Your search keyword '"Kwame Anyane-Yeboa"' showing total 66 results

1. Phenotypic spectrum of the recurrent TRPM3 p.( <scp>Val837Met</scp> ) substitution in seven individuals with global developmental delay and hypotonia

Author

Matthew A, Lines, Paula, Goldenberg, Ashley, Wong, Siddharth, Srivastava, Allan, Bayat, Hanne, Hove, Helena Gásdal, Karstensen, Kwame, Anyane-Yeboa, Jun, Liao, Nan, Jiang, Alison, May, Edwin, Guzman, Manuela, Morleo, Stefano, D'Arrigo, Claudia, Ciaccio, Chiara, Pantaleoni, Raffaele, Castello, Shane, McKee, Jinfon, Ong, Hana, Zibdeh-Lough, Frederic, Tran-Mau-Them, Anna, Gerasimenko, Delphine, Heron, Boris, Keren, Henri, Margot, Jean-Madeleine, de Sainte Agathe, Lydie, Burglen, Thomas, Voets, Joris, Vriens, A Micheil, Innes, David A, Dyment, Lines, M. A., Goldenberg, P., Wong, A., Srivastava, S., Bayat, A., Hove, H., Karstensen, H. G., Anyane-Yeboa, K., Liao, J., Jiang, N., May, A., Guzman, E., Morleo, M., D'Arrigo, S., Ciaccio, C., Pantaleoni, C., Castello, R., Mckee, S., Ong, J., Zibdeh-Lough, H., Tran-Mau-Them, F., Gerasimenko, A., Heron, D., Keren, B., Margot, H., de Sainte Agathe, J. -M., Burglen, L., Voets, T., Vriens, J., Innes, A. M., and Dyment, D. A.

Subjects

Epilepsy, Developmental Disabilities, seizure, Infant, Newborn, Mutation, Missense, TRPM Cation Channels, global developmental delay, Infant, Newborn, Diseases, Genematcher, intellectual disability, Exome Sequencing, Genetics, Humans, Muscle Hypotonia, TRPM3, Child, Genetics (clinical)

Abstract

TRPM3 encodes a transient receptor potential cation channel of the melastatin family, expressed in the central nervous system and in peripheral sensory neurons of the dorsal root ganglia. The recurrent substitution in TRPM3: c.2509G>A, p.(Val837Met) has been associated with syndromic intellectual disability and seizures. In this report, we present the clinical and molecular features of seven previously unreported individuals, identified by exome sequencing, with the recurrent p.(Val837Met) variant and global developmental delay. Other shared clinical features included congenital hypotonia, dysmorphic facial features (broad forehead, deep-set eyes, and down turned mouth), exotropia, and musculoskeletal issues (hip dysplasia, hip dislocation, scoliosis). Seizures were observed in two of seven individuals (febrile seizure in one and generalized tonic–clonic seizures with atonic drops in another), and epileptiform activity was observed in an additional two individuals. This report extends the number of affected individuals to 16 who are heterozygous for the de novo recurrent substitution p.(Val837Met). In contrast with the initial report, epilepsy was not a mandatory feature observed in this series. TRPM3 pathogenic variation should be considered in individuals with global developmental delays, moderate–severe intellectual disability with, or without, childhood-onset epilepsy.

Published

2022

2. Assessment of the beliefs, needs, and expectations for genetic counseling of patients with hypermobile Ehlers-Danlos syndrome

Author

Priyanka Ahimaz, Tamar Kramer, Pooja Swaroop, McKenzie Mitchell, Rebecca Hernan, Kwame Anyane‐Yeboa, and Elaine M. Pereira

Subjects

Joint Instability, Motivation, Genetics, Humans, Ehlers-Danlos Syndrome, Genetic Counseling, Genetics (clinical)

Abstract

Ehlers-Danlos syndrome, hypermobility type (hEDS) is a heritable connective tissue disorder that currently does not have a known molecular etiology. Previous studies have explored the complex symptomology, clinical diagnosis, and psychological aspects of hEDS. Genetics providers currently aid in the diagnosis and management guidance of patients with hEDS, but there is limited data describing the needs and expectations of individuals with hEDS from a clinical genetics appointment. Our study sought to explore these items through the use of an online survey to assess participants' beliefs, needs and expectations (BNE) for genetic counseling as well as questions about demographics, hEDS symptoms, and current medical care. A total of 460 respondents with hEDS completed the survey. Most participants felt joint pain/weakness (n = 392; 88%) was one of the most disruptive symptoms of hEDS and 63% (n = 289) reported having psychiatric conditions. BNE scores were highest in two domains: expectations to have psychosocial concerns addressed during a genetic counseling appointment (mean score = 4.4/5; SD = 0.56) and desire for positive feelings after a genetic counseling session (mean score = 4.3/5; SD = 0.59). Participants who previously had genetic counseling felt less unsure about their diagnosis (p = 0.02) and had lower need for information about hEDS (p 0.001). Majority of participants did not feel that their doctors were knowledgeable about hEDS (n = 269; 58%) and strongly supported a multidisciplinary approach to their care (n = 445; 97%). This research provides a framework for genetics providers and other healthcare professionals to assess the needs and expectations of patients with hEDS and consider re-structuring their appointment formats to service this population.

Published

2022

3. Whole-exome sequencing in the evaluation of fetal structural anomalies: a prospective cohort study

Author

David Goldstein, Melissa Stosic, Odelia Nahum, Louise Bier, Vimla S. Aggarwal, Colin D. Malone, Erica Spiegel, Brynn Levy, Jessica L. Giordano, Caroline Mebane, Ronald J. Wapner, Karen Wou, Kelly Brennan, Russell Miller, Nicholas Stong, Slavé Petrovski, Xiaolin Zhu, Quanli Wang, Sitharthan Kamalakaran, Kwame Anyane-Yeboa, Zhong Ren, and Vaidehi Jobanputra

Subjects

Male, medicine.medical_specialty, DNA Copy Number Variations, Genetic Carrier Screening, Abnormal Karyotype, Aneuploidy, Chorionic villus sampling, 030204 cardiovascular system & hematology, Ultrasonography, Prenatal, Fetal Development, 03 medical and health sciences, Fetus, 0302 clinical medicine, Pregnancy, Exome Sequencing, medicine, Humans, Abnormalities, Multiple, Prospective Studies, 030212 general & internal medicine, Copy-number variation, Prospective cohort study, Exome sequencing, medicine.diagnostic_test, Obstetrics, business.industry, General Medicine, medicine.disease, Chorionic Villi Sampling, Cohort, Amniocentesis, Female, business

Abstract

Summary Background Identification of chromosomal aneuploidies and copy number variants that are associated with fetal structural anomalies has substantial value. Although whole-exome sequencing (WES) has been applied to case series of a few selected prenatal cases, its value in routine clinical settings has not been prospectively assessed in a large unselected cohort of fetuses with structural anomalies. We therefore aimed to determine the incremental diagnostic yield (ie, the added value) of WES following uninformative results of standard investigations with karyotype testing and chromosomal microarray in an unselected cohort of sequential pregnancies showing fetal structural anomalies. Methods In this prospective cohort study, the parents of fetuses who were found to have a structural anomaly in a prenatal ultrasound were screened for possible participation in the study. These participants were predominantly identified in or were referred to the Columbia University Carmen and John Thain Center for Prenatal Pediatrics (New York, NY, USA). Fetuses with confirmed aneuploidy or a causal pathogenic copy number variant were excluded from WES analyses. By use of WES of the fetuses and parents (parent–fetus trios), we identified genetic variants that indicated an underlying cause (diagnostic genetic variants) and genetic variants that met the criteria of bioinformatic signatures that had previously been described to be significantly enriched among diagnostic genetic variants. Findings Between April 24, 2015, and April 19, 2017, 517 sequentially identified pregnant women found to have fetuses with a structural anomaly were screened for their eligibility for inclusion in our study. 71 (14%) couples declined testing, 87 (17%) trios were missing at least one DNA sample (from either parent or the fetus), 69 (13%) trios had a clinically relevant abnormal karyotype or chromosomal microarray finding, 51 (10%) couples did not consent to WES or withdrew consent, and five (1%) samples were not of good enough quality for analysis. DNA samples from 234 (45%) eligible trios were therefore used for analysis of the primary outcome. By use of trio sequence data, we identified diagnostic genetic variants in 24 (10%) families. Mutations with bioinformatic signatures that were indicative of pathogenicity but with insufficient evidence to be considered diagnostic were also evaluated; 46 (20%) of the 234 fetuses assessed were found to have such signatures. Interpretation Our analysis of WES data in a prospective cohort of unselected fetuses with structural anomalies shows the value added by WES following the use of routine genetic tests. Our findings suggest that, in cases of fetal anomalies in which assessment with karyotype testing and chromosomal microarray fail to determine the underlying cause of a structural anomaly, WES can add clinically relevant information that could assist current management of a pregnancy. The unique challenges of WES-based prenatal diagnostics require analysis by a multidisciplinary team of perinatal practitioners and laboratory specialists. Funding Institute for Genomic Medicine (Columbia University Irving Medical Center).

Published

2019

4. Bi-allelic KARS1 pathogenic variants affecting functions of cytosolic and mitochondrial isoforms are associated with a progressive and multisystem disease

Author

Paola Goffrini, Felice D'Arco, Enrico Baruffini, Adeline Vanderver, Tamison Jewett, Enrico Bertini, Anya Revah-Politi, Eirik Bratland, Vandana Shashi, Alessandra D'Amico, Camilla Ceccatelli Berti, Vimla Aggarwal, Silvia Maitz, Kwame Anyane-Yeboa, Tara H. Stamper, Francesco Canonico, Gabriel S Kupchik, Andreas Benneche, César Augusto Pinheiro Ferreira Alves, Daniela Longo, Gerarda Cappuccio, Annalaura Torella, Vincenzo Nigro, Nicola Brunetti-Pierri, Marjo S van der Knaap, Siren Berland, Jennifer A. Sullivan, Pediatrics, Amsterdam Neuroscience - Cellular & Molecular Mechanisms, Functional Genomics, Cappuccio, G., Ceccatelli Berti, C., Baruffini, E., Sullivan, J., Shashi, V., Jewett, T., Stamper, T., Maitz, S., Canonico, F., Revah-Politi, A., Kupchik, G. S., Anyane-Yeboa, K., Aggarwal, V., Benneche, A., Bratland, E., Berland, S., D'Arco, F., Alves, C. A., Vanderver, A., Longo, D., Bertini, E., Torella, A., Nigro, V., D'Amico, A., van der Knaap, M. S., Goffrini, P., Brunetti Pierri, N., and Brunetti-Pierri, N.

Subjects

Lysine-tRNA Ligase, Male, Mitochondrion, lysyl-transfer RNA synthetase, Cohort Studies, Cytosol, KARS, lysyl‐transfer RNA synthetase, Child, Research Articles, Muscular Dystrophie, Genetics (clinical), Allele, Genetics, 0303 health sciences, Progressive microcephaly, Homozygote, 030305 genetics & heredity, Phenotype, Mitochondria, Pedigree, Isoenzymes, mitochondrial disease, Child, Preschool, Transfer RNA, Disease Progression, Microcephaly, Female, KARS1, Research Article, Human, Gene isoform, Adolescent, Mitochondrial disease, Saccharomyces cerevisiae, Biology, 03 medical and health sciences, SDG 3 - Good Health and Well-being, medicine, Humans, Abnormalities, Multiple, Alleles, 030304 developmental biology, Organisms, Genetically Modified, Leukodystrophy, Brain Diseases, Metabolic, Inborn, Infant, LysRS, medicine.disease, Isoenzyme, Cohort Studie

Abstract

KARS1 encodes a lysyl-transfer RNA synthetase (LysRS) that links lysine to its cognate tRNA. Two different KARS1 isoforms exert functional effects in cytosol and mitochondria. Bi-allelic pathogenic variants in KARS1 have been associated to sensorineural hearing and visual loss, neuropathy, seizures, and leukodystrophy. We report the clinical, biochemical and neuroradiological features of nine individuals with KARS1-related disorder carrying 12 different variants with nine of them being novel. The consequences of these variants on the cytosol and/or mitochondrial LysRS were functionally validated in yeast mutants. Most cases presented with severe neurological features including congenital and progressive microcephaly, seizures, developmental delay/intellectual disability, and cerebral atrophy. Oculo-motor dysfunction and immuno-hematological problems were present in six and three cases, respectively. A yeast growth defect of variable severity was detected for most variants on both cytosolic and mitochondrial isoforms. The detrimental effects of two variants on yeast growth were partially rescued by lysine supplementation. Congenital progressive microcephaly, oculo-motor dysfunction and immuno-hematological problems are emerging phenotypes in KARS1-related disorders. The data in yeast emphasize the role of both mitochondrial and cytosolic isoforms in the pathogenesis of KARS1-related disorder and supports the therapeutic potential of lysine supplementation at least in a subset of patients. This article is protected by copyright. All rights reserved.

Published

2021

5. Truncating variants in the SHANK1 gene are associated with a spectrum of neurodevelopmental disorders

Author

Chong Ae Kim, Marwan Shinawi, Naomichi Matsumoto, Anya Revah-Politi, Julia Baptista, Halie J. May, Julie S. Cohen, Julia Rankin, Samantha Toy, Kwame Anyane-Yeboa, Michelle Primiano, Evan H. Baugh, David Goldstein, Richard E. Person, Constance Smith-Hicks, Louise Bier, Katherine W. Roche, Anna Chassevent, Yuri Uchiyama, Michel Guipponi, Joel Victor Fluss, Charles Conlon, Armand Bottani, Jaehoon Jeong, Vimla Aggarwal, Maria resa Te Carminho A. Rodrigues, and Aida Telegrafi

Subjects

Genetics, Neurons, Dendritic spine, HEK 293 cells, HOMER1, Nerve Tissue Proteins, Biology, Phenotype, Article, HEK293 Cells, Cell culture, Neurodevelopmental Disorders, Complementary DNA, Exome Sequencing, Humans, Gene, Genetics (clinical), Exome sequencing

Abstract

Purpose In this study, we aimed to characterize the clinical phenotype of a SHANK1-related disorder and define the functional consequences of SHANK1 truncating variants. Methods Exome sequencing (ES) was performed for six individuals who presented with neurodevelopmental disorders. Individuals were ascertained with the use of GeneMatcher and Database of Chromosomal Imbalance and Phenotype in Humans Using Ensembl Resources (DECIPHER). We evaluated potential nonsense-mediated decay (NMD) of two variants by making knock-in cell lines of endogenous truncated SHANK1, and expressed the truncated SHANK1 complementary DNA (cDNA) in HEK293 cells and cultured hippocampal neurons to examine the proteins. Results ES detected de novo truncating variants in SHANK1 in six individuals. Evaluation of NMD resulted in stable transcripts, and the truncated SHANK1 completely lost binding with Homer1, a linker protein that binds to the C-terminus of SHANK1. These variants may disrupt protein–protein networks in dendritic spines. Dispersed localization of the truncated SHANK1 variants within the spine and dendritic shaft was also observed when expressed in neurons, indicating impaired synaptic localization of truncated SHANK1. Conclusion This report expands the clinical spectrum of individuals with truncating SHANK1 variants and describes the impact these variants may have on the pathophysiology of neurodevelopmental disorders.

