Jayne Y. Hehir-Kwa, Ronald J.E. Pennings, Mieke Wesdorp, Hannie Kremer, Marcel R. Nelen, Lies H. Hoefsloot, Human genetics, AGEM - Endocrinology, metabolism and nutrition, AGEM - Inborn errors of metabolism, Amsterdam Neuroscience - Complex Trait Genetics, APH - Quality of Care, ACS - Atherosclerosis & ischemic syndromes, Clinical Genetics, MUMC+: DA KG Bedrijfsbureau (9), RS: GROW - R4 - Reproductive and Perinatal Medicine, Klinische Genetica, MUMC+: DA KG Polikliniek (9), Human Genetics, and Paediatric Genetics

Subjects

0301 basic medicine, MYO15A, 030105 genetics & heredity, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], Connexins, Exome, Copy-number variation, MUTATION, Genetics (clinical), Exome sequencing, Netherlands, Genetics, COPY NUMBER VARIANTS, Extracellular Matrix Proteins, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], EAR, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Connexin 26, Intercellular Signaling Peptides and Proteins, Neurodevelopmental disorders Radboud Institute for Molecular Life Sciences [Radboudumc 7], DEAFNESS, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], STRC, medicine.medical_specialty, DNA Copy Number Variations, OTOGELIN, Genetic counseling, Biology, Myosins, GPI-Linked Proteins, FREQUENCY, Article, 03 medical and health sciences, Molecular genetics, Journal Article, medicine, Humans, Genetic Testing, Sensory disorders Radboud Institute for Molecular Life Sciences [Radboudumc 12], Hearing Loss, SPECTRUM, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Myosin Heavy Chains, IDENTIFICATION, Genetic heterogeneity, Other Research Radboud Institute for Health Sciences [Radboudumc 0], Membrane Proteins, Sequence Analysis, DNA, 030104 developmental biology

Abstract

Contains fulltext : 169850.pdf (Publisher’s version ) (Closed access) Hearing impairment (HI) is genetically heterogeneous which hampers genetic counseling and molecular diagnosis. Testing of several single HI-related genes is laborious and expensive. In this study, we evaluate the diagnostic utility of whole-exome sequencing (WES) targeting a panel of HI-related genes. Two hundred index patients, mostly of Dutch origin, with presumed hereditary HI underwent WES followed by targeted analysis of an HI gene panel of 120 genes. We found causative variants underlying the HI in 67 of 200 patients (33.5%). Eight of these patients have a large homozygous deletion involving STRC, OTOA or USH2A, which could only be identified by copy number variation detection. Variants of uncertain significance were found in 10 patients (5.0%). In the remaining 123 cases, no potentially causative variants were detected (61.5%). In our patient cohort, causative variants in GJB2, USH2A, MYO15A and STRC, and in MYO6 were the leading causes for autosomal recessive and dominant HI, respectively. Segregation analysis and functional analyses of variants of uncertain significance will probably further increase the diagnostic yield of WES.

Published

2017

22. Novel

Author

Stijn L M, In 't Groen, Douglas O S, de Faria, Alessandro, Iuliano, Johanna M P, van den Hout, Hannie, Douben, Trijnie, Dijkhuizen, David, Cassiman, Peter, Witters, Miguel-Ángel, Barba Romero, Annelies, de Klein, Galhana M, Somers-Bolman, Jasper J, Saris, Lies H, Hoefsloot, Ans T, van der Ploeg, Atze J, Bergsma, and W W M Pim, Pijnappel

Subjects

mosaicism, glycogen storage disease type II, diagnostics, Pompe disease, segmental uniparental isodisomy, Article

Abstract

Pompe disease is a metabolic disorder caused by a deficiency of the glycogen-hydrolyzing lysosomal enzyme acid α-glucosidase (GAA), which leads to progressive muscle wasting. This autosomal-recessive disorder is the result of disease-associated variants located in the GAA gene. In the present study, we performed extended molecular diagnostic analysis to identify novel disease-associated variants in six suspected Pompe patients from four different families for which conventional diagnostic assays were insufficient. Additional assays, such as a generic-splicing assay, minigene analysis, SNP array analysis, and targeted Sanger sequencing, allowed the identification of an exonic deletion, a promoter deletion, and a novel splicing variant located in the 5′ UTR. Furthermore, we describe the diagnostic process for an infantile patient with an atypical phenotype, consisting of left ventricular hypertrophy but no signs of muscle weakness or motor problems. This led to the identification of a genetic mosaicism for a very severe GAA variant caused by a segmental uniparental isodisomy (UPD). With this study, we aim to emphasize the need for additional analyses to detect new disease-associated GAA variants and non-Mendelian genotypes in Pompe disease where conventional DNA diagnostic assays are insufficient.

Published

2019

23. Residual N-acetyl-α-glucosaminidase activity in fibroblasts correlates with disease severity in patients with mucopolysaccharidosis type IIIB

Author

Tom Wagemans, Lies H. Hoefsloot, Lindsey Welling, Frits A. Wijburg, A. T. van der Ploeg, Olga L. Meijer, N. van Vlies, George J G Ruijter, Hennie T. Brüggenwirth, Marlies J. Valstar, Other departments, Laboratory Genetic Metabolic Diseases, Paediatric Metabolic Diseases, Clinical Genetics, and Pediatrics

Subjects

0301 basic medicine, Adult, Male, Adolescent, Disease, macromolecular substances, medicine.disease_cause, Severity of Illness Index, 03 medical and health sciences, chemistry.chemical_compound, Mucopolysaccharidosis III, Young Adult, 0302 clinical medicine, Severity of illness, Acetylglucosaminidase, medicine, Genetics, Humans, Genetics(clinical), Glucosaminidase, Genetics (clinical), Cells, Cultured, Genetic Association Studies, Aged, Mutation, business.industry, Genetic disorder, Heparan sulfate, Fibroblasts, Middle Aged, medicine.disease, 030104 developmental biology, chemistry, Immunology, Allelic heterogeneity, Female, Original Article, Heparitin Sulfate, business, 030217 neurology & neurosurgery, Biomarkers

Abstract

Background Mucopolysaccharidosis type IIIB (MPS IIIB) is a rare genetic disorder in which the deficiency of the lysosomal enzyme N-acetyl-α-glucosaminidase (NAGLU) results in the accumulation of heparan sulfate (HS), leading to progressive neurocognitive deterioration. In MPS IIIB a wide spectrum of disease severity is seen. Due to a large allelic heterogeneity, establishing genotype-phenotype correlations is difficult. However, reliable prediction of the natural course of the disease is needed, in particular for the assessment of the efficacy of potential therapies. Methods To identify markers that correlate with disease severity, all Dutch patients diagnosed with MPS IIIB were characterised as either rapid (RP; classical, severe phenotype) or slow progressors (SP; non-classical, less severe phenotype), based on clinical data. NAGLU activity and HS levels were measured in patients’ fibroblasts after culturing at different temperatures. Results A small, though significant difference in NAGLU activity was measured between RP and SP patients after culturing at 37 °C (p

Published

2016

24. Heterozygous missense variants of LMX1A lead to nonsyndromic hearing impairment and vestibular dysfunction

Author

Michelle M. van Rossum, Andy J. Beynon, Vitória Piai, Ilse Feenstra, Liselotte J. C. Rotteveel, Stefan H. Lelieveld, Berit M. Verbist, Ronald J.E. Pennings, Mieke Wesdorp, Marieke F. van Dooren, Hannie Kremer, Martijn A. Huynen, Laurens Wiel, Pia A. M. de Koning Gans, Hanka Venselaar, Ronald J.C. Admiraal, Henricus P. M. Kunst, Margit Schraders, Judith van Gaalen, Peter Lichtner, Helger G. Yntema, Nicol C. Voermans, Jaap Oostrik, Bas P. Hartel, Lies H. Hoefsloot, and Clinical Genetics

Subjects

Adult, Male, 0301 basic medicine, Heterozygote, Candidate gene, LIM-Homeodomain Proteins, Mutation, Missense, 030105 genetics & heredity, Biology, Bioinformatics, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], 03 medical and health sciences, Cancer development and immune defence Radboud Institute for Health Sciences [Radboudumc 2], All institutes and research themes of the Radboud University Medical Center, Intellectual disability, Genetics, medicine, Humans, Missense mutation, Hearing Loss, Genetics (clinical), Exome sequencing, Original Investigation, Aged, Aged, 80 and over, Vestibular system, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Neuro- en revalidatiepsychologie, Neuropsychology and rehabilitation psychology, Heterozygote advantage, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], Plasticity and Memory [DI-BCB_DCC_Theme 3], Middle Aged, medicine.disease, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Phenotype, 3. Good health, 030104 developmental biology, Amino Acid Substitution, Vestibular Diseases, Child, Preschool, Female, Age of onset, Nanomedicine Radboud Institute for Molecular Life Sciences [Radboudumc 19], Transcription Factors, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

Unraveling the causes and pathomechanisms of progressive disorders is essential for the development of therapeutic strategies. Here, we identified heterozygous pathogenic missense variants of LMX1A in two families of Dutch origin with progressive nonsyndromic hearing impairment (HI), using whole exome sequencing. One variant, c.721G > C (p.Val241Leu), occurred de novo and is predicted to affect the homeodomain of LMX1A, which is essential for DNA binding. The second variant, c.290G > C (p.Cys97Ser), predicted to affect a zinc-binding residue of the second LIM domain that is involved in protein–protein interactions. Bi-allelic deleterious variants of Lmx1a are associated with a complex phenotype in mice, including deafness and vestibular defects, due to arrest of inner ear development. Although Lmx1a mouse mutants demonstrate neurological, skeletal, pigmentation and reproductive system abnormalities, no syndromic features were present in the participating subjects of either family. LMX1A has previously been suggested as a candidate gene for intellectual disability, but our data do not support this, as affected subjects displayed normal cognition. Large variability was observed in the age of onset (a)symmetry, severity and progression rate of HI. About half of the affected individuals displayed vestibular dysfunction and experienced symptoms thereof. The late-onset progressive phenotype and the absence of cochleovestibular malformations on computed tomography scans indicate that heterozygous defects of LMX1A do not result in severe developmental abnormalities in humans. We propose that a single LMX1A wild-type copy is sufficient for normal development but insufficient for maintenance of cochleovestibular function. Alternatively, minor cochleovestibular developmental abnormalities could eventually lead to the progressive phenotype seen in the families. Electronic supplementary material The online version of this article (10.1007/s00439-018-1880-5) contains supplementary material, which is available to authorized users.

