Your search keyword '"Ann M. Joseph-George"' showing total 14 results

1. Stable transmission of an unbalanced chromosome 21 derived from chromoanasynthesis in a patient with a SYNGAP1 likely pathogenic variant

Author

Peter J. B. Sabatini, Resham Ejaz, Dimitri J. Stavropoulos, Roberto Mendoza-Londono, and Ann M. Joseph-George

Subjects

Chromoanasynthesis, SYNGAP1, Familial transmission, Chromoanagenesis, Genetics, QH426-470

Abstract

Abstract Background Complex genomic structural variations, involving chromoanagenesis, have been implicated in multiple congenital anomalies and abnormal neurodevelopment. Familial inheritance of complex chromosomal structural alteration resulting from germline chromoanagenesis-type mechanisms are limited. Case presentation We report a two-year eleven-month old male presenting with epilepsy, ataxia and dysmorphic features of unknown etiology. Chromosomal microarray identified a complex unbalanced rearrangement involving chromosome 21. G-banding and FISH for targeted regions of chromosome 21 revealed that the copy number imbalances were limited to gains dispersed throughout the long arm of chromosome 21, characteristic of a chromosome derived from chromoanagenesis. Family studies showed that the unbalanced chromosome had been stably inherited, as it was present in both his healthy mother and maternal grandfather. Further molecular testing for non-syndromic intellectual disability genes found a likely pathogenic mutation in SYNGAP1 (NM_006772.2:c.3722_3723del). Conclusions This study indicates that complex rearrangements involving an unbalanced chromosome derived from chromoanasynthesis can be familial and should be not be presumed pathogenic.

Published

2018

2. Complete functional rescue of the ABCA1−/− mouse by human BAC transgenesis

Author

Jonathan M. Coutinho, Roshni R. Singaraja, Martin Kang, David J. Arenillas, Lisa N. Bertram, Nagat Bissada, Bart Staels, Jean-Charles Fruchart, Catherine Fievet, Ann M. Joseph-George, Wyeth W. Wasserman, and Michael R. Hayden

Subjects

ATP binding cassette type A1, humanized mouse, bacterial artificial chromosome, phylogenetic footprinting, liver X receptor, transcription factor binding site, Biochemistry, QD415-436

Abstract

Humanized mouse models are useful tools to explore the functional and regulatory differences between human and murine orthologous genes. We have combined a bioinformatics approach and an in vivo approach to assess the functional and regulatory differences between the human and mouse ABCA1 genes. Computational analysis identified significant differences in potential regulatory sites between the human and mouse genes. The effect of these differences was assessed in vivo, using a bacterial artificial chromosome transgenic humanized ABCA1 mouse model that expresses the human gene in the absence of mouse ABCA1. Humanized mice expressed human ABCA1 protein at levels similar to wild-type mice and fully compensated for cholesterol efflux activity and lipid levels seen in ABCA1-deficient mice. Liver X receptor agonist administration resulted in significant increases in HDL values associated with parallel increases in the hepatic ABCA1 protein and mRNA levels in the humanized ABCA1 mice, as seen in the wild-type animals.Our studies indicate that despite differences in potential regulatory regions, the human ABCA1 gene is able to functionally fully compensate for the mouse gene. Our humanized ABCA1 mice can serve as a useful model system for functional analysis of the human ABCA1 gene in vivo and can be used for the generation of potential new therapeutics that target HDL metabolism.

Published

2005

3. The Personal Genome Project Canada: findings from whole genome sequences of the inaugural 56 participants

Author

Wilson W L Sung, S. Mohsen Hosseini, Brett Trost, Stephen W. Scherer, John Wei, James Ellis, Jeffrey R. MacDonald, Sarah Bowdin, Janet A. Buchanan, M. Stephen Meyn, Miriam S. Reuter, Rohan V. Patel, Giovanna Pellecchia, Allison Hazell, Ryan A. Cook, Sergio L. Pereira, Bhooma Thiruvahindrapuram, Jennifer L. Howe, Iris Cohn, Lisa J. Strug, Ryan K. C. Yuen, Peter Pasceri, Yvonne Bombard, Joe Whitney, Hin C. Lee, Tara Paton, Anne S. Bassett, Rosanna Weksberg, Jill Davies, Barbara Kellam, Dimitri J. Stavropoulos, Wei Wei, Christian R. Marshall, Cheryl Shuman, Marc Fiume, Fred W. Keeley, Richard F. Wintle, Matthew R. Hildebrandt, Jo Anne Herbrick, Zhuozhi Wang, Peter N. Ray, Thomas Nalpathamkalam, Ronald D. Cohn, Sherilyn L. Bell, Neal Sondheimer, Daniele Merico, Susan Walker, Ann M. Joseph-George, Melanie M. Mahtani, Asli Romm, Chao Lu, Michael J. Szego, and Nasim Monfared