Published

2021

6. COVID-19’s Impact on Genetics at One Medical Center in New York

Author

Elaine M. Pereira, Priyanka Ahimaz, Carli Andrews, Kwame Anyane-Yeboa, Todor Arsov, Sara M. Berger, Ilana Chilton, Diana M. Cory, Wendy K. Chung, Katia R. Dergham, Michele M. Disco, Michelle E. Ernst, Tamar Forman, Stephanie Galloway, Alexa R. Geltzeiler, Jessica L. Giordano, Emily Griffin, Edwin Guzman, Nina Harkavy, Rebecca Hernan, Anah K. Hetzler, Alejandro Iglesias, Rupinder Kakar, Catherine Kentros, Thandiwe C. Khonje, Carrie Koval, Elana Levinson, Scott Robinson, Meredith J. Ross, Fatema Sadeque-Iqbal, Erica Spiegel, Elana Spitz, and Ronald J. Wapner

Subjects

medicine.medical_specialty, 2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), business.industry, Genetics, Medical, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Comment, New York, COVID-19, Family medicine, medicine, Humans, Center (algebra and category theory), Genetics(clinical), business, Genetics (clinical)

Published

2020

7. Impact of patient education videos on genetic counseling outcomes after exome sequencing

Author

Kwame Anyane-Yeboa, Catherine Au, Josue Natanael Martinez, Rebecca Hernan, Michelle Primiano, Robert L. Klitzman, Priyanka Ahimaz, Sara M. Berger, Edwin Guzman, Leyla Tabanfar, Wendy K. Chung, Alejandro D. Iglesias, Ilana Chilton, Laura Pisani, Julia Wynn, Ruth Ottman, Paul S. Appelbaum, Jessica E. Shaw, Jimmy Duong, Jasmin Roohi, Ashley Wilson, Megan T. Cho, Meredith Ross, Chana Ratner, and Emily Griffin

Subjects

Parents, medicine.medical_specialty, Genetic counseling, Genetic counselors, Patient education--Evaluation, Article, 03 medical and health sciences, 0302 clinical medicine, Patient Education as Topic, Patient experience, medicine, Humans, Exome, Patient education--Audio-visual aids, 030212 general & internal medicine, Routine care, Exome sequencing, 030503 health policy & services, General Medicine, Counselors, Family medicine, 0305 other medical science, Psychology, Video education, Patient education

Abstract

Objective Growing use of clinical exome sequencing (CES) has led to an increased burden of genomic education. Self-guided educational tools can minimize the educational burden for genetic counselors (GCs). The effectiveness of these tools must be evaluated. Methods Parents of patients offered CES were randomized to watch educational videos before their visit or to receive routine care. Parents and GCs were surveyed about their experiences following the sessions. The responses of the video (n = 102) and no-video (n = 105) groups were compared. Results GCs reported no significant differences between parents in the video and no-video groups on genetics knowledge or CES knowledge. In contrast, parents’ scores on genetics knowledge questions were lower in the video than no-video group (p = 0.007). Most parents reported the videos were informative, and the groups did not differ in satisfaction with GCs or decisions to have CES. Conclusion GCs and parents perceived the videos to be beneficial. However, lower scores on genetics knowledge questions highlight the need for careful development of educational tools. Practice implications Educational tools should be developed and assessed for effectiveness with the input of all stakeholders before widespread implementation. Better measures of the effectiveness of these educational tools are needed.

Published

2020

8. New diagnosis of atypical ataxia-telangiectasia in a 17-year-old boy with T-cell acute lymphoblastic leukemia and a novel ATM mutation

Author

Jennifer Levine, Denis G Loredan, Shan Zha, Mahesh M. Mansukhani, Lenore Omesi, Kwame Anyane-Yeboa, Jasmin Roohi, Anya Revah Politi, and Jennifer Crowe

Subjects

Male, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Adolescent, Ataxia Telangiectasia Mutated Proteins, Disease, Biology, Malignancy, Article, Ataxia Telangiectasia, 03 medical and health sciences, Genetics, medicine, Humans, Missense mutation, Child, Telangiectasia, Genetics (clinical), Immunodeficiency, Infant, Karyotype, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, 3. Good health, 030104 developmental biology, Child, Preschool, Mutation, Ataxia-telangiectasia, Immunology, Chromosome breakage, medicine.symptom

Abstract

Ataxia-telangiectasia (A-T) is an autosomal recessive chromosome breakage disorder caused by mutations in the ATM gene. Typically, it presents in early childhood with progressive cerebellar dysfunction along with immunodeficiency and oculocutaneous telangiectasia. An increased risk of malignancy is also associated with the syndrome and, rarely, may be the presenting feature in small children. We describe a 17-year-old boy with slurred speech, mild motor delays and learning disability diagnosed with atypical A-T in the setting of T-cell acute lymphoblastic leukemia. Suspicion for A-T was raised after review of a peripheral blood karyotype demonstrating rearrangements involving chromosomes 7 and/or 14. The diagnosis was confirmed after molecular testing identified a novel homozygous missense variant in ATM (c.5585T>A; p.Leu1862His) that resulted in protein instability and abolished serine/threonine protein kinase activity. To our knowledge, this is the first report of concurrent A-T and lymphoid malignancy diagnoses in an older child or adult with only mild neurological disease. Our experience suggests that screening for the disorder should be considered in any individual with lymphoid malignancy and neurological findings, especially as radiation and certain chemotherapy protocols are contraindicated in A-T.

Published

2017

9. Familial X-Linked Acrogigantism: Postnatal Outcomes and Tumor Pathology in a Prenatally Diagnosed Infant and His Mother

Author

Rebecca J Gordon, George Zanazzi, Sharon L. Wardlaw, Jeffrey H. Wisoff, Brittany K. Wise-Oringer, Raphael David, Christopher William, Wendy K. Chung, Brenda Kohn, Sharon E. Oberfield, and Kwame Anyane-Yeboa

Subjects

Adenoma, Adult, Male, medicine.medical_specialty, Proliferation index, Somatotropic cell, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Physiology, 030209 endocrinology & metabolism, Case Report, Biochemistry, Gigantism, Prolactin cell, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Pituitary adenoma, Pregnancy, Internal medicine, Prenatal Diagnosis, medicine, Humans, Pituitary Neoplasms, business.industry, Biochemistry (medical), Pituitary tumors, Pregnancy Outcome, Infant, Genetic Diseases, X-Linked, medicine.disease, Tumor Pathology, Bromocriptine, Prolactin, Mother-Child Relations, 030220 oncology & carcinogenesis, Acromegaly, Female, business, medicine.drug

Abstract

ContextX-linked acrogigantism (X-LAG), a condition of infant-onset acrogigantism marked by elevated GH, IGF-1, and prolactin (PRL), is extremely rare. Thirty-three cases, including three kindreds, have been reported. These patients have pituitary adenomas that are thought to be mixed lactotrophs and somatotrophs.Case DescriptionThe patient’s mother, diagnosed with acrogigantism at 21 months, underwent pituitary tumor excision at 24 months. For more than 30 years, stable PRL, GH, and IGF-1 concentrations and serial imaging studies indicated no tumor recurrence. During preconception planning, X-LAG was diagnosed: single-nucleotide polymorphism microarray showed chromosome Xq26.3 microduplication. After conception, single-nucleotide polymorphism microarray on a chorionic villus sample showed the same microduplication in the fetus, confirming familial X-LAG. The infant grew rapidly with rising PRL, GH, and IGF-1 concentrations and an enlarging suprasellar pituitary mass, despite treatment with bromocriptine. At 15 months, he underwent tumor resection. The pituitary adenoma resembled the mother’s pituitary adenoma, with tumor cells arranged in trabeculae and glandular structures. In both cases, many tumor cells expressed PRL, GH, and pituitary-specific transcription factor-1. Furthermore, the tumor expressed other lineage-specific transcription factors, as well as SOX2 and octamer-binding transcription factor 4, demonstrating the multipotentiality of X-LAG tumors. Both showed an elevated Ki-67 proliferation index, 5.6% in the mother and 8.5% in the infant, the highest reported in X-LAG.ConclusionsThis is a prenatally diagnosed case of X-LAG. Clinical follow-up and biochemical evaluation have provided insight into the natural history of this disease. Expression of stem cell markers and several cell lineage-specific transcription factors suggests that these tumors are multipotential.

Published

2019

10. A CCR4-NOT Transcription Complex, Subunit 1, CNOT1, Variant Associated with Holoprosencephaly

Author

Paul Kruszka, Seth I. Berger, Robert J. Lipinski, Maximilian Muenke, Sung-Kook Hong, Kwame Anyane-Yeboa, Joshua L. Everson, Ariel F. Martinez, and Karin Weiss

Subjects

0301 basic medicine, Male, Mutation, Missense, In situ hybridization, Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, Prosencephalon, Holoprosencephaly, Report, Genetics, medicine, Missense mutation, Animals, Humans, Child, Gene, Genetics (clinical), Neural fold, Infant, Semilobar holoprosencephaly, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, Phenotype, Forebrain, Transcription preinitiation complex, Female, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Holoprosencephaly is the incomplete separation of the forebrain during embryogenesis. Both genetic and environmental etiologies have been determined for holoprosencephaly; however, a genetic etiology is not found in most cases. In this report, we present two unrelated individuals with semilobar holoprosencephaly who have the identical de novo missense variant in the gene CCR4-NOT transcription complex, subunit 1 (CNOT1). The variant (c.1603C>T [p.Arg535Cys]) is predicted to be deleterious and is not present in public databases. CNOT1 has not been previously associated with holoprosencephaly or other brain malformations. In situ hybridization analyses of mouse embryos show that Cnot1 is expressed in the prosencephalic neural folds at gestational day 8.25 during the critical period for subsequent forebrain division. Combining human and mouse data, we show that CNOT1 is associated with incomplete forebrain division.

Published

2019

11. Germline De Novo Mutations in GNB1 Cause Severe Neurodevelopmental Disability, Hypotonia, and Seizures

Author

Louise Bier, Fan Xia, Zhong Ren, Susan Schelley, Geoffrey Wallace, Amy L Schneider, Thomas Besnard, Tracy Dudding-Byth, David Goldstein, Benjamin Cogné, Gregory M. Enns, Xiaolin Zhu, Jill A. Rosenfeld, Edwin Guzman, Xenia Latypova, Joanne M. Nguyen, Anya Revah Politi, James J. Riviello, Sophie Colombo, Erin L. Heinzen, Candace T. Myers, Bertrand Isidor, Joline C. Dalton, Theresa A. Grebe, Michele G. Mehaffey, Peter I. Karachunski, Kwame Anyane-Yeboa, Jonathan A. Bernstein, Slavé Petrovski, Klaas J. Wierenga, Alice Basinger, Heather C Mefford, Martin G. Bialer, Pierre Corre, Ingrid E. Scheffer, Emily Becraft, Stéphane Bézieau, Natasha Shur, Sandra Mercier, Aaron Rosen, Christine Moore, Sébastien Schmitt, Sébastien Küry, Alexandrea Wadley, Parisa Hemati, and Ian Andrews

Subjects

Adult, Male, 0301 basic medicine, Adolescent, Protein Conformation, Developmental Disabilities, Biology, Bioinformatics, medicine.disease_cause, Germline, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Neurodevelopmental disorder, Germline mutation, Seizures, Intellectual Disability, Report, Genetics, medicine, Humans, Missense mutation, Exome, Genetics(clinical), Child, Germ-Line Mutation, Genetics (clinical), Mutation, GTP-Binding Protein beta Subunits, Infant, medicine.disease, Hypotonia, Phenotype, 030104 developmental biology, Child, Preschool, Muscle Hypotonia, Female, medicine.symptom, GNB1, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Whole-exome sequencing of 13 individuals with developmental delay commonly accompanied by abnormal muscle tone and seizures identified de novo missense mutations enriched within a sub-region of GNB1, a gene encoding the guanine nucleotide-binding protein subunit beta-1, Gβ. These 13 individuals were identified among a base of 5,855 individuals recruited for various undiagnosed genetic disorders. The probability of observing 13 or more de novo mutations by chance among 5,855 individuals is very low (p = 7.1 × 10(-21)), implicating GNB1 as a genome-wide-significant disease-associated gene. The majority of these 13 mutations affect known Gβ binding sites, which suggests that a likely disease mechanism is through the disruption of the protein interface required for Gα-Gβγ interaction (resulting in a constitutively active Gβγ) or through the disruption of residues relevant for interaction between Gβγ and certain downstream effectors (resulting in reduced interaction with the effectors). Strikingly, 8 of the 13 individuals recruited here for a neurodevelopmental disorder have a germline de novo GNB1 mutation that overlaps a set of five recurrent somatic tumor mutations for which recent functional studies demonstrated a gain-of-function effect due to constitutive activation of G protein downstream signaling cascades for some of the affected residues.