Published

2018

25. Mucolipidosis type III, a series of adult patients

Author

Mario Maas, Esmee Oussoren, George J. G. Ruijter, Ans T. van der Ploeg, David van Eerd, Janneke G. Langendonk, Mirjam Langeveld, Robin H. Lachmann, Lies H. Hoefsloot, Carla E. M. Hollak, Jan C. van der Meijden, Elaine Murphy, Robert M. Verdijk, Pediatrics, Internal Medicine, Erasmus MC other, Clinical Genetics, Pathology, Radiology and Nuclear Medicine, AGEM - Endocrinology, metabolism and nutrition, AMS - Sports & Work, Endocrinology, AGEM - Inborn errors of metabolism, and ACS - Diabetes & metabolism

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Mucopolysaccharidosis, Disease, Osteoarthritis, Young Adult, 03 medical and health sciences, Mucolipidoses, Internal medicine, Activities of Daily Living, Genetics, medicine, Humans, Cognitive Dysfunction, Young adult, Carpal tunnel syndrome, Genetics (clinical), Aged, Retrospective Studies, business.industry, Cartilage, Retrospective cohort study, Middle Aged, medicine.disease, Carpal Tunnel Syndrome, 3. Good health, Natural history, 030104 developmental biology, medicine.anatomical_structure, Female, Original Article, business

Abstract

Background Mucolipidosis type III α/β or γ (MLIII) are rare autosomal recessive diseases, in which reduced activity of the enzyme UDP-N-acetyl glucosamine-1-phosphotransferase (GlcNAc-PTase) leads to intra-lysosomal accumulation of different substrates. Publications on the natural history of MLIII, especially the milder forms, are scarce. This study provides a detailed description of the disease characteristics and its natural course in adult patients with MLIII. Methods In this retrospective chart study, the clinical, biochemical and molecular findings in adult patients with a confirmed diagnosis of MLIII from three treatment centres were collected. Results Thirteen patients with MLIII were included in this study. Four patients (31%) were initially misdiagnosed with a type of mucopolysaccharidosis (MPS). Four patients (31%) had mild cognitive impairment. Six patients (46%) needed help with activities of daily living (ADL) or were wheelchair-dependent. All patients had dysostosis multiplex and progressive secondary osteoarthritis, characterised by cartilage destruction and bone lesions in multiple joints. All patients underwent multiple orthopaedic surgical interventions as early as the second or third decades of life, of which total hip replacement (THR) was the most common procedure (61% of patients). Carpal tunnel syndrome (CTS) was found in 12 patients (92%) and in eight patients (61%), CTS release was performed. Conclusions Severe skeletal abnormalities, resulting from abnormal bone development and severe progressive osteoarthritis, are the hallmark of MLIII, necessitating surgical orthopaedic interventions early in life. Future therapies for this disease should focus on improving cartilage and bone quality, preventing skeletal complications and improving mobility. Electronic supplementary material The online version of this article (10.1007/s10545-018-0186-z) contains supplementary material, which is available to authorized users.

Published

2018

26. Is it feasible to select fetuses for prenatal WES based on the prenatal phenotype?

Author

Attie T.J.I. Go, Malgorzata I. Srebniak, Marieke Joosten, Diane Van Opstal, Robert-Jan H. Galjaard, Lutgarde C.P. Govaerts, Karin E. M. Diderich, Maarten F. C. M. Knapen, and Lies H. Hoefsloot

Subjects

Fetus, Pregnancy, business.industry, MEDLINE, Obstetrics and Gynecology, Prenatal diagnosis, Bioinformatics, medicine.disease, Phenotype, Text mining, Medicine, business, Genetics (clinical), Exome sequencing

Published

2019

27. Early-Onset Stargardt Disease

Author

B. Jeroen Klevering, Lies H. Hoefsloot, Camiel J. F. Boon, Frans P.M. Cremers, Nathalie M. Bax, Stanley Lambertus, Ramon A. C. van Huet, and Carel B. Hoyng

Subjects

medicine.medical_specialty, Visual acuity, genetic structures, medicine.diagnostic_test, business.industry, Fundus photography, Foveal atrophy, medicine.disease, Fluorescein angiography, eye diseases, Stargardt disease, Ophthalmoscopy, Ophthalmology, medicine.anatomical_structure, Atrophy, medicine, sense organs, Choroid, medicine.symptom, business

Abstract

Objective To describe the phenotype and genotype of patients with early-onset Stargardt disease. Design Retrospective cohort study. Participants Fifty-one Stargardt patients with age at onset ≤10 years. Methods We reviewed patient medical records for age at onset, medical history, initial symptoms, best-corrected visual acuity (BCVA), ophthalmoscopy, fundus photography, fundus autofluorescence (FAF), fluorescein angiography (FA), spectral-domain optical coherence tomography (SD-OCT), and full-field electroretinography (ffERG). The ABCA4 gene was screened for mutations. Main Outcome Measures Age at onset, BCVA, fundus appearance, FAF, FA, SD-OCT, ffERG, and presence of ABCA4 mutations. Results The mean age at onset was 7.2 years (range, 1–10). The median times to develop BCVA of 20/32, 20/80, 20/200, and 20/500 were 3, 5, 12, and 23 years, respectively. Initial ophthalmoscopy in 41 patients revealed either no abnormalities or foveal retinal pigment epithelium (RPE) changes in 10 and 9 patients, respectively; the other 22 patients had foveal atrophy, atrophic RPE lesions, and/or irregular yellow-white fundus flecks. On FA, there was a "dark choroid" in 21 out of 29 patients. In 14 out of 50 patients, foveal atrophy occurred before flecks developed. On FAF, there was centrifugal expansion of disseminated atrophic spots, which progressed to the eventual profound chorioretinal atrophy. Spectral-domain OCT revealed early photoreceptor damage followed by atrophy of the outer retina, RPE, and choroid. On ffERG in 26 patients, 15 had normal amplitudes, and 11 had reduced photopic and/or scotopic amplitudes at their first visit. We found no correlation between ffERG abnormalities and the rate of vision loss. Thirteen out of 25 patients had progressive ffERG abnormalities. Finally, genetic screening of 44 patients revealed ≥2 ABCA4 mutations in 37 patients and single heterozygous mutations in 7. Conclusions In early-onset Stargardt, initial ophthalmoscopy can reveal no abnormalities or minor retinal abnormalities. Yellow-white flecks can be preceded by foveal atrophy and may be visible only on FAF. Although ffERG is insufficient for predicting the rate of vision loss, abnormalities can develop. Over time, visual acuity declines rapidly in parallel with progressive retinal degeneration, resulting in profound chorioretinal atrophy. Thus, early-onset Stargardt lies at the severe end of the spectrum of ABCA4 -associated retinal phenotypes.

Published

2015

28. Progressive hearing loss and vestibular dysfunction caused by a homozygous nonsense mutation in CLIC5

Author

Ronald J.C. Admiraal, Jaap Oostrik, Ronald J.E. Pennings, Kornelia Neveling, María Domínguez-Ruiz, Ignacio del Castillo, Hannie Kremer, Henricus P. M. Kunst, Margit Schraders, Jos M. T. Draaisma, Celia Zazo Seco, Anne M.M. Oonk, Lies H. Hoefsloot, and Marta Gandía

Subjects

Male, Candidate gene, Adolescent, Hearing loss, media_common.quotation_subject, Mutant, Nonsense, Nonsense mutation, Sensory disorders Radboud Institute for Health Sciences [Radboudumc 12], Biology, Deafness, Article, Healthcare improvement science Radboud Institute for Health Sciences [Radboudumc 18], Cell Line, Chloride Channels, Genetics, medicine, otorhinolaryngologic diseases, Humans, RNA, Messenger, Sensory disorders Radboud Institute for Molecular Life Sciences [Radboudumc 12], Child, Progressive hearing impairment, Genetics (clinical), media_common, Vestibular areflexia, Other Research Radboud Institute for Health Sciences [Radboudumc 0], Homozygote, Microfilament Proteins, Infant, Nonsense Mediated mRNA Decay, Pedigree, Vestibular Diseases, Codon, Nonsense, Mutation testing, Female, medicine.symptom

Abstract

Contains fulltext : 153746.pdf (Publisher’s version ) (Closed access) In a consanguineous Turkish family diagnosed with autosomal recessive nonsyndromic hearing impairment (arNSHI), a homozygous region of 47.4 Mb was shared by the two affected siblings on chromosome 6p21.1-q15. This region contains 247 genes including the known deafness gene MYO6. No pathogenic variants were found in MYO6, neither with sequence analysis of the coding region and splice sites nor with mRNA analysis. Subsequent candidate gene evaluation revealed CLIC5 as an excellent candidate gene. The orthologous mouse gene is mutated in the jitterbug mutant that exhibits progressive hearing impairment and vestibular dysfunction. Mutation analysis of CLIC5 revealed a homozygous nonsense mutation c.96T>A (p.(Cys32Ter)) that segregated with the hearing loss. Further analysis of CLIC5 in 213 arNSHI patients from mostly Dutch and Spanish origin did not reveal any additional pathogenic variants. CLIC5 mutations are thus not a common cause of arNSHI in these populations. The hearing loss in the present family had an onset in early childhood and progressed from mild to severe or even profound before the second decade. Impaired hearing is accompanied by vestibular areflexia and in one of the patients with mild renal dysfunction. Although we demonstrate that CLIC5 is expressed in many other human tissues, no additional symptoms were observed in these patients. In conclusion, our results show that CLIC5 is a novel arNSHI gene involved in progressive hearing impairment, vestibular and possibly mild renal dysfunction in a family of Turkish origin.

