Your search keyword '"Ana S A Cohen"' showing total 22 results

1. Complex trait associations in rare diseases and impacts on Mendelian variant interpretation

Author

Craig Smail, Bing Ge, Marissa R. Keever-Keigher, Carl Schwendinger-Schreck, Warren A. Cheung, Jeffrey J. Johnston, Cassandra Barrett, Genomic Answers for Kids Consortium, Keith Feldman, Ana S. A. Cohen, Emily G. Farrow, Isabelle Thiffault, Elin Grundberg, and Tomi Pastinen

Subjects

Science

Abstract

Abstract Emerging evidence implicates common genetic variation - aggregated into polygenic scores (PGS) - in the onset and phenotypic presentation of rare diseases. Here, we comprehensively map individual polygenic liability for 1102 open-source PGS in a cohort of 3059 probands enrolled in the Genomic Answers for Kids (GA4K) rare disease study, revealing widespread associations between rare disease phenotypes and PGSs for common complex diseases and traits, blood protein levels, and brain and other organ morphological measurements. Using this resource, we demonstrate increased polygenic liability in probands with an inherited candidate disease variant (VUS) compared to unaffected carrier parents. Further, we show an enrichment for large-effect rare variants in putative core PGS genes for associated complex traits. Overall, our study supports and expands on previous findings of complex trait associations in rare diseases, implicates polygenic liability as a potential mechanism underlying variable penetrance of candidate causal variants, and provides a framework for identifying novel candidate rare disease genes.

Published

2024

2. Direct haplotype-resolved 5-base HiFi sequencing for genome-wide profiling of hypermethylation outliers in a rare disease cohort

Author

Warren A. Cheung, Adam F. Johnson, William J. Rowell, Emily Farrow, Richard Hall, Ana S. A. Cohen, John C. Means, Tricia N. Zion, Daniel M. Portik, Christopher T. Saunders, Boryana Koseva, Chengpeng Bi, Tina K. Truong, Carl Schwendinger-Schreck, Byunggil Yoo, Jeffrey J. Johnston, Margaret Gibson, Gilad Evrony, William B. Rizzo, Isabelle Thiffault, Scott T. Younger, Tom Curran, Aaron M. Wenger, Elin Grundberg, and Tomi Pastinen

Subjects

Science

Abstract

Abstract Long-read HiFi genome sequencing allows for accurate detection and direct phasing of single nucleotide variants, indels, and structural variants. Recent algorithmic development enables simultaneous detection of CpG methylation for analysis of regulatory element activity directly in HiFi reads. We present a comprehensive haplotype resolved 5-base HiFi genome sequencing dataset from a rare disease cohort of 276 samples in 152 families to identify rare (~0.5%) hypermethylation events. We find that 80% of these events are allele-specific and predicted to cause loss of regulatory element activity. We demonstrate heritability of extreme hypermethylation including rare cis variants associated with short (~200 bp) and large hypermethylation events (>1 kb), respectively. We identify repeat expansions in proximal promoters predicting allelic gene silencing via hypermethylation and demonstrate allelic transcriptional events downstream. On average 30–40 rare hypermethylation tiles overlap rare disease genes per patient, providing indications for variation prioritization including a previously undiagnosed pathogenic allele in DIP2B causing global developmental delay. We propose that use of HiFi genome sequencing in unsolved rare disease cases will allow detection of unconventional diseases alleles due to loss of regulatory element activity.

Published

2023

3. Author Correction: CHD3 helicase domain mutations cause a neurodevelopmental syndrome with macrocephaly and impaired speech and language

Author

Lot Snijders Blok, Justine Rousseau, Joanna Twist, Sophie Ehresmann, Motoki Takaku, Hanka Venselaar, Lance H. Rodan, Catherine B. Nowak, Jessica Douglas, Kathryn J. Swoboda, Marcie A. Steeves, Inderneel Sahai, Connie T. R. M. Stumpel, Alexander P. A. Stegmann, Patricia Wheeler, Marcia Willing, Elise Fiala, Aaina Kochhar, William T. Gibson, Ana S. A. Cohen, Ruky Agbahovbe, A. Micheil Innes, P. Y. Billie Au, Julia Rankin, Ilse J. Anderson, Steven A. Skinner, Raymond J. Louie, Hannah E. Warren, Alexandra Afenjar, Boris Keren, Caroline Nava, Julien Buratti, Arnaud Isapof, Diana Rodriguez, Raymond Lewandowski, Jennifer Propst, Ton van Essen, Murim Choi, Sangmoon Lee, Jong H. Chae, Susan Price, Rhonda E. Schnur, Ganka Douglas, Ingrid M. Wentzensen, Christiane Zweier, André Reis, Martin G. Bialer, Christine Moore, Marije Koopmans, Eva H. Brilstra, Glen R. Monroe, Koen L. I. van Gassen, Ellen van Binsbergen, Ruth Newbury-Ecob, Lucy Bownass, Ingrid Bader, Johannes A. Mayr, Saskia B. Wortmann, Kathy J. Jakielski, Edythe A. Strand, Katja Kloth, Tatjana Bierhals, The DDD study, John D. Roberts, Robert M. Petrovich, Shinichi Machida, Hitoshi Kurumizaka, Stefan Lelieveld, Rolph Pfundt, Sandra Jansen, Pelagia Deriziotis, Laurence Faivre, Julien Thevenon, Mirna Assoum, Lawrence Shriberg, Tjitske Kleefstra, Han G. Brunner, Paul A. Wade, Simon E. Fisher, and Philippe M. Campeau

Subjects

Science

Abstract

The HTML and PDF versions of this Article were updated after publication to remove images of one individual from Figure 1.