Subjects

Male, 0301 basic medicine, Genetics, Whole genome sequencing, Canada, Whole Genome Sequencing, Genome, Human, Genetic Variation, Genes, Recessive, Sequence Analysis, DNA, General Medicine, Biology, Genome, Personal Genome Project, 03 medical and health sciences, 030104 developmental biology, Genotype, Genetic variation, Humans, Female, Genetic Predisposition to Disease, Human genome, Letters, Copy-number variation, Allele

Abstract

BACKGROUND: The Personal Genome Project Canada is a comprehensive public data resource that integrates whole genome sequencing data and health information. We describe genomic variation identified in the initial recruitment cohort of 56 volunteers. METHODS: Volunteers were screened for eligibility and provided informed consent for open data sharing. Using blood DNA, we performed whole genome sequencing and identified all possible classes of DNA variants. A genetic counsellor explained the implication of the results to each participant. RESULTS: Whole genome sequencing of the first 56 participants identified 207 662 805 sequence variants and 27 494 copy number variations. We analyzed a prioritized disease-associated data set (n = 1606 variants) according to standardized guidelines, and interpreted 19 variants in 14 participants (25%) as having obvious health implications. Six of these variants (e.g., in BRCA1 or mosaic loss of an X chromosome) were pathogenic or likely pathogenic. Seven were risk factors for cancer, cardiovascular or neurobehavioural conditions. Four other variants — associated with cancer, cardiac or neurodegenerative phenotypes — remained of uncertain significance because of discrepancies among databases. We also identified a large structural chromosome aberration and a likely pathogenic mitochondrial variant. There were 172 recessive disease alleles (e.g., 5 individuals carried mutations for cystic fibrosis). Pharmacogenomics analyses revealed another 3.9 potentially relevant genotypes per individual. INTERPRETATION: Our analyses identified a spectrum of genetic variants with potential health impact in 25% of participants. When also considering recessive alleles and variants with potential pharmacologic relevance, all 56 participants had medically relevant findings. Although access is mostly limited to research, whole genome sequencing can provide specific and novel information with the potential of major impact for health care.

Published

2018

4. Warsaw breakage syndrome: Further clinical and genetic delineation

Author

Ebba Alkhunaizi, Ann M. Joseph-George, Fowzan S. Alkuraya, Susan Blaser, Sanjay Kumar Bharti, Mais Hashem, Nicole Martin, Ranad Shaheen, Robert M. Brosh, David Chitayat, Mohammed Al-Owain, Mohammed A. Butt, Ghada M H Abdel-Salam, Karen Chong, Blake C. Papsin, and Ruth Godoy

Subjects

0301 basic medicine, Male, Models, Molecular, Microcephaly, Hearing loss, Biology, Article, DEAD-box RNA Helicases, 03 medical and health sciences, 0302 clinical medicine, DDX11, Genotype, Genetics, medicine, Humans, Abnormalities, Multiple, Amino Acid Sequence, Child, Genetics (clinical), Exome sequencing, Protein Stability, DNA Helicases, Infant, Newborn, Facies, Infant, Chromosome Breakage, Syndrome, medicine.disease, Phenotype, Magnetic Resonance Imaging, Hypoplasia, 030104 developmental biology, Gene Expression Regulation, Child, Preschool, Ear, Inner, Sensorineural hearing loss, Female, medicine.symptom, Tomography, X-Ray Computed, Proteasome Inhibitors, 030217 neurology & neurosurgery