Published

2015

29. Heterozygous Deep-Intronic Variants and Deletions in ABCA4 in Persons with Retinal Dystrophies and One Exonic ABCA4 Variant

Author

Carel B. Hoyng, Caroline C W Klaver, Susanne Roosing, Lies H. Hoefsloot, Anneke I. den Hollander, L. Ingeborgh van den Born, Nathalie M. Bax, Frans P.M. Cremers, B. Jeroen Klevering, Marijke N. Zonneveld-Vrieling, Merve Mutlu, Ilse J. de Wijs, Riccardo Sangermano, Carla S. Westeneng-van Haaften, Edwin M. Stone, Terry A. Braun, Alberta A H J Thiadens, Milan Phan, and Ophthalmology

Subjects

Male, Proband, Sequence analysis, ABCA4, Sensory disorders Radboud Institute for Health Sciences [Radboudumc 12], Biology, Genetic Heterogeneity, Macular Degeneration, Exon, Genetics, medicine, Humans, Stargardt Disease, Genetic Predisposition to Disease, splice, Sensory disorders Radboud Institute for Molecular Life Sciences [Radboudumc 12], Genetic Association Studies, Genetics (clinical), Sequence Deletion, Genetic heterogeneity, Intron, High-Throughput Nucleotide Sequencing, Exons, Sequence Analysis, DNA, medicine.disease, Molecular biology, Introns, Pedigree, Stargardt disease, biology.protein, ATP-Binding Cassette Transporters, Female, Retinitis Pigmentosa

Abstract

Item does not contain fulltext Variants in ABCA4 are responsible for autosomal-recessive Stargardt disease and cone-rod dystrophy. Sequence analysis of ABCA4 exons previously revealed one causative variant in each of 45 probands. To identify the "missing" variants in these cases, we performed multiplex ligation-dependent probe amplification-based deletion scanning of ABCA4. In addition, we sequenced the promoter region, fragments containing five deep-intronic splice variants, and 15 deep-intronic regions containing weak splice sites. Heterozygous deletions spanning ABCA4 exon 5 or exons 20-22 were found in two probands, heterozygous deep-intronic variants were identified in six probands, and a deep-intronic variant was found together with an exon 20-22 deletion in one proband. Based on ophthalmologic findings and characteristics of the identified exonic variants present in trans, the deep-intronic variants V1 and V4 were predicted to be relatively mild and severe, respectively. These findings are important for proper genetic counseling and for the development of variant-specific therapies.

Published

2015

30. Exome Sequencing Extends the Phenotypic Spectrum for ABHD12 Mutations

Author

Wendy A. G. van Zelst-Stams, Carlo Rivolta, Maria Isabel Lopez-Molina, Marta Corton, Raquel Perez-Carro, Carlos Vazquez, Esther Martín-Garrido, B. Jeroen Klevering, Javier del Val, Ramon A. C. van Huet, Silvio Alessandro Di Gioia, Bart P.C. van de Warrenburg, Carel B. Hoyng, Blanca Garcia-Sandoval, Rob W.J. Collin, Koji M. Nishiguchi, Pedro J. García-Ruiz, Fiona Blanco-Kelly, Carmen Ayuso, Frans P.M. Cremers, Lies H. Hoefsloot, and Almudena Avila-Fernandez

Subjects

Retinal degeneration, Genetics, 0303 health sciences, Ataxia, genetic structures, Cerebellar ataxia, Hearing loss, business.industry, Compound heterozygosity, medicine.disease, eye diseases, 3. Good health, 03 medical and health sciences, Ophthalmology, 0302 clinical medicine, Retinitis pigmentosa, medicine, Sensorineural hearing loss, medicine.symptom, business, 030217 neurology & neurosurgery, Exome sequencing, 030304 developmental biology

Abstract

Objective To identify the genetic causes underlying autosomal recessive retinitis pigmentosa (arRP) and to describe the associated phenotype. Design Case series. Participants Three hundred forty-seven unrelated families affected by arRP and 33 unrelated families affected by retinitis pigmentosa (RP) plus noncongenital and progressive hearing loss, ataxia, or both, respectively. Methods A whole exome sequencing (WES) analysis was performed in 2 families segregating arRP. A mutational screening was performed in 378 additional unrelated families for the exon–intron boundaries of the ABHD12 gene. To establish a genotype–phenotype correlation, individuals who were homozygous or compound heterozygotes of mutations in ABHD12 underwent exhaustive clinical examinations by ophthalmologists, neurologists, and otologists. Main Outcome Measures DNA sequence variants, best-corrected visual acuity, visual field assessments, electroretinogram responses, magnetic resonance imaging, and audiography. Results After a WES analysis, we identified 4 new mutations (p.Arg107Glufs*8, p.Trp159*, p.Arg186Pro, and p.Thr202Ile) in ABHD12 in 2 families (RP-1292 and W08-1833) previously diagnosed with nonsyndromic arRP, which cosegregated with the disease among the family members. Another homozygous mutation (p.His372Gln) was detected in 1 affected individual (RP-1487) from a cohort of 378 unrelated arRP and syndromic RP patients. After exhaustive clinical examinations by neurologists and otologists, the 4 affected members of the RP-1292 had no polyneuropathy or ataxia, and the sensorineural hearing loss and cataract were attributed to age or the normal course of the RP, whereas the affected members of the families W08-1833 and RP-1487 showed clearly symptoms associated with polyneuropathy, hearing loss, cerebellar ataxia, RP, and early-onset cataract (PHARC) syndrome. Conclusions Null mutations in the ABHD12 gene lead to PHARC syndrome, a neurodegenerative disease including polyneuropathy, hearing loss, cerebellar ataxia, RP, and early-onset cataract. Our study allowed us to report 5 new mutations in ABHD12 . This is the first time missense mutations have been described for this gene. Furthermore, these findings are expanding the spectrum of phenotypes associated with ABHD12 mutations ranging from PHARC syndrome to a nonsyndromic form of retinal degeneration.

Published

2014

31. Genotype phenotype correlations for hearing impairment: Approaches to management

Author

Hannie Kremer, Ilse Feenstra, Lies H. Hoefsloot, and Henricus P. M. Kunst

Subjects

Genetics, Massive parallel sequencing, Genotype, otorhinolaryngologic diseases, Approaches of management, Biology, Phenotype, Gene, Genotype-Phenotype Correlations, Exome, Genetics (clinical), Heterogeneous disorder

Abstract

Hearing impairment is an extremely heterogeneous disorder, with both environmental as well as genetic causes. This review describes the known genes involved in non-syndromic hearing impairment and their genotype-phenotype correlations where possible. Furthermore, some of the more frequent syndromic forms of hearing impairment are described, in particular where they overlap with the non-syndromic forms. Given the heterogeneity of the disorder, together with the indistinguishable phenotypes for many of the genes, it is suggested that testing for mutations is performed using massive parallel sequencing techniques, either by a large targeted set of genes or by an exome wide analysis.

Published

2014

32. Audiometric Characteristics of a Dutch Family with a New Mutation in GATA3 Causing HDR Syndrome

Author

Ronald J.E. Pennings, Patrick L. M. Huygen, Henricus P. M. Kunst, Lies H. Hoefsloot, Ad F. M. Snik, Ronald J.C. Admiraal, E. van Beelen, and Joop M. Leijendeckers

Subjects

Vestibular system, medicine.medical_specialty, Physiology, business.industry, GATA3, Audiogram, Audiology, medicine.disease, Sensory Systems, Loudness, Speech and Hearing, medicine.anatomical_structure, Otorhinolaryngology, Hypoparathyroidism, New mutation, otorhinolaryngologic diseases, medicine, Hair cell, business, Flat audiogram

Abstract

We present the case of a Dutch family with a new mutation (c523_528dup) in GATA3 causing HDR syndrome. HDR syndrome is characterised by hypoparathyroidism, deafness and renal defects. In this study, we describe the audiometric characteristics of 5 patients from this family. Their hearing impairment was congenital, bilateral and symmetric. Audiograms showed mild-to-moderate hearing impairment with a flat audiogram configuration. Higher frequencies tended to be affected more strongly. Cross-sectional analyses showed no progression, and a mean audiogram was established. Psychophysical measurements in 3 HDR patients - including speech reception in noise, loudness scaling, gap detection and difference limen for frequency - were obtained to assess hearing function in greater detail. Overall, the results of the psychophysical measurements indicated characteristics of outer hair cell loss. CT scanning showed no anomalies in 3 of the HDR patients. Although 2 patients displayed vestibular symptoms, no anomalies in the vestibular system were found by vestibulo-ocular examination. Our results are in agreement with the theory that outer hair cell malfunctioning can play a major role in HDR syndrome.