Published

2016

12. Gain-of-function variants in the ODC1 gene cause a syndromic neurodevelopmental disorder associated with macrocephaly, alopecia, dysmorphic features, and neuroimaging abnormalities

Author

Lance H. Rodan, Farrah Rajabi, Ashley Wilson, Sanjeev V. Kothare, Jolien S. Klein Wassink-Ruiter, Karen Chong, Annapurna Poduri, Susan Blaser, Gerard T. Berry, Ralph J. DeBerardinis, Kwame Anyane-Yeboa, Lacey Smith, and Min Ni

Subjects

0301 basic medicine, Male, Neuropsychological Tests, Bioinformatics, Corpus callosum, Mitochondrial Membrane Transport Proteins, Ornithine decarboxylase, chemistry.chemical_compound, 0302 clinical medicine, Neurodevelopmental disorder, putrescine, Global developmental delay, Child, Genetics (clinical), Dicarboxylic Acid Transporters, Brain, Electroencephalography, Body Dysmorphic Disorders, Phenotype, Gain of Function Mutation, Female, medicine.symptom, ornithine decarboxylase 1 (ODC1), Adolescent, Genotype, polyamines, Neuroimaging, METABOLISM, Polymorphism, Single Nucleotide, 03 medical and health sciences, Genetics, medicine, Humans, Alleles, business.industry, Macrocephaly, Cancer, Facies, medicine.disease, alopecia, neurodevelopmental disorder, Megalencephaly, 030104 developmental biology, chemistry, Neurodevelopmental Disorders, Mutation, Polyamine, business, 030217 neurology & neurosurgery

Abstract

Polyamines serve a number of vital functions in humans, including regulation of cellular proliferation, intracellular signaling, and modulation of ion channels. Ornithine decarboxylase 1 (ODC1) is the rate-limiting enzyme in endogenous polyamine synthesis. In this report, we present four patients with a distinct neurometabolic disorder associated with de novo heterozygous, gain-of-function variants in the ODC1 gene. This disorder presents with global developmental delay, ectodermal abnormalities including alopecia, absolute or relative macrocephaly, and characteristic facial dysmorphisms. Neuroimaging variably demonstrates white matter abnormalities, prominent Virchow-Robin spaces, periventricular cysts, and abnormalities of the corpus callosum. Plasma clinical metabolomics analysis demonstrates elevation of N-acetylputrescine, the acetylated form of putrescine, with otherwise normal polyamine levels. Therapies aimed at reducing putrescine levels, including ODC1 inhibitors, dietary interventions, and antibiotics to reduce polyamine production by gastrointestinal flora could be considered as disease-modifying therapies. As the ODC1 gene has been implicated in neoplasia, cancer surveillance may be important in this disorder.

Published

2018

13. De novo variants in HK1 associated with neurodevelopmental abnormalities and visual impairment

Author

Aida Telegrafi, Kwame Anyane-Yeboa, Megan T. Cho, Ian D. Krantz, Wendy K. Chung, Kinga M. Bujakowska, Kyle Retterer, Ganka Douglas, Ashley Wilson, Dorothy K. Grange, Kristin G. Monaghan, Linda Manwaring, Amber Begtrup, Brigitte A. van Oirschot, Eric A. Pierce, Peter J. Hulick, Holley May, Volkan Okur, Colleen Clark Muraresku, Richard van Wijk, Stephanie A. Coury, Emily Place, and Jonathan Picker

Subjects

Hemolytic anemia, Adult, Male, medicine.medical_specialty, Erythrocytes, Adolescent, Mutation, Missense, medicine.disease_cause, Article, 03 medical and health sciences, chemistry.chemical_compound, Neurodevelopmental disorder, Internal medicine, Hexokinase, Intellectual disability, Genetics, Medicine, Missense mutation, Humans, Glycolysis, Child, Genetics (clinical), 0303 health sciences, Mutation, business.industry, 030305 genetics & heredity, Infant, medicine.disease, eye diseases, Pedigree, Endocrinology, chemistry, Female, business, Hereditary motor and sensory neuropathy, Hereditary Sensory and Motor Neuropathy, Retinitis Pigmentosa

Abstract

Hexokinase 1 (HK1) phosphorylates glucose to glucose-6-phosphate, the first rate-limiting step in glycolysis. Homozygous and heterozygous variants in HK1 have been shown to cause autosomal recessive non-spherocytic hemolytic anemia, autosomal recessive Russe type hereditary motor and sensory neuropathy, and autosomal dominant retinitis pigmentosa (adRP). We report seven patients from six unrelated families with a neurodevelopmental disorder associated with developmental delay, intellectual disability, structural brain abnormality, and visual impairments in whom we identified four novel, de novo missense variants in the N-terminal half of HK1. Hexokinase activity in red blood cells of two patients was normal, suggesting that the disease mechanism is not due to loss of hexokinase enzymatic activity.

Published

2018

14. Mutations inSLC1A4, encoding the brain serine transporter, are associated with developmental delay, microcephaly and hypomyelination

Author

Wendy K. Chung, Motee Al-Ashhab, Nadirah Damseh, Matthias A. Hediger, Barak Yaacov, Alexandre Simonin, Orly Elpeleg, Aida Telegrafi, Julie Neidich, Jane Juusola, John Pappas, Sherri J. Bale, Kyle Retterer, Joseph A. Picoraro, Bassam Abu-Libdeh, Ellen Moran, Kwame Anyane Yeboa, Avraham Shaag, Simon Edvardson, Megan T. Cho, Chaim Jalas, and Joshua Cappell

Subjects

Amino Acid Transport System ASC, Male, Heterozygote, medicine.medical_specialty, Microcephaly, Adolescent, Developmental Disabilities, DNA Mutational Analysis, Population, Biology, medicine.disease_cause, Serine, Molecular genetics, Genetics, medicine, Humans, Serine transport, Child, 610 Medicine & health, education, Exome, Myelin Sheath, Genetics (clinical), chemistry.chemical_classification, Mutation, education.field_of_study, Genetic Carrier Screening, Biological Transport, medicine.disease, Pedigree, Amino acid, Cell biology, HEK293 Cells, chemistry, Child, Preschool, 570 Life sciences, biology, Female

Abstract

Background L-serine plays an essential role in neuronal development and function. Although a non-essential amino acid, L-serine must be synthesised within the brain because of its poor permeability by the blood–brain barrier. Within the brain, its synthesis is confined to astrocytes, and its shuttle to neuronal cells is performed by a dedicated neutral amino acid transporter, ASCT1. Methods and results Using exome analysis we identified the recessive mutations, p.E256K, p.L315fs, and p.R457W, in SLC1A4 , the gene encoding ASCT1, in patients with developmental delay, microcephaly and hypomyelination; seizure disorder was variably present. When expressed in a heterologous system, the mutations did not affect the protein level at the plasma membrane but abolished or markedly reduced L-serine transport for p.R457W and p.E256K mutations, respectively. Interestingly, p.E256K mutation displayed a lower L-serine and alanine affinity but the same substrate selectivity as wild-type ASCT1. Conclusions The clinical phenotype of ASCT1 deficiency is reminiscent of defects in L-serine biosynthesis. The data underscore that ASCT1 is essential in brain serine transport. The SLC1A4 p.E256K mutation has a carrier frequency of 0.7% in the Ashkenazi-Jewish population and should be added to the carrier screening panel in this community.

Published

2015

15. Diagnostic exome sequencing in children: A survey of parental understanding, experience and psychological impact

Author

Jimmy Duong, Ashley Wilson, Julia Wynn, R. Rabin, Josue Natanael Martinez, Robert L. Klitzman, Wendy K. Chung, U. Lichter‐Konecki, Alejandro Iglesias, M. Primiano, Megan T. Cho, Rachel Webster, Priyanka Ahimaz, Edwin Guzman, Kwame Anyane-Yeboa, C. Egan, Paul S. Appelbaum, E. Rosen, J.E. Shaw, Ruth Ottman, and R. Sisson

Subjects

0301 basic medicine, Adult, Male, Parents, Genetic counseling, Developmental Disabilities, Genetic Counseling, Disclosure, 030105 genetics & heredity, Article, law.invention, 03 medical and health sciences, law, Surveys and Questionnaires, Exome Sequencing, Genetics, medicine, Humans, Exome, Genetic Testing, Child, Genetics (clinical), Exome sequencing, Depression (differential diagnoses), business.industry, Regret, Test (assessment), CLARITY, Anxiety, Female, Personalized medicine, medicine.symptom, Psychology, business, Clinical psychology

Abstract

Clinical exome sequencing (CES) is increasingly being used as an effective diagnostic tool in the field of pediatric genetics. We sought to evaluate the parental experience, understanding and psychological impact of CES by conducting a survey study of English-speaking parents of children who had diagnostic CES. Parents of 192 unique patients participated. The parent's interpretation of the child's result agreed with the clinician's interpretation in 79% of cases, with more frequent discordance when the clinician's interpretation was uncertain. The majority (79%) reported no regret with the decision to have CES. Most (65%) reported complete satisfaction with the genetic counseling experience, and satisfaction was positively associated with years of genetic counselor (GC) experience. The psychological impact of CES was greatest for parents of children with positive results and for parents with anxiety or depression. The results of this study are important for helping clinicians to prepare families for the possible results and variable psychological impact of CES. The frequency of parental misinterpretation of test results indicates the need for additional clarity in the communication of results. Finally, while the majority of patients were satisfied with their genetic counseling, satisfaction was lower for new GCs, suggesting a need for targeted GC training for genomic testing.

Published

2017

16. Loss-of-function variants in NFIA provide further support that NFIA is a critical gene in 1p32-p31 deletion syndrome: A four patient series

Author

Kwame Anyane-Yeboa, Anya Revah-Politi, Alejandro Iglesias, Louise Bier, Slavé Petrovski, Megan T. Cho, Parisa Hemati, David Goldstein, Vimla S. Aggarwal, Mythily Ganapathi, Ashley Wilson, John Pappas, and Jane Juusola

Subjects

0301 basic medicine, Adult, Male, Adolescent, Developmental Disabilities, Haploinsufficiency, Biology, Nervous System Malformations, Frameshift mutation, Cohort Studies, 03 medical and health sciences, Loss of Function Mutation, Exome Sequencing, Genetics, medicine, Humans, Child, Genetics (clinical), Exome sequencing, Macrocephaly, Microdeletion syndrome, medicine.disease, Hypotonia, Megalencephaly, Arnold-Chiari Malformation, NFI Transcription Factors, 030104 developmental biology, NFIA, Chromosomes, Human, Pair 1, Female, medicine.symptom, Agenesis of Corpus Callosum, Chromosome Deletion, Ventriculomegaly

Abstract

The association between 1p32-p31 contiguous gene deletions and a distinct phenotype that includes anomalies of the corpus callosum, ventriculomegaly, developmental delay, seizures, and dysmorphic features has been long recognized and described. Recently, the observation of overlapping phenotypes in patients with chromosome translocations that disrupt NFIA (Nuclear factor I/A), a gene within this deleted region, and NFIA intragenic deletions has led to the hypothesis that NFIA is a critical gene within this region. The wide application and increasing accessibility of whole exome sequencing (WES) has helped identify new cases to support this hypothesis. Here, we describe four patients with loss-of-function variants in the NFIA gene identified through WES. The clinical presentation of these patients significantly overlaps with the phenotype described in previously reported cases of 1p32-p31 deletion syndrome, NFIA gene disruptions and intragenic NFIA deletions. Our cohort includes a mother and daughter as well as an unrelated individual who share the same nonsense variant (c.205C>T, p.Arg69Ter; NM_001145512.1). We also report a patient with a frameshift NFIA variant (c.159_160dupCC, p.Gln54ProfsTer49). We have compared published cases of 1p32-p31 microdeletion syndrome, translocations resulting in NFIA gene disruption, intragenic deletions, and loss-of-function mutations (including our four patients) to reveal that abnormalities of the corpus callosum, ventriculomegaly/hydrocephalus, macrocephaly, Chiari I malformation, dysmorphic features, developmental delay, hypotonia, and urinary tract defects are common findings. The consistent overlap in clinical presentation provides further evidence of the critical role of NFIA haploinsufficiency in the development of the 1p32-p31 microdeletion syndrome phenotype.

Published

2017

17. The genomic landscape of balanced cytogenetic abnormalities associated with human congenital anomalies

Author

Bert Callewaert, Robert J. Hopkin, David A. Koolen, Hennie T. Brüggenwirth, Dezso David, Heather L. Ferguson, Helen Cox, Claire Redin, Joseph V. Thakuria, Ryan L. Collins, Mary-Alice Abbott, Michael E. Talkowski, Sjors Middelkamp, Michael J. Macera, Salmo Raskin, William J. Rhead, Heather Fisher, Han G. Brunner, Emmanuelle Lemyre, Margo Grady, Elyse Mitchell, Tarja Mononen, Sofia L. Alcaraz-Estrada, Cristin Griffis, Emily Moe, Samantha L.P. Schilit, Matthew J. Waterman, Colby Chiang, Aggie W. M. Nieuwint, Ivo Renkens, Joan F. Atkin, Jessie C. Jacobsen, Shehla Mohammed, Ernie M.H.F. Bongers, Maria de la Concepcion A Yerena-de Vega, Wigard P. Kloosterman, Jiddeke M. van de Kamp, Ton van Essen, Liya R Mikami, Tom Cushing, Conny M. A. van Ravenswaaij-Arts, Melita Irving, Kwame Anyane-Yeboa, Diane Masser-Frye, Catarina M. Seabra, Daniela Giachino, Bert B.A. de Vries, Brynn Levy, Caroline Antolik, Tina M. Bartell, Erika Aberg, Edwin Cuppen, Pamela Gerrol, Shahrin Pereira, Megan Mortenson, Raul Eduardo Pina Aguilar, Zehra Ordulu, Jennelle C. Hodge, Nicole de Leeuw, Troy J. Gliem, Michael W. McClellan, Sarah Vergult, Julia Tagoe, Giulia Pregno, Sandhya Parkash, David R. FitzPatrick, Giorgia Mandrile, Catharina M L Volker-Touw, Joseph T. Glessner, Danielle Perrin, Haibo Li, Peter M. Kroisel, Rhett Adley, Jodi D. Hoffman, Dorothy Warburton, Lauren Margolin, David J. Harris, Omar A. Abdul-Rahman, Ineke van der Burgt, Benjamin Currall, Monika Weisz Hubshman, Marjolijn C.J. Jongmans, Roberto T. Zori, William Lawless, Cynthia Lim, Andrea Hanson-Kahn, Vamsee Pillalamarri, Ken Corning, Tamara Mason, Yu An, Pino J. Poddighe, Susan P. Pauker, Cinthya J Zepeda Mendoza, Fowzan S. Alkuraya, Mira Irons, Sandra Janssens, Ranad Shaheen, Kathleen A. Leppig, Erica Spiegel, Chester W. Brown, Cynthia C. Morton, Filip Roelens, Ron Hochstenbach, Tamison Jewett, James F. Gusella, John P. Johnson, Brett H. Graham, Björn Menten, Annelies Dheedene, Rosamund Hill, Eva H. Brilstra, Alex V. Levin, Carlo Marcelis, Anna Wilson, A. Micheil Innes, Matthew A. Deardorff, Marc D'Hooghe, Elizabeth Beyer, Katy Phelan, Jayla Ruliera, Carrie Hanscom, Mark A. Hayden, Debra Rita, Edward J. Lose, Poornima Manavalan, Jerome Korzelius, Susan Wiley, Harrison Brand, Matthew R. Stone, Diane Lucente, Markus J. van Roosmalen, Tammy Kammin, Rebecca Sparkes, Patrick Rump, Stephen G. Kahler, Graciela Moya, Bregje W.M. van Bon, Blair Stevens, Eric C. Liao, Karen W. Gripp, Yves Lacassie, Dawn L. Earl, Erik C. Thorland, Linda M. Reis, Andrea L. Gropman, Jonathan A. Bernstein, Ian Blumenthal, Mary-Anne Anderson, Hong Li, Erasmus MC other, Klinische Genetica, RS: GROW - R4 - Reproductive and Perinatal Medicine, MUMC+: DA Klinische Genetica (5), Human genetics, AGEM - Endocrinology, metabolism and nutrition, AGEM - Inborn errors of metabolism, Amsterdam Neuroscience - Complex Trait Genetics, and Clinical Cognitive Neuropsychiatry Research Program (CCNP)

