Your search keyword '"Dmitriy Niyazov"' showing total 47 results

1. P245: Oldest reported patients with RAB18 deficiency due to RAB3GAP1 gene mutations

Author

Dmitriy Niyazov and Jane Juusola

Subjects

Genetics, QH426-470, Medicine

Published

2024

2. Novel NUDT2 variant causes intellectual disability and polyneuropathy

Author

Frank Diaz, Shaweta Khosa, Dmitriy Niyazov, Hane Lee, Richard Person, Michelle M. Morrow, Rebecca Signer, Naghmeh Dorrani, Allison Zheng, Matthew Herzog, Robert Freundlich, Undiagnosed Diseases Network, J. Brandon Birath, Yurivia Cervantes‐Manzo, Julian A. Martinez‐Agosto, Christina Palmer, Stanley F. Nelson, Brent L. Fogel, and Shri K. Mishra

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Exome or genome sequencing was performed to identify the genetic etiology for the clinical presentation of global developmental delay, intellectual disability, and sensorimotor neuropathy with associated distal weakness in two unrelated families. A homozygous frameshift variant c.186delA (p.A63Qfs*3) in the NUDT2 gene was identified in cases 1 and 2 from one family and a third case from another family. Variants in NUDT2 were previously shown to cause intellectual disability, but here we expand the phenotype by demonstrating its association with distal upper and lower extremity weakness due to a sensorimotor polyneuropathy with demyelinating and/or axonal features.

Published

2020

3. Abnormal Bone Collagen Cross‐Linking in Osteogenesis Imperfecta/Bruck Syndrome Caused by Compound Heterozygous PLOD2 Mutations

Author

Charlotte Gistelinck, MaryAnn Weis, Jyoti Rai, Ulrike Schwarze, Dmitriy Niyazov, Kit M Song, Peter H Byers, and David R Eyre

Subjects

BRUCK SYNDROME, COLLAGEN, LYSYL HYDROXYLASE 2, OSTEOGENESIS IMPERFECTA, PLOD2, Orthopedic surgery, RD701-811, Diseases of the musculoskeletal system, RC925-935

Abstract

ABSTRACT Bruck syndrome (BS) is a congenital disorder characterized by joint flexion contractures, skeletal dysplasia, and increased bone fragility, which overlaps clinically with osteogenesis imperfecta (OI). On a genetic level, BS is caused by biallelic mutations in either FKBP10 or PLOD2. PLOD2 encodes the lysyl hydroxylase 2 (LH2) enzyme, which is responsible for the hydroxylation of cross‐linking lysine residues in fibrillar collagen telopeptide domains. This modification enables collagen to form chemically stable (permanent) intermolecular cross‐links in the extracellular matrix. Normal bone collagen develops a unique mix of such stable and labile lysyl‐oxidase–mediated cross‐links, which contribute to bone strength, resistance to microdamage, and crack propagation, as well as the ordered deposition of mineral nanocrystals within the fibrillar collagen matrix. Bone from patients with BS caused by biallelic FKBP10 mutations has been shown to have abnormal collagen cross‐linking; however, to date, no direct studies of human bone from BS caused by PLOD2 mutations have been reported. Here the results from a study of a 4‐year‐old boy with BS caused by compound heterozygous mutations in PLOD2 are discussed. Diminished hydroxylation of type I collagen telopeptide lysines but normal hydroxylation at triple‐helical sites was found. Consequently, stable trivalent cross‐links were essentially absent. Instead, allysine aldol dimeric cross‐links dominated as in normal skin collagen. Furthermore, in contrast to the patient's bone collagen, telopeptide lysines in cartilage type II collagen cross‐linked peptides from the patient's urine were normally hydroxylated. These findings shed light on the complex mechanisms that control the unique posttranslational chemistry and cross‐linking of bone collagen, and how, when defective, they can cause brittle bones and related connective tissue problems. © 2020 The Authors. JBMR Plus published by Wiley Periodicals LLC. on behalf of American Society for Bone and Mineral Research.

Published

2021

4. Novel Variants in Individuals with RYR1-Related Congenital Myopathies: Genetic, Laboratory, and Clinical Findings

Author

Joshua J. Todd, Muslima S. Razaqyar, Jessica W. Witherspoon, Tokunbor A. Lawal, Ami Mankodi, Irene C. Chrismer, Carolyn Allen, Mary D. Meyer, Anna Kuo, Monique S. Shelton, Kim Amburgey, Dmitriy Niyazov, Pierre Fequiere, Carsten G. Bönnemann, James J. Dowling, and Katherine G. Meilleur

Subjects

genotype, phenotype, RYR1, neuromuscular, magnetic resonance imaging, Neurology. Diseases of the nervous system, RC346-429

Abstract

The ryanodine receptor 1-related congenital myopathies (RYR1-RM) comprise a spectrum of slow, rare neuromuscular diseases. Affected individuals present with a mild-to-severe symptomatology ranging from proximal muscle weakness, hypotonia and joint contractures to scoliosis, ophthalmoplegia, and respiratory involvement. Although there is currently no FDA-approved treatment for RYR1-RM, our group recently conducted the first clinical trial in this patient population (NCT02362425). This study aimed to characterize novel RYR1 variants with regard to genetic, laboratory, muscle magnetic resonance imaging (MRI), and clinical findings. Genetic and histopathology reports were obtained from participant’s medical records. Alamut Visual Software was used to determine if participant’s variants had been previously reported and to assess predicted pathogenicity. Physical exams, pulmonary function tests, T1-weighted muscle MRI scans, and blood measures were completed during the abovementioned clinical trial. Six novel variants (two de novo, three dominant, and one recessive) were identified in individuals with RYR1-RM. Consistent with established RYR1-RM histopathology, cores were observed in all biopsies, except Case 6 who exhibited fiber-type disproportion. Muscle atrophy and impaired mobility with Trendelenburg gait were the most common clinical symptoms and were identified in all cases. Muscle MRI revealed substantial inter-individual variation in fatty infiltration corroborating the heterogeneity of the disease. Two individuals with dominant RYR1 variants exhibited respiratory insufficiency: a clinical symptom more commonly associated with recessive RYR1-RM cases. This study demonstrates that a genetics-led approach is suitable for the diagnosis of suspected RYR1-RM which can be corroborated through histopathology, muscle MRI and clinical examination.

Published

2018

5. Bi-allelic variants in the ER quality-control mannosidase gene EDEM3 cause a congenital disorder of glycosylation

Author

Ana Berta Sousa, Anneke J.A. Kievit, Marjon van Slegtenhorst, Nicholas J. Hand, Kosuke Izumi, Paula Jorge, Andrew C. Edmondson, Elisa De Franco, Linlea Armstrong, Michael E. March, Dirk Lefeber, Hans van Bokhoven, Miao He, Sian Ellard, Marina P Hommersom, Serwet Demirdas, Elaine H. Zackai, Fleur S van Dijk, Anna Lehman, Avni Santani, Daniel L. Polla, Daniel J. Rader, Arjan P.M. de Brouwer, Sandrine Duvet, Xin Bi, Sophie C. Huffels, Dmitriy Niyazov, Céline Schulz, Clinical Genetics, and Repositório da Universidade de Lisboa

Subjects

Male, Glycosylation, Mouse, Developmental Disabilities, Endoplasmic Reticulum, Compound heterozygosity, chemistry.chemical_compound, Congenital Disorders of Glycosylation, 0302 clinical medicine, EIF2AK3, Child, Genetics (clinical), Exome sequencing, 0303 health sciences, Tunicamycin, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Pedigree, Mannosidase, Child, Preschool, N-glycan, Female, Adolescent, Biology, Cell Line, 03 medical and health sciences, Polysaccharides, alpha-Mannosidase, Intellectual Disability, Report, Genetics, medicine, Humans, Proteostasis Deficiencies, Gene, Alleles, Glycoproteins, 030304 developmental biology, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Endoplasmic reticulum, Calcium-Binding Proteins, Infant, medicine.disease, Molecular biology, carbohydrates (lipids), Dysmorphism, chemistry, Mutation, Unfolded protein response, High-mannose, CDG, EDEM3, Congenital disorder of glycosylation, 030217 neurology & neurosurgery

Abstract

© 2021 American Society of Human Genetics, EDEM3 encodes a protein that converts Man8GlcNAc2 isomer B to Man7-5GlcNAc2. It is involved in the endoplasmic reticulum-associated degradation pathway, responsible for the recognition of misfolded proteins that will be targeted and translocated to the cytosol and degraded by the proteasome. In this study, through a combination of exome sequencing and gene matching, we have identified seven independent families with 11 individuals with bi-allelic protein-truncating variants and one individual with a compound heterozygous missense variant in EDEM3. The affected individuals present with an inherited congenital disorder of glycosylation (CDG) consisting of neurodevelopmental delay and variable facial dysmorphisms. Experiments in human fibroblast cell lines, human plasma, and mouse plasma and brain tissue demonstrated decreased trimming of Man8GlcNAc2 isomer B to Man7GlcNAc2, consistent with loss of EDEM3 enzymatic activity. In human cells, Man5GlcNAc2 to Man4GlcNAc2 conversion is also diminished with an increase of Glc1Man5GlcNAc2. Furthermore, analysis of the unfolded protein response showed a reduced increase in EIF2AK3 (PERK) expression upon stimulation with tunicamycin as compared to controls, suggesting an impaired unfolded protein response. The aberrant plasma N-glycan profile provides a quick, clinically available test for validating variants of uncertain significance that may be identified by molecular genetic testing. We propose to call this deficiency EDEM3-CDG., This work was supported by the EU FP7 large-scale integrating project Genetic and Epigenetic Networks in Cognitive Dysfunction (241995) (to H.v.B.); National Institutes of Health (NIH) grants 5R01GM115730-03 (to M.H.), U54 NS115198 (to A.C.E. and M.H.), and T32GM008638 (to A.C.E.); and the Transatlantic Network of Excellence grant (10CVD03) from the Fondation Leducq and NIH NHGRI U01HG006398 (to D.J.R.). Family 4 was enrolled in the CAUSES Study; investigators include Shelin Adam, Christele Du Souich, Alison Elliott, Anna Lehman, Jill Mwenifumbo, Tanya Nelson, Clara Van Karnebeek, and Jan Friedman; it is funded by Mining for Miracles, British Columbia Children’s Hospital Foundation (grant number F15-01355) and Genome British Columbia (grant number F16-02276). D.L.P. is recipient of a CAPES Fellowship (99999.013311/2013-01). X.B. is supported by an AHA career development award (19CDA34630032).

Published

2021

6. Hypotrichosis‐lymphedema‐telangiectasia syndrome: Report of ileal atresia associated with a <scp> SOX18 </scp> de novo pathogenic variant and review of the phenotypic spectrum

Author

Miikka Vikkula, Dmitriy Niyazov, Elodie Fastré, Pascal Brouillard, Michael J. Gambello, Richard Coulie, and UCL - SSS/DDUV/GEHU - Génétique

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, phenotype, 030105 genetics & heredity, 03 medical and health sciences, Gene duplication, Genetics, Medicine, transcription factor, Genetics (clinical), HLTRS, business.industry, Alopecia totalis, Ileal Atresia, medicine.disease, Pulmonary hypertension, Lymphangiogenesis, lymphangiogenesis, 030104 developmental biology, Lymphatic system, Lymphedema, Hypotrichosis–lymphedema–telangiectasia syndrome, genetic, business, HLTS

Abstract

Hypotrichosis-lymphedema-telangiectasia syndrome (HLTS) is a rare condition caused by pathogenic variants in the SOX18 gene. SOX18 plays a key role in angio- and lymphangiogenesis due to its expression in venous endothelial cells from which the lymphatic system develops. It is also expressed in embryonic hair follicles, heart, and vascular smooth muscle cells. The main clinical symptoms of HLTS include sparse hair, alopecia totalis, lymphedema, most often affecting lower limbs, and telangiectatic lesions. Only 10 patients with a SOX18 pathogenic variant have been described that presented with additional features such as hydrocele, renal failure, arterial or pulmonary hypertension, aortic dilatation, and facial dysmorphism. Here, we summarize these phenotypic variations and report an additional HLTS patient, with a 14-nucleotide de novo duplication in SOX18 and congenital ileal atresia, a feature not previously associated with HLTS.