Abstract

Warsaw breakage syndrome (WBS) is a recently recognized DDX11-related rare cohesinopathy, characterized by severe prenatal and postnatal growth restriction, microcephaly, developmental delay, cochlear anomalies and sensorineural hearing loss. Only seven cases have been reported in the English literature, and thus the information on the phenotype and genotype of this interesting condition is limited. We provide clinical and molecular information on five additional unrelated patients carrying novel bi-allelic variants in the DDX11 gene, identified via whole exome sequencing. One of the variants was found to be a novel Saudi founder variant. All identified variants were classified as pathogenic or likely pathogenic except for one which was initially classified as a variant of unknown significance (VOUS) (p.Arg378Pro). Functional characterization of this VOUS using heterologous expression of wild type and mutant DDX11 revealed a marked effect on protein stability, thus confirming pathogenicity of this variant. The phenotypic data of the seven WBS reported patients were compared to our patients for further phenotypic delineation. Although all the reported patients had cochlear hypoplasia, one patient also had posterior labyrinthine anomaly. We conclude that while the cardinal clinical features in WBS (microcephaly, growth retardation and cochlear anomalies) are almost universally present, the “breakage” phenotype is highly variable and can be absent in some cases. This report further expands the knowledge of the phenotypic and molecular features of WBS.

Published

2018

5. Indexing Effects of Copy Number Variation on Genes Involved in Developmental Delay

Author

Stephen W. Scherer, Bhooma Thiruvahindrapuram, Ann M. Joseph-George, Peter Kannu, Emmanuelle Lemyre, Ada Chan, Susan Walker, Mary Shago, Grace Yoon, Janet A. Buchanan, Abdul Noor, Lia D’Abate, Christian R. Marshall, Melissa T. Carter, Sonia Nizard, Mehdi Zarrei, Géraldine Mathonnet, Kristiina Tammimies, Thomas Nalpathamkalam, Ryan K. C. Yuen, Mohammed Uddin, Frédérique Tihy, Daniele Merico, Dimitri J. Stavropoulos, Giovanna Pellecchia, Matthew J. Gazzellone, Erik C. Thorland, Koenraad Devriendt, and Marsha Speevak

Subjects

Adult, Male, Proteomics, 0301 basic medicine, Candidate gene, DNA Copy Number Variations, Developmental Disabilities, Cell Cycle Proteins, Genome-wide association study, Biology, Gene dosage, Article, 03 medical and health sciences, Exon, 0302 clinical medicine, Humans, Genetic Predisposition to Disease, Copy-number variation, Child, Gene, Adaptor Proteins, Signal Transducing, Genetics, Regulation of gene expression, Multidisciplinary, Gene Expression Profiling, Brain, Gene Expression Regulation, Developmental, Gene expression profiling, 030104 developmental biology, Female, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

A challenge in clinical genomics is to predict whether copy number variation (CNV) affecting a gene or multiple genes will manifest as disease. Increasing recognition of gene dosage effects in neurodevelopmental disorders prompted us to develop a computational approach based on critical-exon (highly expressed in brain, highly conserved) examination for potential etiologic effects. Using a large CNV dataset, our updated analyses revealed significant (P −15) enrichment of critical-exons within rare CNVs in cases compared to controls. Separately, we used a weighted gene co-expression network analysis (WGCNA) to construct an unbiased protein module from prenatal and adult tissues and found it significantly enriched for critical exons in prenatal (P −50, OR = 2.11) and adult (P −18, OR = 1.55) tissues. WGCNA yielded 1,206 proteins for which we prioritized the corresponding genes as likely to have a role in neurodevelopmental disorders. We compared the gene lists obtained from critical-exon and WGCNA analysis and found 438 candidate genes associated with CNVs annotated as pathogenic, or as variants of uncertain significance (VOUS), from among 10,619 developmental delay cases. We identified genes containing CNVs previously considered to be VOUS to be new candidate genes for neurodevelopmental disorders (GIT1, MVB12B and PPP1R9A) demonstrating the utility of this strategy to index the clinical effects of CNVs.