Published

2014

33. Foveal sparing in stargardt disease

Author

Sarah C. Westeneng-van Haaften, Carel B. Hoyng, Frans P.M. Cremers, B. Jeroen Klevering, Camiel J. F. Boon, Lies H. Hoefsloot, Nathalie M. Bax, Muhamad Muhamad, Marijke N. Zonneveld-Vrieling, and Ramon A. C. van Huet

Subjects

Adult, Male, medicine.medical_specialty, Fovea Centralis, Visual acuity, genetic structures, Fundus Oculi, DNA Mutational Analysis, Visual Acuity, Sensory disorders Radboud Institute for Health Sciences [Radboudumc 12], Retinal Pigment Epithelium, ABCA4, Ophthalmoscopy, Macular Degeneration, Foveal, Ophthalmology, medicine, Electroretinography, Humans, Fluorescein Angiography, Sensory disorders Radboud Institute for Molecular Life Sciences [Radboudumc 12], Aged, medicine.diagnostic_test, business.industry, Fundus photography, Fovea centralis, DNA, Middle Aged, Fluorescein angiography, medicine.disease, Rod Cell Outer Segment, foveal sparing, eye diseases, Stargardt disease, medicine.anatomical_structure, Mutation, Optometry, ATP-Binding Cassette Transporters, Female, sense organs, medicine.symptom, business, Tomography, Optical Coherence

Abstract

Contains fulltext : 138884.pdf (Publisher’s version ) (Open Access) PURPOSE: To provide a clinical and genetic description of a patient cohort with Stargardt disease (STGD1) with identifiable foveal sparing. METHODS: Patients with retinal atrophy (defined as an absence of autofluorescence) that surrounded the fovea by at least 180 degrees and did not include the fovea were defined as having foveal sparing; eyes with visual acuity (VA) worse than 20/200 were excluded. We reviewed the medical files and extracted data regarding medical history, VA, ophthalmoscopy, static perimetry, fundus photography, spectral-domain optical coherence tomography (SD-OCT), fluorescein angiography (FA), fundus autofluorescence (FAF), and electroretinography (ERG). We screened each patient's ABCA4 gene for mutations. RESULTS: Seventeen eyes with foveal sparing were identified in 13 unrelated patients. In 4 eyes, the fovea gradually became atrophic after the initial foveal sparing. The mean age at onset was 51 years (range, 32-67 years). Visual acuity was 20/40 or better in all foveal sparing eyes and was 20/25 or better in 41%. Fundus autofluorescence imaging revealed hyperautofluorescent flecks and parafoveal retinal atrophy; SD-OCT revealed sharply delineated atrophy; and perimetry revealed parafoveal scotomas with intact foveal sensitivity. Finally, genetic screening identified mutations in 19 of the 26 ABCA4 gene alleles. CONCLUSIONS: Foveal sparing occurs mainly in patients with late-onset STGD1 and represents the milder end of the clinical spectrum in STGD1. The anatomy, metabolism, and biochemistry of the retina, as well as genetic variations in genes other than ABCA4, can influence the etiology of foveal sparing. Identifying these fovea-protecting factors will facilitate the future development of strategies designed to treat STGD1.

Published

2014

34. Osteoporotic Vertebral Fractures During Pregnancy: Be Aware of a Potential Underlying Genetic Cause

Author

Ling Oei, Marleen Simon, Natalia Campos-Obando, Lies H. Hoefsloot, Caroline C W Klaver, M. Carola Zillikens, Rosalie M. Kiewiet, Internal Medicine, Ophthalmology, and Clinical Genetics

Subjects

Adult, medicine.medical_specialty, Familial Exudative Vitreoretinopathies, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Osteoporosis, Context (language use), Biochemistry, Endocrinology, Pregnancy, Internal medicine, medicine, Back pain, Humans, Medical history, Family history, Past medical history, business.industry, Vitreoretinopathy, Proliferative, Biochemistry (medical), Osteogenesis Imperfecta, medicine.disease, Pedigree, Pregnancy Complications, Spinal Fractures, Female, medicine.symptom, business, Osteoporotic Fractures, Postpartum period

Abstract

Context: Although the baby growing in its mother's womb needs calcium for skeletal development, osteoporosis and fractures very rarely occur during pregnancy. Case Presentation: A 27-year-old woman in the seventh month of her first pregnancy contracted midthoracic back pain after lifting an object. The pain was attributed to her pregnancy, but it remained postpartum. Her past medical history was uneventful, except for severely reduced vision of her left eye since birth. Family history revealed that her maternal grandmother had postmenopausal osteoporosis and her half-brother had three fractures during childhood after minor trauma. Her height was 1.58 m; she had no blue sclerae or joint hyperlaxity. Laboratory examination including serum calcium, phosphate, alkaline phosphatase, creatinine, beta-carboxyterminal cross-linking telopeptide of type I collagen, 25-hydroxyvitamin D, and TSH was normal. Multiple thoracic vertebral fractures were diagnosed on x-ray examination, and dual-energy x-ray absorptiometry scanning showed severe osteoporosis (Z-scores: L2-L4, -5.6 SD; femur neck, -3.9 SD). DNA analyses revealed two compound heterozygous missense mutations in LRP5. The patient's mother carried one of the LRP5 mutations and was diagnosed with osteoporosis. Her half-brother, treated with cabergoline for a microprolactinoma, also had osteoporosis of the lumbar spine on dual-energy x-ray absorptiometry and carried the same LRP5 mutation. The patient was treated with risedronate for 2.5 years. Bone mineral density and back pain improved. She stopped bisphosphonate use 6 months before planning a second pregnancy. Conclusion: Our patient was diagnosed with osteoporosis pseudoglioma syndrome/familial exudative vitreoretinopathy. Potential underlying genetic causes should be considered in pregnancy-associated osteoporosis with implications for patients and relatives. More studies regarding osteoporosis treatment preceding conception are desirable.

Published

2014

35. Mutations in the Mevalonate Kinase (MVK) Gene Cause Nonsyndromic Retinitis Pigmentosa

Author

Lies H. Hoefsloot, P. Martin van Hagen, L. Ingeborgh van den Born, Carel B. Hoyng, Kornelia Neveling, Frans P.M. Cremers, Mieke Kipping-Geertsema, Anna M. Siemiatkowska, Anneke I. den Hollander, Rob W.J. Collin, Monique Stoffels, Anna Simon, Arjen Henkes, Immunology, and Ophthalmology

Subjects

Adult, Male, Proband, Oncology, medicine.medical_specialty, Pathology, Genetics and epigenetic pathways of disease [NCMLS 6], DNA Mutational Analysis, Visual Acuity, Mevalonic Acid, Compound heterozygosity, Genomic disorders and inherited multi-system disorders [IGMD 3], Evaluation of complex medical interventions Genomic disorders and inherited multi-system disorders [NCEBP 2], Internal medicine, Retinitis pigmentosa, Electroretinography, medicine, Humans, Exome, Fluorescein Angiography, Exome sequencing, Mevalonate kinase deficiency, biology, business.industry, Genetic heterogeneity, Mevalonate kinase, Middle Aged, medicine.disease, Pedigree, Pathogenesis and modulation of inflammation [N4i 1], Phosphotransferases (Alcohol Group Acceptor), Ophthalmology, Mutation, biology.protein, Female, Genetics and epigenetic pathways of disease Genomic disorders and inherited multi-system disorders [NCMLS 6], business, Retinitis Pigmentosa, Tomography, Optical Coherence

Abstract

Contains fulltext : 125691.pdf (Publisher’s version ) (Closed access) OBJECTIVE: Retinitis pigmentosa (RP) is a clinically and genetically heterogeneous disorder characterized by night blindness and peripheral vision loss, and in many cases leads to blindness. Despite extensive knowledge about genes involved in the pathogenesis of RP, the genetic cause remains elusive in many patients. In this study, we aimed to identify novel genes that are involved in the cause of RP. DESIGN: We present a case series with mutations in the mevalonate kinase (MVK) gene. PARTICIPANTS: A total of 769 patients with nonsyndromic RP and 174 Dutch control individuals participated in this study. METHODS: Exome sequencing analysis was performed in a proband of Dutch origin who was initially diagnosed with nonsyndromic autosomal recessive RP. Mutations in MVK were identified and subsequently tested for segregation within the patient's family and screened in a large cohort of patients with genetically unsolved RP. Patients with mutations underwent extensive clinical reexamination. MAIN OUTCOME MEASURES: Digital fundus photography, spectral-domain optical coherence tomography (OCT), and fundus autofluorescence analysis were performed in patients with MVK mutations. Mevalonate kinase (MK) enzyme activity was analyzed in cultured lymphoblastoid cells, and mevalonic acid levels were measured in urine samples. RESULTS: Exome variant filtering and prioritization led to the identification of compound heterozygous mutations in MVK (p.I268T and p.A334T) in the proband and her affected brother. Screening of our nonsyndromic RP patient cohort revealed an additional individual who was homozygous for the p.A334T alteration. Clinical reevaluation of all 3 patients showed a classic form of RP with variable extraocular symptoms, such as history of recurrent childhood febrile crises in 2 patients, mild ataxia in 1, and renal failure in 1. All 3 affected individuals showed a significantly decreased MK activity and highly elevated levels of urinary mevalonic acid. CONCLUSIONS: Although the MK activity in cells and mevalonic acid concentrations in urine are strongly aberrant and comparable to that in patients with systemic mevalonate kinase deficiency (MKD), only mild clinical symptoms related to this syndrome were observed in our patients. In the current article, we add another phenotype to the spectrum of diverging disorders associated with mutations in MVK. FINANCIAL DISCLOSURE(S): The author(s) have no proprietary or commercial interest in any materials discussed in this article.