Published

2021

7. Phenotypic expansion of<scp>Bosch–Boonstra–Schaaf</scp>optic atrophy syndrome and further evidence for genotype–phenotype correlations

Author

Philip J. Lupo, Megan E. Rech, Linford Williams, Suneeta Madan-Khetarpal, Veeral Shah, Erin Kovar, Gerard T. Berry, Dmitriy Niyazov, Christian P. Schaaf, Daniëlle G. M. Bosch, Charles Shaw-Smith, Jane C. Edmond, Chun-An Chen, and John M. McCarthy

Subjects

Male, Cortical visual impairment, Alacrima, Neurodevelopmental disorder, Atrophy, Optic Atrophies, Hereditary, Seizures, Intellectual Disability, Intellectual disability, Genetics, medicine, Humans, Point Mutation, Frameshift Mutation, Genetic Association Studies, Genetics (clinical), Optic nerve hypoplasia, COUP Transcription Factor I, business.industry, medicine.disease, Hypotonia, DNA-Binding Proteins, Codon, Nonsense, Autism spectrum disorder, Mutation, Female, medicine.symptom, business, Neuroscience

Abstract

Bosch-Boonstra-Schaaf Optic Atrophy Syndrome (BBSOAS) is an autosomal dominant neurodevelopmental disorder caused by loss-of-function variants in NR2F1 and characterized by visual impairment, developmental delay, and intellectual disability. Here we report 18 new cases, provide additional clinical information for 9 previously reported individuals, and review an additional 27 published cases to present a total of 54 patients. Among these are 22 individuals with point mutations or in-frame deletions in the DNA-binding domain (DBD), and 32 individuals with other types of variants including whole-gene deletions, nonsense and frameshift variants, and point mutations outside the DBD. We corroborate previously described clinical characteristics including developmental delay, intellectual disability, autism spectrum disorder diagnoses/features thereof, cognitive/behavioral anomalies, hypotonia, feeding difficulties, abnormal brain MRI findings, and seizures. We also confirm a vision phenotype that includes optic nerve hypoplasia, optic atrophy, and cortical visual impairment. Additionally, we expand the vision phenotype to include alacrima and manifest latent nystagmus (fusional maldevelopment), and we broaden the behavioral phenotypic spectrum to include a love of music, an unusually good long-term memory, sleep difficulties, a high pain tolerance, and touch sensitivity. Furthermore, we provide additional evidence for genotype-phenotype correlations, specifically supporting a more severe phenotype associated with DBD variants.

Published

2020

8. Biallelic variants in AGMO with diminished enzyme activity are associated with a neurodevelopmental disorder

Author

Volkan Okur, Donald Basel, Martin Hermann, Ernst R. Werner, Wendy K. Chung, Katrin Watschinger, Dmitriy Niyazov, and Julie McCarrier

Subjects

Male, Microcephaly, Biology, medicine.disease_cause, Mixed Function Oxygenases, Frameshift mutation, 03 medical and health sciences, Neurodevelopmental disorder, Genetics, medicine, Humans, Missense mutation, Allele, Alleles, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Mutation, 030305 genetics & heredity, HEK 293 cells, Alkylglycerol monooxygenase, Prognosis, medicine.disease, HEK293 Cells, Neurodevelopmental Disorders

Abstract

Alkylglycerol monooxygenase (AGMO) is the only enzyme known to cleave the O-alkyl bonds of ether lipids (alkylglycerols) which are essential components of cell membranes. A homozygous frameshift variant [p.(Glu324LysfsTer12)] in AGMO has recently been reported in two male siblings with syndromic microcephaly. In this study, we identified rare nonsense, in frame deletion, and missense biallelic variants in AGMO in two unrelated individuals with neurodevelopmental disabilities. We assessed the activity of seven disease associated AGMO variants including the four variants identified in our two affected individuals expressed in human embryonic kidney (HEK293T) cells. We demonstrated significantly diminished enzyme activity for all disease-associated variants, supporting the mechanism as decreased AGMO activity. Future mechanistic studies are necessary to understand how decreased AGMO activity leads to the neurologic manifestations.

Published

2019

9. Phenotype and mutation expansion of the PTPN23 associated disorder characterized by neurodevelopmental delay and structural brain abnormalities

Author

Jennifer A. Lee, Carlos Ferreira, Kym M. Boycott, Lina Basel-Salmon, Yue Si, Richard E. Person, Michael J. Lyons, Melissa T. Carter, Dmitriy Niyazov, Claudia Gonzaga-Jauregui, Renee Bend, Erin Torti, Lior Cohen, Samantha K Rojas, Ingrid M. Wentzensen, and Mohamad A. Mikati

Subjects

Male, Microcephaly, Adolescent, Biology, medicine.disease_cause, Compound heterozygosity, Article, 03 medical and health sciences, Atrophy, Genetics, medicine, Humans, DNA sequencing, Allele, Child, 10. No inequality, Genetics (clinical), Loss function, 0303 health sciences, Mutation, Neurodevelopmental disorders, Medical genetics, 030305 genetics & heredity, Brain, Infant, Protein Tyrosine Phosphatases, Non-Receptor, medicine.disease, Phenotype, Child, Preschool, Female, Ventriculomegaly

Abstract

PTPN23 is a His-domain protein-tyrosine phosphatase implicated in ciliogenesis, the endosomal sorting complex required for transport (ESCRT) pathway, and RNA splicing. Until recently, no defined human phenotype had been associated with alterations in this gene. We identified and report a cohort of seven patients with either homozygous or compound heterozygous rare deleterious variants in PTPN23. Combined with four patients previously reported, a total of 11 patients with this disorder have now been identified. We expand the phenotypic and variation spectrum associated with defects in this gene. Patients have strong phenotypic overlap, suggesting a defined autosomal recessive syndrome caused by reduced function of PTPN23. Shared characteristics of affected individuals include developmental delay, brain abnormalities (mainly ventriculomegaly and/or brain atrophy), intellectual disability, spasticity, language disorder, microcephaly, optic atrophy, and seizures. We observe a broad range of variants across patients that are likely strongly reducing the expression or disrupting the function of the protein. However, we do not observe any patients with an allele combination predicted to result in complete loss of function of PTPN23, as this is likely incompatible with life, consistent with reported embryonic lethality in the mouse. None of the observed or reported variants are recurrent, although some have been identified in homozygosis in patients from consanguineous populations. This study expands the phenotypic and molecular spectrum of PTPN23 associated disease and identifies major shared features among patients affected with this disorder, while providing additional support to the important role of PTPN23 in human nervous and visual system development and function.

Published

2019

10. Biallelic loss-of-function variants in PLD1 cause congenital right-sided cardiac valve defects and neonatal cardiomyopathy

Author

Gijs W. E. Santen, Damara Ortiz, Elisabeth M. Lodder, Francesca Clementina Radio, Michael V. Airola, Monique C. Haak, Dominic S Zimmerman, Quinn Gunst, Peter de Knijff, Katherine H. Kim, Viktor Stránecký, Stanislav Kmoch, Hiba Mustafa, Dmitriy Niyazov, H. Alex Brown, Najim Lahrouchi, Jamille Y. Robinson, Rick H. de Leeuw, Anne Sophie Denommé-Pichon, Sara Cherny, George A. Tanteles, Mariam Hababa, Joey V. Barnett, Doris Škorić-Milosavljević, Annemiek C. Dutman, Timothy J. Moss, Daniel M. de Laughter, Connie R. Bezzina, Zeev Perles, Fleur V.Y. Tjong, Matthew Ambrose, Forrest Z. Bowling, Arend D. J. ten Harkel, Katelijne Bouman, Barry Wolf, Monia Magliozzi, Asaf Ta-Shma, Lenka Piherová, Aho Ilgun, Sabrina C. Burn, Orly Elpeleg, Michael A. Frohman, Alex V. Postma, Maurice J.B. van den Hoff, Christian M. Salazar, Johanna C. Herkert, Christine Francannet, Jennifer Jacober, Andreas Rousounides, Leander Beekman, Barbara J.M. Mulder, Viktor Tomek, Bruel Ange-Line, Aphrodite Aristidou-Kallika, S. A. Clur, Gwendolyn T. R. Manten, Cardiology, ACS - Heart failure & arrhythmias, Human Genetics, Medical Biology, ACS - Pulmonary hypertension & thrombosis, ACS - Amsterdam Cardiovascular Sciences, ARD - Amsterdam Reproduction and Development, Graduate School, APH - Aging & Later Life, APH - Personalized Medicine, Paediatric Cardiology, and APH - Amsterdam Public Health

Subjects

Heart Defects, Congenital, Male, 0301 basic medicine, Heart disease, Heart Valve Diseases, Cardiomyopathy, HEART-DISEASE, PHOSPHOLIPASE-D DEFINES, 03 medical and health sciences, 0302 clinical medicine, DESIGN, Loss of Function Mutation, Phospholipase D, Humans, Medicine, Missense mutation, CRYSTAL-STRUCTURE, Allele frequency, Alleles, Loss function, Genetics, business.industry, GROWTH-FACTOR-BETA, MUTATIONS, INDUCTION, FACTOR-ALPHA, General Medicine, medicine.disease, Phenotype, Ashkenazi jews, TRANSFORMATION, 030104 developmental biology, D1, 030220 oncology & carcinogenesis, Heart failure, Female, business, Research Article

Abstract

Congenital heart disease is the most common type of birth defect, accounting for one-third of all congenital anomalies. Using whole-exome sequencing of 2718 patients with congenital heart disease and a search in GeneMatcher, we identified 30 patients from 21 unrelated families of different ancestries with biallelic phospholipase D1 (PLD1) variants who presented predominantly with congenital cardiac valve defects. We also associated recessive PLD1 variants with isolated neonatal cardiomyopathy. Furthermore, we established that p.1668F is a founder variant among Ashkenazi Jews (allele frequency of -.2%) and describe the phenotypic spectrum of PLD1-associated congenital heart defects. PLD1 missense variants were overrepresented in regions of the protein critical for catalytic activity, and, correspondingly, we observed a strong reduction in enzymatic activity for most of the mutant proteins in an enzymatic assay. Finally, we demonstrate that PLD1 inhibition decreased endothelial-mesenchymal transition, an established pivotal early step in valvulogenesis. In conclusion, our study provides a more detailed understanding of disease mechanisms and phenotypic expression associated with PLD1 loss of function.

Published

2021

11. Haploinsufficiency of the Sin3/HDAC corepressor complex member SIN3B causes a syndromic intellectual disability/autism spectrum disorder

Author

Erica E. Davis, Xenia Latypova, Damien Lederer, LaDonna Immken, Bertrand Isidor, Carmen Orellana, Nicolette S. den Hollander, Shannon Bell, Francisco Martínez, Alice Molle, Oluwadamilare A. Adebambo, Thomas Besnard, Dmitriy Niyazov, Anne Claude Tabet, Marie Deprez, Kamran Moradkhani, Alfonso Caro, Sandra Mercier, Solène Conrad, Philippe M. Campeau, Xiang-Jiao Yang, Christelle Retière, Nicholas Katsanis, Marie Vincent, Kirsty McWalter, Jill A. Rosenfeld, Raymond J. Louie, Stéphane Bézieau, Cynthia Fourgeux, Sharon F. Suchy, Jagdeep S. Walia, Mónica Roselló, Cédric Le Caignec, Emmelien Aten, Jeremie Poschmann, Benjamin Cogné, Peter Kannu, Miranda Splitt, Pawel Stankiewicz, Yline Capri, Catherine Willem, Tahir N. Khan, Justine Rousseau, Sébastien Küry, Jonathan I. Levy, Roger E. Stevenson, Centre hospitalier universitaire de Nantes (CHU Nantes), Duke University Medical Center, unité de recherche de l'institut du thorax UMR1087 UMR6291 (ITX), Université de Nantes - UFR de Médecine et des Techniques Médicales (UFR MEDECINE), Université de Nantes (UN)-Université de Nantes (UN)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Centre de Recherche en Transplantation et Immunologie (U1064 Inserm - CRTI), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Nantes - UFR de Médecine et des Techniques Médicales (UFR MEDECINE), Université de Nantes (UN)-Université de Nantes (UN), Hospital Universitario y Politécnico La Fe [Valencia, Spain], Ochsner Medical Center [New Orleans, Louisiana, USA], Institut de Pathologie et Génétique [Gosselies] (I.P.G.), Hôpital Robert Debré, The Hospital for sick children [Toronto] (SickKids), Leiden University Medical Center (LUMC), Institute of Genetic Medicine [Newcastle], Newcastle University [Newcastle], Kingston General Health Research Institute [Kingston, ON, Canada] (KGHRI), Dell Children's Medical Group [Austin, TX, USA] (DCMG), Baylor College of Medicine (BCM), Baylor University, GeneDx [Gaithersburg, MD, USA], The Greenwood Genetic Center, Centre Hospitalier Universitaire Sainte-Justine [Montréal, QC, Canada] (CHU Sainte-Justine), EFS Centre-Pays de la Loire [Nantes], Immunobiology of Human αβ and γδ T Cells and Immunotherapeutic Applications (CRCINA-ÉQUIPE 1), Centre de Recherche en Cancérologie et Immunologie Nantes-Angers (CRCINA), Université de Nantes (UN)-Université de Nantes (UN)-Centre hospitalier universitaire de Nantes (CHU Nantes)-Centre National de la Recherche Scientifique (CNRS)-Université d'Angers (UA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Nantes - UFR de Médecine et des Techniques Médicales (UFR MEDECINE), Université de Nantes (UN)-Université de Nantes (UN)-Centre hospitalier universitaire de Nantes (CHU Nantes)-Centre National de la Recherche Scientifique (CNRS)-Université d'Angers (UA), LabEX IGO Immunothérapie Grand Ouest, McGill University = Université McGill [Montréal, Canada], Ann & Robert H. Lurie Children's Hospital of Chicago, Northwestern University Medical School [Chicago], Unité de recherche de l'institut du thorax (ITX-lab), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université de Nantes - UFR de Médecine et des Techniques Médicales (UFR MEDECINE), Hospital Universitari i Politècnic La Fe = University and Polytechnic Hospital La Fe, CHU Sainte Justine [Montréal], Université d'Angers (UA)-Université de Nantes (UN)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Centre hospitalier universitaire de Nantes (CHU Nantes)-Université d'Angers (UA)-Université de Nantes (UN)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Centre hospitalier universitaire de Nantes (CHU Nantes), Nantes Université (Nantes Univ), and RETIERE, Christelle

