Your search keyword '"Michael O. Dorschner"' showing total 13 results

1. Somatic Mosaicism of a PDGFRB Activating Variant in Aneurysms of the Intracranial, Coronary, Aortic, and Radial Artery Vascular Beds

Author

Carolina A. Parada, Fatima M. El‐Ghazali, Daphne Toglia, Jacob Ruzevick, Malia McAvoy, Samuel Emerson, Yigit Karasozen, Tina Busald, Ahmad A. Nazem, Shaun M. Suranowitz, Sherene Shalhub, Desiree A. Marshall, Luis F. Gonzalez‐Cuyar, Michael O. Dorschner, and Manuel Ferreira

Subjects

cerebral aneurysm, fusiform, mosaic, PDGFRB, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background Activating variants in platelet‐derived growth factor receptor beta (PDGFRB), including a variant we have previously described (p.Tyr562Cys [g.149505130T>C [GRCh37/hg19]; c.1685A>G]), are associated with development of multiorgan pathology, including aneurysm formation. To investigate the association between the allele fraction genotype and histopathologic phenotype, we performed an expanded evaluation of post‐mortem normal and aneurysmal tissue specimens from the previously published index patient. Methods and Results Following death due to diffuse subarachnoid hemorrhage in a patient with mosaic expression of the above PDGFRB variant, specimens from the intracranial, coronary, radial and aortic arteries were harvested. DNA was extracted and alternate allele fractions (AAF) of PDGFRB were determined using digital droplet PCR. Radiographic and histopathologic findings, together with genotype expression of PDGFRB were then correlated in aneurysmal tissue and compared to non‐aneurysmal tissue. The PDGFRB variant was identified in the vertebral artery, basilar artery, and P1 segment aneurysms (AAF: 28.7%, 16.4%, and 17.8%, respectively). It was also identified in the coronary and radial artery aneurysms (AAF: 22.3% and 20.6%, respectively). In phenotypically normal intracranial and coronary artery tissues, the PDGFRB variant was not present. The PDGFRB variant was absent from lymphocyte DNA and normal tissue, confirming it to be a non‐germline somatic variant. Primary cell cultures from a radial artery aneurysm localized the PDGFRB variant to CD31‐, non‐endothelial cells. Conclusions Constitutive expression of PDGFRB within the arterial wall is associated with the development of human fusiform aneurysms. The role of targeted therapy with tyrosine kinase inhibitors in fusiform aneurysms with PDGFRB mutations should be further studied.

Published

2022

2. Spinal cord‐predominant neuropathology in an adult‐onset case of <scp> POLR3A </scp> ‐related spastic ataxia

Author

Thomas D. Bird, Jing Zhang, C. Dirk Keene, Caitlin S. Latimer, Michael O. Dorschner, Suman Jayadev, Dong-Hui Chen, Bradley Rolf, and Trevor M. Sytsma

Subjects

Proband, congenital, hereditary, and neonatal diseases and abnormalities, Pathology, medicine.medical_specialty, Spinocerebellar tract, Ataxia, Hereditary spastic paraplegia, business.industry, General Medicine, Neuropathology, Spinal cord, Compound heterozygosity, medicine.disease, Pathology and Forensic Medicine, medicine.anatomical_structure, medicine, Neurology (clinical), medicine.symptom, Differential diagnosis, business

Abstract

Biallelic mutations in POLR3A have been associated with childhood-onset hypomyelinating leukodystrophies and adolescent-to-adult-onset spastic ataxia, the latter of which has been linked to the intronic variant c.1909 + 22G>A. We report a case of adult-onset spastic ataxia in a 75-year-old man, being a compound heterozygous carrier of this variant, whose brain and spinal cord were for the first time investigated by neuropathological examination. We describe prominent degeneration of the posterior columns, spinocerebellar tracts, and anterior corticospinal tracts of the spinal cord in a pattern resembling Friedreich's ataxia, with a notable lack of significant white matter pathology throughout the brain, in marked contrast with childhood-onset cases. Immunohistochemical examination for the POLR3A protein demonstrated no apparent differences in localization or staining intensity between the proband and an age-matched control subject. We demonstrate the clinicopathologic description of POLR3A-related neurodegenerative disease and also mention the differential diagnosis of the childhood-onset hypomyelinating leukodystrophy and late-onset spastic ataxia phenotypes.