Published

2016

6. Co-occurrence of 16p13.11 microdeletion and ring chromosome 20 syndrome

Author

Lance H. Rodan, Ann M. Joseph-George, Maria Zak, James Stavropoulos, and Berge A. Minassian

Subjects

0301 basic medicine, Pediatrics, medicine.medical_specialty, Activities of daily living, media_common.quotation_subject, Ring chromosome 20, Bioinformatics, Irritability, Mood Lability, 03 medical and health sciences, 0302 clinical medicine, medicine, Girl, Clinical/Scientific Notes, Genetics (clinical), media_common, Sleep attacks, business.industry, medicine.disease, Sleep in non-human animals, 030104 developmental biology, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery, Altered level of consciousness

Abstract

A previously healthy 16-year-old girl of Jamaican descent presented with a 1-year history of progressive daytime somnolence, sleep attacks (sudden irresistible episodes of sleep), and paroxysms of altered level of consciousness. Her parents also reported irritability, mood lability, and hyperphagia. Her history was notable for a mild learning disability diagnosed at 9 years of age. Before symptom onset, she attended regular class at school with average academic performance and was independent in instrumental activities of daily living. On examination, she was normocephalic and nondysmorphic and had no focal neurologic deficits.

Published

2015

7. Genome assembly comparison identifies structural variants in the human genome

Author

Charles Lee, Matthew E. Hurles, Xavier Estivill, Muhammad Rafiq, Lars Feuk, Yongshu He, Stephen W. Scherer, Lorena Pantano, Ann M. Joseph-George, Keith W. Jones, Richard J. Mural, Richard Redon, Razi Khaja, John Wei, Junjun Zhang, Lluís Armengol, Mary Shago, Hiroyuki Aburatani, Cheng Qian, and Jeffrey R. MacDonald

Subjects

Genetics, Base Sequence, Genome, Human, Genetic Variation, Sequence assembly, Genomics, DNA, Computational biology, Biology, Polymerase Chain Reaction, Genome, Article, DNA sequencing, Structural variation, Humans, Human genome, Copy-number variation, Sequence Alignment, In Situ Hybridization, Fluorescence, Segmental duplication

Abstract

Numerous types of DNA variation exist, ranging from SNPs to larger structural alterations such as copy number variants (CNVs) and inversions. Alignment of DNA sequence from different sources has been used to identify SNPs1,2 and intermediate-sized variants (ISVs)3. However, only a small proportion of total heterogeneity is characterized, and little is known of the characteristics of most smaller-sized (1.5 million SNPs. Some differences were simple insertions and deletions, but in regions containing CNVs, segmental duplication and repetitive DNA, they were more complex. Our results uncover substantial undescribed variation in humans, highlighting the need for comprehensive annotation strategies to fully interpret genome scanning and personalized sequencing projects.

Published

2006

8. PGD for a carrier of an intrachromosomal insertion using aCGH

Author

Ann M. Joseph-George, Claire Jones, David Chitayat, Matthew Vlasschaert, Georges Maire, Karen Chong, Elena Kolomietz, Rebecca Arthur, and Diane Myles-Reid

Subjects

Adult, Abortion, Habitual, Heterozygote, Urology, medicine.medical_treatment, Biopsy, Fertilization in Vitro, Biology, Preimplantation genetic diagnosis, Predictive Value of Tests, Pregnancy, medicine, Humans, Genetic Testing, Treatment Failure, Genetic risk, In Situ Hybridization, Fluorescence, Preimplantation Diagnosis, Genetics, Chromosome Aberrations, Comparative Genomic Hybridization, In vitro fertilisation, Chromosome, Embryo, Embryo Transfer, Blastocyst, Reproductive Medicine, Chromosomes, Human, Pair 1, embryonic structures, Female, Ploidy, Trophectoderm biopsy, Comparative genomic hybridization

Abstract

Intrachromosomal insertions are rare and difficult to diagnose. However, making the correct diagnosis is critical for genetic risk assessment, and prenatal and preimplantation genetic diagnosis outcomes. We present a case of preimplantation genetic diagnosis (PGD) using array comparative genomic hybridization (aCGH) following trophectoderm biopsy of embryos created after in vitro fertilization for a carrier of an intrachromosomal insertion on chromosome 1 [46,XX, ins(1)(q44q23q32.1)]. The PGD analysis of 6 blastocysts demonstrated 67% unbalanced embryos. No pregnancy was achieved after the transfer of 2 euploid embryos. To the best of our knowledge, this is the first reported case of PGD using aCGH following trophectoderm biopsy for a carrier of an intrachromosomal insertion.