Subjects

Male, Models, Molecular, Autism Spectrum Disorder, [SDV]Life Sciences [q-bio], Haploinsufficiency, medicine.disease_cause, Histones, 0302 clinical medicine, HDAC, Intellectual disability, Child, Zebrafish, Genetics (clinical), Exome sequencing, Genetics, 0303 health sciences, Mutation, HDAC, SIN3A, SINB, acetylation, autism, epigenetics, intellectual disability, mutation, transcription, zebrafish, Syndrome, Middle Aged, Magnetic Resonance Imaging, [SDV] Life Sciences [q-bio], intellectual disability, Child, Preschool, Larva, Female, transcription, Adolescent, DNA Copy Number Variations, autism, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Biology, Histone Deacetylases, Frameshift mutation, Young Adult, 03 medical and health sciences, Report, medicine, Animals, Humans, Epigenetics, [SDV.BC] Life Sciences [q-bio]/Cellular Biology, 030304 developmental biology, SIN3A, acetylation, epigenetics, Infant, Zebrafish Proteins, SINB, biology.organism_classification, medicine.disease, zebrafish, Repressor Proteins, Histone deacetylase, mutation, 030217 neurology & neurosurgery

Abstract

International audience; Proteins involved in transcriptional regulation harbor a demonstrated enrichment of mutations in neurodevelopmental disorders. The Sin3 (Swi-independent 3)/histone deacetylase (HDAC) complex plays a central role in histone deacetylation and transcriptional repression. Among the two vertebrate paralogs encoding the Sin3 complex, SIN3A variants cause syndromic intellectual disability, but the clinical consequences of SIN3B haploinsufficiency in humans are uncharacterized. Here, we describe a syndrome hallmarked by intellectual disability, developmental delay, and dysmorphic facial features with variably penetrant autism spectrum disorder, congenital malformations, corpus callosum defects, and impaired growth caused by disruptive SIN3B variants. Using chromosomal microarray or exome sequencing, and through international data sharing efforts, we identified nine individuals with heterozygous SIN3B deletion or single-nucleotide variants. Five individuals harbor heterozygous deletions encompassing SIN3B that reside within a $230 kb minimal region of overlap on 19p13.11, two individuals have a rare nonsynonymous substitution, and two individuals have a single-nucleotide deletion that results in a frameshift and predicted premature termination codon. To test the relevance of SIN3B impairment to measurable aspects of the human phenotype, we disrupted the orthologous zebrafish locus by genome editing and transient suppression. The mutant and morphant larvae display altered craniofacial patterning, commissural axon defects, and reduced body length supportive of an essential role for Sin3 function in growth and patterning of anterior structures. To investigate further the molecular consequences of SIN3B variants, we quantified genome-wide enhancer and promoter activity states by using H3K27ac ChIP-seq. We show that, similar to SIN3A mutations, SIN3B disruption causes hyperacetylation of a subset of enhancers and promoters in peripheral blood mononuclear cells. Together, these data demonstrate that SIN3B haploinsufficiency leads to a hitherto unknown intellectual disability/autism syndrome, uncover a crucial role of SIN3B in the central nervous system, and define the epigenetic landscape associated with Sin3 complex impairment.

Published

2021

12. Novel NUDT2 variant causes intellectual disability and polyneuropathy

Author

Allison Zheng, J Brandon Birath, Frank Diaz, Yurivia Cervantes-Manzo, Richard E. Person, Michelle M. Morrow, Brent L. Fogel, Robert Freundlich, Matthew R. Herzog, Hane Lee, Stanley F. Nelson, Christina G.S. Palmer, Shaweta Khosa, Shri K. Mishra, Dmitriy Niyazov, Rebecca Signer, Naghmeh Dorrani, and Julian A. Martinez-Agosto

Subjects

0301 basic medicine, Adult, Male, Weakness, Pediatrics, medicine.medical_specialty, Developmental Disabilities, Neurosciences. Biological psychiatry. Neuropsychiatry, Brief Communication, Frameshift mutation, 03 medical and health sciences, Polyneuropathies, Young Adult, 0302 clinical medicine, Genetic etiology, Intellectual Disability, Intellectual disability, Exome Sequencing, Medicine, Humans, Global developmental delay, RC346-429, Child, Frameshift Mutation, Exome, business.industry, Electromyography, General Neuroscience, Electroencephalography, medicine.disease, Phenotype, Magnetic Resonance Imaging, Phosphoric Monoester Hydrolases, Pedigree, 030104 developmental biology, Female, Neurology. Diseases of the nervous system, Neurology (clinical), medicine.symptom, business, Brief Communications, Polyneuropathy, 030217 neurology & neurosurgery, RC321-571

Abstract

Exome or genome sequencing was performed to identify the genetic etiology for the clinical presentation of global developmental delay, intellectual disability, and sensorimotor neuropathy with associated distal weakness in two unrelated families. A homozygous frameshift variant c.186delA (p.A63Qfs*3) in the NUDT2 gene was identified in cases 1 and 2 from one family and a third case from another family. Variants in NUDT2 were previously shown to cause intellectual disability, but here we expand the phenotype by demonstrating its association with distal upper and lower extremity weakness due to a sensorimotor polyneuropathy with demyelinating and/or axonal features.

Published

2020

13. TANGO2: expanding the clinical phenotype and spectrum of pathogenic variants

Author

Alison M. Muir, Dianne Laboy Cintrón, Katherine H. Kim, Amber Begtrup, Peter I. Karachunski, Almuth Caliebe, Heather C Mefford, Amy Lacroix, J. Lawrence Merritt, Kirsty McWalter, Angela Sun, Sharon F. Suchy, Barbara K. Burton, Ingo Helbig, René Santer, Joline C. Dalton, Dmitriy Niyazov, Rachel Westman, Ganka Douglas, Leah Fleming, Hiltrud Muhle, Kristin G. Monaghan, Alice Basinger, Katherine L. Helbig, Jenny Thies, Kolja Becker, Manuela Pendziwiat, Can Ficicioglu, Megan T. Cho, Jennifer N. Dines, Francisca Millan, and Katie Golden-Grant

Subjects

Male, 0301 basic medicine, Adolescent, DNA Copy Number Variations, Genotype, Developmental Disabilities, Encephalopathy, developmental delay DNA copy-number variation, 030105 genetics & heredity, Compound heterozygosity, Bioinformatics, Article, 03 medical and health sciences, Epilepsy, Genotype-phenotype distinction, Seizures, Intellectual Disability, Intellectual disability, medicine, Humans, Exome, Family, intragenic deletion, Child, Genetics (clinical), Exome sequencing, Brain Diseases, business.industry, Aryl Hydrocarbon Receptor Nuclear Translocator, Correction, medicine.disease, Phenotype, Pedigree, 3. Good health, 030104 developmental biology, Child, Preschool, epilepsy, Female, business, exome sequencing

Abstract

Purpose TANGO2-related disorders were first described in 2016 and prior to this publication, only 15 individuals with TANGO2-related disorder were described in the literature. Primary features include metabolic crisis with rhabdomyolysis, encephalopathy, intellectual disability, seizures, and cardiac arrhythmias. We assess whether genotype and phenotype of TANGO2-related disorder has expanded since the initial discovery and determine the efficacy of exome sequencing (ES) as a diagnostic tool for detecting variants. Methods We present a series of 14 individuals from 11 unrelated families with complex medical and developmental histories, in whom ES or microarray identified compound heterozygous or homozygous variants in TANGO2. Results The initial presentation of patients with TANGO2-related disorders can be variable, including primarily neurological presentations. We expand the phenotype and genotype for TANGO2, highlighting the variability of the disorder. Conclusion TANGO2-related disorders can have a more diverse clinical presentation than previously anticipated. We illustrate the utility of routine ES data reanalysis whereby discovery of novel disease genes can lead to a diagnosis in previously unsolved cases and the need for additional copy-number variation analysis when ES is performed.

Published

2018

14. Improvement in Cardiac Function With Enzyme Replacement Therapy in a Patient With Infantile-Onset Pompe Disease

Author

Dmitriy Niyazov and Diego A. Lara

Subjects

0301 basic medicine, Cardiac function curve, medicine.medical_specialty, business.industry, Diastole, Hypertrophic cardiomyopathy, Enzyme replacement therapy, General Medicine, medicine.disease, Hypotonia, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Inborn error of metabolism, Internal medicine, Glycogen storage disease type II, Cardiology, Medicine, medicine.symptom, business, Case Reports and Clinical Observations, Alglucosidase alfa, 030217 neurology & neurosurgery, medicine.drug

Abstract

Background: Pompe disease is a lysosomal storage disorder that results from an inborn error of metabolism involving abnormal glycogen storage. Infantile-onset Pompe disease is the most severe phenotype, and enzyme replacement therapy with alglucosidase alfa (Lumizyme) improves medical and functional outcomes in patients with infantile-onset Pompe disease. Case Report: We report the case of a patient with infantile-onset Pompe disease who presented with severe hypertrophic cardiomyopathy, systolic and diastolic cardiac dysfunction, and hypotonia. She experienced significant improvement in cardiac systolic function while receiving enzyme replacement therapy. Conclusion: Typically, patients with infantile-onset Pompe disease and severe hypertrophic cardiomyopathy are not as responsive to enzyme replacement therapy as patients with mild or no hypertrophic cardiomyopathy. We demonstrated the efficacy of enzyme replacement therapy in a patient with severe hypertrophic cardiomyopathy.

Published

2018

15. Missense variants in the chromatin remodeler CHD1 are associated with neurodevelopmental disability

Author

Maria J. Guillen Sacoto, Hilary J. Vernon, Meron Azage, Leandros Boukas, Berivan Baskin, Gregory D. Bowman, Dmitriy Niyazov, Ingrid M. Wentzensen, Megan T. Cho, Hans T. Bjornsson, Erin Beaver, Christina A. Gurnett, Genay Pilarowski, Paul J. Benke, Livija Medne, Jennifer M. Heeley, Ian D. Krantz, Carolyn D. Applegate, and Lindsay B. Henderson

Subjects

0301 basic medicine, Genetics, Mechanism (biology), Disease, Biology, medicine.disease, Bioinformatics, Phenotype, Chromatin, 03 medical and health sciences, 030104 developmental biology, medicine, Missense mutation, Autism, Epigenetics, Gene, Genetics (clinical)

Abstract

BackgroundThe list of Mendelian disorders of the epigenetic machinery has expanded rapidly during the last 5 years. A few missense variants in the chromatin remodeler CHD1 have been found in several large-scale sequencing efforts focused on uncovering the genetic aetiology of autism.ObjectivesTo explore whether variants in CHD1 are associated with a human phenotype.MethodsWe used GeneMatcher to identify other physicians caring for patients with variants in CHD1. We also explored the epigenetic consequences of one of these variants in cultured fibroblasts.ResultsHere we describe six CHD1 heterozygous missense variants in a cohort of patients with autism, speech apraxia, developmental delay and facial dysmorphic features. Importantly, three of these variants occurred de novo. We also report on a subject with a de novo deletion covering a large fraction of the CHD1 gene without any obvious neurological phenotype. Finally, we demonstrate increased levels of the closed chromatin modification H3K27me3 in fibroblasts from a subject carrying a de novo variant in CHD1.ConclusionsOur results suggest that variants in CHD1 can lead to diverse phenotypic outcomes; however, the neurodevelopmental phenotype appears to be limited to patients with missense variants, which is compatible with a dominant negative mechanism of disease.