Published

2013

36. Genotype and clinical care correlations in craniosynostosis: Findings from a cohort of 630 Australian and New Zealand patients

Author

Susan M. White, Tiong Yang Tan, Lisa Worgan, Emma L. Hackett, Michael Gattas, David Mowat, Michael Field, Hanka Venselaar, George McGillivray, Felicity Collins, Edwin P. Kirk, Michael F. Buckley, Alison Colley, David J. David, Julie McGaughran, Trang T. Le, Michael T. Gabbett, David J. Amor, Timothy C. Cox, Rani Sachdev, Anne M. Turner, Mary-Louise Freckmann, Eric Haan, Peter J. Anderson, Kate Gibson, Ian A. Glass, Benjamin Kamien, Mark P. Gianoutsos, Joanne Dixon, David J. Moon, Tony Roscioli, Meredith Wilson, Matthew S. Edwards, Elizabeth Thompson, Lies H. Hoefsloot, Anna Hackett, George Elakis, Ravi Savarirayan, and L. C. Adès

Subjects

Proband, Sanger sequencing, Genetics, medicine.medical_specialty, Acrocephalosyndactylia, Apert syndrome, Biology, medicine.disease, Craniosynostosis, symbols.namesake, Genotype, medicine, symbols, Pfeiffer syndrome, Medical genetics, Genetics (clinical)

Abstract

Craniosynostosis is one of the most common craniofacial disorders encountered in clinical genetics practice, with an overall incidence of 1 in 2,500. Between 30% and 70% of syndromic craniosynostoses are caused by mutations in hotspots in the fibroblast growth factor receptor (FGFR) genes or in the TWIST1 gene with the difference in detection rates likely to be related to different study populations within craniofacial centers. Here we present results from molecular testing of an Australia and New Zealand cohort of 630 individuals with a diagnosis of craniosynostosis. Data were obtained by Sanger sequencing of FGFR1, FGFR2, and FGFR3 hotspot exons and the TWIST1 gene, as well as copy number detection of TWIST1. Of the 630 probands, there were 231 who had one of 80 distinct mutations (36%). Among the 80 mutations, 17 novel sequence variants were detected in three of the four genes screened. In addition to the proband cohort there were 96 individuals who underwent predictive or prenatal testing as part of family studies. Dysmorphic features consistent with the known FGFR1-3/TWIST1-associated syndromes were predictive for mutation detection. We also show a statistically significant association between splice site mutations in FGFR2 and a clinical diagnosis of Pfeiffer syndrome, more severe clinical phenotypes associated with FGFR2 exon 10 versus exon 8 mutations, and more frequent surgical procedures in the presence of a pathogenic mutation. Targeting gene hot spot areas for mutation analysis is a useful strategy to maximize the success of molecular diagnosis for individuals with craniosynostosis.

Published

2013

37. Buccal cell FISH and blood PCR-Y detect high rates of X chromosomal mosaicism and Y chromosomal derivatives in patients with Turner syndrome

Author

Ad R. M. M. Hermus, K. Freriks, Hanneke Mieloo, Maaike A.F. Traas, Henri J L M Timmers, Dominique Smeets, Romana T. Netea-Maier, Janiëlle A E M van Alfen-van der Velden, Barto J. Otten, Catharina C. M. Beerendonk, Guillaume van de Zande, and Lies H. Hoefsloot

Subjects

Adult, Monosomy, Pathology, medicine.medical_specialty, Buccal swab, Turner Syndrome, Gonadoblastoma, Biology, Real-Time Polymerase Chain Reaction, Y chromosome, Genomic disorders and inherited multi-system disorders [IGMD 3], Turner syndrome, Tissue mosaicism, Genetics, medicine, Humans, Hormonal regulation Translational research [IGMD 6], Genetic Predisposition to Disease, Lymphocytes, In Situ Hybridization, Fluorescence, Genetics (clinical), X chromosome, Ovarian Neoplasms, Chromosomes, Human, X, Chromosomes, Human, Y, Mosaicism, Hormonal regulation [IGMD 6], Mouth Mucosa, Karyotype, General Medicine, medicine.disease, Human Reproduction [NCEBP 12], Female, Genetics and epigenetic pathways of disease Genomic disorders and inherited multi-system disorders [NCMLS 6]

Abstract

Item does not contain fulltext Turner syndrome (TS) is the result of (partial) X chromosome monosomy. In general, the diagnosis is based on karyotyping of 30 blood lymphocytes. This technique, however, does not rule out tissue mosaicism or low grade mosaicism in the blood. Because of the associated risk of gonadoblastoma, mosaicism is especially important in case this involves a Y chromosome. We investigated different approaches to improve the detection of mosaicisms in 162 adult women with TS (mean age 29.9 +/- 10.3). Standard karyotyping identified 75 patients (46.3%) with a non-mosaic monosomy 45,X. Of these 75 patients, 63 underwent additional investigations including FISH on buccal cells with X- and Y-specific probes and PCR-Y on blood. FISH analysis of buccal cells revealed a mosaicism in 19 of the 63 patients (30.2%). In five patients the additional cell lines contained a (derivative) Y chromosome. With sensitive real-time PCR we confirmed the presence of this Y chromosome in blood in three of the five cases. Although Y chromosome material was established in ovarian tissue in two patients, no gonadoblastoma was found. Our results confirm the notion that TS patients with 45,X on conventional karyotyping often have tissue specific mosaicisms, some of which include a Y chromosome. Although further investigations are needed to estimate the risk of gonadoblastoma in patients with Y chromosome material in buccal cells, we conclude that FISH or real-time PCR on buccal cells should be considered in TS patients with 45,X on standard karyotyping.

Published

2013

38. New TRPC6 gain-of-function mutation in a non-consanguineous Dutch family with late-onset focal segmental glomerulosclerosis

Author

Willie H.M. van Kuijk, Jo H. M. Berden, Jack F.M. Wetzels, Lies H. Hoefsloot, Sergio Lainez, René J. M. Bindels, Johan van der Vlag, Marijke P. Baltissen, Jeroen Schoots, Tom Nijenhuis, Julia M. Hofstra, Nine V A M Knoers, and Joost G. J. Hoenderop

Subjects

Male, Time Factors, Sequence Homology, medicine.disease_cause, TRPC6, Exon, Consanguinity, Focal segmental glomerulosclerosis, Glomerulosclerosis, Tissue engineering and pathology Renal disorder [NCMLS 3], Age of Onset, Child, Renal disorder [IGMD 9], Netherlands, Genetics, Mutation, TRPC Cation Channels/genetics, Glomerulosclerosis, Focal Segmental, Tissue engineering and pathology Auto-immunity, transplantation and immunotherapy [NCMLS 3], Middle Aged, Prognosis, Infection and autoimmunity Auto-immunity, transplantation and immunotherapy [NCMLS 1], Pedigree, Electrophysiology, Amino Acid, Nephrology, Child, Preschool, Female, Focal Segmental/etiology, Glomerular Filtration Rate, Adult, Mutation/genetics, Molecular Sequence Data, Biology, Genomic disorders and inherited multi-system disorders [IGMD 3], medicine, TRPC6 Cation Channel, Humans, Family, Amino Acid Sequence, Preschool, TRPC Cation Channels, Aged, Transplantation, Sequence Homology, Amino Acid, Glomerulosclerosis, Focal Segmental/etiology, medicine.disease, Membrane transport and intracellular motility Renal disorder [NCMLS 5], HEK293 Cells, Age of onset, Nephrotic syndrome, Follow-Up Studies

Abstract

Contains fulltext : 118864.pdf (Publisher’s version ) (Closed access) BackgroundFocal segmental glomerulosclerosis (FSGS) is a leading cause of steroid-resistant nephrotic syndrome. Hereditary FSGS is frequently caused by mutations in important structural podocyte proteins, including the slit diaphragm-associated transient receptor potential channel C6 (TRPC6).MethodsIn five patients with biopsy-proven autosomal-dominant FSGS from five different Dutch families, all 13 exons of TRPC6 were sequenced. Upon identification of a novel TRPC6 sequence variant, the resultant amino acid change was introduced in the wild-type TRPC6 protein and functionally tested using patch-clamp analyses and cell-surface biotinylation experiments.ResultsNone of the previously described TRPC6 mutations were found in our cohort. In one family, we identified a novel c.524G>A sequence variant resulting in a p.Arg175Gln (R175Q) substitution in the TRPC6 protein. This sequence variant was absent in 449 control subjects and from public SNP databases. The mutation was located in the third ankyrin repeat domain (ANK3) in the cytoplasmic N-tail of TRPC6, important for protein-protein interaction and regulation of ion channel activity. Patch-clamp analyses of the mutant channel indeed showed an increased TRPC6 channel-mediated current. However, cell-surface expression of the mutant channel was not increased.ConclusionsWe identified a novel TRPC6 p.Arg175Gln gain-of-function mutation that shows increased TRPC6-mediated current, which is not due to altered cell-surface expression. This is the first mutation identified in ANK3 of the TRPC6 N-tail and is most likely responsible for the late-onset autosomal dominant FSGS in this family.

Published

2013

39. The Cardiac Phenotype in Patients With a CHD7 Mutation

Author

Nicole Corsten-Janssen, Maria E. Baardman, Jorieke E. H. Bergman, Gideon J. du Marchie Sarvaas, Ketil Heimdal, Wilhelmina S. Kerstjens-Frederikse, Raoul C.M. Hennekam, Lies H. Hoefsloot, Livia Kapusta, Hanne Hove, Conny M. A. van Ravenswaaij-Arts, Robert M.W. Hofstra, Marian K. Bakker, Cecilie F. Rustad, Amsterdam Neuroscience, Amsterdam Public Health, Human Genetics, Paediatrics, Faculteit Medische Wetenschappen/UMCG, Ethical, Legal, Social Issues in Genetics (ELSI), Methods in Medicines evaluation & Outcomes research (M2O), Reproductive Origins of Adult Health and Disease (ROAHD), and Clinical Genetics

Subjects

Heart Defects, Congenital, Male, medicine.medical_specialty, Heart disease, FEATURES, heart defect, congenital, medicine.disease_cause, COLOBOMA, Cohort Studies, Genomic disorders and inherited multi-system disorders [IGMD 3], CHARGE syndrome, Internal medicine, CHD7 protein, Genetics, medicine, Humans, In patient, human, ATRESIA, Genetics (clinical), CHD7 protein, human, SPECTRUM, Coloboma, Mutation, NEURAL CREST, business.industry, DNA Helicases, congenital, Infant, Neural crest, Heart, Functional imaging [IGMD 1], ASSOCIATION, DEFECTS, medicine.disease, heart defect, GENE, DNA-Binding Proteins, CONGENITAL HEART-DISEASE, Phenotype, CHARGE-SYNDROME, Atresia, Cardiology, Female, Cardiology and Cardiovascular Medicine, Cardiac phenotype, business