Published

2014

9. MuLV-related endogenous retroviral elements and Flt3 participate in aberrant end-joining events that promote B-cell leukemogenesis

Author

Cynthia J. Guidos, Eniko Papp, Jayne S. Danska, Paul E. Kowalski, Raymond C.C. Wong, Ildiko Grandal, Radia M. Johnson, Lauryl M. J. Nutter, and Ann M. Joseph-George

Subjects

DNA End-Joining Repair, Endogenous retrovirus, Biology, medicine.disease_cause, Receptor tyrosine kinase, Mice, hemic and lymphatic diseases, Genetics, medicine, STAT5 Transcription Factor, Tumor Cells, Cultured, Animals, Phosphorylation, B cell, STAT5, Cell Proliferation, Recombination, Genetic, Mutation, B-Lymphocytes, Leukemia, Gene Expression Regulation, Leukemic, hemic and immune systems, Hematopoietic Stem Cells, Long terminal repeat, Protein Structure, Tertiary, Non-homologous end joining, medicine.anatomical_structure, fms-Like Tyrosine Kinase 3, Fms-Like Tyrosine Kinase 3, embryonic structures, Cancer research, biology.protein, Moloney murine leukemia virus, Developmental Biology, Signal Transduction, Research Paper

Abstract

During V(D)J recombination of immunoglobulin genes, p53 and nonhomologous end-joining (NHEJ) suppress aberrant rejoining of DNA double-strand breaks induced by recombinase-activating genes (Rags)-1/2, thus maintaining genomic stability and limiting malignant transformation during B-cell development. However, Rag deficiency does not prevent B-cell leukemogenesis in p53/NHEJ mutant mice, revealing that p53 and NHEJ also suppress Rag-independent mechanisms of B-cell leukemogenesis. Using several cytogenomic approaches, we identified a novel class of activating mutations in Fms-like tyrosine kinase 3 (Flt3), a receptor tyrosine kinase important for normal hematopoiesis in Rag/p53/NHEJ triple-mutant (TM) B-cell leukemias. These mutant Flt3 alleles were created by complex genomic rearrangements with Moloney leukemia virus (MuLV)-related endogenous retroviral (ERV) elements, generating ERV-Flt3 fusion genes encoding an N-terminally truncated mutant form of Flt3 (trFlt3) that was transcribed from ERV long terminal repeats. trFlt3 protein lacked most of the Flt3 extracellular domain and induced ligand-independent STAT5 phosphorylation and proliferation of hematopoietic progenitor cells. Furthermore, expression of trFlt3 in p53/NHEJ mutant hematopoietic progenitor cells promoted development of clinically aggressive B-cell leukemia. Thus, repetitive MuLV-related ERV sequences can participate in aberrant end-joining events that promote development of aggressive B-cell leukemia.

Published

2014

10. Euchromatic 9q13-q21 duplication variants are tandem segmental amplifications of sequence reciprocal to 9q13-q21 deletions

Author

Yongshu He, Ann M. Joseph-George, Christian R. Marshall, Kathy Chun, Ciara A Fahey, David Chitayat, Jeffrey R. MacDonald, Greg Ryan, Elizabeth J.T. Winsor, Raymond C.C. Wong, Anne Summers, and Stephen W. Scherer

Subjects

Genetics, Adult, medicine.medical_specialty, Euchromatin, DNA Copy Number Variations, Cytogenetics, Gene Amplification, Chromosome 9, Context (language use), Biology, Microarray Analysis, Molecular cytogenetics, Fetus, Gene mapping, Gene duplication, Chromosome Duplication, medicine, Humans, Chromosome Deletion, Chromosomes, Human, Pair 9, Genetics (clinical), In Situ Hybridization, Fluorescence, Segmental duplication

