Your search keyword '"Monica H. Wojcik"' showing total 84 results

1. Integrating rapid exome sequencing into NICU clinical care after a pilot research study

Author

Alissa M. D’Gama, Maya C. Del Rosario, Mairead A. Bresnahan, Timothy W. Yu, Monica H. Wojcik, and Pankaj B. Agrawal

Subjects

Medicine, Genetics, QH426-470

Abstract

Abstract Genomic sequencing is a powerful diagnostic tool in critically ill infants, but performing exome or genome sequencing (ES/GS) in the context of a research study is different from implementing these tests clinically. We investigated the integration of rapid ES into routine clinical care after a pilot research study in a Level IV Neonatal Intensive Care Unit (NICU). We performed a retrospective cohort analysis of infants admitted with suspected genetic disorders to the NICU from December 1, 2018 to March 31, 2021 and compared results to those obtained from a previous research study cohort (March 1, 2017 to November 30, 2018). Clinical rapid ES was performed in 80/230 infants (35%) with a suspected genetic disorder and identified a genetic diagnosis in 22/80 infants (28%). The majority of diagnoses acutely impacted clinical management (14/22 (64%)). Compared to the previous research study, clinically integrated rapid ES had a significantly lower diagnostic yield and increased time from NICU admission and genetics consult to ES report, but identified four genetic diagnoses that may have been missed by the research study selection criteria. Compared to other genetic tests, rapid ES had similar or higher diagnostic yield and similar or decreased time to result. Overall, rapid ES was utilized in the NICU after the pilot research study, often as the first-tier sequencing test, and could identify the majority of disease-causing variants, shorten the diagnostic odyssey, and impact clinical care. Based on our experience, we have identified strategies to optimize the clinical implementation of rapid ES in the NICU.

Published

2022

2. AXIN2‐related oligodontia‐colorectal cancer syndrome with cleft palate as a possible new feature

Author

Laura Roht, Hanne K. Hyldebrandt, Astrid T. Stormorken, Hilde Nordgarden, Rolf H. Sijmons, Dennis K. Bos, Douglas Riegert‐Johnson, Sarah Mantia‐Macklin, Pilvi Ilves, Kai Muru, Monica H. Wojcik, Tiina Kahre, and Katrin Õunap

Subjects

AXIN2, cancer predisposition syndrome, cleft palate, oligodontia, Genetics, QH426-470

Abstract

Abstract Background Pathogenic variants in AXIN2 have been associated with tooth agenesis, colon polyps, and colon cancer. Given the rare nature of this phenotype, we set out to collect additional genotypic and phenotypic information. Methods Data were collected via a structured questionnaire. Sequencing was performed in these patients mostly due to diagnostic purpose. A little more than half of the AXIN2 variant carriers were identified by NGS; other six were family members. Results Here, we report 13 individuals with a heterozygous AXIN2 pathogenic/likely pathogenic variant who have a variable expression of oligodontia‐colorectal cancer syndrome (OMIM 608615) or oligodontia‐cancer predisposition syndrome (ORPHA 300576). Three individuals from one family also had cleft palate, which might represent a new clinical feature of AXIN2 phenotype, also given the fact that AXIN2 polymorphisms have been found in association with oral clefting in population studies. AXIN2 has already been added to multigene cancer panel tests; further research should be conducted to determine whether it should be added to cleft lip/palate multigene panels. Conclusion More clarity about oligodontia‐colorectal cancer syndrome, about the variable expression, and associated cancer risks is needed to improve clinical management and to establish guidelines for surveillance. We collected information about the surveillance that was advised, which might support clinical management of these patients.

Published

2023

3. The fundamental need for unifying phenotypes in sudden unexpected pediatric deaths

Author

Monica H. Wojcik, Annapurna H. Poduri, Ingrid A. Holm, Calum A. MacRae, and Richard D. Goldstein

Subjects

SUDC, SUEND, SIDS, SUDEP, genetics, molecular autopsy, Medicine (General), R5-920