Published

2021

3. Genetic counseling for early onset and familial dementia: Patient perspectives on exome sequencing

Author

Michael O. Dorschner, Suman Jayadev, Elizabeth E. Blue, Stephanie A. Bucks, and Bradley Rolf

Subjects

Genetic counseling, Population, Genetic Counseling, Context (language use), 03 medical and health sciences, 0302 clinical medicine, Exome Sequencing, Humans, Medicine, Dementia, Exome, Genetic Testing, education, Genetics (clinical), Exome sequencing, Genetic testing, 0303 health sciences, education.field_of_study, medicine.diagnostic_test, business.industry, 030305 genetics & heredity, Regret, medicine.disease, 030220 oncology & carcinogenesis, Observational study, business, Clinical psychology

Abstract

Genetic testing has become routine for many inherited conditions; however, little is known about the unique issues that arise when offering genetic testing for inherited forms of dementia. To better understand the patient perspective, we surveyed study participants about their experiences as they underwent genetic counseling and genetic testing for dementia. We recruited 50 pairs of subjects. Each pair was comprised of one person with cognitive impairment and a cognitively intact co-participant. Study participants received pre- and post-test genetic counseling and comprehensive genetic testing for dementia. During the study, participant pairs completed four surveys which asked about their experience. Testing began with a 38 gene dementia panel. Participants with negative panel results or variants of uncertain significance (VUS) were reflexed to exome sequencing (ES). Twenty-nine participants (58%) reported that their primary motivation to join the study was for the benefit to their families. Fifty-two percent of participants initially planned to use their test results to make health and wellness changes, but, six months after disclosure, only 31% had done so. Six months after result disclosure, approximately 90% of participant pairs accurately recalled their genetic test results. Overall satisfaction with testing was high, and decision regret was negligible. This observational study describes the experiences of study participants undergoing genetic counseling and genetic testing for dementia and found that most participant pairs accurately recalled their results up to six months following disclosure while also maintaining high levels of satisfaction without decision regret. These findings suggest that, in the context of genetic counseling, genetic testing can be effectively used in this population.

Published

2021

4. Homozygous CADPS2 Mutations Cause Neurodegenerative Disease with Lewy Body-like Pathology in Parrots

Author

Oswaldo Lorenzo‐Betancor, Livio Galosi, Laura Bonfili, Anna Maria Eleuteri, Valentina Cecarini, Ranieri Verin, Fabrizio Dini, Anna‐Rita Attili, Sara Berardi, Lucia Biagini, Patrizia Robino, Maria Cristina Stella, Dora Yearout, Michael O. Dorschner, Debby W. Tsuang, Giacomo Rossi, and Cyrus P. Zabetian

Subjects

CADPS2, Lewy body, Neurology, Parkinson's disease, animal model, Neurology (clinical), parkinsonism, parrot

Abstract

Several genetic models that recapitulate neurodegenerative features of Parkinson's disease (PD) exist, which have been largely based on genes discovered in monogenic PD families. However, spontaneous genetic mutations have not been linked to the pathological hallmarks of PD in non-human vertebrates.To describe the genetic and pathological findings of three Yellow-crowned parrot (Amazona ochrocepahala) siblings with a severe and rapidly progressive neurological phenotype.The phenotype of the three parrots included severe ataxia, rigidity, and tremor, while their parents were phenotypically normal. Tests to identify avian viral infections and brain imaging studies were all negative. Due to their severe impairment, they were all euthanized at age 3 months and their brains underwent neuropathological examination and proteasome activity assays. Whole genome sequencing (WGS) was performed on the three affected parrots and their parents.The brains of affected parrots exhibited neuronal loss, spongiosis, and widespread Lewy body-like inclusions in many regions including the midbrain, basal ganglia, and neocortex. Proteasome activity was significantly reduced in these animals compared to a control (P 0.05). WGS identified a single homozygous missense mutation (p.V559L) in a highly conserved amino acid within the pleckstrin homology (PH) domain of the calcium-dependent secretion activator 2 (CADPS2) gene.Our data suggest that a homozygous mutation in the CADPS2 gene causes a severe neurodegenerative phenotype with Lewy body-like pathology in parrots. Although CADPS2 variants have not been reported to cause PD, further investigation of the gene might provide important insights into the pathophysiology of Lewy body disorders. © 2022 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society. This article has been contributed to by U.S. Government employees and their work is in the public domain in the USA.