Subjects

0301 basic medicine, Male, INTELLECTUAL DISABILITY, Autism, Genome-wide association study, 030105 genetics & heredity, OF-FUNCTION MUTATIONS, balanced chromosomal abnormalities (BCAs), MEF2C, Genetics, Gene Rearrangement, Cytogenetic Abnormalities, Chromothripsis, DEVELOPMENTAL DELAY, Inversion, karyotypes, Microdeletion syndrome, Doenças Genómicas, Structural Variation, Medical genetics, Female, Topologically Associated Domain (TAD), Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Genetic Markers, medicine.medical_specialty, Human Congenital Anomalies, MICRODELETION SYNDROME, Translocation, Genomics, Biology, Article, Congenital Abnormalities, Structural variation, 03 medical and health sciences, Cytogenetics, Intellectual Disability, medicine, Journal Article, Humans, Genetic Predisposition to Disease, Chromosome Aberrations, Whole-genome sequencing, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], CHROMOSOME REARRANGEMENTS, karyotypes, balanced chromosomal abnormalities (BCAs), Whole-genome sequencing, AUTISM SPECTRUM DISORDER, CANCER GENOMES, Gene rearrangement, Balanced Chromosomal Abnormality, Doenças Genéticas, STRUCTURAL VARIATION, 030104 developmental biology, Congenital Anomaly, SEVERE MENTAL-RETARDATION, DE-NOVO MUTATIONS, Genome-Wide Association Study

Abstract

Despite the clinical significance of balanced chromosomal abnormalities (BCAs), their characterization has largely been restricted to cytogenetic resolution. We explored the landscape of BCAs at nucleotide resolution in 273 subjects with a spectrum of congenital anomalies. Whole-genome sequencing revised 93% of karyotypes and demonstrated complexity that was cryptic to karyotyping in 21% of BCAs, highlighting the limitations of conventional cytogenetic approaches. At least 33.9% of BCAs resulted in gene disruption that likely contributed to the developmental phenotype, 5.2% were associated with pathogenic genomic imbalances, and 7.3% disrupted topologically associated domains (TADs) encompassing known syndromic loci. Remarkably, BCA breakpoints in eight subjects altered a single TAD encompassing MEF2C, a known driver of 5q14.3 microdeletion syndrome, resulting in decreased MEF2C expression. We propose that sequence-level resolution dramatically improves prediction of clinical outcomes for balanced rearrangements and provides insight into new pathogenic mechanisms, such as altered regulation due to changes in chromosome topology. info:eu-repo/semantics/publishedVersion

Published

2017

18. The usefulness of whole-exome sequencing in routine clinical practice

Author

Ashley Wilson, Alejandro Iglesias, Edwin Guzman, Wendy K. Chung, Claire Egan, Rebecca Sisson, Megan T. Cho, Kwame Anyane-Yeboa, and Julia Wynn

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, Adolescent, Developmental Disabilities, DNA Mutational Analysis, MEDLINE, Consanguinity, Young Adult, Pregnancy, Humans, Medicine, Exome, Genetic Testing, Family history, Child, Genetics (clinical), Exome sequencing, Retrospective Studies, Genetic testing, medicine.diagnostic_test, business.industry, Infant, Newborn, High-Throughput Nucleotide Sequencing, Infant, Reproducibility of Results, Retrospective cohort study, Pedigree, Discontinuation, Phenotype, Child, Preschool, Karyotyping, Family medicine, Mutation, Female, business

Abstract

Reports of the use of whole-exome sequencing in clinical practice are limited. We report our experience with whole-exome sequencing in 115 patients in a single center and evaluate its feasibility and clinical usefulness in clinical care. Whole-exome sequencing was utilized based on the judgment of three clinical geneticists. We describe age, gender, ethnicity, consanguinity, indication for testing, family history, insurance, laboratory results, clinician interpretation of results, and impact on patient care. Most patients were children (78.9%). The most common indications for testing were birth defects (24.3%) and developmental delay (25.2%). We identified four new candidate human disease genes and possibly expanded the disease phenotypes associated with five different genes. Establishing a diagnosis led to discontinuation of additional planned testing in all patients, screening for additional manifestations in eight, altered management in fourteen, novel therapy in two, identification of other familial mutation carriers in five, and reproductive planning in six. Our results show that whole-exome sequencing is feasible, has clinical usefulness, and allows timely medical interventions, informed reproductive choices, and avoidance of additional testing. Our results also suggest phenotype expansion and identification of new candidate disease genes that would have been impossible to diagnose by other targeted testing methods. Genet Med 16 12, 922–931.

Published

2014

19. Tetratricopeptide Repeat Domain 7A (TTC7A) Mutation in a Newborn with Multiple Intestinal Atresia and Combined Immunodeficiency

Author

Lesley E. Northrop, Peter L. Nagy, Yesim Yilmaz Demirdag, Vimla S. Aggarwal, Niti Sardana Agarwal, and Kwame Anyane-Yeboa

Subjects

Adult, Male, Genotype, DNA Mutational Analysis, Molecular Sequence Data, Immunology, Intestinal Atresia, Mutation, Missense, Biology, Compound heterozygosity, Sepsis, medicine, Humans, Immunology and Allergy, Genetic Predisposition to Disease, In patient, Intestinal Mucosa, Gene, Immunodeficiency, Genetics, Polymorphism, Genetic, Base Sequence, Intestinal atresia, Infant, Newborn, Proteins, medicine.disease, Virology, Pedigree, Tetratricopeptide, Multiple intestinal atresia, Female, Severe Combined Immunodeficiency

Abstract

In the past year, two centers reported autosomal recessive mutations in tetratricopeptide repeat domain 7A (TTC7A) gene in patients with multiple intestinal atresia and immunodeficiency. Here, we present clinical progress of an infant with multiple intestinal atresia and combined immunodeficiency who carries novel compound heterozygote mutations in TTC7A gene.

Published

2014

20. Expanding the clinical and mutational spectrum of Kaufman oculocerebrofacial syndrome with biallelic UBE3B mutations

Author

Kwame Anyane-Yeboa, Patrick P. Koty, Wenqi Zeng, Christiane Zweier, Guntram Borck, Nils Rahner, Rüstem Yilmaz, Dorothy K. Grange, Heinrich Sticht, Lina Basel-Vanagaite, Nathalie Boddaert, Christian Kubisch, Heather Feenstra, Tamison Jewett, André Reis, Sha Tang, Megan Mortenson, Miriam S. Reuter, Julie Désir, and Kelly Gonzalez

Subjects

Adult, Male, Heterozygote, Adolescent, Ubiquitin-Protein Ligases, DNA Mutational Analysis, Limb Deformities, Congenital, Biology, medicine.disease_cause, Compound heterozygosity, Kaufman oculocerebrofacial syndrome, Intellectual Disability, Intellectual disability, Genetics, medicine, Humans, Missense mutation, Eye Abnormalities, Child, Genetics (clinical), Exome sequencing, Mutation, Homozygote, Facies, Infant, medicine.disease, Magnetic Resonance Imaging, Hypotonia, Cholesterol, Phenotype, Child, Preschool, Failure to thrive, Microcephaly, Female, medicine.symptom

Abstract

Biallelic mutations of UBE3B have recently been shown to cause Kaufman oculocerebrofacial syndrome (also reported as blepharophimosis-ptosis-intellectual disability syndrome), an autosomal recessive condition characterized by hypotonia, developmental delay, intellectual disability, congenital anomalies, characteristic facial dysmorphic features, and low cholesterol levels. To date, six patients with either missense mutations affecting the UBE3B HECT domain or truncating mutations have been described. Here, we report on the identification of homozygous or compound heterozygous UBE3B mutations in six additional patients from five unrelated families using either targeted UBE3B sequencing in individuals with suggestive facial dysmorphic features, or exome sequencing. Our results expand the clinical and mutational spectrum of the UBE3B-related disorder in several ways. First, we have identified UBE3B mutations in individuals who previously received distinct clinical diagnoses: two sibs with Toriello-Carey syndrome as well as the patient reported to have a "new" syndrome by Buntinx and Majewski in 1990. Second, we describe the adult phenotype and clinical variability of the syndrome. Third, we report on the first instance of homozygous missense alterations outside the HECT domain of UBE3B, observed in a patient with mildly dysmorphic facial features. We conclude that UBE3B mutations cause a clinically recognizable and possibly underdiagnosed syndrome characterized by distinct craniofacial features, hypotonia, failure to thrive, eye abnormalities, other congenital malformations, low cholesterol levels, and severe intellectual disability. We review the UBE3B-associated phenotypes, including forms that can mimick Toriello-Carey syndrome, and suggest the single designation "Kaufman oculocerebrofacial syndrome".

Published

2014

21. Megacystis-Microcolon-Intestinal Hypoperistalsis Syndrome: Case Report and Review of Prenatal Ultrasonographic Findings

Author

Russell Miller, Ashley Mills, Kwame Anyane-Yeboa, Kenneth Glassberg, and Lea Tuzovic

Subjects

Adult, Male, Embryology, medicine.medical_specialty, Amniotic fluid, Colon, Urinary Bladder, Prenatal diagnosis, Oligohydramnios, Ultrasonography, Prenatal, Pregnancy, Colon surgery, Fetal megacystis, medicine, Humans, Abnormalities, Multiple, Radiology, Nuclear Medicine and imaging, Obstetrics, business.industry, Intestinal Pseudo-Obstruction, Infant, Newborn, Obstetrics and Gynecology, General Medicine, Megacystis, Microcolon, medicine.disease, Pediatrics, Perinatology and Child Health, Female, Berdon syndrome, business

Abstract

Objective: To investigate prenatal ultrasonographic findings associated with megacystis-microcolon-intestinal hypoperistalsis syndrome (MMIHS). Methods: A PubMed search was performed using the terms ‘MMIHS', ‘MMIH' and ‘prenatal diagnosis'. Results: A total of 50 cases were analyzed. Prenatal diagnosis was achieved in 26% of cases. In 54% of patients with a correct antenatal diagnosis there was a previously affected sibling. Fetal megacystis with or without hydroureteronephrosis was the most common initial ultrasonographic finding (88%). While megacystis eventually complicated all fetal presentations, isolated bilateral hydronephrosis and isolated dilated stomach were noted (in 10 and 2% of cases, respectively) prior to megacystis. The initial sonographic abnormality was most commonly detected (in 70% of patients) in the second trimester. Amniotic fluid was normal in 69% and increased in 27% of cases. Gastrointestinal abnormalities were noted in 24% of pregnancies. Conclusion: MMIHS should be prenatally suspected when fetal megacystis is associated with a normal or increased amount of amniotic fluid and normal external genitalia, especially in the setting of a suggestive family history. Associated gastrointestinal findings support this diagnosis. Isolated bilateral hydronephrosis may precede the development of megacystis. Due to preserved renal function and a general absence of oligohydramnios, no rationale exists for vesicoamniotic shunt placement.

Published

2014

22. Phylloid terminal hair nevus: A unique clinical entity

Author

Christine T. Lauren, Maria C. Garzon, Nicole W. Kittler, Kwame Anyane-Yeboa, Tessa B. Scripps, and Nina K. Antonov

Subjects

medicine.medical_specialty, Dermoscopy, Dermatology, Terminal hair, Diagnosis, Differential, 030207 dermatology & venereal diseases, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Nevus, Skin, Hypopigmentation, integumentary system, Mosaicism, business.industry, Infant, Newborn, medicine.disease, 030220 oncology & carcinogenesis, Pediatrics, Perinatology and Child Health, Phylloid hypomelanosis, Female, medicine.symptom, business

Abstract

We present a case of an otherwise healthy infant with a localized patch of phylloid hypopigmentation bordered by terminal hairs on the back. We believe that this is a unique clinical entity and propose the term "phylloid terminal hair nevus." We believe that this is a localized form of phylloid hypomelanosis that is not associated with extracutaneous abnormalities.

Published

2018

23. Homozygous noncanonical splice variant in LSM1 in two siblings with multiple congenital anomalies and global developmental delay

Author

Charles A. LeDuc, Kwame Anyane-Yeboa, Zaheer Valivullah, Edwin Guzman, Wendy K. Chung, and Volkan Okur

Subjects

Research Report, Male, cupped ear, Triphalangeal thumb, Developmental Disabilities, RNA Stability, perimembranous ventricular septal defect, craniofacial asymmetry, Global developmental delay, congenital strabismus, Child, Genetics, 0303 health sciences, penile hypospadias, Homozygote, 030305 genetics & heredity, RNA-Binding Proteins, Exons, General Medicine, Phenotype, intellectual disability, moderate, RNA splicing, Knockout mouse, Female, Gene isoform, intermittent microsaccadic pursuits, bicuspid aortic valve, Adolescent, RNA Splicing, lumbar hemivertebrae, hydroureter, Biology, Congenital Abnormalities, 03 medical and health sciences, hydronephrosis, Proto-Oncogene Proteins, medicine, Animals, Humans, Abnormalities, Multiple, Gene, 030304 developmental biology, congenital mitral stenosis, Siblings, Alternative splicing, bilateral cryptorchidism, triphalangeal thumb, medicine.disease, moderate global developmental delay, primum atrial septal defect, inguinal hernia, Mutation

Abstract

Two siblings, one male and one female, ages 6 and 13 yr old, have similar clinical features of global developmental delay, multiple congenital anomalies affecting the cardiac, genitourinary, and skeletal systems, and abnormal eye movements. Whole-genome sequencing revealed a homozygous splice variant (NM_014462.3:c.231+4A>C) in LSM1 that segregated with the phenotype in the family. LSM1 has a role in pre-mRNA splicing and degradation. Expression studies revealed absence of expression of the canonical isoform in the affected individuals. The Lsm1 knockout mice have a partially overlapping phenotype that affects the brain, heart, and eye. To our knowledge, LSM1 has not been associated with any human disorder; however, the tissue expression pattern, gene constraint, and the similarity of the phenotype in our patients and the knockout mice models suggest it has a role in the development of multiple organ systems in humans.