Published

2019

4. CHD3 helicase domain mutations cause a neurodevelopmental syndrome with macrocephaly and impaired speech and language

Author

Lot Snijders Blok, Justine Rousseau, Joanna Twist, Sophie Ehresmann, Motoki Takaku, Hanka Venselaar, Lance H. Rodan, Catherine B. Nowak, Jessica Douglas, Kathryn J. Swoboda, Marcie A. Steeves, Inderneel Sahai, Connie T. R. M. Stumpel, Alexander P. A. Stegmann, Patricia Wheeler, Marcia Willing, Elise Fiala, Aaina Kochhar, William T. Gibson, Ana S. A. Cohen, Ruky Agbahovbe, A. Micheil Innes, P. Y. Billie Au, Julia Rankin, Ilse J. Anderson, Steven A. Skinner, Raymond J. Louie, Hannah E. Warren, Alexandra Afenjar, Boris Keren, Caroline Nava, Julien Buratti, Arnaud Isapof, Diana Rodriguez, Raymond Lewandowski, Jennifer Propst, Ton van Essen, Murim Choi, Sangmoon Lee, Jong H. Chae, Susan Price, Rhonda E. Schnur, Ganka Douglas, Ingrid M. Wentzensen, Christiane Zweier, André Reis, Martin G. Bialer, Christine Moore, Marije Koopmans, Eva H. Brilstra, Glen R. Monroe, Koen L. I. van Gassen, Ellen van Binsbergen, Ruth Newbury-Ecob, Lucy Bownass, Ingrid Bader, Johannes A. Mayr, Saskia B. Wortmann, Kathy J. Jakielski, Edythe A. Strand, Katja Kloth, Tatjana Bierhals, The DDD study, John D. Roberts, Robert M. Petrovich, Shinichi Machida, Hitoshi Kurumizaka, Stefan Lelieveld, Rolph Pfundt, Sandra Jansen, Pelagia Deriziotis, Laurence Faivre, Julien Thevenon, Mirna Assoum, Lawrence Shriberg, Tjitske Kleefstra, Han G. Brunner, Paul A. Wade, Simon E. Fisher, and Philippe M. Campeau

Subjects

Science

Abstract

Chromodomain Helicase DNA-binding (CHD) proteins have been implicated in neurodevelopmental processes. Here, the authors identify missense variants in CHD3 that disturb its chromatin remodeling activities and cause a neurodevelopmental disorder with macrocephaly and speech and language impairment.

Published

2018

5. Loss of maternal EED results in postnatal overgrowth

Author

Lexie Prokopuk, Jessica M. Stringer, Craig R. White, Rolf H. A. M. Vossen, Stefan J. White, Ana S. A. Cohen, William T. Gibson, and Patrick S. Western

Subjects

Epigenetic inheritance, Germ, Oocyte, Polycomb, Histone, Weaver, Medicine, Genetics, QH426-470

Abstract

Abstract Background Investigating how epigenetic information is transmitted through the mammalian germline is the key to understanding how this information impacts on health and disease susceptibility in offspring. EED is essential for regulating the repressive histone modification, histone 3 lysine 27 tri-methylation (H3K27me3) at many developmental genes. Results In this study, we used oocyte-specific Zp3-Cre recombinase (Zp3Cre) to delete Eed specifically in mouse growing oocytes, permitting the study of EED function in oocytes and the impact of depleting EED in oocytes on outcomes in offspring. As EED deletion occurred only in growing oocytes and females were mated to normal wild type males, this model allowed the study of oocyte programming without confounding factors such as altered in utero environment. Loss of EED from growing oocytes resulted in a significant overgrowth phenotype that persisted into adult life. Significantly, this involved increased adiposity (total fat) and bone mineral density in offspring. Similar overgrowth occurs in humans with Cohen-Gibson (OMIM 617561) and Weaver (OMIM 277590) syndromes, that result from de novo germline mutations in EED or its co-factor EZH2, respectively. Consistent with a role for EZH2 in human oocytes, we demonstrate that de novo germline mutations in EZH2 occurred in the maternal germline in some cases of Weaver syndrome. However, deletion of Ezh2 in mouse oocytes resulted in a distinct phenotype compared to that resulting from oocyte-specific deletion of Eed. Conclusions This study provides novel evidence that altering EED-dependent oocyte programming leads to compromised offspring growth and development in the next generation.

Published

2018

6. Phenotypic expansion and variable expressivity in individuals with JARID2 ‐related intellectual disability: A case series

Author

Maxime Cadieux‐Dion, Emily Farrow, Isabelle Thiffault, Ana S. A. Cohen, Holly Welsh, Lauren Bartik, Caitlin Schwager, Kendra Engleman, Dihong Zhou, Lei Zhang, Elena Repnikova, Shivarajan M. Amudhavalli, and Carol J. Saunders

Subjects

Phenotype, DNA Copy Number Variations, Intellectual Disability, Polycomb Repressive Complex 2, Genetics, Humans, Exons, Autistic Disorder, Genetics (clinical)

Abstract

Loss of function variants in JARID2 were recently reported in 16 patients with a neurodevelopmental disorder characterized by delays, intellectual and learning disability, autism, behavioral abnormalities, and dysmorphic features. Most cases were de novo, with only one variant inherited from an affected parent. Here, we present seven additional individuals from five families with pathogenic or likely pathogenic JARID2 variants, confirming this gene-disease association and highlighting palatal abnormalities and heart defects as part of the phenotype. In addition, we report inheritance of JARID2 variants from mildly affected parents, demonstrating the variable expressivity of the disease. We also note the high prevalence of intragenic JARID2 copy number variants, emphasizing the importance of exon-level analysis.