Published

2017

16. De novo heterozygous missense and loss-of-function variants in CDC42BPB are associated with a neurodevelopmental phenotype

Author

Michelle Steinraths, Dominique Campion, Andrea Accogli, Koen L.I. van Gassen, Volkan Okur, Guillaume Sébire, Austin Larson, Solveig Heide, Angelo Selicorni, Carol J Saunders, Thomas Husson, Giuseppina Vitiello, Joseph T Alaimo, Christel Depienne, Rebecca O. Littlejohn, Myriam Srour, Caroline Nava, Jennifer Rice, Daniel Groepper, Klaske D. Lichtenbelt, Dmitriy Niyazov, Janda L Jenkins, Meron Azage, Karen W. Gripp, George E. Hoganson, Alice Goldenberg, Ilana Chilton, Wendy K. Chung, Milena Mariani, Julie Fleischer, Delphine Héron, Jennifer Burton, Elizabeth Roeder, Isabelle Thiffault, and Eric T. Rush

Subjects

Adult, Male, Heterozygote, Adolescent, Developmental Disabilities, Protein domain, Medizin, Mutation, Missense, Haploinsufficiency, Biology, Myotonin-Protein Kinase, Frameshift mutation, Neurodevelopmental disorder, Loss of Function Mutation, Intellectual Disability, Genetics, medicine, Missense mutation, Humans, Amino Acid Sequence, Autistic Disorder, Child, Frameshift Mutation, Genetics (clinical), Exome sequencing, Infant, Newborn, Infant, medicine.disease, Hypotonia, Phenotype, Protein kinase domain, Neurodevelopmental Disorders, Child, Preschool, Female, medicine.symptom

Abstract

CDC42BPB encodes MRCKβ (myotonic dystrophy-related Cdc42-binding kinase beta), a serine/threonine protein kinase, and a downstream effector of CDC42, which has recently been associated with Takenouchi-Kosaki syndrome, an autosomal dominant neurodevelopmental disorder. We identified 12 heterozygous predicted deleterious variants in CDC42BPB (9 missense, 2 frameshift, and 1 nonsense) in 14 unrelated individuals (confirmed de novo in 11/14) with neurodevelopmental disorders including developmental delay/intellectual disability, autism, hypotonia, and structural brain abnormalities including cerebellar vermis hypoplasia and agenesis/hypoplasia of the corpus callosum. The frameshift and nonsense variants in CDC42BPB are expected to be gene-disrupting and lead to haploinsufficiency via nonsense-mediated decay. All missense variants are located in highly conserved and functionally important protein domains/regions: 3 are found in the protein kinase domain, 2 are in the citron homology domain, and 4 in a 20-amino acid sequence between 2 coiled-coil regions, 2 of which are recurrent. Future studies will help to delineate the natural history and to elucidate the underlying biological mechanisms of the missense variants leading to the neurodevelopmental and behavioral phenotypes.

Published

2019

17. Pathogenic WDFY3 variants cause neurodevelopmental disorders and opposing effects on brain size

Author

Meron Azage, David B. Everman, Brooke T. Smith, Steffen Syrbe, Stephen W. Scherer, Jennifer Keller-Ramey, Gregory M. Cooper, Verónica Martínez-Cerdeño, Susan M. Hiatt, Mathew J Wallis, Dmitriy Niyazov, Benjamin Büttner, Rami Abou Jamra, Ryan K. C. Yuen, Johannes R. Lemke, Natasha J Brown, Amber Begtrup, Richard E. Person, Barbara Kellam, Chloé Quélin, Heinrich Sticht, Laurence J. Walsh, Angelo Harlan De Crescenzo, Konstantinos Zarbalis, Jonathan B. Strober, Susan Walker, Alexios A Panoutsopoulos, Shuxi Liu, Diana Le Duc, Urania Kotzaeridou, Michael S. Hildebrand, Michael C. Pride, Eleonora Napoli, Jacqueline N. Crawley, Francis Jeshira Reynoso Santos, Katelyn Payne, Renee Bend, Sandra Yang, Megan T. Cho, Evdokia Anagnostou, Cecilia R Giulivi, Rhonda E. Schnur, Lori Orosco, Andreas Ziegler, Jan H Doering, Christèle Dubourg, Jill L. Silverman, Universität Leipzig [Leipzig], University of California [Davis] (UC Davis), University of California, GeneDx [Gaithersburg, MD, USA], Institut de Génétique et Développement de Rennes (IGDR), 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), Service de génétique clinique [Rennes], Université de Rennes 1 (UR1), Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES)-CHU Pontchaillou [Rennes]-hôpital Sud, Shriners Hospitals for Children, U54 HD079125, National Institute of Child Health and Human Development, R21MH115347, National Institute of Mental Health, 286567, Simons Foundation, Nancy Lurie Marks Family Foundation, UM1HG007301, National Human Genome Research Institute, Clinician Scientist Programm, Medizinische Fakultät der Universität Leipzig, Shriners Hospitals for Children Postdoctoral Fellowship, The MIND Institute IDDRC, Universität Leipzig, University of California (UC), 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 ), and Université de Rennes (UR)-CHU Pontchaillou [Rennes]-hôpital Sud

Subjects

0301 basic medicine, Proband, Male, Microcephaly, Secondary, [SDV]Life Sciences [q-bio], Autophagy-Related Proteins, Medical and Health Sciences, Transgenic, Mice, 0302 clinical medicine, Intellectual disability, 2.1 Biological and endogenous factors, Aetiology, Child, Exome, ComputingMilieux_MISCELLANEOUS, Pediatric, Brain, Adaptor Proteins, Organ Size, Mental Health, WDFY3, Autism spectrum disorder, intellectual disability, brain size, Neurological, Female, medicine.symptom, Haploinsufficiency, Biotechnology, Protein Structure, Adolescent, Intellectual and Developmental Disabilities (IDD), Biology, neurodevelopmental delay, 03 medical and health sciences, Clinical Research, medicine, Genetics, Animals, Humans, Preschool, Neurology & Neurosurgery, Psychology and Cognitive Sciences, Macrocephaly, Signal Transducing, Neurosciences, Genetic Variation, medicine.disease, Stem Cell Research, Associative learning, Brain Disorders, 030104 developmental biology, Neurodevelopmental Disorders, Neurology (clinical), Neuroscience, 030217 neurology & neurosurgery

Abstract

The underpinnings of mild to moderate neurodevelopmental delay remain elusive, often leading to late diagnosis and interventions. Here, we present data on exome and genome sequencing as well as array analysis of 13 individuals that point to pathogenic, heterozygous, mostly de novo variants in WDFY3 (significant de novo enrichment P = 0.003) as a monogenic cause of mild and non-specific neurodevelopmental delay. Nine variants were protein-truncating and four missense. Overlapping symptoms included neurodevelopmental delay, intellectual disability, macrocephaly, and psychiatric disorders (autism spectrum disorders/attention deficit hyperactivity disorder). One proband presented with an opposing phenotype of microcephaly and the only missense-variant located in the PH-domain of WDFY3. Findings of this case are supported by previously published data, demonstrating that pathogenic PH-domain variants can lead to microcephaly via canonical Wnt-pathway upregulation. In a separate study, we reported that the autophagy scaffolding protein WDFY3 is required for cerebral cortical size regulation in mice, by controlling proper division of neural progenitors. Here, we show that proliferating cortical neural progenitors of human embryonic brains highly express WDFY3, further supporting a role for this molecule in the regulation of prenatal neurogenesis. We present data on Wnt-pathway dysregulation in Wdfy3-haploinsufficient mice, which display macrocephaly and deficits in motor coordination and associative learning, recapitulating the human phenotype. Consequently, we propose that in humans WDFY3 loss-of-function variants lead to macrocephaly via downregulation of the Wnt pathway. In summary, we present WDFY3 as a novel gene linked to mild to moderate neurodevelopmental delay and intellectual disability and conclude that variants putatively causing haploinsufficiency lead to macrocephaly, while an opposing pathomechanism due to variants in the PH-domain of WDFY3 leads to microcephaly.

Published

2019

18. Solid organ transplantation in primary mitochondrial disease: Proceed with caution

Author

Sumit Parikh, Helen Mundy, Mark A. Tarnopolsky, Amel Karaa, Richard Haas, Yi Shiau Ng, Courtney J. Wusthoff, Amy Goldstein, Annette Feigenbaum, Dmitriy Niyazov, John Christodoulou, Mark S. Wainwright, Robert McFarland, Mary Kay Koenig, Russell P. Saneto, Bruce K. Cohen, David Dimmock, Grainne S. Gorman, Fernando Scaglia, and Timothy Feyma

Subjects

Adult, Graft Rejection, Male, 0301 basic medicine, medicine.medical_specialty, Mitochondrial Diseases, Adolescent, Heart Diseases, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Mitochondrial disease, Disease, Liver transplantation, Biochemistry, Kearns–Sayre syndrome, Young Adult, 03 medical and health sciences, Endocrinology, Risk Factors, Internal medicine, Genetics, medicine, Humans, Child, Molecular Biology, Survival rate, Kidney transplantation, Heart transplantation, business.industry, Liver Diseases, Infant, Middle Aged, medicine.disease, Kidney Transplantation, Liver Transplantation, Surgery, Survival Rate, Transplantation, Treatment Outcome, surgical procedures, operative, 030104 developmental biology, Child, Preschool, Heart Transplantation, Female, Kidney Diseases, business

Abstract

Solid organ transplants are rarely performed in both adult and pediatric patients with primary mitochondrial disease. Poor outcomes have been described in case reports and small case series. It is unclear whether the underlying genetic disease has a significant impact on post-transplant morbidity and mortality. Data were obtained for 35 patients from 17 Mitochondrial Disease Centers across North America, the United Kingdom and Australia. Patient outcomes were noted after liver, kidney or heart transplantation. Excluding patients with POLG-related disease, post-transplant survival approached or met outcomes seen in non-mitochondrial disease transplant patients. The majority of mitochondrial disease patients did not have worsening of their mitochondrial disease within 90-days post-transplant. Post-transplant complications, including organ rejection, were not a common occurrence and were generally treatable. Many patients did not have a mitochondrial disease considered or diagnosed prior to transplantation. In conclusion, patients with mitochondrial disease in this cohort generally tolerated solid-organ transplantation. Such patients may not need to be excluded from transplant solely for their mitochondrial diagnosis; additional caution may be needed for patients with POLG-related disease. Transplant teams should be aware of mitochondrial disease as an etiology for organ-failure and consider appropriate consultation in patients without a known cause of their symptoms.

Published

2016

19. Clinical and Molecular Characteristics of Mitochondrial Dysfunction in Autism Spectrum Disorder

Author

Dmitriy Niyazov, Stephen G. Kahler, Richard E. Frye, Shannon Rose, Michael J. Goldenthal, and Daniel A. Rossignol

Subjects

0301 basic medicine, Mitochondrial DNA, Mitochondrial Diseases, genetic structures, Autism Spectrum Disorder, Mitochondrial disease, Buccal swab, Review Article, Mitochondrion, Environment, Bioinformatics, behavioral disciplines and activities, 03 medical and health sciences, 0302 clinical medicine, Stress, Physiological, mental disorders, Genetics, Medicine, Humans, Genetic Predisposition to Disease, Microbiome, Pharmacology, business.industry, Fatty Acids, Brain, General Medicine, medicine.disease, Human genetics, Mitochondria, Gastrointestinal Tract, 030104 developmental biology, Autism spectrum disorder, Etiology, Molecular Medicine, business, 030217 neurology & neurosurgery, Biomarkers

Abstract

Autism spectrum disorder (ASD) affects ~ 2% of children in the United States. The etiology of ASD likely involves environmental factors triggering physiological abnormalities in genetically sensitive individuals. One of these major physiological abnormalities is mitochondrial dysfunction, which may affect a significant subset of children with ASD. Here we systematically review the literature on human studies of mitochondrial dysfunction related to ASD. Clinical aspects of mitochondrial dysfunction in ASD include unusual neurodevelopmental regression, especially if triggered by an inflammatory event, gastrointestinal symptoms, seizures, motor delays, fatigue and lethargy. Traditional biomarkers of mitochondrial disease are widely reported to be abnormal in ASD, but appear non-specific. Newer biomarkers include buccal cell enzymology, biomarkers of fatty acid metabolism, non-mitochondrial enzyme function, apoptosis markers and mitochondrial antibodies. Many genetic abnormalities are associated with mitochondrial dysfunction in ASD, including chromosomal abnormalities, mitochondrial DNA mutations and large-scale deletions, and mutations in both mitochondrial and non-mitochondrial nuclear genes. Mitochondrial dysfunction has been described in immune and buccal cells, fibroblasts, muscle and gastrointestinal tissue and the brains of individuals with ASD. Several environmental factors, including toxicants, microbiome metabolites and an oxidized microenvironment are shown to modulate mitochondrial function in ASD tissues. Investigations of treatments for mitochondrial dysfunction in ASD are promising but preliminary. The etiology of mitochondrial dysfunction and how to define it in ASD is currently unclear. However, preliminary evidence suggests that the mitochondria may be a fruitful target for treatment and prevention of ASD. Further research is needed to better understand the role of mitochondrial dysfunction in the pathophysiology of ASD.