Abstract

Background There are four known pericentromeric euchromatic variants of chromosome 9 in the literature that are increasingly being observed in diagnostic cytogenetic laboratories. These variants pose diagnostic and counselling dilemmas, especially in prenatal settings, as distinction of a pathogenic alteration from a euchromatic variant is difficult. The molecular characterisation of three of these four variants has been reported. In this study, the genomic structure of the fourth variant, an additional G-positive band at 9q13-q21, is characterised. Methods Two unrelated families with the 9q13-q21 duplication variant, and a third individual with a cytogenetically visible 9q13-q21 deletion, were studied using conventional and molecular cytogenetics techniques, as well as microarrays. The highly repetitive nature of the segmental duplications in the region also necessitated the use of both interphase and metaphase fluorescence in situ hybridisation (FISH). Results It was determined that the DNA that constitutes this variant was ∼15–20 megabases in size and tandemly repeated as 3–4 cassettes of intrachromosomal segmental duplication. The variant appeared constitutively similar in sequence content and organisation between the two unrelated individuals, and it was inherited without apparent change. Sequences found amplified in the two duplication carriers were absent in the carrier of the deletion variant. Conclusions The sequences involved in both the 9q13-q21 duplication and deletion appear the same, implying reciprocity and suggesting non-allelic homologous recombination as the underlying mechanism. All four known euchromatic variants of chromosome 9 have now been shown to encompass segmental duplications. Importantly, a set of validated FISH probes was defined for the detection and characterisation of this 9q13-q21 amplification in the context of other chromosome 9 variants, allowing apparently benign variants to be distinguished from pathogenic changes.

Published

2011

11. Hemizygous deletions on chromosome 1p21.3 involving the DPYD gene in individuals with autism spectrum disorder

Author

Abdul Noor, Christian R. Marshall, Sarah M. Nikkel, Rosanna Weksberg, Melissa T. Carter, Wendy Roberts, Dalila Pinto, Stephen W. Scherer, Aparna Prasad, C Fairbrother-Davies, John B. Vincent, Carolyn Noakes, Ann M. Joseph-George, Bridget A. Fernandez, and Anath C. Lionel

Subjects

Proband, Adult, Male, Adolescent, Locus (genetics), Biology, Exon, Genetics, medicine, Missense mutation, Humans, Copy-number variation, Child, Genetics (clinical), Dihydrouracil Dehydrogenase (NADP), Chromosomes, Human, Pair 10, medicine.disease, Pedigree, Child Development Disorders, Pervasive, Chromosomes, Human, Pair 1, Child, Preschool, Speech delay, Autism, DPYD, Female, medicine.symptom, Chromosome Deletion

Abstract

We describe the identification and clinical presentation of four individuals from three unrelated families with hemizygous deletions involving the DPYD gene at chromosome 1p21.3. DPYD encodes dihydropyrimidine dehydrogenase, which is the initial and rate-limiting enzyme in the catabolism of pyrimidine bases. All four individuals described met diagnostic criteria for autism spectrum disorder with severe speech delay. Patient 1's deletion was originally reported in 2008, and more detailed clinical information is provided. Subsequently, this male individual was found to have a missense mutation in the X-linked PTCHD1 autism susceptibility gene, which may also contribute to the phenotype. Patients 2 and 3 are siblings with a novel deletion encompassing the DPYD gene. In their mother, the genomic region deleted from chromosome 1p21.3 was inserted into chromosome 10. A fourth proband had a novel 10-kb intragenic deletion of exon 6 of the DPYD gene detected on a higher resolution microarray. Our study suggests that hemizygous deletions involving the DPYD locus present with variable phenotypes which can include speech delay and autistic features, and may also be influenced by additional mutations in other genes, issues which need to be considered in genetic counseling.

Published

2010

12. Phenotypic spectrum associated with de novo and inherited deletions and duplications at 16p11.2 in individuals ascertained for diagnosis of autism spectrum disorder

Author

Barbara Noble, Sandra Luscombe, Cathy Vardy, Lesley Turner, Victoria Crosbie, Eva Tucker, Sara MacKay, Stephen W. Scherer, Peter Szatmari, Stephen Meyn, Brian H.Y. Chung, Christian R. Marshall, Rosanna Weksberg, Kathy Whitten, Bridget A. Fernandez, Wendy Roberts, and Ann M. Joseph-George