Published

2022

7. Variants in the zinc transporter TMEM163 cause a hypomyelinating leukodystrophy

Author

Michelle C do Rosario, Guillermo Rodriguez Bey, Bruce Nmezi, Fang Liu, Talia Oranburg, Ana S A Cohen, Keith A Coffman, Maya R Brown, Kirill Kiselyov, Quinten Waisfisz, Myrthe T Flohil, Shahyan Siddiqui, Jill A Rosenfeld, Alejandro Iglesias, Katta Mohan Girisha, Nicole I Wolf, Quasar Saleem Padiath, Anju Shukla, Human genetics, CCA - Cancer biology and immunology, Pediatrics, and Amsterdam Neuroscience - Cellular & Molecular Mechanisms

Subjects

Zinc, Pelizaeus-Merzbacher Disease, Mutation, Missense, Humans, Membrane Proteins, Neurology (clinical), Myelin Sheath

Abstract

Hypomyelinating leukodystrophies comprise a subclass of genetic disorders with deficient myelination of the CNS white matter. Here we report four unrelated families with a hypomyelinating leukodystrophy phenotype harbouring variants in TMEM163 (NM_030923.5). The initial clinical presentation resembled Pelizaeus–Merzbacher disease with congenital nystagmus, hypotonia, delayed global development and neuroimaging findings suggestive of significant and diffuse hypomyelination. Genomic testing identified three distinct heterozygous missense variants in TMEM163 with two unrelated individuals sharing the same de novo variant. TMEM163 is highly expressed in the CNS particularly in newly myelinating oligodendrocytes and was recently revealed to function as a zinc efflux transporter. All the variants identified lie in highly conserved residues in the cytoplasmic domain of the protein, and functional in vitro analysis of the mutant protein demonstrated significant impairment in the ability to efflux zinc out of the cell. Expression of the mutant proteins in an oligodendroglial cell line resulted in substantially reduced mRNA expression of key myelin genes, reduced branching and increased cell death. Our findings indicate that variants in TMEM163 cause a hypomyelinating leukodystrophy and uncover a novel role for zinc homeostasis in oligodendrocyte development and myelin formation.

Published

2022

8. Haploinsufficiency of the basic helix–loop–helix transcription factor HAND2 causes congenital heart defects

Author

Wahab A. Khan, Stuart A. Scott, Huanzhi Shi, Ram Singh, Christopher Simotas, Bryn D. Webb, Ana S. A. Cohen, and Lisa Edelmann

Subjects

0301 basic medicine, Genetics, Proband, Heart morphogenesis, animal structures, biology, Pulmonic stenosis, GATA4, 030105 genetics & heredity, medicine.disease, 03 medical and health sciences, Exon, 030104 developmental biology, embryonic structures, biology.protein, medicine, HAND2, Haploinsufficiency, Genetics (clinical), Tetralogy of Fallot

Abstract

Congenital heart defects (CHDs) are caused by a disruption in heart morphogenesis, which is dependent, in part, on a network of transcription factors (TFs) that regulate myocardial development. Heterozygous sequence variants in the basic helix-loop-helix TF gene heart and neural crest derivatives expressed 2 (HAND2) have been reported among some patients with CHDs; however, HAND2 has not yet been established as a Mendelian disease gene. We report a 31-month-old male with unicommissural unicuspid aortic valve, moderate aortic stenosis, and mild pulmonic stenosis. Chromosome analysis revealed a normal 46,XY karyotype, and a CHD sequencing panel was negative for pathogenic variants in NKX2.5, GATA4, TBX5, and CHD7. However, chromosomal microarray (CMA) testing identified a heterozygous 546.0-kb deletion on chromosome 4q34.1 (174364195_174910239[GRCh37/hg19]) that included exons 1 and 2 of SCRG1, HAND2, and HAND2-AS1. Familial CMA testing determined that the deletion was paternally inherited, which supported a likely pathogenic classification as the proband's father had previously undergone surgery for Tetralogy of Fallot. The family history was also notable for a paternal uncle who had previously died from complications related to an unknown heart defect. Taken together, this first report of a HAND2 and HAND2-AS1 deletion in a family with CHDs strongly supports haploinsufficiency of HAND2 as an autosomal dominant cause of CHD.

Published

2020

9. Clinical Validation of Genome Reference Consortium Human Build 38 in a Laboratory Utilizing Next-Generation Sequencing Technologies

Author

Lisa A Lansdon, Maxime Cadieux-Dion, John C Herriges, Jeffrey Johnston, Byunggil Yoo, Joseph T Alaimo, Isabelle Thiffault, Neil Miller, Ana S A Cohen, Elena A Repnikova, Lei Zhang, Midhat S Farooqi, Emily G Farrow, and Carol J Saunders

Subjects

3-Oxo-5-alpha-Steroid 4-Dehydrogenase, Genome, Human, Biochemistry (medical), Clinical Biochemistry, Receptor-Like Protein Tyrosine Phosphatases, Class 3, High-Throughput Nucleotide Sequencing, Humans, Membrane Proteins, Cell Cycle Proteins, Exome, Laboratories, Alleles