Published

2022

5. Alternative splicing in a presenilin 2 variant associated with Alzheimer disease

Author

Caitlin S. Latimer, Kiel Shuey, Carole L. Smith, Chloe G Cross, Bryce L. Sopher, Michael O. Dorschner, Stephanie A. Bucks, Thomas J. Grabowski, Suman Jayadev, Debby W. Tsuang, Kimiko Domoto-Reilly, Kristoffer Rhoads, Michael Lardelli, Thomas D. Bird, Chizuru Kinoshita, Paul N. Valdmanis, Meredith M. Course, Christopher Dirk Keene, Jessica E. Young, Luis F. Gonzalez-Cuyar, Leah Osnis, Gwenn A. Garden, Kathryn P Scherpelz, Morgan Newman, James B. Leverenz, Jacquelyn E. Braggin, Ellen M. Wijsman, Seyyed H. M. Nik, Richard S. Morrison, and Christina Caso

Subjects

Adult, Male, 0301 basic medicine, Presenilin, Frameshift mutation, Amyloid beta-Protein Precursor, 03 medical and health sciences, 0302 clinical medicine, Alzheimer Disease, Presenilin-2, PSEN2, Presenilin-1, PSEN1, Amyloid precursor protein, medicine, Humans, Research Articles, Genetics, Amyloid beta-Peptides, biology, business.industry, General Neuroscience, Alternative splicing, Middle Aged, medicine.disease, Peptide Fragments, 3. Good health, Alternative Splicing, 030104 developmental biology, Mutation, biology.protein, Neurology (clinical), Amyloid Precursor Protein Secretases, Alzheimer's disease, business, Amyloid precursor protein secretase, 030217 neurology & neurosurgery, Research Article

Abstract

Objective Autosomal‐dominant familial Alzheimer disease (AD) is caused by by variants in presenilin 1 (PSEN1), presenilin 2 (PSEN2), and amyloid precursor protein (APP). Previously, we reported a rare PSEN2 frameshift variant in an early‐onset AD case (PSEN2 p.K115Efs*11). In this study, we characterize a second family with the same variant and analyze cellular transcripts from both patient fibroblasts and brain lysates. Methods We combined genomic, neuropathological, clinical, and molecular techniques to characterize the PSEN2 K115Efs*11 variant in two families. Results Neuropathological and clinical evaluation confirmed the AD diagnosis in two individuals carrying the PSEN2 K115Efs*11 variant. A truncated transcript from the variant allele is detectable in patient fibroblasts while levels of wild‐type PSEN2 transcript and protein are reduced compared to controls. Functional studies to assess biological consequences of the variant demonstrated that PSEN2 K115Efs*11 fibroblasts secrete less Aβ 1–40 compared to controls, indicating abnormal γ‐secretase activity. Analysis of PSEN2 transcript levels in brain tissue revealed alternatively spliced PSEN2 products in patient brain as well as in sporadic AD and age‐matched control brain. Interpretation These data suggest that PSEN2 K115Efs*11 is a likely pathogenic variant associated with AD. We uncovered novel PSEN2 alternative transcripts in addition to previously reported PSEN2 splice isoforms associated with sporadic AD. In the context of a frameshift, these alternative transcripts return to the canonical reading frame with potential to generate deleterious protein products. Our findings suggest novel potential mechanisms by which PSEN variants may influence AD pathogenesis, highlighting the complexity underlying genetic contribution to disease risk.