Published

2018

20. An immune tolerance approach using transient low-dose methotrexate in the ERT-naïve setting of patients treated with a therapeutic protein: experience in infantile-onset Pompe disease

Author

R. Bradley Troxler, Marta Sabbadini, Neerja Gupta, David Kronn, Ankit K. Desai, Katalin Scherer, Susan M. Richards, Alison McVie-Wylie, Priya S. Kishnani, Reeval Segel, Langston Sherry, Alexandra Joseph, Pranoot Tanpaiboon, William B. Rizzo, Crystal Sung, Seymour Packman, Sheela Nampoothiri, Zoheb B. Kazi, Omar A. Abdul-Rahman, Annette Feigenbaum, and Dmitriy Niyazov

Subjects

0301 basic medicine, Male, medicine.medical_specialty, alglucosidase alfa, Disease, 030105 genetics & heredity, Cross Reactions, Low dose methotrexate, Gastroenterology, Article, methotrexate, Immune tolerance, 03 medical and health sciences, Internal medicine, medicine, Immune Tolerance, Humans, prophylactic immune tolerance induction, Enzyme Replacement Therapy, Age of Onset, Alglucosidase alfa, Genetics (clinical), business.industry, Glycogen Storage Disease Type II, Infant, Newborn, Therapeutic protein, Infant, Pompe disease, alpha-Glucosidases, 3. Good health, Titer, 030104 developmental biology, anti-drug antibodies, Methotrexate, Female, Infantile onset, business, medicine.drug

Abstract

Purpose: To investigate immune tolerance induction with transient low-dose methotrexate (TLD-MTX) initiated with recombinant human acid α-glucosidase (rhGAA), in treatment-naïve cross-reactive immunologic material (CRIM)-positive infantile-onset Pompe disease (IOPD) patients. Methods: Newly-diagnosed IOPD patients received subcutaneous or oral 0.4 mg/kg TLD-MTX for 3 cycles (3 doses/cycle) with the first 3 rhGAA infusions. Anti-rhGAA IgG titers, classified as high-sustained (HSAT; ≥51,200, ≥2 times after 6 months), sustained intermediate (SIT; ≥12,800 and

Published

2018

21. Mutations in SPATA5 Are Associated with Microcephaly, Intellectual Disability, Seizures, and Hearing Loss

Author

Alisha Wilkins, Akemi J. Tanaka, Adolfo Garnica, Xilma R. Ortiz-Gonzalez, Kyle Retterer, Ada Hamosh, Jane Juusola, Catharina M L Volker-Touw, Kristin G. Monaghan, Charuta Joshi, Dianalee McKnight, Koen L.I. van Gassen, Megan T. Cho, Edward Gratz, Ellen van Binsbergen, Matthew A. Deardorff, Katherine D. Mathews, Nara Sobreira, Dmitriy Niyazov, Wendy K. Chung, Karin Panzer, Francisca Millan, and Eva H. Brilstra

Subjects

Male, Microcephaly, Hearing loss, Molecular Sequence Data, Genes, Recessive, Cortical visual impairment, Biology, Research Support, medicine.disease_cause, Bioinformatics, N.I.H, Gene Frequency, Research Support, N.I.H., Extramural, Seizures, Report, Intellectual Disability, Intellectual disability, Journal Article, medicine, Genetics, Humans, Abnormalities, Multiple, Exome, Genetics(clinical), Amino Acid Sequence, Hearing Loss, Non-U.S. Gov't, Genetics (clinical), Homeodomain Proteins, Mutation, Base Sequence, Research Support, Non-U.S. Gov't, Extramural, Sequence Analysis, DNA, medicine.disease, Hypotonia, ATPases Associated with Diverse Cellular Activities, Female, Sensorineural hearing loss, medicine.symptom, Sequence Alignment

Abstract

Using whole-exome sequencing, we have identified in ten families 14 individuals with microcephaly, developmental delay, intellectual disability, hypotonia, spasticity, seizures, sensorineural hearing loss, cortical visual impairment, and rare autosomal-recessive predicted pathogenic variants in spermatogenesis-associated protein 5 (SPATA5). SPATA5 encodes a ubiquitously expressed member of the ATPase associated with diverse activities (AAA) protein family and is involved in mitochondrial morphogenesis during early spermatogenesis. It might also play a role in post-translational modification during cell differentiation in neuronal development. Mutations in SPATA5 might affect brain development and function, resulting in microcephaly, developmental delay, and intellectual disability.

Published

2015

22. Mutations Impairing GSK3-Mediated MAF Phosphorylation Cause Cataract, Deafness, Intellectual Disability, Seizures, and a Down Syndrome-like Facies

Author

Philippe M. Campeau, Alice Traversa, Maria Teresa Fiorenza, Nicholas Katsanis, Nicole Philip, Stephen R. Braddock, Karen W. Gripp, Antonio Palleschi, Serena Cecchetti, Marcello Niceta, Carla Boitani, Lorenzo Stella, Alessandro Bruselles, Viviana Caputo, Chiara Leoni, Gabriele Gillessen-Kaesbach, Kim M. Keppler-Noreuil, Gianfranco Bocchinfuso, Maria Kousi, Takaya Nakane, Marco Tartaglia, Dmitriy Niyazov, Emilia Stellacci, Massimiliano Anselmi, Giuseppe Zampino, Celio Pouponnot, Katia Sol-Church, Deborah L. Stabley, Andrea Ciolfi, Sabrina Prudente, and Brendan Lee

Subjects

Down syndrome, Deafness, Biology, Cataract, Down Syndrome, Glycogen Synthase Kinase 3, Humans, Intellectual Disability, Mutation, Phenotype, Phosphorylation, Proto-Oncogene Proteins c-maf, Seizures, MAF, mutations, developmental defects, aimé-gripp syndrome, Transactivation, Report, Genetics, medicine, Missense mutation, Genetics(clinical), Transcription factor, Genetics (clinical), Loss function, Settore CHIM/02 - Chimica Fisica, medicine.disease, AP-1 transcription factor, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA

Abstract

Transcription factors operate in developmental processes to mediate inductive events and cell competence, and perturbation of their function or regulation can dramatically affect morphogenesis, organogenesis, and growth. We report that a narrow spectrum of amino-acid substitutions within the transactivation domain of the v-maf avian musculoaponeurotic fibrosarcoma oncogene homolog (MAF), a leucine zipper-containing transcription factor of the AP1 superfamily, profoundly affect development. Seven different de novo missense mutations involving conserved residues of the four GSK3 phosphorylation motifs were identified in eight unrelated individuals. The distinctive clinical phenotype, for which we propose the eponym Aymé-Gripp syndrome, is not limited to lens and eye defects as previously reported for MAF/Maf loss of function but includes sensorineural deafness, intellectual disability, seizures, brachycephaly, distinctive flat facial appearance, skeletal anomalies, mammary gland hypoplasia, and reduced growth. Disease-causing mutations were demonstrated to impair proper MAF phosphorylation, ubiquitination and proteasomal degradation, perturbed gene expression in primary skin fibroblasts, and induced neurodevelopmental defects in an in vivo model. Our findings nosologically and clinically delineate a previously poorly understood recognizable multisystem disorder, provide evidence for MAF governing a wider range of developmental programs than previously appreciated, and describe a novel instance of protein dosage effect severely perturbing development.

Published

2015

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

Author

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

Subjects

Genetics (clinical)

Abstract

This corrects the article DOI: 10.1038/gim.2016.18.

Published

2017

24. Missense variants in the chromatin remodeler

Author

Genay O, Pilarowski, Hilary J, Vernon, Carolyn D, Applegate, Leandros, Boukas, Megan T, Cho, Christina A, Gurnett, Paul J, Benke, Erin, Beaver, Jennifer M, Heeley, Livija, Medne, Ian D, Krantz, Meron, Azage, Dmitriy, Niyazov, Lindsay B, Henderson, Ingrid M, Wentzensen, Berivan, Baskin, Maria J Guillen, Sacoto, Gregory D, Bowman, and Hans T, Bjornsson

Subjects

Models, Molecular, Protein Conformation, Developmental Disabilities, DNA Helicases, Mutation, Missense, Facies, Infant, Fibroblasts, Chromatin Assembly and Disassembly, Article, DNA-Binding Proteins, Histones, Structure-Activity Relationship, Phenotype, Child, Preschool, Humans, Female, Genetic Predisposition to Disease, Child, Genetic Association Studies

Abstract

The list of Mendelian disorders of the epigenetic machinery has expanded rapidly during the last five years. A few missense variants in the chromatin remodeler CHD1 have been found in several large scale sequencing efforts focused on uncovering the genetic etiology of autism. Here we describe CHD1 heterozygous missense variants in a cohort of patients with autism, speech apraxia, developmental delay and facial dysmorphic features. Importantly three of these variants occurred de novo. We also report on a patient with a de novo deletion covering a large fraction of the CHD1 gene without any obvious neurological phenotype. Our results suggest that variants in CHD1 can lead to diverse phenotypic outcomes; however, the neurodevelopmental phenotype appears to be limited to patients with missense variants, which is compatible with a dominant negative mechanism of disease.

Published

2017

25. Clinical spectrum of POLR3-related leukodystrophy caused by biallelic POLR1C pathogenic variants

Author

Ferdy K. Cayami, L Gauquelin, Dagmar Timmann, Marjo S. van der Knaap, Stefano D'Arrigo, László Sztriha, Nivedita Thakur, Gessica Vasco, Geneviève Bernard, Heike Philippi, Nicole I. Wolf, Richard Webster, Bart P.C. van de Warrenburg, François Hocke, Julia Rankin, Enrico Bertini, Adeline Vanderver, Abhijit Dixit, Penny Fallon, Kara Stuart Lewis, Dmitriy Niyazov, Sébastien Fribourg, Luan T. Tran, Trine Prescott, Rosalina M. L. van Spaendonk, Michael C. Kruer, Richard E. Person, Grace Yoon, Cyril Goizet, Eva Lai-Wah Fung, Isabelle Thiffault, Davide Tonduti, Evangeline Wassmer, Suvasini Sharma, Meriel McEntagart, Kether Guerrero, Claire Searle, and Ddd Study

Subjects

Pathology, medicine.medical_specialty, Medizin, Article, White matter, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, 0302 clinical medicine, medicine, Craniofacial, Genetics (clinical), 030304 developmental biology, 0303 health sciences, business.industry, Leukodystrophy, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], medicine.disease, Hyperintensity, 3. Good health, medicine.anatomical_structure, Severe phenotype, Male patient, Cohort, Neurology (clinical), business, Treacher Collins syndrome, 030217 neurology & neurosurgery

Abstract

ObjectiveTo determine the clinical, radiologic, and molecular characteristics of RNA polymerase III-related leukodystrophy (POLR3-HLD) caused by biallelic POLR1C pathogenic variants.MethodsA cross-sectional observational study involving 25 centers worldwide was conducted. Clinical and molecular information was collected on 23 unreported and previously reported patients with POLR3-HLD and biallelic pathogenic variants in POLR1C. Brain MRI studies were reviewed.ResultsFourteen female and 9 male patients aged 7 days to 23 years were included in the study. Most participants presented early in life (birth to 6 years), and motor deterioration was seen during childhood. A notable proportion of patients required a wheelchair before adolescence, suggesting a more severe phenotype than previously described in POLR3-HLD. Dental, ocular, and endocrine features were not invariably present (70%, 50%, and 50%, respectively). Five patients (22%) had a combination of hypomyelinating leukodystrophy and abnormal craniofacial development, including 1 individual with clear Treacher Collins syndrome (TCS) features. Brain MRI revealed hypomyelination in all cases, often with areas of pronounced T2 hyperintensity corresponding to T1 hypointensity of the white matter. Twenty-nine different pathogenic variants (including 12 new disease-causing variants) in POLR1C were identified.ConclusionsThis study provides a comprehensive description of POLR3-HLD caused by biallelic POLR1C pathogenic variants based on the largest cohort of patients to date. These results suggest distinct characteristics of POLR1C-related disorder, with a spectrum of clinical involvement characterized by hypomyelinating leukodystrophy with or without abnormal craniofacial development reminiscent of TCS.