Abstract

Background Laboratories utilizing next-generation sequencing align sequence data to a standardized human reference genome (HRG). Several updated versions, or builds, have been released since the original HRG in 2001, including the Genome Reference Consortium Human Build 38 (GRCh38) in 2013. However, most clinical laboratories still use GRCh37, which was released in 2009. We report our laboratory’s clinical validation of GRCh38. Methods Migration to GRCh38 was validated by comparing the coordinates (lifting over) of 9443 internally curated variants from GRCh37 to GRCh38, globally comparing protein coding sequence variants aligned with GRCh37 vs GRCh38 from 917 exomes, assessing genes with known discrepancies, comparing coverage differences, and establishing the analytic sensitivity and specificity of variant detection using Genome in a Bottle data. Results Eight discrepancies, due to strand swap or reference base, were observed. Three clinically relevant variants had the GRCh37 alternate allele as the reference allele in GRCh38. A comparison of 88 295 calls between builds identified 8 disease-associated genes with sequence differences: ABO, BNC2, KIZ, NEFL, NR2E3, PTPRQ, SHANK2, and SRD5A2. Discrepancies in coding regions in GRCh37 were resolved in GRCh38. Conclusions There were a small number of clinically significant changes between the 2 genome builds. GRCh38 provided improved detection of nucleotide changes due to the resolution of discrepancies present in GRCh37. Implementation of GRCh38 results in more accurate and consistent reporting.

Published

2022

10. Rare SUZ12 variants commonly cause an overgrowth phenotype

Author

Shawn E. McCandless, Ana S A Cohen, Causes Study, William T. Gibson, E. Lopez-Rangel, Ruky Agbahovbe, Michael J. Gambello, KS Yeung, Shayna Svihovec, Brian H.Y. Chung, Stephen R. Braddock, Margarita Saenz, Lynne M. Bird, Rhonda E. Schnur, Sanaa Choufani, Rosanna Weksberg, Hailey Pinz, Sanjiv K Bhalla, Nataliya Tkachenko, Steven J.M. Jones, Kathleen Brown, Sharri Cyrus, HM Luk, Kristiina Avela, Jianghong An, Aixa Gonzalez Garcia, and Kirsty McWalter

Subjects

Male, media_common.quotation_subject, Nonsense, Biology, Frameshift mutation, 03 medical and health sciences, 0302 clinical medicine, Intellectual Disability, Intellectual disability, Genetics, SUZ12, medicine, Humans, Missense mutation, Epigenetics, Child, Growth Disorders, Genetics (clinical), 030304 developmental biology, media_common, Weaver syndrome, 0303 health sciences, Infant, Newborn, Polycomb Repressive Complex 2, Infant, medicine.disease, Phenotype, Neoplasm Proteins, Child, Preschool, Mutation, Female, 030217 neurology & neurosurgery, Transcription Factors

Abstract

The Polycomb repressive complex 2 is an epigenetic writer and recruiter with a role in transcriptional silencing. Constitutional pathogenic variants in its component proteins have been found to cause two established overgrowth syndromes: Weaver syndrome (EZH2-related overgrowth) and Cohen-Gibson syndrome (EED-related overgrowth). Imagawa et al. (2017) initially reported a singleton female with a Weaver-like phenotype with a rare coding SUZ12 variant-the same group subsequently reported two additional affected patients. Here we describe a further 10 patients (from nine families) with rare heterozygous SUZ12 variants who present with a Weaver-like phenotype. We report four frameshift, two missense, one nonsense, and two splice site variants. The affected patients demonstrate variable pre- and postnatal overgrowth, dysmorphic features, musculoskeletal abnormalities and developmental delay/intellectual disability. Some patients have genitourinary and structural brain abnormalities, and there may be an association with respiratory issues. The addition of these 10 patients makes a compelling argument that rare pathogenic SUZ12 variants frequently cause overgrowth, physical abnormalities, and abnormal neurodevelopmental outcomes in the heterozygous state. Pathogenic SUZ12 variants may be de novo or inherited, and are sometimes inherited from a mildly-affected parent. Larger samples sizes will be needed to elucidate whether one or more clinically-recognizable syndromes emerge from different variant subtypes.

Published

2019

11. Deletion of

Author

Ram, Singh, Ana S A, Cohen, Cathryn, Poulton, Tina Duelund, Hjortshøj, Moe, Akahira-Azuma, Geetu, Mendiratta, Wahab A, Khan, Dimitar N, Azmanov, Karen J, Woodward, Maria, Kirchhoff, Lisong, Shi, Lisa, Edelmann, Gareth, Baynam, Stuart A, Scott, and Ethylin Wang, Jabs

Subjects

Male, Research Report, Heterozygote, Adolescent, DNA Copy Number Variations, Developmental Disabilities, widely patent coronal suture, global developmental delay, Proto-Oncogene Protein c-ets-2, Intellectual Disability, Humans, Genetic Predisposition to Disease, Genetic Testing, congenital strabismus, Child, Genetic Association Studies, Skull, Membrane Proteins, Repressor Proteins, craniosynostosis, Phenotype, Neurodevelopmental Disorders, intellectual disability, Child, Preschool, Female, Sodium-Potassium-Exchanging ATPase, macrocephaly at birth, Gene Deletion, Transcription Factors

Abstract

The ETS2 repressor factor (ERF) is a transcription factor in the RAS-MEK-ERK signal transduction cascade that regulates cell proliferation and differentiation, and pathogenic sequence variants in the ERF gene cause variable craniosynostosis inherited in an autosomal dominant pattern. The reported ERF variants are largely loss-of-function, implying haploinsufficiency as a primary disease mechanism; however, ERF gene deletions have not been reported previously. Here we describe three probands with macrocephaly, craniofacial dysmorphology, and global developmental delay. Clinical genetic testing for fragile X and other relevant sequencing panels were negative; however, chromosomal microarray identified heterozygous deletions (63.7–583.2 kb) on Chromosome 19q13.2 in each proband that together included five genes associated with Mendelian diseases (ATP1A3, ERF, CIC, MEGF8, and LIPE). Parental testing indicated that the aberrations were apparently de novo in two of the probands and were inherited in the one proband with the smallest deletion. Deletion of ERF is consistent with the reported loss-of-function ERF variants, prompting clinical copy-number-variant classifications of likely pathogenic. Moreover, the recent characterization of heterozygous loss-of-function CIC sequence variants as a cause of intellectual disability and neurodevelopmental disorders inherited in an autosomal dominant pattern is also consistent with the developmental delays and intellectual disabilities identified among the two probands with CIC deletions. Taken together, this case series adds to the previously reported patients with ERF and/or CIC sequence variants and supports haploinsufficiency of both genes as a mechanism for a variable syndromic cranial phenotype with developmental delays and intellectual disability inherited in an autosomal dominant pattern.