Published

2019

6. CTC1 mutations in a Brazilian family with progeroid features and recurrent bone fractures

Author

David Sillence, Fuki M. Hisama, Christian Kubisch, Davor Lessel, Michael O. Dorschner, Débora Rossi Precioso, George M. Martin, Forough Sargolzaeiaval, Junko Oshima, Jennifer Schleit, and Jiaming Zhang

Subjects

Adult, Male, 0301 basic medicine, Telomere-Binding Proteins, Biology, Compound heterozygosity, Cell Line, Fractures, Bone, 03 medical and health sciences, Genetics, medicine, Humans, Missense mutation, DNA Breaks, Double-Stranded, Allele, progeroid syndrome, Molecular Biology, Genetics (clinical), Exome sequencing, Werner syndrome, Telomere-binding protein, Mendelian disorders, Progeria, Original Articles, Middle Aged, Telomere, genomic instability, telomeres, medicine.disease, GC Rich Sequence, Pedigree, 3. Good health, Phenotype, 030104 developmental biology, molecular genetics, Mutation, Original Article, CTC1, Female, Werner Syndrome, Cerebroretinal microangiopathy with calcifications and cysts, Protein Binding

Abstract

Background Cerebroretinal microangiopathy with calcifications and cysts (CRMCC) is an autosomal recessive disorder caused by pathogenic variants of the conserved telomere maintenance component 1 (CTC1) gene. The CTC1 forms the telomeric capping complex, CST, which functions in telomere homeostasis and replication. Methods A Brazilian pedigree and an Australian pedigree were referred to the International Registry of Werner Syndrome (Seattle, WA, USA), with clinical features of accelerated aging and recurrent bone fractures. Whole exome sequencing was performed to identify the genetic causes. Results Whole exome sequencing of the Brazilian pedigree revealed compound heterozygous pathogenic variants in CTC1: a missense mutation (c.2959C>T, p.Arg987Trp) and a novel stop codon change (c.322C>T, p.Arg108*). The Australian patient carried two novel heterozygous CTC1 variants, c.2916G>T, p.Val972Gly and c.2926G>T, p.Val976Phe within the same allele. Both heterozygous variants were inherited from the unaffected father, excluding the diagnosis of CRMCC in this pedigree. Cell biological studies demonstrated accumulation of double strand break foci in lymphoblastoid cell lines derived from the patients. Increased DSB foci were extended to non‐telomeric regions of the genome, in agreement with previous biochemical studies showing a preferential binding of CTC1 protein to GC‐rich sequences. Conclusion CTC1 pathogenic variants can present with unusual manifestations of progeria accompanied with recurrent bone fractures. Further studies are needed to elucidate the disease mechanism leading to the clinical presentation with intra‐familial variations of CRMCC.

Published

2018

7. Building a family network from genetic testing

Author

Aaron Scrol, David Carrel, Heidi Thiese, Gail P. Jarvik, James D. Ralston, Andrea L. Hartzler, Michael O. Dorschner, Eric B. Larson, Adam S. Gordon, David R. Crosslin, and Kathleen A. Leppig

Subjects

0301 basic medicine, Proband, medicine.medical_specialty, Genetic counseling, Genomics, 03 medical and health sciences, 0302 clinical medicine, Health care, RYR1, Genetics, medicine, Family network, family network, Molecular Biology, SCN5A, Genetics (clinical), Genetic testing, medicine.diagnostic_test, business.industry, Original Articles, 3. Good health, LDLR, 030104 developmental biology, Electronic medical record and genomics, Family medicine, Medical genetics, Original Article, business, 030217 neurology & neurosurgery, Pharmacogenetics