Published

2019

26. Corrigendum

Author

Rami Abou Jamra, Diana Le Duc, Renee Bend, Jennifer Keller-Ramey, Sandra Yang, Mathew Wallis, Megan T. Cho, Jonathan B. Strober, Rhonda E. Schnur, Susan Walker, Stephen W. Scherer, David B. Everman, Susan M. Hiatt, Michael C. Pride, Konstantinos Zarbalis, Dmitriy Niyazov, Meron Azage, Brooke T. Smith, Steffen Syrbe, Jill L. Silverman, Verónica Martínez-Cerdeño, Benjamin Büttner, Ryan K. C. Yuen, Natasha J Brown, Urania Kotzaeridou, Jacqueline N. Crawley, Francis Jeshira Reynoso Santos, Cecilia R Giulivi, Gregory M. Cooper, Laurence J. Walsh, Jan H Doering, Johannes R. Lemke, Amber Begtrup, Richard E. Person, Alexios A Panoutsopoulos, Angelo Harlan De Crescenzo, Shuxi Liu, Chloé Quélin, Michael S. Hildebrand, Eleonora Napoli, Katelyn Payne, Christèle Dubourg, Evdokia Anagnostou, Lori Orosco, Heinrich Sticht, Barbara Kellam, and Andreas Ziegler

Subjects

Male, Adolescent, Autophagy-Related Proteins, Brain, Genetic Variation, Mice, Transgenic, Organ Size, Original Articles, Biology, Corrigenda, Protein Structure, Secondary, Mice, Neurodevelopmental Disorders, Child, Preschool, Brain size, Animals, Humans, Female, Neurology (clinical), Child, Neuroscience, Adaptor Proteins, Signal Transducing

Abstract

The underpinnings of mild to moderate neurodevelopmental delay remain elusive, often leading to late diagnosis and interventions. Here, we present data on exome and genome sequencing as well as array analysis of 13 individuals that point to pathogenic, heterozygous, mostly de novo variants in WDFY3 (significant de novo enrichment P = 0.003) as a monogenic cause of mild and non-specific neurodevelopmental delay. Nine variants were protein-truncating and four missense. Overlapping symptoms included neurodevelopmental delay, intellectual disability, macrocephaly, and psychiatric disorders (autism spectrum disorders/attention deficit hyperactivity disorder). One proband presented with an opposing phenotype of microcephaly and the only missense-variant located in the PH-domain of WDFY3. Findings of this case are supported by previously published data, demonstrating that pathogenic PH-domain variants can lead to microcephaly via canonical Wnt-pathway upregulation. In a separate study, we reported that the autophagy scaffolding protein WDFY3 is required for cerebral cortical size regulation in mice, by controlling proper division of neural progenitors. Here, we show that proliferating cortical neural progenitors of human embryonic brains highly express WDFY3, further supporting a role for this molecule in the regulation of prenatal neurogenesis. We present data on Wnt-pathway dysregulation in Wdfy3-haploinsufficient mice, which display macrocephaly and deficits in motor coordination and associative learning, recapitulating the human phenotype. Consequently, we propose that in humans WDFY3 loss-of-function variants lead to macrocephaly via downregulation of the Wnt pathway. In summary, we present WDFY3 as a novel gene linked to mild to moderate neurodevelopmental delay and intellectual disability and conclude that variants putatively causing haploinsufficiency lead to macrocephaly, while an opposing pathomechanism due to variants in the PH-domain of WDFY3 leads to microcephaly.

Published

2019

27. Correction: TANGO2: expanding the clinical phenotype and spectrum of pathogenic variants

Author

Amber Begtrup, Heather C Mefford, Hiltrud Muhle, Sharon F. Suchy, Barbara K. Burton, Angela Sun, Ingo Helbig, René Santer, J. Lawrence Merritt, Kolja Becker, Megan T. Cho, Katherine L. Helbig, Katie Golden-Grant, Amy Lacroix, Rachel Westman, Alison M. Muir, Ganka Douglas, Dmitriy Niyazov, Kristin G. Monaghan, Jennifer N. Dines, Almuth Caliebe, Jenny Thies, Leah Fleming, Manuela Pendziwiat, Can Ficicioglu, Alice Basinger, Dianne Laboy Cintrón, Katherine H. Kim, Kirsty McWalter, Francisca Millan, Joline C. Dalton, and Peter I. Karachunski

Subjects

Computer science, business.industry, Artificial intelligence, Clinical phenotype, business, computer.software_genre, Spectrum (topology), computer, Genetics (clinical), Natural language processing, Spelling

Abstract

The original version of this Article contained an error in the spelling of the author J. Lawrence Merritt, which was incorrectly given as Lawrence Merritt. This has now been corrected in both the PDF and HTML versions of the Article.

Published

2019

28. P.075 Clinical spectrum of POLR3-related leukodystrophy caused by biallelic POLR1C pathogenic variants

Author

Kether Guerrero, Claire Searle, L Gauquelin, Adeline Vanderver, Geneviève Bernard, Isabelle Thiffault, Dmitriy Niyazov, KS Lewis, Meriel McEntagart, Suvasini Sharma, Nicole I. Wolf, Dagmar Timmann, Davide Tonduti, E. Bertini, F Hocke, Julia Rankin, Richard Webster, Richard E. Person, Heike Philippi, P Fallon, Evangeline Wassmer, Stefano D'Arrigo, Gessica Vasco, Abhijit Dixit, El Fung, Sébastien Fribourg, R.M.L. van Spaendonk, van der Knaap, B van de Warrenburg, Ferdy K. Cayami, Grace Yoon, László Sztriha, MC Kruer, N Thakur, Cyril Goizet, Ddd Study, Trine Prescott, and Luan T. Tran

Subjects

Pediatrics, medicine.medical_specialty, business.industry, Leukodystrophy, General Medicine, medicine.disease, Hypomyelinating leukodystrophy, Hypodontia, Neurology, Hypogonadotropic hypogonadism, Cohort, medicine, Neurology (clinical), ENDOCRINE FEATURES, Craniofacial, business, Treacher Collins syndrome

Abstract

Background: Biallelic variants in POLR1C are associated with POLR3-related leukodystrophy (POLR3-HLD), or 4H leukodystrophy (Hypomyelination, Hypodontia, Hypogonadotropic Hypogonadism), and Treacher Collins syndrome (TCS). The clinical spectrum of POLR3-HLD caused by variants in this gene has not been described. Methods: A cross-sectional observational study involving 25 centers worldwide was conducted between 2016 and 2018. The clinical, radiologic and molecular features of 23 unreported and previously reported cases of POLR3-HLD caused by POLR1C variants were reviewed. Results: Most participants presented between birth and age 6 years with motor difficulties. Neurological deterioration was seen during childhood, suggesting a more severe phenotype than previously described. The dental, ocular and endocrine features often seen in POLR3-HLD were not invariably present. Five patients (22%) had a combination of hypomyelinating leukodystrophy and abnormal craniofacial development, including one individual with clear TCS features. Several cases did not exhibit all the typical radiologic characteristics of POLR3-HLD. A total of 29 different pathogenic variants in POLR1C were identified, including 13 new disease-causing variants. Conclusions: Based on the largest cohort of patients to date, these results suggest novel characteristics of POLR1C-related disorder, with a spectrum of clinical involvement characterized by hypomyelinating leukodystrophy with or without abnormal craniofacial development reminiscent of TCS.

Published

2019

29. Familial ebstein anomaly, left ventricular hypertrabeculation, and ventricular septal defect associated with a MYH7 mutation

Author

Theodorus J. Mulder, Audra L. Bettinelli, Sherri Longo, Birgit Funke, Dmitriy Niyazov, and Katherine A Lafferty

Subjects

Adult, Heart Septal Defects, Ventricular, Male, Heterozygote, medicine.medical_specialty, Ventricular Dysfunction, Left, Exon, Genetic etiology, Internal medicine, Genetics, medicine, Humans, Left ventricular hypertrabeculation, Child, Genetics (clinical), Likely pathogenic, Genetic testing, Myosin Heavy Chains, medicine.diagnostic_test, business.industry, Infant, Ebstein Anomaly, Endocrinology, EBSTEIN ANOMALY, Echocardiography, Child, Preschool, Mutation, Mutation (genetic algorithm), Cardiology, Female, MYH7, business, Cardiac Myosins

Abstract

Ebstein anomaly is a rare congenital heart defect that most often occurs sporadically within a kindred. Familial cases, although reported, are uncommon. At this time, the genetic etiology of Ebstein anomaly is not fully elucidated. Here, we describe clinical and molecular investigations of a rare case of familial Ebstein anomaly in association with a likely pathogenic mutation of the MYH7 gene. The severity of presentation varies, and Ebstein anomaly can be observed in association with such other heart defects as ventricular septal defect and left ventricular (LV) hypertrabeculation, as seen in our family of study. In our family of study, the 31-year-old father and four of his children have been diagnosed with Ebstein anomaly. Genetic testing revealed that the father was heterozygous for the Glu1220del variant detected in exon 27 of the MYH7 gene. The MYH7 gene encodes the β-myosin heavy chain and is expressed in cardiac muscle. DNA sequencing of three of his affected children confirmed that they carried the same variant while the fourth affected child was not available for testing. This is the first report of familial Ebstein anomaly associated with the Glu1220del mutation of the MYH7 gene. The mutation segregates with disease in a family with autosomal dominant transmission of congenital heart defects including Ebstein anomaly and other associated cardiovascular defects including LV hypertrabeculation and ventricular septal defect.

Published

2013

30. Primary Mitochondrial Disease and Secondary Mitochondrial Dysfunction: Importance of Distinction for Diagnosis and Treatment

Author

Stephan G. Kahler, Richard E. Frye, and Dmitriy Niyazov

Subjects

0301 basic medicine, Genetics, Mutation, Mitochondrial DNA, Muscle biopsy, medicine.diagnostic_test, business.industry, Mitochondrial disease, Review Article, Mitochondrion, medicine.disease_cause, medicine.disease, Human mitochondrial genetics, Phenotype, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine, Clinical significance, business, 030217 neurology & neurosurgery, Genetics (clinical)

Abstract

Mitochondrial disease refers to a heterogeneous group of disorders resulting in defective cellular energy production due to abnormal oxidative phosphorylation (oxphos). Primary mitochondrial disease (PMD) is diagnosed clinically and ideally, but not always, confirmed by a known or indisputably pathogenic mitochondrial DNA (mtDNA) or nuclear DNA (nDNA) mutation. The PMD genes either encode oxphos proteins directly or they affect oxphos function by impacting production of the complex machinery needed to run the oxphos process. However, many disorders have the ‘mitochondrial' phenotype without an identifiable mtDNA or nDNA mutation or they have a variant of unknown clinical significance. Secondary mitochondrial dysfunction (SMD) can be caused by genes encoding neither function nor production of the oxphos proteins and accompanies many hereditary non-mitochondrial diseases. SMD may also be due to nongenetic causes such as environmental factors. In our practice, we see many patients with clinical signs of mitochondrial dysfunction based on phenotype, biomarkers, imaging, muscle biopsy, or negative/equivocal mtDNA or nDNA test results. In these cases, it is often tempting to assign a patient's phenotype to ‘mitochondrial disease', but SMD is often challenging to distinguish from PMD. Fortunately, rapid advances in molecular testing, made possible by next generation sequencing, have been effective at least in some cases in establishing accurate diagnoses to distinguish between PMD and SMD. This is important, since their treatments and prognoses can be quite different. However, even in the absence of the ability to distinguish between PMD and SMD, treating SMD with standard treatments for PMD can be effective. We review the latest findings regarding mitochondrial disease/dysfunction and give representative examples in which differentiation between PMD and SMD has been crucial for diagnosis and treatment.

Published

2016

31. Mitochondrial Dysfunction in a Patient with 8q21.11 Deletion and Charcot-Marie-Tooth Disease Type 2K due to GDAP1 Haploinsufficiency

Author

Diane Africk and Dmitriy Niyazov

Subjects

Genetics, Proband, Biology, medicine.disease, Short stature, Contiguous gene syndrome, Tooth disease, Intellectual disability, Failure to thrive, medicine, medicine.symptom, Haploinsufficiency, Developmental regression, Genetics (clinical)

Abstract

Unbalanced chromosomal rearrangements typically cause multiple organ system involvement including neurodevelopmental deficits. It is atypical, however, to experience developmental and neurological regression. We describe a female with intellectual disability, failure to thrive, short stature, multiple congenital anomalies, and dysmorphic features and a previously diagnosed de novo 8q21.11 deletion at the age of 7. However, at the age of 11, she experienced neurological and developmental regression. The GDAP1 gene encoding ganglioside-induced differentiation-associated protein 1 was deleted in the patient as a part of the contiguous gene syndrome. We argue that haploinsufficiency of GDAP1 could have contributed to the proband's regression based on its involvement in mitochondrial function and a signal transduction pathway in neuronal development.