Abstract

A definitive, authoritative approach to evaluate the causes of unexpected, and ultimately unexplained, pediatric deaths remains elusive, relegating final conclusions to diagnoses of exclusion in the vast majority of cases. Research into unexplained pediatric deaths has focused primarily on sudden infant deaths (under 1 year of age) and led to the identification of several potential, albeit incompletely understood, contributory factors: nonspecific pathology findings, associations with sleep position and environment that may not be uniformly relevant, and the elucidation of a role for serotonin that is practically difficult to estimate in any individual case. Any assessment of progress in this field must also acknowledge the failure of current approaches to substantially decrease mortality rates in decades. Furthermore, potential commonalities with pediatric deaths across a broader age spectrum have not been widely considered. Recent epilepsy-related observations and genetic findings, identified post-mortem in both infants and children who died suddenly and unexpectedly, suggest a role for more intense and specific phenotyping efforts as well as an expanded role for genetic and genomic evaluation. We therefore present a new approach to reframe the phenotype in sudden unexplained deaths in the pediatric age range, collapsing many distinctions based on arbitrary factors (such as age) that have previously guided research in this area, and discuss its implications for the future of postmortem investigation.

Published

2023

4. Impaired protein hydroxylase activity causes replication stress and developmental abnormalities in humans

Author

Sally C. Fletcher, Charlotte Hall, Tristan J. Kennedy, Sander Pajusalu, Monica H. Wojcik, Uncaar Boora, Chan Li, Kaisa Teele Oja, Eline Hendrix, Christian A.E. Westrip, Regina Andrijes, Sonia K. Piasecka, Mansi Singh, Mohammed E. El-Asrag, Anetta Ptasinska, Vallo Tillmann, Martin R. Higgs, Deanna A. Carere, Andrew D. Beggs, John Pappas, Rachel Rabin, Stephen J. Smerdon, Grant S. Stewart, Katrin Õunap, and Mathew L. Coleman

Subjects

Cell biology, Genetics, Medicine

Abstract

Although protein hydroxylation is a relatively poorly characterized posttranslational modification, it has received significant recent attention following seminal work uncovering its role in oxygen sensing and hypoxia biology. Although the fundamental importance of protein hydroxylases in biology is becoming clear, the biochemical targets and cellular functions often remain enigmatic. JMJD5 is a “JmjC-only” protein hydroxylase that is essential for murine embryonic development and viability. However, no germline variants in JmjC-only hydroxylases, including JMJD5, have yet been described that are associated with any human pathology. Here we demonstrate that biallelic germline JMJD5 pathogenic variants are deleterious to JMJD5 mRNA splicing, protein stability, and hydroxylase activity, resulting in a human developmental disorder characterized by severe failure to thrive, intellectual disability, and facial dysmorphism. We show that the underlying cellular phenotype is associated with increased DNA replication stress and that this is critically dependent on the protein hydroxylase activity of JMJD5. This work contributes to our growing understanding of the role and importance of protein hydroxylases in human development and disease.

Published

2023

5. Copy Number Variation and Structural Genomic Findings in 116 Cases of Sudden Unexplained Death between 1 and 28 Months of Age

Author

Catherine A. Brownstein, Elise Douard, Robin L. Haynes, Hyun Yong Koh, Alireza Haghighi, Christine Keywan, Bree Martin, Sanda Alexandrescu, Elisabeth A. Haas, Sara O. Vargas, Monica H. Wojcik, Sébastien Jacquemont, Annapurna H. Poduri, Richard D. Goldstein, and Ingrid A. Holm

Subjects

autism spectrum disorder, chromosomal microarray, death, genetics, genomics, sudden infant death syndrome, Genetics, QH426-470

Abstract

Abstract In sudden unexplained death in pediatrics (SUDP) the cause of death is unknown despite an autopsy and investigation. The role of copy number variations (CNVs) in SUDP has not been well‐studied. Chromosomal microarray (CMA) data are generated for 116 SUDP cases with age at death between 1 and 28 months. CNVs are classified using the American College of Medical Genetics and Genomics guidelines and CNVs in our cohort are compared to an autism spectrum disorder (ASD) cohort, and to a control cohort. Pathogenic CNVs are identified in 5 of 116 cases (4.3%). Variants of uncertain significance (VUS) favoring pathogenic CNVs are identified in 9 cases (7.8%). Several CNVs are associated with neurodevelopmental phenotypes including seizures, ASD, developmental delay, and schizophrenia. The structural variant 47,XXY is identified in two cases (2/69 boys, 2.9%) not previously diagnosed with Klinefelter syndrome. Pathogenicity scores for deletions are significantly elevated in the SUDP cohort versus controls (p = 0.007) and are not significantly different from the ASD cohort. The finding of pathogenic or VUS favoring pathogenic CNVs, or structural variants, in 12.1% of cases, combined with the observation of higher pathogenicity scores for deletions in SUDP versus controls, suggests that CMA should be included in the genetic evaluation of SUDP.