Abstract

Background Genetic testing has multigenerational and familial repercussions. However, the “trickle-down effect” of providing genetic counseling and testing to family members at risk after an initial identification of a pathogenic variant in a medically actionable gene has been poorly understood. Methods Three probands were identified during the pharmacogenetics research phase of eMERGEII (electronic MEdical Record and Genomics, phase II) to have variants in genes associated with autosomal dominant adult-onset disorders determined to be actionable by the American College of Medical Genetics (ACMG). Two of the three probands had variants that were classified as pathogenic and the third proband had a variant ultimately classified of uncertain significance, but of concern due to the proband's own phenotype. All probands had additional family members at risk for inheriting the variant. Two of the three probands had family members who received their medical care from the same health care system, Group Health Cooperative (GHC). It was recommended that the proband contact their family members at risk to be referred to genetic counseling for consideration of genetic testing. Results The two probands with pathogenic variants contacted some of their family members at risk. Individuals contacted included children and adult grandchildren, particularly if they received their medical care at GHC. To the best of our knowledge, siblings and more distant relatives at risk were not informed by the proband of their genetic risk. Conclusions Establishing a family network is essential to disseminate knowledge of genetic risk. These three initial cases describe our experience of contacting eMERGE participants with identified variants, providing the probands with appropriate genetic counseling and care coordination, and recommendations for contacting family members at risk. Greater challenges were observed for coordinating genetics care for family members and extending the family network to include other relatives at risk.

Published

2016

8. P3‐162: IPSC‐DERIVED CORTICAL NEURONS WITH A NOVEL FRAMESHIFT PSEN2 MUTATION INCREASE THE RATIO OF AGGREGATE PRONE AMYLOID BETA

Author

Bryce L. Sopher, Debby W. Tsuang, James B. Leverenz, Jessica E. Young, Leah Osnis, Stephanie A. Bucks, Kevin Green, Jacquelyn E. Braggin, Refugio A. Martinez, Suman Jayadev, Thomas D. Bird, Carole L. Smith, Paul N. Valdmanis, and Michael O. Dorschner

Subjects

biology, Epidemiology, Amyloid beta, Health Policy, Cortical neurons, Frameshift mutation, Cell biology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, PSEN2, Mutation (genetic algorithm), biology.protein, Neurology (clinical), Geriatrics and Gerontology

Published

2018

9. P4‐230: A GENOMIC AND CELL FUNCTION APPROACH TO IDENTIFYING CELL‐TYPE‐SPECIFIC BIOLOGICAL NETWORKS IN ALZHEIMER'S DISEASE

Author

Elizabeth Blue, Gwenn A. Garden, Brad Rolf, Michael O. Dorschner, Allison Knupp, Caitlin S. Latimer, Shannon E. Rose, Harald Frankowski, Kevin Green, Benjamin A. Logsdon, Suman Jayadev, Jessica E. Young, and C. Dirk Keene

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Cell type specific, Neurology (clinical), Disease, Computational biology, Geriatrics and Gerontology, Biology, Cell function, Biological network

Published

2018

10. Refining the structure and content of clinical genomic reports

Author

Joseph Salama, Brian H. Shirts, Peter Tarczy-Hornoch, Laura M. Amendola, Lesli A. Kiedrowski, Michael O. Dorschner, Gail P. Jarvik, Peter H. Byers, Adam S. Gordon, and Stephanie M. Fullerton

Subjects

Structure (mathematical logic), business.industry, Molecular genetic testing, MEDLINE, Genomics, Bioinformatics, Data science, DNA sequencing, Genetics, Medicine, Standard test, business, Exome, Genetics (clinical), Exome sequencing

Abstract

To effectively articulate the results of exome and genome sequencing we refined the structure and content of molecular test reports. To communicate results of a randomized control trial aimed at the evaluation of exome sequencing for clinical medicine, we developed a structured narrative report. With feedback from genetics and non-genetics professionals, we developed separate indication-specific and incidental findings reports. Standard test report elements were supplemented with research study-specific language, which highlighted the limitations of exome sequencing and provided detailed, structured results, and interpretations. The report format we developed to communicate research results can easily be transformed for clinical use by removal of research-specific statements and disclaimers. The development of clinical reports for exome sequencing has shown that accurate and open communication between the clinician and laboratory is ideally an ongoing process to address the increasing complexity of molecular genetic testing.