Published

2015

32. High-resolution array CGH defines critical regions and candidate genes for microcephaly, abnormalities of the corpus callosum, and seizure phenotypes in patients with microdeletions of 1q43q44

Author

Patricia I. Bader, Allen N. Lamb, Rhonda E. Schnur, Deepti Babu, Jill A. Rosenfeld, Lisa G. Shaffer, Michael L. Netzloff, John S. Bamforth, Beth S. Torchia, Sandra A. Farrell, Raymond C. Tervo, Kristen Hanson, Ryan N. Traylor, Tracy Stroud, Michael Marble, Roger A. Schultz, Dmitriy Niyazov, Shelley Williams, Arthur S. Aylsworth, Susan Sell, Lauren B. Coffey, Michelle Steinraths, J. Britt Ravnan, James J. Filiano, Urvashi Surti, Blake C. Ballif, Aaron Theisen, Marianne McGuire, Roger L. Ladda, and Bassem A. Bejjani

Subjects

Male, Microcephaly, Candidate gene, Adolescent, Biology, Corpus callosum, Seizures, Intellectual Disability, Genetics, medicine, Humans, Abnormalities, Multiple, Child, In Situ Hybridization, Fluorescence, Genetics (clinical), Oligonucleotide Array Sequence Analysis, Comparative Genomic Hybridization, Infant, Syndrome, Microdeletion syndrome, medicine.disease, Penetrance, Phenotype, Genes, Chromosomes, Human, Pair 1, Child, Preschool, Female, Agenesis of Corpus Callosum, Chromosome Deletion, Haploinsufficiency, Biomarkers, Comparative genomic hybridization

Abstract

Microdeletions of 1q43q44 result in a recognizable clinical disorder characterized by moderate to severe intellectual disability (ID) with limited or no expressive speech, characteristic facial features, hand and foot anomalies, microcephaly (MIC), abnormalities (agenesis/hypogenesis) of the corpus callosum (ACC), and seizures (SZR). Critical regions have been proposed for some of the more prominent features of this disorder such as MIC and ACC, yet conflicting data have prevented precise determination of the causative genes. In this study, the largest of pure interstitial and terminal deletions of 1q43q44 to date, we characterized 22 individuals by high-resolution oligonucleotide microarray-based comparative genomic hybridization. We propose critical regions and candidate genes for the MIC, ACC, and SZR phenotypes associated with this microdeletion syndrome. Three cases with MIC had small overlapping or intragenic deletions of AKT3, an isoform of the protein kinase B family. The deletion of only AKT3 in two cases implicates haploinsufficiency of this gene in the MIC phenotype. Likewise, based on the smallest region of overlap among the affected individuals, we suggest a critical region for ACC that contains ZNF238, a transcriptional and chromatin regulator highly expressed in the developing and adult brain. Finally, we describe a critical region for the SZR phenotype which contains three genes (FAM36A, C1ORF199, and HNRNPU). Although ~90% of cases in this study and in the literature fit these proposed models, the existence of phenotypic variability suggests other mechanisms such as variable expressivity, incomplete penetrance, position effects, or multigenic factors could account for additional complexity in some cases.

Published

2011

33. An immune tolerance approach using methotrexate in the naïve setting of patients treated with a therapeutic protein: Experience in infantile Pompe disease

Author

Sherry Langston, Neerja Gupta, James Weisfield-Adams, Marta Sabbadini, Zoheb B. Kazi, Sheela Nampoothiri, Seymour Packman, Diana Ballhausen, Priya S. Kishnani, Bradley Troxler, Jean-Marc Nuoffer, Alexandra Joseph, Marianne Rohrbach, Ankit K. Desai, Katalin Scherer, Susan M. Richards, Clarisa Maxit, Angelika Erwin, Annette Feigenbaum, Dmitriy Niyazov, Pranoot Tanpaiboon, William B. Rizzo, David Kronn, Alison McVie-Wylie, Crystal Sung, and Omar A. Abdul-Rahman

Subjects

0301 basic medicine, business.industry, Endocrinology, Diabetes and Metabolism, Therapeutic protein, Disease, Biochemistry, Immune tolerance, 03 medical and health sciences, 030104 developmental biology, Endocrinology, Immunology, Genetics, medicine, Methotrexate, business, Molecular Biology, medicine.drug

Published

2018

34. De novo mutations in CSNK2A1 are associated with neurodevelopmental abnormalities and dysmorphic features

Author

Wendy K. Chung, Volkan Okur, Michael C. Schneider, Lauren Brady, Meron Azage, Jonathan Picker, Sharyn A. Lincoln, Amy Dameron, Dmitriy Niyazov, Carolyn D. Applegate, Berivan Baskin, Mark A. Tarnopolsky, Hans T. Bjornsson, Megan T. Cho, Rebecca Willaert, Jane Juusola, Sharon R. Smith, Shannon Sattler, Kyle Retterer, and Lindsay B. Henderson

Subjects

0301 basic medicine, Microcephaly, Adolescent, Biology, medicine.disease_cause, Bioinformatics, 03 medical and health sciences, Germline mutation, Dysmorphic feature, Intellectual Disability, Intellectual disability, Genetics, medicine, Humans, Exome, Genetic Predisposition to Disease, Casein Kinase II, Child, Genetics (clinical), Exome sequencing, Germ-Line Mutation, Mutation, Pachygyria, High-Throughput Nucleotide Sequencing, medicine.disease, Body Dysmorphic Disorders, Hypotonia, 030104 developmental biology, Neurodevelopmental Disorders, Child, Preschool, Female, medicine.symptom

Abstract

Whole exome sequencing (WES) can be used to efficiently identify de novo genetic variants associated with genetically heterogeneous conditions including intellectual disabilities. We have performed WES for 4102 (1847 female; 2255 male) intellectual disability/developmental delay cases and we report five patients with a neurodevelopmental disorder associated with developmental delay, intellectual disability, behavioral problems, hypotonia, speech problems, microcephaly, pachygyria and dysmorphic features in whom we have identified de novo missense and canonical splice site mutations in CSNK2A1, the gene encoding CK2α, the catalytic subunit of protein kinase CK2, a ubiquitous serine/threonine kinase composed of two regulatory (β) and two catalytic (α and/or α') subunits. Somatic mutations in CSNK2A1 have been implicated in various cancers; however, this is the first study to describe a human condition associated with germline mutations in any of the CK2 subunits.

Published

2016

35. 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

36. Mitochondrial Dysfunction in a Patient with 8q21.11 Deletion and Charcot-Marie-Tooth Disease Type 2K due to GDAP1 Haploinsufficiency

Author

Dmitriy, Niyazov and Diane, Africk

Subjects

Short Report

Abstract

Unbalanced chromosomal rearrangements typically cause multiple organ system involvement including neurodevelopmental deficits. It is atypical, however, to experience developmental and neurological regression. We describe a female with intellectual disability, failure to thrive, short stature, multiple congenital anomalies, and dysmorphic features and a previously diagnosed de novo 8q21.11 deletion at the age of 7. However, at the age of 11, she experienced neurological and developmental regression. The GDAP1 gene encoding ganglioside-induced differentiation-associated protein 1 was deleted in the patient as a part of the contiguous gene syndrome. We argue that haploinsufficiency of GDAP1 could have contributed to the proband's regression based on its involvement in mitochondrial function and a signal transduction pathway in neuronal development.

Published

2015

37. Heart Transplantation for a Patient With Kearns-Sayre Syndrome and End-Stage Heart Failure

Author

Michael Bates, Hector O. Ventura, David J. Homan, Hamang Patel, Patrick W. Fisher, Stacy Mandras, Dmitriy Niyazov, and Gene Parrino

Subjects

Heart transplantation, medicine.medical_specialty, business.industry, medicine.medical_treatment, MEDLINE, Emergency Nursing, medicine.disease, Kearns–Sayre syndrome, Internal medicine, Heart failure, Emergency Medicine, medicine, Cardiology, End stage heart failure, Young adult, Cardiology and Cardiovascular Medicine, business

Published

2011

38. Practice patterns of mitochondrial disease physicians in North America. Part 2: treatment, care and management

Author

Sumit Parikh, Amy Goldstein, Mary Kay Koenig, Fernando Scaglia, Gregory M. Enns, Russell Saneto, Irina Anselm, Abigail Collins, Bruce H. Cohen, Suzanne D. DeBrosse, David Dimmock, Marni J. Falk, Jaya Ganesh, Carol Greene, Andrea L. Gropman, Richard Haas, Stephen G. Kahler, John Kamholz, Fran Kendall, Mark S. Korson, Andre Mattman, Margherita Milone, Dmitriy Niyazov, Phillip L. Pearl, Tyler Reimschisel, Ramona Salvarinova-Zivkovic, Katherine Sims, Mark Tarnopolsky, Chang-Yong Tsao, Johan van Hove, Laurence Walsh, and Lynne A. Wolfe

Subjects

medicine.medical_specialty, Mitochondrial Diseases, Practice patterns, business.industry, Mitochondrial disease, Consensus criteria, Cell Biology, Vitamins, medicine.disease, Subspecialty, Preventive care, Insurance Coverage, Xenobiotics, Clinical Practice, Family medicine, North America, Molecular Medicine, Medicine, Humans, Limited evidence, Practice Patterns, Physicians', business, Molecular Biology, Routine care, Exercise

Abstract

Mitochondrial medicine is a young subspecialty. Clinicians have limited evidence-based guidelines on which to formulate clinical decisions regarding diagnosis, treatment and management for patients with mitochondrial disorders. Mitochondrial medicine specialists have cobbled together an informal set of rules and paradigms for preventive care and management based in part on anecdotal experience. The Mitochondrial Medicine Society (MMS) assessed the current state of clinical practice including diagnosis, preventive care and treatment, as provided by various mitochondrial disease providers in North America. In this second of two reports, we present data related to clinical practice that highlight the challenges clinicians face in the routine care of patients with established mitochondrial disease. Concerning variability in treatment and preventative care approaches were noted. We hope that sharing this information will be a first step toward formulating a set of consensus criteria and establishing standards of care.

Published

2013

39. Practice patterns of mitochondrial disease physicians in North America. Part 1: diagnostic and clinical challenges

Author

Abigail Collins, Andre Mattman, Marni J. Falk, Mark A. Tarnopolsky, David Dimmock, Phillip L. Pearl, Ramona Salvarinova-Zivkovic, Johan L.K. Van Hove, Russell P. Saneto, Suzanne D. DeBrosse, Sumit Parikh, John Kamholz, Andrea L. Gropman, Dmitriy Niyazov, Jaya Ganesh, Richard Haas, Irina Anselm, Katherine B. Sims, Laurence E. Walsh, Chang Yong Tsao, Stephen G. Kahler, Gregory M. Enns, Mark S. Korson, Fran Kendall, Amy Goldstein, Tyler Reimschisel, Bruce H. Cohen, Carol L. Greene, Lynne A. Wolfe, Margherita Milone, Fernando Scaglia, and Mary Kay Koenig

Subjects

medicine.medical_specialty, Mitochondrial Diseases, Practice patterns, business.industry, Mitochondrial disease, MEDLINE, Consensus criteria, Cell Biology, medicine.disease, Subspecialty, Preventive care, Patient management, Family medicine, Physicians, North America, medicine, Molecular Medicine, Humans, Limited evidence, Practice Patterns, Physicians', business, Molecular Biology

Abstract

Mitochondrial medicine is a young subspecialty. Clinicians have a limited evidence base on which to formulate clinical decisions regarding diagnosis, treatment and patient management. Mitochondrial medicine specialists have cobbled together an informal set of rules and paradigms for preventive care and management based in part on anecdotal experience. The Mitochondrial Medicine Society (MMS) assessed the current state of clinical practice from diagnosis, to preventive care and treatment, as provided by various mitochondrial disease specialists in North America. We hope that by obtaining this information we can begin moving towards formulating a set of consensus criteria and establishing standards of care.