Published

2019

24. Mutations in GMPPA Cause a Glycosylation Disorder Characterized by Intellectual Disability and Autonomic Dysfunction

Author

J. Christopher Hennings, Yoshinao Wada, Christian A. Hübner, Ingo Kurth, Thorsten Marquardt, Christine Coubes, Dieter Vanderschaeghe, Kwame Anyane-Yeboa, Dusica Babovic-Vuksanovic, Emile Van Schaftingen, Reinhard Mühlenberg, Pierre Sarda, Christian Beetz, Antje K. Huebner, Alma Sikiric, Janine Altmüller, Rizwan Mumtaz, Jürgen Brämswig, Avraham Zeharia, Ammi Grahn, Peter Nürnberg, Arsalan Ahmad, Meera Malik, Guntram Borck, Saqib Mahmood, Katrin Koehler, Holger Thiele, Sebastian Gießelmann, Gudrun Nürnberg, Angela Huebner, Janine Reunert, and Lina Basel-Vanagaite

Subjects

Adult, Guanosine Diphosphate Mannose, medicine.medical_specialty, Glycosylation, Adolescent, Nonsense mutation, Genes, Recessive, Consanguinity, Triple-A syndrome, Biology, Alacrima, Young Adult, chemistry.chemical_compound, Report, Intellectual Disability, Internal medicine, Intellectual disability, Genetics, medicine, Adrenal insufficiency, Humans, Genetics(clinical), Child, Genetics (clinical), Lacrimal Apparatus Diseases, Homozygote, Eye Diseases, Hereditary, medicine.disease, Nucleotidyltransferases, Pedigree, Esophageal Achalasia, Endocrinology, chemistry, Codon, Nonsense, Nervous System Diseases, Guanosine diphosphate mannose, Adrenal Insufficiency

Abstract

In guanosine diphosphate (GDP)-mannose pyrophosphorylase A (GMPPA), we identified a homozygous nonsense mutation that segregated with achalasia and alacrima, delayed developmental milestones, and gait abnormalities in a consanguineous Pakistani pedigree. Mutations in GMPPA were subsequently found in ten additional individuals from eight independent families affected by the combination of achalasia, alacrima, and neurological deficits. This autosomal-recessive disorder shows many similarities with triple A syndrome, which is characterized by achalasia, alacrima, and variable neurological deficits in combination with adrenal insufficiency. GMPPA is a largely uncharacterized homolog of GMPPB. GMPPB catalyzes the formation of GDP-mannose, which is an essential precursor of glycan moieties of glycoproteins and glycolipids and is associated with congenital and limb-girdle muscular dystrophies with hypoglycosylation of α-dystroglycan. Surprisingly, GDP-mannose pyrophosphorylase activity was unchanged and GDP-mannose levels were strongly increased in lymphoblasts of individuals with GMPPA mutations. This suggests that GMPPA might serve as a GMPPB regulatory subunit mediating feedback inhibition of GMPPB instead of displaying catalytic enzyme activity itself. Thus, a triple-A-like syndrome can be added to the growing list of congenital disorders of glycosylation, in which dysregulation rather than mere enzyme deficiency is the basal pathophysiological mechanism.

Published

2013

25. Phenotypic Heterogeneity of Neutropenia and Gastrointestinal Illness Associated with G6PC3 Founder Mutation

Author

Kara Gross Margolis, Sivan Kinberg, Alejandro Iglesias, Evelyn Rustia, Chana L. Glasser, Joseph A. Picoraro, Preti Jain, Kwame Anyane-Yeboa, and Nancy S. Green

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Neutropenia, Adolescent, Gastrointestinal Diseases, G6PC3, Intermittent thrombocytopenia, macromolecular substances, Gene mutation, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, Internal medicine, Granulocyte Colony-Stimulating Factor, medicine, Congenital Bone Marrow Failure Syndromes, Humans, Congenital Neutropenia, Child, Genetic heterogeneity, Prominent superficial veins, business.industry, Hematology, medicine.disease, Failure to Thrive, 030104 developmental biology, Phenotype, nervous system, Oncology, 030220 oncology & carcinogenesis, Child, Preschool, Pediatrics, Perinatology and Child Health, Failure to thrive, Mutation, Glucose-6-Phosphatase, medicine.symptom, business

Abstract

Severe congenital neutropenia type IV (SCN IV) is a syndrome of severe neutropenia, cardiac and urogenital defects, prominent superficial veins, facial dysmorphism, failure to thrive (FTT), and intermittent thrombocytopenia, caused by a glucose-6-phosphatase catalytic subunit 3 (G6PC3) gene mutation. SCN IV has been linked to glycogen storage disease type 1b as both disorders involve disruption of the glucose-6-phosphatase/glucose-6-phosphate transporter complex, leading to arrested neutrophil maturation. Emerging evidence suggests that neutrophil function plays an important role in intestinal integrity, evidenced by inflammatory bowel disease in certain neutropenic patients. Here, we report 3 unrelated Hispanic males from the Dominican Republic with classic features of SCN IV found to share an identical inherited canonical splice-site mutation of the G6PC3 gene (c.218+1GA). All 3 patients presented with severe FTT and gastrointestinal manifestations. Two of the patients had significant improvement in growth and resolution of gastrointestional symptoms with initiation of granulocyte colony-stimulating factor. We hypothesize that the gene variant described represents a founder mutation in the Dominican Republic, the first to be described in this geographical region. We discuss the potential associations between neutropenia and gastrointestinal disease with FTT and the role of granulocyte colony-stimulating factor in improving neutrophil count and intestinal integrity and growth.

Published

2016

26. The expanding clinical phenotype of Bosch-Boonstra-Schaaf optic atrophy syndrome: 20 new cases and possible genotype-phenotype correlations

Author

Kwame Anyane-Yeboa, Juan M. Pascual, Ganka Douglas, Kristin G. Monaghan, Fuki M. Hisama, Frans P.M. Cremers, Timothy J. Moss, Laurence E. Walsh, Marwan Shinawi, Jill A. Rosenfeld, Elfrida Malkin, Jane Juusola, Keri Ramsey, Parul Jayakar, Fran Kendall, John Mann, Wendy K. Chung, Daniëlle G.M. Bosch, Christian P. Schaaf, Cheri Schoonveld, Dianalee McKnight, Chun-An Chen, Bert B.A. de Vries, Dmitriy Niyazov, Katelyn Payne, F. Nienke Boonstra, Magdalena Walkiewicz, Megan T. Cho, Richard A. Lewis, Frances Elmslie, Vivekanand Veluchamy, Chumei Li, Gabriele Richard, Allison Schreiber, and Francisca Millan

Subjects

Adult, Male, 0301 basic medicine, Nonsynonymous substitution, Adolescent, Autism Spectrum Disorder, Mutation, Missense, Biology, medicine.disease_cause, Corpus callosum, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], 03 medical and health sciences, 0302 clinical medicine, Atrophy, medicine, Humans, Missense mutation, Child, Genetic Association Studies, Genetics (clinical), Genetics, Mutation, COUP Transcription Factor I, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], medicine.disease, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Phenotype, Hypotonia, Pedigree, Optic Atrophy, 030104 developmental biology, Autism spectrum disorder, Child, Preschool, Female, medicine.symptom, Gene Deletion, 030217 neurology & neurosurgery

Abstract

Item does not contain fulltext PURPOSE: Bosch-Boonstra-Schaaf optic atrophy syndrome (BBSOAS) is an autosomal-dominant disorder characterized by optic atrophy and intellectual disability caused by loss-of-function mutations in NR2F1. We report 20 new individuals with BBSOAS, exploring the spectrum of clinical phenotypes and assessing potential genotype-phenotype correlations. METHODS: Clinical features of individuals with pathogenic NR2F1 variants were evaluated by review of medical records. The functional relevance of coding nonsynonymous NR2F1 variants was assessed with a luciferase assay measuring the impact on transcriptional activity. The effects of two start codon variants on protein expression were evaluated by western blot analysis. RESULTS: We recruited 20 individuals with novel pathogenic NR2F1 variants (seven missense variants, five translation initiation variants, two frameshifting insertions/deletions, one nonframeshifting insertion/deletion, and five whole-gene deletions). All the missense variants were found to impair transcriptional activity. In addition to visual and cognitive deficits, individuals with BBSOAS manifested hypotonia (75%), seizures (40%), autism spectrum disorder (35%), oromotor dysfunction (60%), thinning of the corpus callosum (53%), and hearing defects (20%). CONCLUSION: BBSOAS encompasses a broad range of clinical phenotypes. Functional studies help determine the severity of novel NR2F1 variants. Some genotype-phenotype correlations seem to exist, with missense mutations in the DNA-binding domain causing the most severe phenotypes.Genet Med 18 11, 1143-1150.

Published

2016

27. Mutation abolishing the ZMPSTE24 cleavage site in prelamin A causes a progeroid disorder

Author

Gregg G. Gundersen, Kwame Anyane-Yeboa, Yuexia Wang, Howard J. Worman, Jonathan T. Lu, Ji-Yeon Shin, Uta Lichter-Konecki, Peter L. Nagy, Cecilia Östlund, Jessica E. Shaw, and Lorraine N. Clark

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Arginine, Protein Prenylation, Short Report, Biology, LMNA, 03 medical and health sciences, Progeria, medicine, Humans, Genetic Predisposition to Disease, Gene, Genetics, integumentary system, Farnesyltransferase inhibitor, High-Throughput Nucleotide Sequencing, Membrane Proteins, Metalloendopeptidases, nutritional and metabolic diseases, Cell Biology, Fibroblasts, Lamin Type A, medicine.disease, Cell biology, 030104 developmental biology, Amino Acid Substitution, Membrane protein, Mutation, Protein prenylation, Female, Lamin

Abstract

In 1994 in the Journal of Cell Science, Hennekes and Nigg reported that changing valine to arginine at the endoproteolytic cleavage site in chicken prelamin A abolishes its conversion to lamin A. The consequences of this mutation in an organism have remained unknown. We now report that the corresponding mutation in a human subject leads to accumulation of prelamin A and causes a progeroid disorder. Next generation sequencing of the subject and her parents' exomes identified a de novo mutation in the lamin A/C gene (LMNA) that resulted in a leucine to arginine amino acid substitution at residue 647 in prelamin A. The subject's fibroblasts accumulated prelamin A, a farnesylated protein, which led to an increased percentage of cultured cells with morphologically abnormal nuclei. Treatment with a protein farnesyltransferase inhibitor improved abnormal nuclear morphology. This case demonstrates that accumulation of prelamin A, independent of the loss of function of ZMPSTE24 metallopeptidase that catalyzes processing of prelamin A, can cause a progeroid disorder and that a cell biology assay could be used in precision medicine to identify a potential therapy.

Published

2016

28. A Novel Mutation Causing Pseudohypoparathyroidism 1A with Congenital Hypothyroidism and Osteoma Cutis

Author

Maria Garzon, Kwame Anyane Yeboa, Bina Shah, and Tamar Lubell

Subjects

Male, medicine.medical_specialty, Pseudohypoaldosteronism, Endocrinology, Diabetes and Metabolism, Parathyroid hormone, Bone Neoplasms, Case Reports, Short stature, Frameshift mutation, Endocrinology, Internal medicine, Chromogranins, GTP-Binding Protein alpha Subunits, Gs, Humans, Medicine, Osteoma cutis, Frameshift Mutation, Pseudohypoparathyroidism, Psychomotor retardation, business.industry, Brachydactyly, congenital hypothyroidism, Calcinosis, Osteoma, medicine.disease, Congenital hypothyroidism, osteoma cutis, Child, Preschool, Pediatrics, Perinatology and Child Health, medicine.symptom, business

Abstract

Various inactivating mutations in guanine nucleotide−binding protein, alpha−stimulating activity polypeptide1 (GNAS1) gene have been described with poor phenotype correlation. Pseudohypoparathyroidism type 1a (PHP1a) results from an inactivating mutation in the GNAS1 gene. Hormone resistance occurs not only to parathyroid hormone (PTH), but typically also to other hormones which signal via G protein coupled receptors including thyroid stimulating hormone (TSH), gonadotropins, and growth hormone releasing hormone. In addition, the phenotype of Albright hereditary osteodystrophy (AHO) is observed, which may include short stature, round facies, brachydactyly, obesity, ectopic soft tissue or dermal ossification (osteoma cutis) and psychomotor retardation with variable expression. We present a 2−year−old boy with PHP 1A who initially presented at age 3 weeks with congenital hypothyroidism. By 17 months of age, he manifested osteoma cutis, psychomotor retardation, obesity, brachydactyly and resistance to PTH with normocalcemia and mild hyperphosphatemia. Genetic analysis revealed a novel mutation in exon 13 of GNAS1 in our patient. This mutation, c.1100_1101insA, resulted in a frameshift and premature truncation of bases downstream. This mutation was also found in the mother of this patient who was also noted to have short stature, obesity, brachydactyly and non progressive osteoma cutis, but no hormone resistance. We report a novel heterozygous mutation causing PHP1A with PTH and TSH resistance and AHO which has not been described previously. PHP1A is also a rare presentation of congenital hypothyroidism. Conflict of interest:None declared.

Published

2009

29. Congenital hypothyroidism and thyroid dyshormonogenesis: a case report of siblings with a newly identified mutation in thyroperoxidase

Author

Kendra Fabian, Vaidehi Jobanputra, David P. Sparling, Sharon E. Oberfield, Kwame Anyane-Yeboa, Ilene Fennoy, and Lara Harik

Subjects

0301 basic medicine, Male, endocrine system, Pathology, medicine.medical_specialty, Pediatrics, Thyroid Hormones, Goiter, endocrine system diseases, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Thyroid Gland, 030209 endocrinology & metabolism, Autoantigens, Iodide Peroxidase, Article, Frameshift mutation, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Thyroid dyshormonogenesis, Thyroid peroxidase, Iron-Binding Proteins, medicine, Congenital Hypothyroidism, Humans, Thyroid cancer, Exome sequencing, biology, business.industry, Siblings, Thyroidectomy, Infant, Newborn, medicine.disease, Prognosis, Congenital hypothyroidism, 030104 developmental biology, Pediatrics, Perinatology and Child Health, Mutation, biology.protein, business

Abstract

Thyroid dyshormonogenesis continues to be a significant cause of congenital hypothyroidism. Over time, forms of thyroid dyshormonogenesis can result in goiter, which can lead to difficult management decisions as the pathologic changes can both mimic or lead to thyroid cancer.Herein we describe the cases of two brothers diagnosed with congenital hypothyroidism, with initial findings consistent with thyroid dyshormonogenesis. One brother eventually developed multinodular goiter with complex pathology on biopsy, resulting in thyroidectomy.Whole exome sequencing revealed the brothers carry a novel frameshift mutation in thyroperoxidase; the mutation, while not previously described, was likely both deleterious and pathogenic.These cases highlight the complex pathology that can occur within thyroid dyshormonogenesis, with similar appearance to possible thyroid cancer, leading to complex management decisions. They also highlight the role that a genetic diagnosis can play in interpreting the impact of dyshormonogenesis on nodular thyroid development, and the need for long-term follow-up in these patients.