Abstract

Background— Loss-of-function mutations in CHD7 cause Coloboma, Heart Disease, Atresia of Choanae, Retardation of Growth and/or Development, Genital Hypoplasia, and Ear Abnormalities With or Without Deafness (CHARGE) syndrome, a variable combination of multiple congenital malformations including heart defects. Heart defects are reported in 70% to 92% of patients with a CHD7 mutation, but most studies are small and do not provide a detailed classification of the defects. We present the first, detailed, descriptive study on the cardiac phenotype of 299 patients with a CHD7 mutation and discuss the role of CHD7 in cardiac development. Methods and Results— We collected information on congenital heart defects in 299 patients with a pathogenic CHD7 mutation, of whom 220 (74%) had a congenital heart defect. Detailed information on the heart defects was available for 202 of these patients. We classified the heart defects based on embryonic cardiac development and compared the distribution to 1007 equally classified nonsyndromic heart defects of patients registered by EUROCAT, a European Registry of Congenital Anomalies. Heart defects are highly variable in patients with CHD7 mutations, but atrioventricular septal defects and conotruncal heart defects are over-represented. Sex did not have an effect on the presence of heart defects, but truncating CHD7 mutations resulted in a heart defect significantly more often than missense or splice-site mutations (χ 2 , P Conclusions— CHD7 plays an important role in cardiac development, given that we found a wide range of heart defects in 74% of a large cohort of patients with a CHD7 mutation. Conotruncal defects and atrioventricular septal defects are over-represented in patients with CHD7 mutations compared with patients with nonsyndromic heart defects.

Published

2013

40. More Clinical Overlap between 22q11.2 Deletion Syndrome and CHARGE Syndrome than Often Anticipated

Author

Wilhelmina S. Kerstjens-Frederikse, D A Driscoll, Lies H. Hoefsloot, C.M.A. van Ravenswaaij-Arts, K A Dickinson, Donna M. McDonald-McGinn, Elaine H. Zackai, Sulagna C. Saitta, Nicole Corsten-Janssen, Beverly S. Emanuel, and R Derks

Subjects

TBX1, Coloboma, Mutation, Pathology, medicine.medical_specialty, business.industry, medicine.disease, Bioinformatics, medicine.disease_cause, Phenotype, CHARGE syndrome, Atresia, Journal Article, Genetics, medicine, Original Article, Haploinsufficiency, business, Gene, Genetics (clinical)

Abstract

CHARGE (coloboma, heart defects, atresia of choanae, retardation of growth and development, genital hypoplasia, and ear abnormalities) and 22q11.2 deletion syndromes are variable, congenital malformation syndromes that show considerable phenotypic overlap. We further explored this clinical overlap and proposed recommendations for the genetic diagnosis of both syndromes. We described 2 patients clinically diagnosed with CHARGE syndrome, who were found to carry a 22q11.2 deletion, and searched the literature for more cases. In addition, we screened our cohort of CHD7 mutation carriers (n = 802) for typical 22q11.2 deletion features and studied CHD7 in 20 patients with phenotypically 22q11.2 deletion syndrome but without haploinsufficiency of TBX1. In total, we identified 5 patients with a clinical diagnosis of CHARGE syndrome and a proven 22q11.2 deletion. Typical 22q11.2 deletion features were found in 30 patients (30/802, 3.7%) of our CHD7 mutation-positive cohort. We found truncating CHD7 mutations in 5/20 patients with phenotypically 22q11.2 deletion syndrome. Differentiating between CHARGE and 22q11.2 deletion syndromes can be challenging. CHD7 and TBX1 probably share a molecular pathway or have common target genes in affected organs. We strongly recommend performing CHD7 analysis in patients with a 22q11.2 deletion phenotype without TBX1 haploinsufficiency and conversely, performing a genome-wide array in CHARGE syndrome patients without a CHD7 mutation.

Published

2013

41. The Immune Phenotype of Patients with CHARGE Syndrome

Author

Melanie Wong, Craig F Munns, Elizabeth H Barnes, Alan Ma, Tuula Rinne, Sam Mehr, Meredith Wilson, Peter Hsu, G. L. Williams, Lies H. Hoefsloot, Surgery, and Clinical Genetics

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Heart disease, Lymphocyte, DNA Mutational Analysis, Immunoglobulins, Choanal atresia, Gastroenterology, 03 medical and health sciences, CHARGE syndrome, 0302 clinical medicine, Immune system, 030225 pediatrics, Internal medicine, DiGeorge Syndrome, Humans, Immunology and Allergy, Medicine, Lymphocytes, Prospective Studies, Child, Prospective cohort study, Coloboma, biology, business.industry, DNA Helicases, Infant, Newborn, Infant, medicine.disease, DNA-Binding Proteins, 030104 developmental biology, medicine.anatomical_structure, Child, Preschool, Immunology, biology.protein, Calcium, Female, CHARGE Syndrome, Antibody, business

Abstract

Background Recurrent sinopulmonary infections are common in children with CHARGE (Coloboma, Heart disease, choanal Atresia, growth/mental Retardation, Genitourinary malformations, Ear abnormalities) syndrome, but no prospective studies on immune function have been conducted. Objective This study aims to examine and compare the immune phenotype of patients with CHARGE syndrome to those with 22q11.2 deletion and healthy controls. Methods A total of 21 patients attended a multidisciplinary CHARGE clinic. All patients had CHD7 mutational analysis performed. Patients with CHARGE syndrome had lymphocyte subsets, immunoglobulins (IgG, A, M), functional protein, and polysaccharide vaccine responses measured at initial evaluation. A total of 55 healthy controls were prospectively recruited, whereas 40 patients with 22q11.2 deletion were retrospectively identified through medical records. A separate analysis compared serial lymphocyte counts and ionized calcium levels between patients with CHARGE syndrome and those with 22q11.2 deletion in the first 72 months of life. Results Despite recurrent childhood ear and chest infections, only 2 children with CHARGE syndrome had an identifiable immune defect (reduced serum IgA). In contrast, T-cell lymphopenia, low immunoglobulin levels, and specific antibody deficiency were noted in patients with 22q11.2 deletion. A greater proportion of patients with 22q11.2 deletion had persistent lymphopenia (57% vs 30%) and hypocalcemia (60% vs 37.5%) compared with patients with CHARGE syndrome in the first 72 months of life. Conclusions Although phenotypic overlap exists between CHARGE and 22q11.2 deletion syndromes, no significant immune defects were detected in this cohort of patients with CHARGE syndrome at the time of testing. Lymphopenia and hypocalcemia occur in both conditions early in life, but is more pronounced in patients with 22q11.2 deletion.

Published

2016

42. Homozygosity mapping identifies genetic defects in four consanguineous families with retinal dystrophy from Pakistan

Author

Alamdar Hussain, Muhammad Imran Khan, A.I. den Hollander, Shazia Micheal, Maleeha Azam, Habib Bokhari, R. W. J. Collin, Muhammad Ajmal, Nadia K. Waheed, I. J. de Wijs, Frans P.M. Cremers, Hanka Venselaar, Raheel Qamar, A Shahzad, and Lies H. Hoefsloot

Subjects

Genetics, Retinal dystrophy, Biology, Disease gene identification, Genetics (clinical)

Published

2012

43. Mutation update on the CHD7 gene involved in CHARGE syndrome

Author

Jeroen Schoots, Conny M. A. van Ravenswaaij-Arts, Marianne Lodahl, Jorieke E. H. Bergman, Lies H. Hoefsloot, Morris A. Swertz, Lisbeth Tranebjærg, Nicole Janssen, Robert M.W. Hofstra, Erasmus MC other, and Clinical Genetics

Subjects

PHENOTYPIC SPECTRUM, INTERSTITIAL DELETION, MAJOR CAUSE, Biology, medicine.disease_cause, Chromatin remodeling, Frameshift mutation, Chromodomain, CHD7, CHARGE syndrome, DiGeorge syndrome, KALLMANN-SYNDROME, Genetics, medicine, Coding region, Animals, Humans, 22Q11.2 DELETION SYNDROME, CHOANAL ATRESIA, Genetics (clinical), Mutation, NEURAL CREST, DNA Helicases, Kallmann syndrome, CHD7 database, MOUSE MODEL, medicine.disease, Stop codon, DNA-Binding Proteins, CONGENITAL HEART-DISEASE, mutation spectrum, DIGEORGE-SYNDROME

Abstract

CHD7 is a member of the chromodomain helicase DNA-binding (CHD) protein family that plays a role in transcription regulation by chromatin remodeling. Loss-of-function mutations in CHD7 are known to cause CHARGE syndrome, an autosomal-dominant malformation syndrome in which several organ systems, for example, the central nervous system, eye, ear, nose, and mediastinal organs, are variably involved. In this article, we review all the currently described CHD7 variants, including 183 new pathogenic mutations found by our laboratories. In total, we compiled 528 different pathogenic CHD7 alterations from 508 previously published patients with CHARGE syndrome and 294 unpublished patients analyzed by our laboratories. The mutations are equally distributed along the coding region of CHD7 and most are nonsense or frameshift mutations. Most mutations are unique, but we identified 94 recurrent mutations, predominantly arginine to stop codon mutations. We built a locus-specific database listing all the variants that is easily accessible at . In addition, we summarize the latest data on CHD7 expression studies, animal models, and functional studies, and we discuss the latest clinical insights into CHARGE syndrome. Hum Mutat 33:11491160, 2012. (c) 2012 Wiley Periodicals, Inc.