Published

2020

12. DNA methylation signature for EZH2 functionally classifies sequence variants in three PRC2 complex genes

Author

Michael Brudno, Andrei L. Turinsky, Sharri Cyrus, David Chitayat, Brian H.Y. Chung, Maria Iascone, Luk Ho Ming, Tom Cushing, Eri Imagawa, Ana S A Cohen, Lynne M. Bird, Nobuhiko Okamoto, Vivienne McConnell, Stephen W. Scherer, Rosanna Weksberg, Jack Brzezinski, Kopal Garg, Carol L. Clericuzio, Roberto Mendoza-Londono, Susan M. White, Tianren Wang, Miranda Splitt, Naomichi Matsumoto, Sanaa Choufani, Guiseppe Testa, Romano Tenconi, Alessandro Vitriolo, Jerry Machado, Katrina Tatton-Brown, I. Karen Temple, Cheryl Cytrynbaum, Frances Flinter, William T. Gibson, Oana Caluseriu, Bronwyn Kerr, Eric Chater-Diehl, Sarah J. Goodman, and Sally Ann Lynch

Subjects

0301 basic medicine, DNA methylation signature, Male, medicine.disease_cause, Medical and Health Sciences, Cohort Studies, Craniofacial Abnormalities, Congenital, 0302 clinical medicine, SUZ12, Child, Genetics (clinical), EED, Genetics & Heredity, Mutation, biology, Mosaicism, EZH2, Polycomb Repressive Complex 2, Biological Sciences, overgrowth syndromes, Phenotype, Neoplasm Proteins, 030220 oncology & carcinogenesis, Histone methyltransferase, Child, Preschool, DNA methylation, Female, Abnormalities, PRC2, Multiple, Hand Deformities, Congenital, Adult, Adolescent, Mutation, Missense, Computational biology, macromolecular substances, Article, 03 medical and health sciences, Young Adult, Intellectual Disability, Genetics, medicine, Congenital Hypothyroidism, Humans, Abnormalities, Multiple, Enhancer of Zeste Homolog 2 Protein, Preschool, Gene, dNaM, Infant, Reproducibility of Results, Hand Deformities, DNA Methylation, 030104 developmental biology, biology.protein, Missense, Transcription Factors

Abstract

Weaver syndrome (WS), an overgrowth/intellectual disability syndrome (OGID), is caused by pathogenic variants in the histone methyltransferase EZH2, which encodes a core component of the Polycomb repressive complex-2 (PRC2). Using genome-wide DNA methylation (DNAm) data for 187 individuals with OGID and 969 control subjects, we show that pathogenic variants in EZH2 generate a highly specific and sensitive DNAm signature reflecting the phenotype of WS. This signature can be used to distinguish loss-of-function from gain-of-function missense variants and to detect somatic mosaicism. We also show that the signature can accurately classify sequence variants in EED and SUZ12, which encode two other core components of PRC2, and predict the presence of pathogenic variants in undiagnosed individuals with OGID. The discovery of a functionally relevant signature with utility for diagnostic classification of sequence variants in EZH2, EED, and SUZ12 supports the emerging paradigm shift for implementation of DNAm signatures into diagnostics and translational research.

Published

2020

13. Deletion of ERF and CIC causes abnormal skull morphology and global developmental delay

Author

Ana S. A. Cohen, Gareth Baynam, Ethylin Wang Jabs, Tina Duelund Hjortshøj, Dimitar N. Azmanov, Karen J. Woodward, Wahab A. Khan, Cathryn Poulton, Ram Singh, Maria Kirchhoff, Stuart A. Scott, Lisong Shi, Geetu Mendiratta, Lisa Edelmann, and Moe Akahira-Azuma

Subjects

Proband, Genetics, Macrocephaly, General Medicine, Biology, Phenotype, symbols.namesake, ATP1A3, Mendelian inheritance, symbols, medicine, Global developmental delay, medicine.symptom, Haploinsufficiency, Gene

Abstract

The ETS2 repressor factor (ERF) is a transcription factor in the RAS-MEK-ERK signal transduction cascade that regulates cell proliferation and differentiation, and pathogenic sequence variants in the ERF gene cause variable craniosynostosis inherited in an autosomal dominant pattern. The reported ERF variants are largely loss-of-function, implying haploinsufficiency as a primary disease mechanism; however, ERF gene deletions have not been reported previously. Here we describe three probands with macrocephaly, craniofacial dysmorphology, and global developmental delay. Clinical genetic testing for fragile X and other relevant sequencing panels were negative; however, chromosomal microarray identified heterozygous deletions (63.7–583.2 kb) on Chromosome 19q13.2 in each proband that together included five genes associated with Mendelian diseases (ATP1A3, ERF, CIC, MEGF8, and LIPE). Parental testing indicated that the aberrations were apparently de novo in two of the probands and were inherited in the one proband with the smallest deletion. Deletion of ERF is consistent with the reported loss-of-function ERF variants, prompting clinical copy-number-variant classifications of likely pathogenic. Moreover, the recent characterization of heterozygous loss-of-function CIC sequence variants as a cause of intellectual disability and neurodevelopmental disorders inherited in an autosomal dominant pattern is also consistent with the developmental delays and intellectual disabilities identified among the two probands with CIC deletions. Taken together, this case series adds to the previously reported patients with ERF and/or CIC sequence variants and supports haploinsufficiency of both genes as a mechanism for a variable syndromic cranial phenotype with developmental delays and intellectual disability inherited in an autosomal dominant pattern.