Published

2015

30. Bohring-Opitz syndrome (BOS) with a new ASXL1 pathogenic variant: Review of the most prevalent molecular and phenotypic features of the syndrome

Author

Kwame Anyane-Yeboa, Ashley Wilson, Vaidehi Jobanputra, and Silvana Beatriz Dangiolo

Subjects

Adult, medicine.medical_specialty, Adolescent, Nonsense mutation, Bioinformatics, Frameshift mutation, Craniosynostoses, Intellectual Disability, Genetics, Medicine, Humans, Abnormalities, Multiple, Exome, Hypertelorism, Frameshift Mutation, Genetics (clinical), Exome sequencing, business.industry, High-Throughput Nucleotide Sequencing, medicine.disease, Prognosis, Repressor Proteins, Failure to thrive, Pancreatitis, Medical genetics, Female, medicine.symptom, business, Bohring–Opitz syndrome

Abstract

Bohring-Opitz syndrome (BOS) was first described by Bohring et al. [1999]. The authors reported four cases which had several features in common, including a prominent metopic suture, hypertelorism, exophthalmos, cleft lip and palate, limb anomalies, as well as difficulty feeding with severe developmental delays. In almost 50% of cases that meet the clinical criteria for BOS, de novo frameshift and nonsense mutations in the ASXL1 gene have been detected, suggesting that loss of function of this gene is a major cause. We report on the clinical characterization of one young female patient who was evaluated because of severe developmental delays, failure to thrive, and multiple minor anomalies and was clinically diagnosed with BOS. Whole exome sequencing analysis detected one novel disruptive frameshift mutation in the ASXL1 gene and we were also able to confirm the presence of two CFTR mutations associated with her chronic pancreatitis with acute severe breakthrough attacks requiring multiple ICU admissions. This latter complication of pancreatitis further contributed to the complexity of the clinical presentation and represents an independent genetic finding. Our case report emphasizes the importance of highly specific phenotypic characterization of patients with complex phenotypes before proceeding with molecular studies. That approach will lead to more accurate molecular data interpretation and better clinical genetic diagnosis, particularly for those patients with rare, difficult-to-diagnose disorders.

Published

2015

31. FTO variant associated with malformation syndrome

Author

Mythily Ganapathi, Megan T. Cho, Luis Rohena, Michelle Lawson, Kwame Anyane-Yeboa, Edwin Guzman, and Eden Haverfield

Subjects

0301 basic medicine, Male, medicine.medical_specialty, endocrine system diseases, Alpha-Ketoglutarate-Dependent Dioxygenase FTO, Biology, medicine.disease_cause, Craniosynostosis, 03 medical and health sciences, Internal medicine, Genetics, medicine, Humans, Abnormalities, Multiple, Functional studies, Allele, Genetics (clinical), Exome sequencing, Alleles, Mutation, Homozygote, nutritional and metabolic diseases, Brain, Genetic Variation, Infant, pathological conditions, signs and symptoms, Syndrome, medicine.disease, Phenotype, Eye abnormality, 030104 developmental biology, Endocrinology, Female, Tomography, X-Ray Computed

Abstract

Common FTO variants are associated with obesity. However, it has recently been shown that homozygous FTO c.947G>A variant, which predicts p.R316Q, and c.956C>T, which predicts p.S319F, are associated with a malformation syndrome inherited in an autosomal recessive pattern. We present a similar homozygous FTO c.965G>A variant that predicts p.R322Q, associated with a lethal malformation syndrome in a consanguineous Yemeni family. Functional studies showed that the p.R316Q, p.S219F, and p.R322Q variants render the FTO protein inactive. We further expand on the phenotype of homozygous FTO loss-of-function mutations to include eye abnormalities, gingival overgrowth, craniosynostosis, and cutaneous photosensitivity.

Published

2015

32. Cutis Verticis Gyrata in a Patient with Noonan Syndrome

Author

Kwame Anyane-Yeboa, Lindy P. Fox, Adam S. Geyer, and Maria C. Garzon

Subjects

musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Pathology, medicine.medical_specialty, animal structures, Cutis, Dermatology, Skin Diseases, Turner syndrome, medicine, Edema, Exophthalmos, Humans, Abnormalities, Multiple, cardiovascular diseases, skin and connective tissue diseases, Scalp, Heart Murmurs, Hypertelorism, business.industry, Noonan Syndrome, Infant, Newborn, Ear, medicine.disease, Osteochondrodysplasia, Recien nacido, Pediatrics, Perinatology and Child Health, Muscle Hypotonia, Noonan syndrome, Female, Cutis verticis gyrata, Congenital disease, business

Abstract

We report cutis verticis gyrata in a patient with Noonan syndrome. While cutis vertices gyrata has been shown to have a strong association with chromosomal abnormalities, especially Turner syndrome, this infant represents only the second reported instance of cutis verticis gyrata occurring in a patient with Noonan syndrome.

Published

2005

33. NEUROPSYCHOLOGICAL CHARACTERISTICS OF CHILDREN WITH THE 22Q11 DELETION SYNDROME: A DESCRIPTIVE ANALYSIS

Author

Maria Karayiorgou, Christina Sobin, Kwame Anyane-Yeboa, Karen Kiley-Brabeck, Lisa Taylor, Maude L. Blundell, Sarah Daniels, and Jananne Khuri

Subjects

Male, medicine.medical_specialty, Neuropsychological function, Chromosomes, Human, Pair 22, Stanford-Binet Test, Audiology, Severity of Illness Index, Article, Developmental psychology, 22q11 Deletion Syndrome, DiGeorge Syndrome, Developmental and Educational Psychology, medicine, Humans, Cognitive skill, Child, Memory Disorders, Descriptive statistics, Working memory, Neuropsychology, Brain, Neuropsychology and Physiological Psychology, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, Verbal memory, Cognition Disorders, Psychology, Neurocognitive, Gene Deletion, Follow-Up Studies

Abstract

Previous reports of cognitive functioning in children with the 22q11 Deletion Syndrome have reported marked variability in IQ and achievement subtest scores. Studies have begun to explore neuropsychological function in 22q11 DS however results are inconsistent and the profile incomplete. We assessed 40 children ages 5–12 with 22q11 DS. Consistent with past results, visual-spatial memory was significantly lower than verbal memory. Differentially lowered scores were found only in visual attention, working memory and motor function. Contrary with some past results quantitative, verbal ability, and visual spatial memory scores were within 1 SD from the standardization sample mean. Motor behavior, not typically discussed with regard to 22q11 DS school-age children, may be critical to incorporate in neurocognitive studies of children with 22q11 DS. Implications of these findings are considered with regard to past results.

Published

2005

34. Networks of Attention in Children With the 22q11 Deletion Syndrome

Author

Maude L. Blundell, Karen Kiley-Brabeck, Kwame Anyane-Yeboa, Maria Karayiorgou, Christina Sobin, and Sarah Daniels

Subjects

Male, medicine.medical_specialty, Chromosomes, Human, Pair 22, Population, Neuropsychological Tests, Audiology, Article, Developmental psychology, 22q11 Deletion Syndrome, Reaction Time, Developmental and Educational Psychology, medicine, Humans, Attention, Child, education, Analysis of Variance, education.field_of_study, Learning Disabilities, Siblings, Cognitive disorder, Neuropsychology, medicine.disease, Cross-Sectional Studies, Neuropsychology and Physiological Psychology, Chromosomal deletion syndrome, El Niño, Child, Preschool, Female, Analysis of variance, Chromosome Deletion, Cues, Psychology, Neurocognitive

Abstract

The 22q11 chromosomal deletion syndrome (22q11 DS) is associated with learning disabilities and a complex neuropsychological profile. Previous findings have suggested that executive attention deficits might underlie other neurocognitive anomalies. We administered the child Attention Network Test (ANT) to 52 children ages 5.0 to 11.5, 32 22q11 DS children (19 girls) and 20 controls (13 girls) and assessed the efficiency of segregated executive, orienting, and alerting networks. We hypothesized that 22q11 DS children have impaired executive network efficiency as compared to control siblings. The internal validity of the child ANT was confirmed for this population. Analysis of variance results showed significant main effects for flanker and cue types and no interaction effect in either 22q11 DS children or control siblings. Compared to control siblings, 22q11 DS children had significantly larger (less efficient) executive network scores, significantly increased errors on only incongruent trials, and a significant correlation between executive network scores and accuracy. The implications of these findings for future neurocognitive studies of 22q11 DS children are considered.

Published

2004

35. Homozygosity for Multiple Contiguous Single-Nucleotide Polymorphisms as an Indicator of Large Heterozygous Deletions: Identification of a Novel Heterozygous 8-kb Intragenic Deletion (IVS7–19 to IVS15–17) in a Patient with Glycogen Storage Disease Type II

Author

Edwin Guzman, Maryann L. Huie, Rochelle Hirschhorn, and Kwame Anyane-Yeboa

Subjects

Heterozygote, Sequence analysis, Molecular Sequence Data, Single-nucleotide polymorphism, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, law.invention, Loss of heterozygosity, 03 medical and health sciences, Exon, 0302 clinical medicine, law, Report, Glycogen storage disease type II, medicine, El Salvador, Genetics, Humans, Genetics(clinical), Amino Acid Sequence, Genetics (clinical), Polymerase chain reaction, 030304 developmental biology, Sequence Deletion, 0303 health sciences, Mutation, Base Sequence, Glycogen Storage Disease Type II, Homozygote, alpha-Glucosidases, Exons, medicine.disease, Molecular biology, Introns, 3. Good health, genomic DNA, Glucan 1,4-alpha-Glucosidase, 030217 neurology & neurosurgery

Abstract

Current methods for detection of mutations by polymerase chain reaction (PCR) and sequence analysis frequently are not able to detect heterozygous large deletions. We report the successful use of a novel approach to identify such deletions, based on detection of apparent homozygosity of contiguous single-nucleotide polymorphisms (SNPs). The sequence analysis of genomic DNA PCR products containing all coding exons and flanking introns identified only a single heterozygous mutation (IVS18+2t--a) in a patient with classic infantile-onset autosomal recessive glycogen storage disease type II (GSDII). Apparent homozygosity for multiple contiguous SNPs detected by this sequencing suggested presence of a large deletion as the second mutation; primers flanking the region of homozygous SNPs permitted identification and characterization by PCR of a large genomic deletion (8.26 kb) extending from IVS7 to IVS15. The data clearly demonstrate the utility of SNPs as markers for large deletions in autosomal recessive diseases when only a single mutation is found, thus complementing currently standard DNA PCR sequence methods for identifying the molecular basis of disease.

Published

2002

36. Identification of six novel mutations in the acid alpha-glucosidase gene in three Spanish patients with infantile onset glycogen storage disease type II (Pompe disease)

Author

Rochelle Hirschhorn, Carmen Navarro, Roberto Fernandez-Hojas, Maryann L. Huie, Carmen Domínguez, Manuel Roig, Kwame Anyane-Yeboa, Diana Lopez-Coronas, and Susana Teijeira

Subjects

Male, Nonsense mutation, Muscle disorder, Biology, medicine.disease_cause, chemistry.chemical_compound, Glycogen storage disease type II, medicine, Animals, Humans, Missense mutation, Amino Acid Sequence, Age of Onset, Genetics (clinical), Genetics, Mutation, Splice site mutation, Base Sequence, Glycogen, Glycogen Storage Disease Type II, alpha-Glucosidases, Exons, medicine.disease, Alternative Splicing, Amino Acid Substitution, Neurology, chemistry, Spain, Pediatrics, Perinatology and Child Health, Acid alpha-glucosidase, Female, Neurology (clinical), Lysosomes, Sequence Alignment

Abstract

Glycogen storage disease type II is an autosomal recessive muscle disorder due to deficiency of lysosomal acid α-glucosidase and the resulting intralysosomal accumulation of glycogen. We found six novel mutations in three Spanish classic infantile onset glycogen storage disease type II patients with involvement of both cardiac and skeletal muscle; three missense mutations (G219R, E262K, M408V), a nonsense mutation (Y191X), a donor splice site mutation (IVS18 +2gt>ga) and an in frame deletion of an asparagine residue (nt1408–1410). The missense mutations were not found in 100 normal chromosomes and therefore are not normal polymorphic variants. The splice site mutation was subsequently detected in an additional ‘Spanish’ infantile onset glycogen storage disease type II patient from El Salvador. Further studies will be required to determine if the IVS18 +2gt>ga splice site mutation might in fact be a relatively common Spanish mutation. Mutations among Spanish glycogen storage disease type II patients appear to be genetically heterogeneous and differ from common mutations in neighboring countries.