Published

2012

44. A novel classification system to predict the pathogenic effects of CHD7 missense variants in CHARGE syndrome

Author

Nicole Janssen, Almer M. van der Sloot, Jorieke E. H. Bergman, Jeroen Schoots, Lies H. Hoefsloot, Conny M. A. van Ravenswaaij-Arts, Robert M.W. Hofstra, Nanna Dahl Rendtorff, Hermien E. K. de Walle, Lisbeth Tranebjærg, Clinical Genetics, Ethical, Legal, Social Issues in Genetics (ELSI), and Reproductive Origins of Adult Health and Disease (ROAHD)

Subjects

Genotype, Kallmann syndrome, PHENOTYPIC SPECTRUM, Genetic counseling, Mutation, Missense, SEQUENCE-ALIGNMENT, Sequence alignment, genotype-phenotype correlation, Biology, DISEASE, CHD7, prediction pathogenicity, CHARGE syndrome, KALLMANN-SYNDROME, Genetics, medicine, Humans, Missense mutation, Gene, Genetics (clinical), DOUBLE CHROMODOMAINS, PROTEIN FUNCTION, MUTATIONS, missense mutation, DNA Helicases, medicine.disease, GENE, Phenotype, DNA-Binding Proteins, SUBSTITUTIONS, FORCE-FIELD, classification system

Abstract

CHARGE syndrome is characterized by the variable occurrence of multisensory impairment, congenital anomalies, and developmental delay, and is caused by heterozygous mutations in the CHD7 gene. Correct interpretation of CHD7 variants is essential for genetic counseling. This is particularly difficult for missense variants because most variants in the CHD7 gene are private and a functional assay is not yet available. We have therefore developed a novel classification system to predict the pathogenic effects of CHD7 missense variants that can be used in a diagnostic setting. Our classification system combines the results from two computational algorithms (PolyPhen-2 and Align-GVGD) and the prediction of a newly developed structural model of the chromo- and helicase domains of CHD7 with segregation and phenotypic data. The combination of different variables will lead to a more confident prediction of pathogenicity than was previously possible. We have used our system to classify 145 CHD7 missense variants. Our data show that pathogenic missense mutations are mainly present in the middle of the CHD7 gene, whereas benign variants are mainly clustered in the 5' and 3' regions. Finally, we show that CHD7 missense mutations are, in general, associated with a milder phenotype than truncating mutations. Hum Mutat 33:12511260, 2012. (c) 2012 Wiley Periodicals, Inc.

Published

2012

45. Audiometric characteristics of two Dutch families with non-ocular Stickler syndrome (COL11A2)

Author

E. van Beelen, R. Leuwer, Henricus P. M. Kunst, Ronald J.E. Pennings, Patrick L. M. Huygen, L. Stöbe, K.D. Lichtenbelt, Lies H. Hoefsloot, Joop M. Leijendeckers, Ad F. M. Snik, and Ronald J.C. Admiraal

Subjects

Male, Heterozygote, medicine.medical_specialty, Tectorial Membrane, Hearing loss, Hearing Loss, Conductive, Gene Expression, DCN PAC - Perception action and control, Audiology, Collagen Type XI, Conductive hearing impairment, Loudness, Genomic disorders and inherited multi-system disorders [IGMD 3], otorhinolaryngologic diseases, Humans, Medicine, Missense mutation, Stickler syndrome, TECTA, Connective Tissue Diseases, Netherlands, medicine.diagnostic_test, business.industry, Arthritis, Audiogram, medicine.disease, Sensory Systems, eye diseases, Pedigree, Phenotype, Mutation, Audiometry, Pure-Tone, Female, Audiometry, medicine.symptom, Audiometry, Speech, business, Psychoacoustics

Abstract

Item does not contain fulltext OBJECTIVE: To evaluate hearing impairment and cochlear function in non-ocular Stickler syndrome. STUDY DESIGN: Multifamily study. PATIENTS & METHODS: Ten patients from two different families with non-ocular Stickler syndrome (Stickler syndrome type 3) were included. Six members of the first family and four members of the second family participated in this study. Otorhinolaryngologic examinations were performed. Pure-tone and speech audiograms were obtained. Longitudinal analysis was performed. Psychophysical measurements, including loudness scaling, gap detection, difference limen for frequency and speech perception in noise were administered to assess cochlear function at a deeper level. RESULTS: Affected individuals in the first family were carriers of a heterozygous splice donor mutation in the COL11A2 gene. Affected individuals in the second family were carriers of a novel heterozygous missense mutation in COL11A2. Both families showed bilateral, non-progressive hearing impairment with childhood onset. The severity of the hearing impairment exhibited inter- and intrafamilial variability and was mostly mild to moderate. The results of the psychophysical measurements were similar to those previously published for DFNA8/12 (TECTA) and DFNA13 (COL11A2) patients and thus consistent with an intra-cochlear conductive hearing impairment. This is in line with the theory that mutations in COL11A2 affect tectorial membrane function. CONCLUSION: Hearing impairment in non-ocular Stickler syndrome is characterized by non-progressive hearing loss, present since childhood, and mostly mild to moderate in severity. Psychophysical measurements in non-ocular Stickler patients were suggestive of intra-cochlear conductive hearing impairment. 01 september 2012

Published

2012

46. Mutations in the pre-replication complex cause Meier-Gorlin syndrome

Author

Hans van Bokhoven, John M. Opitz, Andrea Leitch, Stephen Brown, Jumana Y. Al-Aama, Michael B. Bober, Paul A.J. Brown, Salim Aftimos, Annick Toutain, Murray Feingold, Andrew P. Jackson, Jeroen Schoots, Ernie M.H.F. Bongers, John Dean, Alison Ross, Margaret E. Harley, I. Karen Temple, Michael Wright, Lies H. Hoefsloot, Alan Fryer, Alaa Y Edrees, James MacKenzie, Louise S. Bicknell, Carol Wise, Nine V A M Knoers, Pierre Sarda, and Nikolaus Kau

Subjects

Male, Microcephaly, Micrognathism/genetics, Origin Recognition Complex, Basal Cell Nevus Syndrome, Sequence Homology, Cell Cycle Proteins, Pre-replication complex, medicine.disease_cause, Ear/abnormalities, Patella/abnormalities, Locus heterogeneity, Origin Recognition Complex/genetics, Micrognathism, Frameshift Mutation, Growth Disorders, Renal disorder [IGMD 9], Genetics, Mutation, Nuclear Proteins, Ear, Patella, Pedigree, Amino Acid, Phenotype, Female, Functional Neurogenomics [DCN 2], Molecular Sequence Data, Mutation, Missense, Biology, Article, Genomic disorders and inherited multi-system disorders [IGMD 3], medicine, Humans, Amino Acid Sequence, DNA Primers, Congenital Microtia, Cell Cycle Proteins/genetics, DNA Primers/genetics, Sequence Homology, Amino Acid, Base Sequence, Growth Disorders/genetics, medicine.disease, Nuclear Proteins/genetics, Haplotypes, Genetics and epigenetic pathways of disease Renal disorder [NCMLS 6], Origin recognition complex, Missense, Primordial dwarfism

Abstract

Contains fulltext : 97141.pdf (Publisher’s version ) (Closed access) Meier-Gorlin syndrome (ear, patella and short-stature syndrome) is an autosomal recessive primordial dwarfism syndrome characterized by absent or hypoplastic patellae and markedly small ears(1)(3). Both pre- and post-natal growth are impaired in this disorder, and although microcephaly is often evident, intellect is usually normal in this syndrome. We report here that individuals with this disorder show marked locus heterogeneity, and we identify mutations in five separate genes: ORC1, ORC4, ORC6, CDT1 and CDC6. All of these genes encode components of the pre-replication complex, implicating defects in replication licensing as the cause of a genetic syndrome with distinct developmental abnormalities.

Published

2011

47. CHD7 mutations and CHARGE syndrome: the clinical implications of an expanding phenotype

Author

N Janssen, Robert M.W. Hofstra, Marjolijn C.J. Jongmans, Jorieke E. H. Bergman, Lies H. Hoefsloot, C.M.A. van Ravenswaaij-Arts, University Medical Centre Groningen, University of Groningen, Groningen, and Radboud University Medical Center [Nijmegen]

Subjects

medicine.medical_specialty, Kallmann syndrome, Genetic screening/counselling, Choanal atresia, Bioinformatics, COLOBOMA, MULTIPLE ANOMALIES, Genomic disorders and inherited multi-system disorders [IGMD 3], CHARGE syndrome, Molecular genetics, Internal medicine, KALLMANN-SYNDROME, Genotype, Genetics, medicine, DiGeorge Syndrome, otorhinolaryngologic diseases, Outpatient clinic, Humans, HYPOGONADOTROPIC HYPOGONADISM, Clinical genetics, CHOANAL ATRESIA, Genetics (clinical), SPECTRUM, Coloboma, NEURAL CREST, Hereditary cancer and cancer-related syndromes [ONCOL 1], business.industry, DNA Helicases, ASSOCIATION, Kallmann Syndrome, medicine.disease, GENE, CONGENITAL HEART-DISEASE, DNA-Binding Proteins, Endocrinology, Phenotype, Mutation, Medical genetics, CHARGE Syndrome, business

Abstract

Background CHARGE syndrome is a highly variable, multiple congenital anomaly syndrome, of which the complete phenotypic spectrum was only revealed after identification of the causative gene in 2004. CHARGE is an acronym for ocular coloboma, congenital heart defects, choanal atresia, retardation of growth and development, genital hypoplasia, and ear anomalies associated with deafness. This typical combination of clinical features is caused by autosomal dominant mutations in the CHD7 gene. Objective To explore the emerging phenotypic spectrum of CHD7 mutations, with a special focus on the mild end of the spectrum. Methods We evaluated the clinical characteristics in our own cohort of 280 CHD7 positive patients and in previously reported patients with CHD7 mutations and compared these with previously reported patients with CHARGE syndrome but an unknown CHD7 status. We then further explored the mild end of the phenotypic spectrum of CHD7 mutations. Results We discuss that CHARGE syndrome is primarily a clinical diagnosis. In addition, we propose guidelines for CHD7 analysis and indicate when evaluation of the semicircular canals is helpful in the diagnostic process. Finally, we give updated recommendations for clinical surveillance of patients with a CHD7 mutation, based on our exploration of the phenotypic spectrum and on our experience in a multidisciplinary outpatient clinic for CHARGE syndrome. Conclusion CHARGE syndrome is an extremely variable clinical syndrome. CHD7 analysis can be helpful in the diagnostic process, but the phenotype cannot be predicted from the genotype.