Published

2021

14. A novel mutation in EED associated with overgrowth

Author

Sanjiv K Bhalla, Beyhan Tüysüz, Yaoqing Shen, William T. Gibson, Steven J.M. Jones, and Ana S A Cohen

Subjects

Adult, Male, medicine.medical_specialty, DNA Mutational Analysis, Mutation, Missense, macromolecular substances, Biology, medicine.disease_cause, Craniofacial Abnormalities, Diagnosis, Differential, Molecular genetics, Congenital Hypothyroidism, Genetics, medicine, Humans, Abnormalities, Multiple, Epigenetics, Growth Disorders, Genetics (clinical), Weaver syndrome, Mutation, EZH2, Polycomb Repressive Complex 2, medicine.disease, Phenotype, Overgrowth syndrome, Medical genetics, Hand Deformities, Congenital

Abstract

In a patient suspected clinically to have Weaver syndrome, we ruled out mutations in EZH2 and NSD1, then identified a previously undescribed de novo mutation in EZH2's partner protein EED. Both proteins are members of the Polycomb Repressive Complex 2 that maintains gene silencing. On the basis of the similarities of the patient's phenotype to Weaver syndrome, which is caused by de novo mutations in EZH2, and on other lines of evidence including mouse Eed hypomorphs, we characterize this mutation as probably pathogenic for a Weaver-like overgrowth syndrome. This is the first report of overgrowth and related phenotypes associated with a constitutional mutation in human EED.

Published

2015

15. Corrigendum: A novel mutation in EED associated with overgrowth

Author

Ana S A, Cohen, Beyhan, Tuysuz, Yaoqing, Shen, Sanjiv K, Bhalla, Steven J M, Jones, and William T, Gibson

Published

2017

16. Somatic mosaicism for the p.His1047Arg mutation in PIK3CA in a girl with mesenteric lipomatosis

Author

Steven J.M. Jones, Stephen Yip, Christof Senger, William T. Gibson, Patrice Eydoux, Ana S A Cohen, Margaret L. McKinnon, Qing-San Xiang, Scott A. Lear, Jasna Levi, Raj Attariwala, Christof Borchers, Wayne Picker, Katelin N. Townsend, Siu-Li Yong, Amy Lum, Robert Everett, Lila Yewchuk, and Joelle Tan

Subjects

medicine.medical_specialty, Pathology, Mri imaging, Class I Phosphatidylinositol 3-Kinases, Lipomatosis, Adipose tissue, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, Deep sequencing, Phosphatidylinositol 3-Kinases, Internal medicine, Genetics, medicine, Humans, Mesentery, Child, neoplasms, Genetics (clinical), Mutation, Mosaicism, Infant, medicine.disease, Phenotype, 3. Good health, Endocrinology, Adipose Tissue, Somatic mosaicism, Child, Preschool, Female

Abstract

We describe a patient who presented with a localized growth of mature fat tissue, which was surgically removed. MRI imaging identified diffuse increase in visceral adipose tissue. Targeted deep sequencing of the resected tissue uncovered a p.H1047R variant in PIK3CA, which was absent in blood. This report expands the phenotypic spectrum of mosaic PIK3CA mutations. © 2014 Wiley Periodicals, Inc.

Published

2014

17. Weaver Syndrome-Associated EZH2 Protein Variants Show Impaired Histone Methyltransferase Function in Vitro

Author

Ana S A Cohen, Valentina Milano, Natália Tkachenko, M I Van Allen, Damian B. Yap, Chieko Chijiwa, María A Ramos-Arroyo, M. E. Suzanne Lewis, Katelin N. Townsend, Margaret L. McKinnon, Mélanie Fradin, Colin J. D. Ross, Jieqing Xu, William B. Dobyns, William T. Gibson, David D. Weaver, University of British Columbia (UBC), Service de génétique clinique [Rennes], Université de Rennes (UR)-CHU Pontchaillou [Rennes]-hôpital Sud, Institute for Health Research, Centro Hospitalar do Porto, Policlinico Universitario 'A. Gemelli', Institut de Génétique et Développement de Rennes (IGDR), Université de Rennes (UR)-Centre National de la Recherche Scientifique (CNRS)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), University of Washington [Seattle], Seattle Children's Hospital, Department of Medical and Molecular Genetics, Indiana University School of Medicine, Indiana University System-Indiana University System, Contract grant sponsors: Canadian Institutes of Health Research (CIHR MOP-119595) Government of Canada through the Canadian Institutes of Health Research. Grant Number: CIHR MOP-119595, Université de Rennes 1 (UR1), Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES)-CHU Pontchaillou [Rennes]-hôpital Sud, Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique )-Centre National de la Recherche Scientifique (CNRS)-Université de Rennes 1 (UR1), Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES), and Jonchère, Laurent