Published

2013

40. Phenotypic heterogeneity of genomic disorders and rare copy-number variants

Author

Kathleen A. Leppig, Rhonda E. Schnur, Robert Roger Lebel, Santhosh Girirajan, Kisha D. Johnson, Rosemarie Smith, Brad Angle, Robyn A. Filipink, Susie Ball, Dmitriy Niyazov, Luis F. Escobar, J. Edward Spence, Bradley P. Coe, Marjan M. Nezarati, Evan E. Eichler, Wendy S. Meschino, Jill A. Rosenfeld, Juliann Mcconnell, Salmo Raskin, Campbell K. Brasington, Lisa G. Shaffer, Sumit Parikh, Neil R. Friedman, Gordon C. Gowans, Natasha Shur, Dima El-Khechen, Carol L. Clericuzio, Amy Goldstein, Erika Aberg, Donna M. Martin, Laura S. Martin, David W. Stockton, Alexander Asamoah, Lynette S. Penney, Heidi Thiese, Blake C. Ballif, Erin P. Carmany, Kelly E. Jackson, Kiana Siefkas, Judith A. Martin, and Marianne McGuire

Subjects

Male, DNA Copy Number Variations, Developmental Disabilities, Genomics, Biology, Congenital Abnormalities, Genetic Heterogeneity, Sex Factors, Intellectual Disability, Genotype, Humans, Copy-number variation, Genetic variability, Autistic Disorder, Child, Oligonucleotide Array Sequence Analysis, Genetics, Comparative Genomic Hybridization, Genetic heterogeneity, Genome, Human, General Medicine, Phenotype, Human genome, Female, Common disease-common variant, Comparative genomic hybridization

Abstract

Some copy-number variants are associated with genomic disorders with extreme phenotypic heterogeneity. The cause of this variation is unknown, which presents challenges in genetic diagnosis, counseling, and management.We analyzed the genomes of 2312 children known to carry a copy-number variant associated with intellectual disability and congenital abnormalities, using array comparative genomic hybridization.Among the affected children, 10.1% carried a second large copy-number variant in addition to the primary genetic lesion. We identified seven genomic disorders, each defined by a specific copy-number variant, in which the affected children were more likely to carry multiple copy-number variants than were controls. We found that syndromic disorders could be distinguished from those with extreme phenotypic heterogeneity on the basis of the total number of copy-number variants and whether the variants are inherited or de novo. Children who carried two large copy-number variants of unknown clinical significance were eight times as likely to have developmental delay as were controls (odds ratio, 8.16; 95% confidence interval, 5.33 to 13.07; P=2.11×10(-38)). Among affected children, inherited copy-number variants tended to co-occur with a second-site large copy-number variant (Spearman correlation coefficient, 0.66; P0.001). Boys were more likely than girls to have disorders of phenotypic heterogeneity (P0.001), and mothers were more likely than fathers to transmit second-site copy-number variants to their offspring (P=0.02).Multiple, large copy-number variants, including those of unknown pathogenic significance, compound to result in a severe clinical presentation, and secondary copy-number variants are preferentially transmitted from maternal carriers. (Funded by the Simons Foundation Autism Research Initiative and the National Institutes of Health.).

Published

2012

41. A copy number variation morbidity map of developmental delay

Author

Carl Baker, Lisa G. Shaffer, Gregory M. Cooper, Patricia I. Bader, Marybeth Hummel, Krys Johnson, Heather J. Stalker, Santhosh Girirajan, Kathleen A. Leppig, Tiffany H. Vu, Hoda Abdel-Hamid, Blake C. Ballif, Jill A. Rosenfeld, Nora Alexander, Vandana Shashi, Charles A. Williams, Catherine Rehder, Jerome L. Gorski, Dmitriy Niyazov, Evan E. Eichler, Bradley P. Coe, Heidi Thiese, Rizwan Hamid, Elizabeth McCracken, Jennifer Kussmann, and Vickie L. Hannig

Subjects

Adult, endocrine system diseases, Developmental Disabilities, Gene Dosage, Disease, Biology, Article, Congenital Abnormalities, 03 medical and health sciences, 0302 clinical medicine, Genetic variation, Intellectual disability, mental disorders, Genetics, medicine, Humans, Copy-number variation, Exome, 030304 developmental biology, 0303 health sciences, Genetic heterogeneity, Chromosome Mapping, Genetic Variation, Microdeletion syndrome, medicine.disease, 3. Good health, Child, Preschool, Autism, 030217 neurology & neurosurgery

Abstract

To understand the genetic heterogeneity underlying developmental delay, we compared copy number variants (CNVs) in 15,767 children with intellectual disability and various congenital defects (cases) to CNVs in 8,329 unaffected adult controls. We estimate that ∼14.2% of disease in these children is caused by CNVs >400 kb. We observed a greater enrichment of CNVs in individuals with craniofacial anomalies and cardiovascular defects compared to those with epilepsy or autism. We identified 59 pathogenic CNVs, including 14 new or previously weakly supported candidates, refined the critical interval for several genomic disorders, such as the 17q21.31 microdeletion syndrome, and identified 940 candidate dosage-sensitive genes. We also developed methods to opportunistically discover small, disruptive CNVs within the large and growing diagnostic array datasets. This evolving CNV morbidity map, combined with exome and genome sequencing, will be critical for deciphering the genetic basis of developmental delay, intellectual disability and autism spectrum disorders.

Published

2011

42. Distinctive phenotype in 9 patients with deletion of chromosome 1q24-q25

Author

Brad Angle, Maria L. Helgeson, Ralph S. Lachman, Dmitriy Niyazov, Wendy E. Smith, Jill A. Rosenfeld, Jessica Moline, Elaine H. Zackai, Valerie Banks, Douglas G. Ashley, Karen W. Gripp, Robert Roger Lebel, Rocio Moran, Deepika D Cunha Burkardt, Nancy Kramer, John M. Graham, and Cathy A. Stevens

Subjects

Microcephaly, Adolescent, Chromosome Disorders, Biology, Short stature, Article, Young Adult, Intellectual Disability, Genetics, medicine, Humans, Abnormalities, Multiple, Child, Genetics (clinical), In Situ Hybridization, Fluorescence, Comparative Genomic Hybridization, Brachydactyly, Infant, Bone age, Anatomy, Syndrome, Microdeletion syndrome, medicine.disease, Microarray Analysis, DNM3, medicine.anatomical_structure, Seckel syndrome, Phenotype, Chromosomes, Human, Pair 1, Child, Preschool, Face, Eyelid, medicine.symptom, Chromosome Deletion

Abstract

Reports of individuals with deletions of 1q24→q25 share common features of prenatal onset growth deficiency, microcephaly, small hands and feet, dysmorphic face and severe cognitive deficits. We report nine individuals with 1q24q25 deletions, who show distinctive features of a clinically recognizable 1q24q25 microdeletion syndrome: prenatal-onset microcephaly and proportionate growth deficiency, severe cognitive disability, small hands and feet with distinctive brachydactyly, single transverse palmar flexion creases, fifth finger clinodactyly and distinctive facial features: upper eyelid fullness, small ears, short nose with bulbous nasal tip, tented upper lip, and micrognathia. Radiographs demonstrate disharmonic osseous maturation with markedly delayed bone age. Occasional features include cleft lip and/or palate, cryptorchidism, brain and spinal cord defects, and seizures. Using oligonucleotide-based array comparative genomic hybridization, we defined the critical deletion region as 1.9 Mb at 1q24.3q25.1 (chr1: 170,135,865-172,099,327, hg18 coordinates), containing 13 genes and including CENPL, which encodes centromeric protein L, a protein essential for proper kinetochore function and mitotic progression. The growth deficiency in this syndrome is similar to what is seen in other types of primordial short stature with microcephaly, such as Majewski osteodysplastic primordial dwarfism, type II (MOPD2) and Seckel syndrome, which result from loss-of-function mutations in genes coding for centrosomal proteins. DNM3 is also in the deleted region and expressed in the brain, where it participates in the Shank-Homer complex and increases synaptic strength. Therefore, DNM3 is a candidate for the cognitive disability, and CENPL is a candidate for growth deficiency in this 1q24q25 microdeletion syndrome.

Published

2010

43. Mitochondrial genome sequencing: A valuable addition to whole exome sequencing for the molecular diagnosis of mitochondrial disorders

Author

Dolores Arjona, Renkui Bai, Sumit Parikh, Dmitriy Niyazov, Mark A. Tarnopolsky, Kelly Parsons, Yizhou Ye, Kyle Retterer, Wendy K. Chung, Nicole Warren-Mora, Sharon F. Suchy, Sherri J. Bale, Jaimie Higgs, Amanda Balog, and Gabriele Richard

Subjects

Genetics, Cancer genome sequencing, Mitochondrial DNA, Mitochondrial disease, medicine, Molecular Medicine, Cell Biology, Biology, medicine.disease, Molecular Biology, Exome, Exome sequencing

Published

2015

44. Whole exome sequencing and whole mitochondrial genome sequencing for molecular diagnosis of mitochondrial disorders: Lessons from 865 Cases

Author

Mark A. Tarnopolsky, Amy Goldstein, Jane Juusola, Sumit Parikh, Dolores Arjona, Kyle Retterer, William C. Copeland, Sharon F. Suchy, Gregory M. Enns, Amanda Balog, Sherri J. Bale, Jaimie Higgs, Gabriele Richard, Marni J. Falk, Patrik Vitazka, Dmitriy Niyazov, Renkui Bai, Richard Haas, and Wendy K. Chung

Subjects

Genetics, Cancer genome sequencing, Mitochondrial DNA, Mitochondrial disease, medicine, Molecular Medicine, Cell Biology, Biology, medicine.disease, Molecular Biology, Exome, Exome sequencing

Published

2015

45. Diagnosis and treatment of secondary mitochondrial disease

Author

Dmitriy Niyazov and Diane Africk

Subjects

business.industry, Mitochondrial disease, medicine, Cancer research, Molecular Medicine, Cell Biology, medicine.disease, business, Molecular Biology

Published

2012

46. Corrigendum: A copy number variation morbidity map of developmental delay

Author

Elizabeth McCracken, Patricia I. Bader, Krys Johnson, Nora Alexander, Charles A. Williams, Kathleen A. Leppig, Hoda Abdel-Hamid, Marybeth Hummel, Blake C. Ballif, Heidi Thiese, Heather J. Stalker, Evan E. Eichler, Rizwan Hamid, Catherine Rehder, Jill A. Rosenfeld, Lisa G. Shaffer, Bradley P. Coe, Vandana Shashi, Carl Baker, Gregory M. Cooper, Vickie L. Hannig, Dmitriy Niyazov, Santhosh Girirajan, Tiffany H. Vu, Jennifer Kussmann, and Jerome L. Gorski

Subjects

Set (abstract data type), education.field_of_study, Calculation error, Statistics, Population, Genetics, Table (database), Copy-number variation, Biology, education, Penetrance, Population control

Abstract

Nat. Genet. 43, 838–846 (2011); published online 14 August 2011; corrected after print 27 August 2014 In the version of this article initially published, in Table 1 and its associated text, there was a calculation error in which the relative sizes of the case and control populations were set to be equal; because the size of the case population (15,767) was nearly double that of the control population (8,329), this resulted in erroneously inflated penetrance estimates.

Published

2014

47. Confirming TDP2 mutation in spinocerebellar ataxia autosomal recessive 23 (SCAR23)

Author

Guido Zagnoli-Vieira, BSc, Francesco Bruni, PhD, Kyle Thompson, Langping He, Sarah Walker, Arjan P.M. de Brouwer, Robert Taylor, FRCPath, Dmitriy Niyazov, and and Keith W. Caldecott

Subjects

0301 basic medicine, Genetics, Correction, Biology, medicine.disease, Q1, Article, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Mutation (genetic algorithm), Spinocerebellar ataxia, medicine, Neurology (clinical), 030217 neurology & neurosurgery, Genetics (clinical)

Abstract

Objective\ud To address the relationship between mutations in the DNA strand break repair protein tyrosyl DNA phosphodiesterase 2 (TDP2) and spinocerebellar ataxia autosomal recessive 23\ud (SCAR23) and to characterize the cellular phenotype of primary fibroblasts from this disease.\ud \ud Methods\ud We have used exome sequencing, Sanger sequencing, gene editing and cell biology, biochemistry,and subcellular mitochondrial analyses for this study.\ud \ud Results\ud We have identified a patient in the United States with SCAR23 harboring the same homozygous TDP2 mutation as previously reported in 3 Irish siblings (c.425+1G>A). The current and Irish patients share the same disease haplotype, but the current patient lacks a homozygous\ud variant present in the Irish siblings in the closely linked gene ZNF193, eliminating this as a contributor to the disease. The current patient also displays symptoms consistent with mitochondrial dysfunction, although levels of mitochondrial function in patient primary skin fibroblasts are normal. However, we demonstrate an inability in patient primary fibroblasts to rapidly repair topoisomerase-induced DNA double-strand breaks (DSBs) in the nucleus and profound hypersensitivity to this type of DNA damage.\ud \ud Conclusions\ud These data confirm the TDP2 mutation as causative for SCAR23 and highlight the link between defects in nuclear DNA DSB repair, developmental delay, epilepsy, and ataxia.