Subjects

Proband, Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Inheritance Patterns, Biology, behavioral disciplines and activities, Gene Duplication, mental disorders, Genetics, medicine, Pervasive developmental disorder, Humans, Copy-number variation, Genetics (clinical), Genetic Association Studies, Genetic heterogeneity, medicine.disease, Pedigree, Developmental disorder, Phenotype, Molecular Diagnostic Techniques, Asperger syndrome, Autism spectrum disorder, Child Development Disorders, Pervasive, Child, Preschool, Cytogenetic Analysis, Autism, Female, Chromosomes, Human, Pair 16, Gene Deletion

Abstract

Background Recurrent microdeletions and microduplications of ∼555 kb at 16p11.2 confer susceptibility to autism spectrum disorder (ASD) in up to 1% of ASD patients. No physical or behavioural features have been identified that distinguish these individuals as having a distinct ASD subtype, but clinical data are limited. Methods We report five autistic probands identified by microarray analysis with copy number variation (CNV) of 16p11.2 (three deletions, two duplications). Each patient was assessed for ASD and dysmorphic features. We also describe a deletion positive 26-month-old female who has developmental delay (DD) and autistic features. Results Proband 1 (female with ASD, de novo deletion) is not dysmorphic. Proband 2 (male with autism, de novo deletion) and proband 3 and his brother (males with autism, inherited deletions) are dysmorphic, but the two probands do not resemble one another. The mother of proband 3 has mild mental retardation (MR), minor dysmorphism and meets the criteria for ASD. Proband 4 (dysmorphic autistic male, de novo duplication) had a congenital diaphragmatic hernia. Proband 5 (non-dysmorphic ASD female with a duplication) has two apparently healthy duplication positive relatives. Probands 1 and 2 have deletion negative siblings with ASD and Asperger syndrome, respectively. Proband 6 (a female with DD and an inherited duplication) is dysmorphic, but has oligohydramnios sequence. Conclusions The phenotypic spectrum associated with CNV at 16p11.2 includes ASD, MR/DD and/or possibly other primary psychiatric disorders. Compared with the microduplications, the reciprocal microdeletions are more likely to be penetrant and to be associated with non-specific major or minor dysmorphism. There are deletion positive ASD probands with a less severe phenotype than deletion negative ASD siblings underscoring the significant phenotypic heterogeneity.

Published

2009

13. Williams-Beuren Syndrome Diagnosis Using Fluorescence In Situ Hybridization

Author

Lucy R. Osborne, Stephen W. Scherer, and Ann M. Joseph-George

Subjects

Chromosome 7 (human), congenital, hereditary, and neonatal diseases and abnormalities, Williams-beuren syndrome, medicine.diagnostic_test, medicine, Chromosome 7q, Suspected diagnosis, Interphase, cardiovascular diseases, Biology, Molecular biology, Metaphase, Fluorescence in situ hybridization

Abstract

Williams-Beuren syndrome (WBS) is most commonly caused by a 1.5-Mb hemizygous deletion of chromosome 7q 11.23. Other genomic rearrangements of this region have also been described, some as polymorphisms and others as rare variants, the latter often being directly associated with clinical symptoms. Fluorescence in situ hybridization of either metaphase or interphase nuclei can be used to detect all of these chromosomal rearrangements, providing the ability to test this segment of chromosome 7 in families with a suspected diagnosis of WBS.

Published

2006

14. Williams-Beuren syndrome diagnosis using fluorescence in situ hybridization

Author

Lucy R, Osborne, Ann M, Joseph-George, and Stephen W, Scherer

Subjects

Williams Syndrome, Indoles, Tumor Cells, Cultured, Humans, DNA, Nucleic Acid Denaturation, Chromosomes, Human, Pair 7, In Situ Hybridization, Fluorescence, Chromosome Banding

Abstract

Williams-Beuren syndrome (WBS) is most commonly caused by a 1.5-Mb hemizygous deletion of chromosome 7q 11.23. Other genomic rearrangements of this region have also been described, some as polymorphisms and others as rare variants, the latter often being directly associated with clinical symptoms. Fluorescence in situ hybridization of either metaphase or interphase nuclei can be used to detect all of these chromosomal rearrangements, providing the ability to test this segment of chromosome 7 in families with a suspected diagnosis of WBS.

Published

2006