Subjects

0301 basic medicine, Male, Histone methyltransferase activity, Mutant, macromolecular substances, [SDV.GEN.GH] Life Sciences [q-bio]/Genetics/Human genetics, Craniofacial Abnormalities, 03 medical and health sciences, Histone H3, Genetics, medicine, Congenital Hypothyroidism, Humans, childhood cancer, Abnormalities, Multiple, Enhancer of Zeste Homolog 2 Protein, EZH2, Genetics (clinical), Research Articles, Weaver syndrome, H3K27, biology, histone methyltransferase, Infant, Newborn, Polycomb Repressive Complex 2, Infant, Methylation, Histone-Lysine N-Methyltransferase, medicine.disease, 030104 developmental biology, [SDV.GEN.GH]Life Sciences [q-bio]/Genetics/Human genetics, Histone methyltransferase, biology.protein, Histone Methyltransferases, Female, PRC2, Hand Deformities, Congenital, Research Article

Abstract

International audience; Weaver syndrome (WS) is a rare congenital disorder characterized by generalized overgrowth, macrocephaly, specific facial features, accelerated bone age, intellectual disability, and susceptibility to cancers. De novo mutations in the enhancer of zeste homolog 2 (EZH2) have been shown to cause WS. EZH2 is a histone methyltransferase that acts as the catalytic agent of the polycomb-repressive complex 2 (PRC2) to maintain gene repression via methylation of lysine 27 on histone H3 (H3K27). Functional studies investigating histone methyltransferase activity of mutant EZH2 from various cancers have been reported, while WS-associated mutations remain poorly characterized. To investigate the role of EZH2 in WS, we performed functional studies using artificially-assembled PRC2 complexes containing mutagenized human EZH2 that reflected the codon changes predicted from patients with WS. We found that WS-associated amino acid alterations reduce the histone methyltransferase function of EZH2 in this in vitro assay. Our results support the hypothesis that WS is caused by constitutional mutations in EZH2 that alter the histone methyltransferase function of PRC2. However, histone methyltransferase activities of different EZH2 variants do not appear to correlate directly with the phenotypic variability between WS patients and individuals with a common c.553G\textgreaterC (p.Asp185His) polymorphism in EZH2. This article is protected by copyright. All rights reserved

Published

2016

18. EED-associated overgrowth in a second male patient

Author

William T. Gibson and Ana S A Cohen

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, DNA Mutational Analysis, Biology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Molecular genetics, Genetics, medicine, Humans, Genetics (clinical), Growth Disorders, Mutation, Cytogenetics, Polycomb Repressive Complex 2, Brain, Facies, Sequence Analysis, DNA, Phenotype, Magnetic Resonance Imaging, Human genetics, Pedigree, 030104 developmental biology, Genetic epidemiology, Statistical genetics, Child, Preschool, Medical genetics, Female, 030217 neurology & neurosurgery

Abstract

Following our discovery that constitutional mutations in EED can cause overgrowth, we screened our cohort of patients with Weaver-like features for mutations in this gene. Here we describe a second patient with a different, rare and de novo mutation in EED. Phenotypic overlap with our first case of EED-associated overgrowth is significant. Now that we have found two unrelated families of different ethnicities, with a similar rare phenotype, both associated with de novo mutations in this member of the PRC2 complex, we are confident that EED is indeed a novel overgrowth gene.

Published

2015

19. Correction: Corrigendum: A novel mutation in EED associated with overgrowth

Author

Sanjiv K Bhalla, Ana S A Cohen, Beyhan Tüysüz, Steven J.M. Jones, Yaoqing Shen, and William T. Gibson

Subjects

Genetics, medicine.medical_specialty, Developmental genetics, Statistical genetics, medicine, Medical genetics, Biology, Novel mutation, Genetics (clinical), Genealogy, Human genetics

Abstract

Correction to: Journal of Human Genetics (2015) 60, 339–342; doi:10.1038/jhg.2015.26; published online 19 March 2015 Since the publication of the above article, the authors of the above paper have noticed an error in Figure 1. In the pedigree presented (Figure 1i), vertical connectors to individualsII-1 and II-2 were incorrectly omitted.

Published

2017

20. Alternating hypoglycemia and hyperglycemia in a toddler with a homozygous p.R1419H ABCC8 mutation: an unusual clinical picture

Author

Millan S. Patel, Jean-Pierre Chanoine, Shira Harel, Khalid Hussain, Clara D.M. van Karnebeek, Sarah E. Flanagan, Harley T. Kurata, Jaques Courtade, Ana S A Cohen, William T. Gibson, Jenny B.W. Li, Sian Ellard, Kamilla Schlade-Bartusiak, and Other departments

Subjects

Adult, Male, Gerontology, Endocrinology, Diabetes and Metabolism, Mutation, Missense, Clinical science, Library science, Arginine, Sulfonylurea Receptors, Child health, Consanguinity, Endocrinology, Humans, Medicine, Family, Histidine, Toddler, Cells, Cultured, business.industry, Homozygote, Medical school, Infant, Amino acid substitution, Hypoglycemia, Pedigree, Phenotype, Amino Acid Substitution, Hyperglycemia, Pediatrics, Perinatology and Child Health, Female, business