Published

2002

37. New Insights into the Genetics of Fetal Megacystis: ACTG2 Mutations, Encoding γ-2 Smooth Muscle Actin in Megacystis Microcolon Intestinal Hypoperistalsis Syndrome (Berdon Syndrome)

Author

Lea, Tuzovic, Sha, Tang, Russell S, Miller, Luis, Rohena, Layla, Shahmirzadi, Kelly, Gonzalez, Xiang, Li, Charles A, LeDuc, Jiancheng, Guo, Ashley, Wilson, Ashley, Mills, Kenneth, Glassberg, Heidi, Rotterdam, Antonia R, Sepulveda, Wenqi, Zeng, Wendy K, Chung, and Kwame, Anyane-Yeboa

Subjects

Adult, Male, Colon, Duodenum, DNA Mutational Analysis, Intestinal Pseudo-Obstruction, Molecular Sequence Data, Urinary Bladder, Mutation, Missense, Actins, Fetal Diseases, Pregnancy, Prenatal Diagnosis, Intestine, Small, Humans, Abnormalities, Multiple, Female, Sequence Alignment, Ultrasonography

Abstract

To identify the molecular basis for prenatally suspected cases of megacystis microcolon intestinal hypoperistalsis syndrome (MMIHS) (MIM 249210) in 3 independent families with clinical and radiographic evidence of MMIHS.Whole-exome sequencing (WES) and Sanger sequencing of the ACTG2 gene.We identified a novel heterozygous de novo missense variant in ACTG2 c.770GA (p.Arg257His) encoding x03B3;-2 smooth muscle actin (ACTG2) in 2 siblings with MMIHS, suggesting gonadal mosaicism of one of the parents. Two additional de novo missense variants (p.Arg257Cys and p.Arg178His) in ACTG2 were identified in 2 additional MMHIS patients. All of our patients had evidence of fetal megacystis and a normal or slightly increased amniotic fluid volume. Additional findings included bilateral renal hydronephrosis, an enlarged fetal stomach, and transient dilated bowel loops. ACTG2 immunostaining of the intestinal tissue showed an altered muscularis propria, a markedly thinned longitudinal muscle layer, and a reduced amount and abnormal distribution of ACTG2.Our study demonstrates that de novo mutations in ACTG2 are a cause of fetal megacystis in MMIHS and that gonadal mosaicism may be present in a subset of cases. These findings have implications for the counseling of families with a diagnosis of fetal megacystis with a preserved amniotic fluid volume and associated gastrointestinal findings.

Published

2014

38. Mutations in the Cholesterol Transporter Gene ABCA5 Are Associated with Excessive Hair Overgrowth

Author

Heather Feenstra, Kwame Anyane-Yeboa, Anna Vitebsky, Mazen Kurban, Marija Tadin-Strapps, Antonio Sobrino, Claudia Dall'Armi, Angela M. Christiano, Luis Rohena, Julio C. Salas-Alanis, Maija Ht Kiuru, Nanette B. Silverberg, Gina M. DeStefano, Katherine A. Fantauzzo, Larissa D. López-Cepeda, Brynn Levy, Gilbert Di Paolo, Vaidehi Jobanputra, Dorothy Warburton, and Schmidt-Ullrich, Ruth

Subjects

Hypertrichosis, Keratinocytes, Cancer Research, Heredity, Gene Expression, medicine.disease_cause, 2.1 Biological and endogenous factors, Aetiology, Child, Genetics (clinical), Sequence Deletion, Pediatric, Mutation, Genetic Diseases, X-Linked, Phenotype, Pedigree, medicine.anatomical_structure, Cholesterol, Genetic Diseases, Child, Preschool, RNA splicing, Female, Chromosome Deletion, Genetic Engineering, Research Article, Biotechnology, lcsh:QH426-470, RNA Splicing, Biology, Molecular Genetics, Cytogenetics, Clinical Research, Lysosome, medicine, Genetics, Humans, Preschool, Molecular Biology, Gene, Ecology, Evolution, Behavior and Systematics, Point mutation, Neurosciences, Intron, Biology and Life Sciences, Infant, Human Genetics, X-Linked, Mutation (Biology), medicine.disease, Molecular biology, lcsh:Genetics, FOS: Biological sciences, Genetics of Disease, Congenital Structural Anomalies, ATP-Binding Cassette Transporters, Developmental Biology, Hair

Abstract

Inherited hypertrichoses are rare syndromes characterized by excessive hair growth that does not result from androgen stimulation, and are often associated with additional congenital abnormalities. In this study, we investigated the genetic defect in a case of autosomal recessive congenital generalized hypertrichosis terminalis (CGHT) (OMIM135400) using whole-exome sequencing. We identified a single base pair substitution in the 5′ donor splice site of intron 32 in the ABC lipid transporter gene ABCA5 that leads to aberrant splicing of the transcript and a decrease in protein levels throughout patient hair follicles. The homozygous recessive disruption of ABCA5 leads to reduced lysosome function, which results in an accumulation of autophagosomes, autophagosomal cargos as well as increased endolysosomal cholesterol in CGHT keratinocytes. In an unrelated sporadic case of CGHT, we identified a 1.3 Mb cryptic deletion of chr17q24.2-q24.3 encompassing ABCA5 and found that ABCA5 levels are dramatically reduced throughout patient hair follicles. Collectively, our findings support ABCA5 as a gene underlying the CGHT phenotype and suggest a novel, previously unrecognized role for this gene in regulating hair growth., Author Summary Inherited hypertrichoses represent a group of hair overgrowth syndromes that are extremely rare in humans and have remained an area of great interest to evolutionary geneticists since they are considered to be recurrences of an ancestral phenotype. These syndromes often present with additional congenital abnormalities including bone, heart and dental defects; thus, it is crucial to identify the mechanisms and genes underlying the pathology. Copy number variants (CNVs) have previously been reported in several cases of congenital generalized hypertrichosis terminalis (CGHT) with a minimal overlapping region of 555 kb encompassing four genes. However, no point mutations in these or any other single genes have been described to underlie the CGHT phenotype. In this study, we report the first loss-of-function mutation in an ABC transporter, ABCA5 and identified an additional copy number variant in a separate case that lies within the minimal common region. We found high levels of ABCA5 expression in both epithelial and mesenchymal compartments of human and mouse hair follicles, and in CGHT patients, this expression is significantly reduced or completely lost. ABCA5 is a lysosomal protein, and its loss-of-function compromises the integrity of lysosomes and leads to an intra-endolysosomal accumulation of cholesterol. Importantly, our findings support a novel role for ABCA5 in regulating hair growth.

Published

2014

39. Molecular Definition of 22q11 Deletions in 151 Velo-Cardio-Facial Syndrome Patients

Author

Raj K. Pandita, C. Carlson, H. Sirotkin, Raju Kucherlapati, Kwame Anyane-Yeboa, Bernice E. Morrow, Sherman M. Weissman, Sankhavaram R. Patanjali, J McKie, Rosalie Goldberg, Robert J. Shprintzen, R Wadey, Peter J. Scambler, and D. Warburton

Subjects

Genetic Markers, Heart Defects, Congenital, Genotype, Chromosomes, Human, Pair 22, Chromosome Breakpoints, Chromosome Disorders, Biology, Hybrid Cells, Craniofacial Abnormalities, Gene mapping, DiGeorge syndrome, medicine, Genetics, Humans, Abnormalities, Multiple, Genetics(clinical), RNA, Messenger, Genetics (clinical), Sequence Tagged Sites, Chromosome Aberrations, Expressed sequence tag, Haplotype, Chromosome Mapping, Low copy repeats, Syndrome, medicine.disease, Cleft Palate, Phenotype, Chromosome Deletion, Haploinsufficiency, Chromosome 22, Research Article

Abstract

Velo-cardio-facial syndrome (VCFS) is a relatively common developmental disorder characterized by craniofacial anomalies and conotruncal heart defects. Many VCFS patients have hemizygous deletions for a part of 22q11, suggesting that haploinsufficiency in this region is responsible for its etiology. Because most cases of VCFS are sporadic, portions of 22q11 may be prone to rearrangement. To understand the molecular basis for chromosomal deletions, we defined the extent of the deletion, by genotyping 151 VCFS patients and performing haplotype analysis on 105, using 15 consecutive polymorphic markers in 22q11. We found that 83% had a deletion and >90% of these had a similar approximately 3 Mb deletion, suggesting that sequences flanking the common breakpoints are susceptible to rearrangement. We found no correlation between the presence or size of the deletion and the phenotype. To further define the chromosomal breakpoints among the VCFS patients, we developed somatic hybrid cell lines from a set of VCFS patients. An 11-kb resolution physical map of a 1,080-kb region that includes deletion breakpoints was constructed, incorporating genes and expressed sequence tags (ESTs) isolated by the hybridization selection method. The ordered markers were used to examine the two separated copies of chromosome 22 in the somatic hybrid cell lines. In some cases, we were able to map the chromosome breakpoints within a single cosmid. A 480-kb critical region for VCFS has been delineated, including the genes for GSCL, CTP, CLTD, HIRA, and TMVCF, as well as a number of novel ordered ESTs.

Published

1997

40. Lumbar gibbus in storage diseases and bone dysplasias

Author

Walter E. Berdon, Ralph S. Lachman, Terry L. Levin, Kwame Anyane-Yeboa, Carrie Ruzal-Shapiro, and David P. Roye

Subjects

medicine.medical_specialty, Lumbar Vertebrae, biology, business.industry, Mucopolysaccharidosis, Gibbus, Mucopolysaccharidoses, biology.organism_classification, medicine.disease, Magnetic Resonance Imaging, Osteochondrodysplasia, Achondroplasia, Surgery, Dysplasia, Pediatrics, Perinatology and Child Health, Orthopedic surgery, medicine, Etiology, Humans, Radiology, Nuclear Medicine and imaging, Kyphosis, Child, business, Neuroradiology

Abstract

Objective. The objective of this study was to review the problem of lumbar gibbus in children with storage diseases and bone dysplasias utilizing plain films and MR imaging. Materials and methods. Clinical histories and radiographic images in five patients with storage diseases [four mucopolysaccharidosis (MPS) and one mucolipidosis] and two with achondroplasia were reviewed. The International Skeletal Dysplasia Registry (Los Angeles, Calif.), surveyed for all patients with lumbar gibbus and skeletal dysplasias, provided 12 additional cases. Results. All patients had localized gibbus of the upper lumbar spine, characterized by anterior wedging and posterior displacement of the vertebrae at the apex of the curve, producing a beaked appearance. The curve, exaggerated in the sitting or standing position, was most severe in the two patients with MPS-IV (one of whom died). Both developed severe neurologic signs and symptoms requiring surgical intervention. In four patients, MR images demonstrated the apex of the curve to be at or below the conus. Two patients demonstrated anterior herniation of the intervertebral discs at the apex of the curve, though the signal intensity of the intervertebral discs was normal. Conclusion. Lumbar gibbus has important neurologic and orthopedic implications, and is most severe in patients with MPS. The etiology of the gibbus with vertebral beaking is multifactorial and includes poor truncal muscle tone, weight-bearing forces, growth disturbance and anterior disc herniation. The curve is generally at or below the conus. Neurologic complications are unusual, although orthopedic problems can arise. Due to their longer survival, patients with achondroplasia or Morquio's disease are more vulnerable to eventual gibbus-related musculoskeletal complications.

Published

1997

41. The contribution of de novo and rare inherited copy number changes to congenital heart disease in an unselected sample of children with conotruncal defects or hypoplastic left heart disease

Author

Ismee A. Williams, Jennie Kline, Michael Ronemus, Chih-yu Yu, Yoon-ha Lee, Dorothy Warburton, Nancy Wong, Danielle Awad, Boris Yamrom, Anthony Leotta, Michael Wigler, Wendy K. Chung, Lan Yu, Jude Kendall, Dan Levy, Vaidehi Jobanputra, and Kwame Anyane-Yeboa

Subjects

Proband, Heart Defects, Congenital, Male, Candidate gene, congenital, hereditary, and neonatal diseases and abnormalities, DNA Copy Number Variations, Biology, Article, Hypoplastic left heart syndrome, DiGeorge syndrome, Gene Duplication, Conotruncal defect, mental disorders, Hypoplastic Left Heart Syndrome, Genetics, medicine, Humans, Copy-number variation, Genetics (clinical), Comparative Genomic Hybridization, Genome, Human, Intracellular Signaling Peptides and Proteins, Infant, Membrane Proteins, Reproducibility of Results, medicine.disease, Penetrance, Child, Preschool, dup, Intercellular Signaling Peptides and Proteins, Female, Gene Deletion

Abstract

Congenital heart disease (CHD) is the most common congenital malformation, with evidence of a strong genetic component. We analyzed data from 223 consecutively ascertained families, each consisting of at least one child affected by a conotruncal defect (CNT) or hypoplastic left heart disease (HLHS) and both parents. The NimbleGen HD2-2.1 comparative genomic hybridization platform was used to identify de novo and rare inherited copy number variants (CNVs). Excluding 10 cases with 22q11.2 DiGeorge deletions, we validated de novo CNVs in 8 % of 148 probands with CNTs, 12.7 % of 71 probands with HLHS and none in 4 probands with both. Only 2 % of control families showed a de novo CNV. We also identified a group of ultra-rare inherited CNVs that occurred de novo in our sample, contained a candidate gene for CHD, recurred in our sample or were present in an affected sibling. We confirmed the contribution to CHD of copy number changes in genes such as GATA4 and NODAL and identified several genes in novel recurrent CNVs that may point to novel CHD candidate loci. We also found CNVs previously associated with highly variable pheno-types and reduced penetrance, such as dup 1q21.1, dup 16p13.11, dup 15q11.2-13, dup 22q11.2, and del 2q23.1. We found that the presence of extra-cardiac anomalies was not related to the frequency of CNVs, and that there was no significant difference in CNV frequency or specificity between the probands with CNT and HLHS. In agreement with other series, we identified likely causal CNVs in 5.6 % of our total sample, half of which were de novo.

Published

2013

42. Molecular diagnostic dilemmas in Rett syndrome

Author

Debra Rita, Larry White, Ashley Wilson, Kenneth J. Friedman, Val V. Zvereff, Huong Cabral, Lori Carpenter, Dagny Patton, and Kwame Anyane-Yeboa

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, Methyl-CpG-Binding Protein 2, Mutation, Missense, Rett syndrome, Biology, Bioinformatics, medicine.disease_cause, MECP2, Frameshift mutation, Neurodevelopmental disorder, Developmental Neuroscience, medicine, Rett Syndrome, Missense mutation, Humans, Pathology, Molecular, Genetic Association Studies, Genetics, Family Health, Mutation, General Medicine, medicine.disease, Xq28, Pediatrics, Perinatology and Child Health, Autism, Neurology (clinical)

Abstract

Rett syndrome (OMIM 312750) is a progressive, X-linked neurodevelopmental disorder caused by mutations in the MECP2 gene located on chromosome Xq28. The disorder is characterized by a period of normal development during the first 6-18months of life, followed by gradual loss of skills already gained, such as speech and purposeful movement of the hands. The majority of cases are sporadic and represent "de novo" mutations. In this study we summarize the results of diagnostic testing of 30 patients with Rett syndrome (RTT) or mental retardation of unknown etiology using bidirectional sequencing of the open reading frame of the MECP2 gene. Twenty different variants were identified in those patients including 12 missense (R133C, P152R, T158M, V300I, I303M, R306C, T311M, R344W, A358T, P384L, A443T, V481M), four nonsense (R168X, K192X, R255X, R270X), two deletion (E137_L386del, I293_S350del), and two frameshift (S291QfsX26, G343AfsX6) mutations. Seven of the twenty variants identified were novel mutations (E137_L386del, K192X, S291QfsX26, G343AfsX6, I293_S350del, P384L, and A443T). In the cases with novel or non-recurrent missense mutations, family studies were performed to investigate genotype-phenotype correlations. Our results demonstrate the importance of family studies and highlight the complexity of interpretation of MECP2 alterations, which may or may not be disease-associated.