Published

2014

11. P4-479: METHODS TO ASSESS CELL-TYPE-SPECIFIC, BIOLOGICAL NETWORKS OF ALZHEIMER'S DISEASE

Author

Brad Rolf, Elizabeth Blue, Shannon E. Rose, C. Dirk Keene, Kevin Green, Benjamin A. Logsdon, Michael O. Dorschner, Jessica E. Young, Jacquelyn E. Braggin, Suman Jayadev, Harald Frankowski, Gwenn A. Garden, Refugio A. Martinez, and Allison Knupp

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Cell type specific, Neurology (clinical), Disease, Computational biology, Geriatrics and Gerontology, Biology, Biological network

Published

2019

12. 30th International Epilepsy Congress, Montreal, Canada, 23-27 June, 2013

Author

Rodriguez-Casero, Sophie Calvert, Ingrid E. Scheffer, Michael O. Dorschner, Sara Kivity, Simone C. Yendle, N. Zelnick, Dorit Lev, Jay Shendure, Samuel F. Berkovic, Sinéad Heavin, Steensbjerre R. Møller, Geoffrey Wallace, Ann M. E. Bye, Rachel L. Webster, Heather C Mefford, Molly Weaver, Katherine B. Howell, Stephen M. Malone, Thorsten Stanley, Brian J. O'Roak, Jeremy L. Freeman, Lynette G. Sadleir, Joseph Cook, Carvill Gl, Tally Lerman-Sagie, Andrew Bleasel, Mark T Mackay, Danielle M. Andrade, Amos D. Korczyn, and Asma A. Khan

Subjects

Refractory seizures, Novel gene, Genetics, Poor prognosis, Neurology, Genetic heterogeneity, Etiology, Neurology (clinical), Biology, Gene, De novo mutations, Epileptic activity

Abstract

Purpose: Epileptic encephalopathies (EEs) are a devastating group of epilepsies characterized by refractory seizures, cognitive arrest or regression, associated with ongoing epileptic activity, and a poor prognosis. De novo mutations in a number of genes, as well as rare, de novo copy number changes, are known to cause EE. However, the vast majority of cases have an unknown etiology...

Published

2013

13. Genomic context of paralogous recombination hotspots mediating recurrentNF1 region microdeletion

Author

Karen Stephens, Michael O. Dorschner, Rosalynda Le, and Stephen H. Forbes

Subjects

Recombination, Genetic, Genetics, Cancer Research, Neurofibromin 1, Polymorphism, Genetic, Base Sequence, Breakpoint, Gene Conversion, Hot spot (veterinary medicine), Biology, Sequence identity, Multigene Family, Humans, Gene conversion, Sequence Alignment, Gene, Recombination, Sequence Deletion

Abstract

Recombination between paralogs that flank the NF1 gene at 17q11.2 typically results in a 1.5-Mb microdeletion that includes NF1 and at least 13 other genes. We show that the principal sequences responsible are two 51-kb blocks with 97.5% sequence identity (NF1REP-P1-51 and NF1REP-M-51). These blocks belong to a complex group of paralogs with three components on 17q11.2 and another on 19p13.13. Breakpoint sequencing of deleted chromosomes from multiple patients revealed two paralogous recombination hot spots within the 51-kb blocks. Lack of sequence similarity between these sites failed to suggest or corroborate any putative cis-acting recombinogenic motifs. However, the NF1REPs showed relatively high alignment mismatch between recombining paralogs, and we note that the NF1REP hot spots were regions of good alignment bordered by relatively large alignment gaps. Statistical tests for gene conversion detected a single significant tract of perfect match between the NF1REPs that was 700 bp long and coincided with PRS2, the predominant recombination hot spot. Tracts of perfect match occurring by chance may contribute to breakpoint localization, but our result suggests that perfect tracts at recombination hot spots may be a result of gene conversion at sites at which preferential pairing occurs for other, as-yet-unknown reasons. © 2004 Wiley-Liss, Inc.

Published

2004