Abstract

J Pediatr Endocr Met 2015; aop*Corresponding author: William T. Gibson, Child and Family Research Institute, Department of Medical Genetics, British Columbia Children ’ s Hospital, 950 West 28th Avenue, Vancouver, BC, V5Z 4H4, Canada, Phone: + 1-604-875-2000 ext. 5523, ax: F + 1-604-875-2373, mE- ail: wtgibson@cfri.ubc.ca Shira Harel and Jean-Pierre Chanoine: EndocrinologyandDiabetes Unit, Department of Pediatrics, British Columbia Children ’ s Hospital, University of British Columbia, Vancouver, Canada Ana S.A. Cohen, Millan Patel and William T. Gibson: Deparmentt of Medical Genetics, University of British Columbia, Vancouver, Canada ; and Child and Family Research Institute, Vancouver, Canada Khalid Hussain: Institute ofBiomedicalandClinicalSc ience, University of Exeter Medical School, Exeter, UK ; and Developmental Endocrinology Research Group, Clinical and Molecular Genetics, Institute of Child Health, University College London, London, UK Sarah E. Flanagan and Sian Ellard: Institute of Biomedical and Clinical Science, University of Exeter Medical School, Exeter, UK Kamilla Schlade-Bartusiak: Childand amilyF Rese arch Institute, Vancouver, Canada ; and Depar tment of Pathology and Laboratory Medicine, University of British Columbia, Vancouver, Canada Jaques Courtade: ChildandamilyF Research Institute, Vancouver, Canada Jenny B.W. Li and Harley Kurata: Deparmentt ofAnesthesiolog ,yPharmacology and Therapeutics, University of British Columbia, Vancouver, Canada Clara Van Karnebeek: Division ofBiochemicalDiseases, Deparmentt of Pediatrics, British Columbia Children ’ s Hospital, University of British Columbia, Vancouver, Canada

Published

2015

21. Mutations in POLR3A and POLR3B are a major cause of hypomyelinating leukodystrophies with or without dental abnormalities and/or hypogonadotropic hypogonadism

Author

Geneviève Bernard, Cyril Goizet, Adeline Vanderver, Sakkubai Naidu, Cathy A. Stevens, Matthis Synofzik, William T. Gibson, Martine Tétreault, Janina Gburek-Augustat, Ana S A Cohen, Hussein Daoud, Kether Guerrero, Bernard Brais, and Rocío Sánchez-Carpintero

Subjects

DNA Mutational Analysis, Molecular Sequence Data, genetics [Hypogonadism], Biology, medicine.disease_cause, Compound heterozygosity, Frameshift mutation, genetics [Hereditary Central Nervous System Demyelinating Diseases], Exon, Hypogonadotropic hypogonadism, Genetics, medicine, Intronic Mutation, Humans, genetics [RNA Polymerase III], ddc:610, Amino Acid Sequence, POLR3B protein, human, Gene, Genetics (clinical), Mutation, Base Sequence, Tooth Abnormalities, Hypogonadism, RNA Polymerase III, medicine.disease, Phenotype, Hereditary Central Nervous System Demyelinating Diseases, genetics [Tooth Abnormalities]

Abstract

Background Leukodystrophies are a heterogeneous group of inherited neurodegenerative disorders characterised by abnormal central nervous system white matter. Mutations in POLR3A and POLR3B genes were recently reported to cause four clinically overlapping hypomyelinating leukodystrophy phenotypes. Our aim was to investigate the presence and frequency of POLR3A and POLR3B mutations in patients with genetically unexplained hypomyelinating leukodystrophies with typical clinical and/or radiologic features of Pol III-related leukodystrophies. Methods The entire coding region and the flanking exon/intron boundaries of POLR3A and/or POLR3B genes were amplified and sequenced in 14 patients. Results Recessive mutations in POLR3A or POLR3B were uncovered in all 14 patients. Eight novel mutations were identified in POLR3A : six missenses, one nonsense, and one frameshift mutation. Seven patients carried compound heterozygous mutations in POLR3B , of whom six shared the common mutation in exon 15 (p.V523E). Seven novel mutations were identified in POLR3B : four missenses, two splice sites, and one intronic mutation. Conclusions To date, our group has described 37 patients, of whom 27 have mutations in POLR3A and 10 in POLR3B, respectively. Altogether, our results further support the proposal that POLR3A and POLR3B mutations are a major cause of hypomyelinating leukodystrophies and suggest that POLR3A mutations are more frequent.

Published

2013

22. MG-117 Clinical features of prc2 complex-related overgrowth due to mutations in eed

Author

William T. Gibson, Steven J.M. Jones, Yaoqing Shen, and Ana S A Cohen

Subjects

Genetics, Microarray, EZH2, Cancer, Biology, Bioinformatics, medicine.disease, Phenotype, Genotype, medicine, Epigenetics, Genetics (clinical), Exome sequencing, Weaver syndrome

Abstract

Our lab was the first to publish that constitutional mutations in the epigenetic regulator EZH2 cause Weaver Syndrome (WS). WS is characterised by overgrowth, increased height, large head, intellectual disability and susceptibility to various cancers. We found pathogenic mutations in EZH2 among 7 out of 45 individuals with Weaver-like features, of which two had developed malignancies prior to referral. Our efforts focus on determining characteristics that will help us predict the likelihood of WS patients developing cancer, through phenotype/genotype correlations and functional studies. As of yet, it is not clear whether screening for haematological malignancies in patients with Weaver syndrome would increase the patients’ chances of survival. Given that EZH2 is a histone-modifying enzyme known to be mutated in various somatic cancers, we hypothesised that constitutional mutations in other epigenetic regulators could explain the overgrowth features seen in our undiagnosed patients. To investigate this, we carried out whole exome sequencing in patients with paediatric syndromes similar to WS who did not have coding mutations in EZH2 . We have identified novel de novo mutations in EZH2’s partner protein EED in two patients to date. Both proteins are members of the Polycomb Repressive Complex 2 that maintains gene silencing. Based on the similarities of the patients’ phenotypes to WS, and on other lines of evidence including mouse Eed hypomorphs and an epigenetic signature that clustered with Weaver syndrome patients, we characterised these mutations as pathogenic. Here we describe additional features of overgrowth associated with constitutional mutations in human EED , which is also mutated somatically in various cancers. Samples from additional families are required to make a definitive link between mutations in these genes, Weaver-like syndromes, and cancer development. We continue to perform exome sequencing in patients with Weaver-like syndromes who have normal microarray studies and no mutations in EZH2 or NSD1 .

Published

2015