Published

2011

48. Anosmiapredicts hypogonadotropic hypogonadism in CHARGE syndrome

Author

Gianni Bocca, Conny M. A. van Ravenswaaij-Arts, Linda C. Meiners, Jorieke E. H. Bergman, Lies H. Hoefsloot, Faculteit Medische Wetenschappen/UMCG, and Reproductive Origins of Adult Health and Disease (ROAHD)

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Hearing loss, Kallmann syndrome, Hormone Replacement Therapy, PHENOTYPIC SPECTRUM, Anosmia, Choanal atresia, DISEASE, Genomic disorders and inherited multi-system disorders [IGMD 3], CHARGE syndrome, Olfaction Disorders, Hypogonadotropic hypogonadism, Hyposmia, Predictive Value of Tests, Internal medicine, KALLMANN-SYNDROME, medicine, otorhinolaryngologic diseases, Humans, Child, HYPOSMIA, Netherlands, Puberty, Delayed, CHD7 GENE, business.industry, MUTATIONS, Hypogonadism, Micropenis, ASSOCIATION, medicine.disease, Magnetic Resonance Imaging, Olfactory Bulb, VARIABILITY, Endocrinology, Pediatrics, Perinatology and Child Health, UPDATE, Female, medicine.symptom, CHARGE Syndrome, business

Abstract

Objective To test the hypothesis that a smell test could predict the occurrence of hypogonadotropic hypogonadism (HH) in patients with CHARGE syndrome, which is a variable combination of ocular coloboma, heart defects, choanal atresia, retardation of growth/development, genital hypoplasia, and ear anomalies or hearing loss caused by mutations in the CHD7 (chromodomain helicase DNA binding protein 7) gene.Study design We performed endocrine studies and smell testing (University of Pennsylvania Smell Identification Test) in 35 adolescent patients with molecularly confirmed CHARGE syndrome.Results Complete data on smell and puberty were available for 15 patients; 11 patients had both anosmia and HH, whereas 4 patients had normosmia/hyposmia and spontaneous puberty. In addition, 7 boys were highly suspected of having HH (they were too young for definite HH diagnosis, but all had cryptorchidism, micropenis, or both) and had anosmia. The type of CHD7 mutation could not predict HH because a father and daughter with the same CHD7 mutation were discordant for HH and anosmia.Conclusion Anosmia and HH were highly correlated in our cohort, and therefore smell testing seems to be an attractive method for predicting the occurrence of HH in patients with CHARGE syndrome. The use of this test could prevent delay of hormonal pubertal induction, resulting in an age-appropriate puberty. (J Pediatr 2011;158:474-9).

Published

2011

49. Genotype-Phenotype Correlation in DFNB8/10 Families with TMPRSS3 Mutations

Author

Margit Schraders, Mariet W. Elting, Tim M. Strom, Hanka Venselaar, Susanne Granneman, Patrick L. M. Huygen, Cor W. R. J. Cremers, Jaap Oostrik, N.J.D. Weegerink, Henricus P. M. Kunst, Lies H. Hoefsloot, Ronald J.C. Admiraal, Ronald J.E. Pennings, Hannie Kremer, Human genetics, and Other Research

Subjects

Male, Genetic Linkage, Compound heterozygosity, medicine.disease_cause, Protein Structure, Secondary, 0302 clinical medicine, ski-slope audiogram, Perception and Action [DCN 1], Missense mutation, Child, DFNB8/10, Genetics, 0303 health sciences, Mutation, medicine.diagnostic_test, Serine Endopeptidases, Audiogram, TMPRSS3 mutations, Cochlear Implantation, Phenotype, Sensory Systems, Neoplasm Proteins, Pedigree, 3. Good health, Child, Preschool, Audiometry, Pure-Tone, Female, medicine.symptom, Chemical and physical biology [NCMLS 7], Adult, Adolescent, Hearing loss, Mutation, Missense, Biology, Article, genotype–phenotype correlations, Genomic disorders and inherited multi-system disorders [IGMD 3], Hearing Loss, Bilateral, Young Adult, 03 medical and health sciences, medicine, Humans, Profound hearing impairment, Genetic Association Studies, 030304 developmental biology, Family Health, Infant, Membrane Proteins, Genetics and epigenetic pathways of disease Neuroinformatics [NCMLS 6], Protein Structure, Tertiary, Amino Acid Substitution, Otorhinolaryngology, Genetics and epigenetic pathways of disease Functional Neurogenomics [NCMLS 6], cochlear implantation, genotype-phenotype correlations, Audiometry, Audiometry, Speech, 030217 neurology & neurosurgery

Abstract

In the present study, genotype–phenotype correlations in eight Dutch DFNB8/10 families with compound heterozygous mutations in TMPRSS3 were addressed. We compared the phenotypes of the families by focusing on the mutation data. The compound heterozygous variants in the TMPRSS3 gene in the present families included one novel variant, p.Val199Met, and four previously described pathogenic variants, p.Ala306Thr, p.Thr70fs, p.Ala138Glu, and p.Cys107Xfs. In addition, the p.Ala426Thr variant, which had previously been reported as a possible polymorphism, was found in one family. All affected family members reported progressive bilateral hearing impairment, with variable onset ages and progression rates. In general, the hearing impairment affected the high frequencies first, and sooner or later, depending on the mutation, the low frequencies started to deteriorate, which eventually resulted in a flat audiogram configuration. The ski-slope audiogram configuration is suggestive for the involvement of TMPRSS3. Our data suggest that not only the protein truncating mutation p.T70fs has a severe effect but also the amino acid substitutions p.Ala306Thr and p.Val199Met. A combination of two of these three mutations causes prelingual profound hearing impairment. However, in combination with the p.Ala426Thr or p.Ala138Glu mutations, a milder phenotype with postlingual onset of the hearing impairment is seen. Therefore, the latter mutations are likely to be less detrimental for protein function. Further studies are needed to distinguish possible phenotypic differences between different TMPRSS3 mutations. Evaluation of performance of patients with a cochlear implant indicated that this is a good treatment option for patients with TMPRSS3 mutations as satisfactory speech reception was reached after implantation. Electronic supplementary material The online version of this article (doi:10.1007/s10162-011-0282-3) contains supplementary material, which is available to authorized users.

Published

2011

50. Next-generation sequencing identifies mutations of SMPX, which encodes the small muscle protein, X-linked, as a cause of progressive hearing impairment

Author

Margit Schraders, Jaap Oostrik, Patrick L. M. Huygen, N.J.D. Weegerink, Ronald J.E. Pennings, Henricus P. M. Kunst, Hannie Kremer, Vera M. Kalscheuer, Sriram Kannan, Stefan A. Haas, Ronald J.C. Admiraal, Lies H. Hoefsloot, and Hao Hu

Subjects

Adult, Male, Candidate gene, Adolescent, Hearing loss, DNA Mutational Analysis, Nonsense mutation, Muscle Proteins, Locus (genetics), Biology, Bioinformatics, Polymorphism, Single Nucleotide, Frameshift mutation, Genomic disorders and inherited multi-system disorders [IGMD 3], Young Adult, 03 medical and health sciences, 0302 clinical medicine, Genes, X-Linked, Report, medicine, Perception and Action [DCN 1], Genetics, otorhinolaryngologic diseases, Humans, Genetics(clinical), Insulin-Like Growth Factor I, Child, Frameshift Mutation, Hearing Loss, Gene, Progressive hearing impairment, Genetics (clinical), X chromosome, 030304 developmental biology, 0303 health sciences, Molecular Sequence Annotation, Middle Aged, Glycostation disorders [IGMD 4], Pedigree, Genetics and epigenetic pathways of disease Neuroinformatics [NCMLS 6], Codon, Nonsense, Child, Preschool, Genetics and epigenetic pathways of disease Functional Neurogenomics [NCMLS 6], Female, medicine.symptom, Sequence Analysis, 030217 neurology & neurosurgery

Abstract

Contains fulltext : 97159.pdf (Publisher’s version ) (Closed access) In a Dutch family with an X-linked postlingual progressive hearing impairment, a critical linkage interval was determined to span a region of 12.9 Mb flanked by the markers DXS7108 and DXS7110. This interval overlaps with the previously described DFNX4 locus and contains 75 annotated genes. Subsequent next-generation sequencing (NGS) detected one variant within the linkage interval, a nonsense mutation in SMPX. SMPX encodes the small muscle protein, X-linked (SMPX). Further screening was performed on 26 index patients from small families for which X-linked inheritance of nonsyndromic hearing impairment (NSHI) was not excluded. We detected a frameshift mutation in SMPX in one of the patients. Segregation analysis of both mutations in the families in whom they were found revealed that the mutations cosegregated with hearing impairment. Although we show that SMPX is expressed in many different organs, including the human inner ear, no obvious symptoms other than hearing impairment were observed in the patients. SMPX had previously been demonstrated to be specifically expressed in striated muscle and, therefore, seemed an unlikely candidate gene for hearing impairment. We hypothesize that SMPX functions in inner ear development and/or maintenance in the IGF-1 pathway, the integrin pathway through Rac1, or both.

Published

2011