Published

2011

43. Preliminary definition of a 'critical region' of chromosome 13 in q32: Report of 14 cases with 13q deletions and review of the literature

Author

Kwame Anyane-Yeboa, Steven Gersen, Stephen Brown, and Dorothy Warburton

Subjects

Male, Chromosome Disorders, Chromosomal translocation, Biology, Translocation, Genetic, Congenital Abnormalities, Intellectual Disability, medicine, Humans, Growth Disorders, Genetics (clinical), Chromosome 13, Chromosome Aberrations, Genetics, Fetal Growth Retardation, Chromosomes, Human, Pair 13, 13q deletion syndrome, Intermediate phenotype, Breakpoint, Infant, Newborn, Chromosome, Karyotype, medicine.disease, Phenotype, Fetal Diseases, Karyotyping, Female, Chromosome Deletion

Abstract

We report on 14 patients with partial deletions of chromosome 13q. These patients exhibit a wide spectrum of phenotypes. Deletions limited to proximal bands q13-q31 are associated with growth retardation but not with major malformations. We review the literature since 1975 and summarize 13q deletion cases which have a phenotype involving one or more major malformations and mental retardation. Analysis of the breakpoints of these cases, as well as those reported by us, supports the hypothesis that only deletions involving at least part of band q32 are associated with major malformations and digital abnormalities. Patients with more distal deletions have severe mental retardation but do not have major malformations or growth retardation. A group of patients in whom the breakpoint is stated to be within q32 has had an intermediate phenotype. This suggests that it may be possible to define subregions within q32 whose deletion is associated with particular developmental defects.

Published

1993

44. Characterization of the Chromosome 1q41q42.12 region, and the Candidate Gene DISP1, in Patients with CDH

Author

Kristin M. Noonan, Rafael Pieretti Vanmarcke, Sibel Kantarci, Xiaoyun Zhang, Paul S. Dickman, Carrie Sougnez, Mauro Longoni, Meaghan K. Russell, Eli Hatchwell, Kate G. Ackerman, Jay M. Wilson, Kwame Anyane-Yeboa, Barbara R. Pober, and Patricia K. Donahoe

Subjects

Male, Candidate gene, Biology, Article, Congenital Abnormalities, Fryns syndrome, Genetics, medicine, Humans, Hedgehog Proteins, Multiplex ligation-dependent probe amplification, Child, Lung, Genetics (clinical), In Situ Hybridization, Fluorescence, DNA Primers, Sequence Deletion, Hernia, Diaphragmatic, Informed Consent, Mosaicism, Point mutation, Infant, Newborn, Chromosome, Congenital diaphragmatic hernia, Chromosome Mapping, Karyotype, DNA, medicine.disease, Bochdalek hernia, Chromosomes, Human, Pair 1, Female

Abstract

Cytogenetic and molecular cytogenetic studies demonstrate association between congenital diaphragmatic hernia (CDH) and chromosome 1q41q42 deletions. In this study, we screened a large CDH cohort (N=179) for microdeletions in this interval by the multiplex ligation-dependent probe amplification (MLPA) technique, and also sequenced two candidate genes located therein, dispatched 1 (DISP1) and homo sapiens H2.0-like homeobox (HLX). MLPA analysis verified deletions of this region in two cases, an unreported patient with a 46,XY,del(1)(q41q42.13) karyotype and a previously reported patient with a Fryns syndrome phenotype [Kantarci et al., 2006]. HLX sequencing showed a novel but maternally inherited single nucleotide variant (c.27C>G) in a patient with isolated CDH, while DISP1 sequencing revealed a mosaic de novo heterozygous substitution (c.4412C>G; p.Ala1471Gly) in a male with a left-sided Bochdalek hernia plus multiple other anomalies. Pyrosequencing demonstrated the mutant allele was present in 43%, 12%, and 4.5% of the patient's lymphoblastoid, peripheral blood lymphocytes, and saliva cells, respectively. We examined Disp1 expression at day E11.5 of mouse diaphragm formation and confirmed its presence in the pleuroperitoneal fold, as well as the nearby lung which also expresses Sonic hedgehog (Shh). Our report describes the first de novo DISP1 point mutation in a patient with complex CDH. Combining this finding with Disp1 embryonic mouse diaphragm and lung tissue expression, as well as previously reported human chromosome 1q41q42 aberrations in patients with CDH, suggests that DISP1 may warrant further consideration as a CDH candidate gene.

Published

2010

45. The proximal chromosome 14q microdeletion syndrome: delineation of the phenotype using high resolution SNP oligonucleotide microarray analysis (SOMA) and review of the literature

Author

Kwame Anyane-Yeboa, Einat Blumfield, Edina Torgyekes, Sara Pirzadeh, Odelia Nahum, Brynn Levy, Alan L. Shanske, Dorothy Warburton, and Vaidehi Jobanputra

Subjects

Pathology, medicine.medical_specialty, Microcephaly, Chromosomal translocation, Biology, Corpus callosum, Blindness, Polymorphism, Single Nucleotide, Translocation, Genetic, Intellectual Disability, Genetics, medicine, Humans, Abnormalities, Multiple, Hypertelorism, Genetics (clinical), Genetic Association Studies, Oligonucleotide Array Sequence Analysis, Chromosomes, Human, Pair 14, Corpus Callosum Agenesis, Chromosomes, Human, Pair 11, Karyotype, Optic Nerve, Syndrome, Microdeletion syndrome, medicine.disease, Phenotype, Child, Preschool, Face, Karyotyping, Chromosomal region, Female, medicine.symptom, Agenesis of Corpus Callosum, Chromosome Deletion, Chromosomes, Human, Pair 4, Gene Deletion

Abstract

We report on two patients with overlapping small interstitial deletions involving regions 14q12 to 14q13.1. Both children had severe developmental delay, failure to thrive, microcephaly, and distinctive facial features, including abnormal spacing of the eyes, epicanthal folds, sloping forehead, low-set ears, rounded eyebrows with triangular media aspect and outer tapering, depressed and broad nasal bridge, small mouth, a long philtrum, and a prominent Cupid's bow. Brain MRI of both children showed partial agenesis of the corpus callosum. Our first patient had bilateral hypoplastic optic nerves causing blindness, mild hearing impairment, sinus arrhythmia, abnormal temperature regulation, frequent apneic episodes, myoclonic jerks, and opisthotonus. Our second patient had a seizure disorder confirmed by EEG, sleep apnea, chronic interstitial lung disease, and several episodes of pneumonia and gastroenteritis. Cytogenetic analysis showed a normal karyotype in Patient 1 and a unique apparently balanced three-way translocation in Patient 2 involving chromosomes 4, 14, and 11. High resolution SNP Oligonucleotide Microarray Analysis (SOMA) revealed a deletion in the proximal region of chromosome 14q overlapping with the deletion of our first patient, and no copy number changes in chromosomes 4 and 11. Here, we review and compare published cases with a deletion involving the 14q12-22.1 chromosomal region in an effort to correlate phenotype and genotype. We also examine the underlying genomic architecture to identify the possible mechanism of the chromosomal abnormality. Our review found a patient with a mirror duplication of our first patient's deletion, confirming the existence of an underlying genomic structural instability in the region. © 2011 Wiley-Liss, Inc.

Published

2010

46. Changes in an inherited ring (22) due to meiotic recombination? Implications for genetic counseling

Author

Vaidehi Jobanputra, Kwame Anyane-Yeboa, Brynn Levy, Erin Ash, and Dorothy Warburton

Subjects

Adult, Genetic counseling, Chromosomes, Human, Pair 22, Developmental Disabilities, Ring chromosome, Genetic Counseling, Biology, Ring (chemistry), Polymorphism, Single Nucleotide, Meiosis, Genetics, Humans, Base sequence, Ring Chromosomes, Child, Genetics (clinical), In Situ Hybridization, Fluorescence, Oligonucleotide Array Sequence Analysis, Sequence Deletion, Recombination, Genetic, Base Sequence, Extramural, Chromosome Banding, Karyotyping, Female, Homologous recombination, Recombination, Gene Deletion

Published

2009

47. Application of ROMA (representational oligonucleotide microarray analysis) to patients with cytogenetic rearrangements

Author

Jennifer Troge, Wendy K. Chung, Jonathan Sebat, Michael Wigler, Vaidehi Jobanputra, Kwame Anyane-Yeboa, and Dorothy Warburton

Subjects

Male, medicine.medical_specialty, Gene Dosage, Biology, Gene dosage, Sensitivity and Specificity, Cytogenetics, Gene duplication, medicine, Humans, Genetic Testing, Genetics (clinical), In Situ Hybridization, Fluorescence, Oligonucleotide Array Sequence Analysis, Genetics, Chromosome Aberrations, Gene Expression Profiling, Breakpoint, Infant, Subtelomere, Prognosis, Gene expression profiling, Chromosome 4, Child, Preschool, Human genome

Abstract

Purpose: To demonstrate the accuracy and sensitivity of Representational Oligonucleotide Microarray Analysis (ROMA) to describe copy number changes in patients with chromosomal abnormalities. Methods: ROMA was performed using BglII digested DNA from two cases with cytogenetically detected deletions and one case with an unbalanced terminal rearrangement detected only by subtelomeric FISH. Hybridization was to an 85,000-probe oligonucleotide microarray, providing an average resolution of 35 kb. FISH was used to confirm some of the ROMA findings. Results: By ROMA, a del(13)(q14.3q21.2) was shown to be noncontiguous, with deletions extending from 53.08 to 61.40 Mb and from 72.88 to 74.83 Mb. The 10-Mb deletion contained only six known genes. FISH confirmed the noncontiguous nature of the deletion, as well as a small amplification in 6q that was also found in the patient's mother. A del(4)(q12q21.2) was found by ROMA to be 23 Mb in length, from 58.8 to 81.9 Mb on chromosome 4, in agreement with the cytogenetically assigned breakpoints. ROMA showed that an unbalanced “subtelomeric” rearrangement involved a 6-Mb deletion of 22q and an 8-Mb duplication of 16q. Conclusions: ROMA can define cytogenetic aberrations with extraordinary precision. Unexpected findings included the interrupted nature of the deletion in 13q and the large size of the imbalances in the “subtelomeric” rearrangement. Together with the information from the human genome sequence and proteomics, the ability to define rearrangements with “ultra-high” resolution will improve the ability to provide accurate prognosis both prenatally and postnatally to parents of offspring with chromosomal aberrations.

Published

2005

48. Congenital myopathy, recurrent secretory diarrhea, bullous eruption of skin, microcephaly, and deafness: a new genetic syndrome?

Author

Maria C. Garzon, J. Levy, Wendy K. Chung, E. Lieber, M.P. Gallagher, Sharon E. Oberfield, and Kwame Anyane-Yeboa

Subjects

Diarrhea, Male, medicine.medical_specialty, Microcephaly, Hearing loss, Deafness, Pathogenesis, Muscular Diseases, Internal medicine, Pemphigoid, Bullous, otorhinolaryngologic diseases, medicine, Humans, Abnormalities, Multiple, Myopathy, Genetics (clinical), Family Health, business.industry, Infant, Syndrome, medicine.disease, Congenital myopathy, Dermatology, Endocrinology, Child, Preschool, Failure to thrive, Zinc deficiency, Female, medicine.symptom, business

Abstract

We describe three siblings with congenital myopathy, bullous eruption of the skin, secretory diarrhea, apparent zinc deficiency, failure to thrive, deafness, and microcephaly. The parents are not consanguineous and there are no other affected relatives. This new syndrome, which follows an apparent autosomal recessive pattern, appears to be distinct from known syndromes of secretory diarrhea, myopathy, deafness, microcephaly, and zinc deficiency.

Published

2002

49. Paternal germline mosaicism in Herlitz junctional epidermolysis bullosa

Author

Peter B, Cserhalmi-Friedman, Kwame, Anyane-Yeboa, and Angela M, Christiano

Subjects

Male, Mosaicism, Pregnancy, Prenatal Diagnosis, Humans, Point Mutation, Female, Genetic Counseling, Epidermolysis Bullosa, Junctional, Germ-Line Mutation, Sequence Deletion

Abstract

We studied a single patient with the lethal (Herlitz) type of junctional epidermolysis bullosa (H-JEB). Screening for mutations in the LAMB3 gene in the patient revealed the previously described hotspot mutation R635X and a novel one basepair deletion in exon 10. The single basepair deletion 1094delA could be detected in the clinically unaffected mother, while the nonsense mutation R635X could not be found in the peripheral blood DNA of either parent. After excluding non-paternity by microsatellite analysis using random markers on chromosomes 3, 8 and 18, we determined that the mutation R635X in the proband was most likely the result of a de novo event or alternatively, germline mosaicism. The parents requested prenatal diagnosis for a second pregnancy, and while the maternal mutation 1094delA could not be detected in DNA from the fetus, unexpectedly, the mutation R635X was present in the chorionic villus DNA. These findings were most consistent with paternal germline mosaicism for the recessive mutation R635X. The results have had a significant impact on the genetic counseling in this family. To our knowledge, this study represents the first documented case of germline mosaicism in junctional epidermolysis bullosa, and serves as a reminder that germline mosaicism should be considered in cases in which a 'new' mutation is found in the offspring of a clinically and/or genetically unaffected parent.

Published

2002

50. Caveat to genotype-phenotype correlation in mucopolysaccharidosis type II: Discordant clinical severity of R468W and R468Q mutations of the iduronate-2-sulfatase gene

Author

Elena L. Aronovich, Chester B. Whitley, Donna Russo, Dorothy Warburton, Rose Ann Anderson, Kwame Anyane-Yeboa, and Paul Crotty

Subjects

Male, Genetics, Base Sequence, Genotype, Molecular Sequence Data, Infant, Iduronate-2-sulfatase, DNA, Iduronate Sulfatase, Biology, Genotype phenotype, Correlation, Phenotype, Humans, Point Mutation, Clinical severity, Amino Acid Sequence, Mucopolysaccharidosis type II, Gene, Genetics (clinical), Mucopolysaccharidosis II

Published

1993