Published

2023

6. A novel syndrome associated with prenatal fentanyl exposure

Author

Erin Wadman, Erica Fernandes, Candace Muss, Nina Powell-Hamilton, Monica H. Wojcik, Jill A. Madden, Chrystalle Katte Carreon, Robin D. Clark, Annie Stenftenagel, Kamal Chikalard, Virginia Kimonis, William Brucker, Carolina Alves, and Karen W. Gripp

Subjects

Embryopathy, GestaltMatcher, Opioid use disorder, Prenatal fentanyl exposure, Smith-Lemli-Opitz syndrome, Genetics, QH426-470, Medicine

Abstract

A novel syndrome was suspected in individuals sharing short stature, microcephaly, distinctive facial features, and congenital anomalies. We enrolled 6 patients in an institutional review board approved study and evaluated medical history, findings, facial photographs, and test results across this original cohort. Four additional cases with similar findings were contributed by clinicians from outside institutions, bringing the number of reported cases to 10 and supporting the existence of this novel syndrome.The 6 individuals enrolled into the institutional review board approved study shared microcephaly, short stature, and distinctive facial features. Congenital malformations included cleft palate, talipes equinovarus or rocker bottom feet, and chordee or hypospadias. Short, broad thumbs, single palmar crease, and mild 2,3 toe syndactyly were present. A hypoplastic corpus callosum was noted in 3 of 5 with appropriate evaluation. Their growth and physical findings were suggestive of Smith-Lemli-Opitz syndrome. Biochemical studies shortly after delivery indicated abnormalities in the cholesterol metabolism pathway that subsequently resolved. No shared genomic or genetic cause was identified. All individuals were born after a pregnancy complicated by prenatal exposure to nonprescription opioids, particularly fentanyl, suggesting fentanyl as a teratogen.Prenatal fentanyl exposure possibly interfered with cholesterol metabolism, giving rise to findings resembling Smith-Lemli-Opitz syndrome. This novel syndrome is clinically recognizable. Four additional cases contributed clinically shared similar findings, increasing the number of cases to 10 and supporting a novel syndrome associated with prenatal fentanyl exposure. Assessment of Shepard and Bradford Hill criteria could be consistent with fentanyl as teratogen, though caution is necessary before assigning causality and data replication is needed.

Published

2023

7. POLRMT mutations impair mitochondrial transcription causing neurological disease

Author

Monika Oláhová, Bradley Peter, Zsolt Szilagyi, Hector Diaz-Maldonado, Meenakshi Singh, Ewen W. Sommerville, Emma L. Blakely, Jack J. Collier, Emily Hoberg, Viktor Stránecký, Hana Hartmannová, Anthony J. Bleyer, Kim L. McBride, Sasigarn A. Bowden, Zuzana Korandová, Alena Pecinová, Hans-Hilger Ropers, Kimia Kahrizi, Hossein Najmabadi, Mark A. Tarnopolsky, Lauren I. Brady, K. Nicole Weaver, Carlos E. Prada, Katrin Õunap, Monica H. Wojcik, Sander Pajusalu, Safoora B. Syeda, Lynn Pais, Elicia A. Estrella, Christine C. Bruels, Louis M. Kunkel, Peter B. Kang, Penelope E. Bonnen, Tomáš Mráček, Stanislav Kmoch, Gráinne S. Gorman, Maria Falkenberg, Claes M. Gustafsson, and Robert W. Taylor

Subjects

Science

Abstract

POLRMT is key for transcription of the mitochondrial genome, yet has not been implicated in mitochondrial disease to date. Here, the authors identify mutations in POLRMT in individuals with mitochondrial disease-related phenotypes and characterise underlying defects in mitochondrial transcription.

Published

2021

8. Implications of Genomic Newborn Screening for Infant Mortality

Author

Monica H. Wojcik and Nina B. Gold

Subjects

mortality, infant, neonate, sequencing, exome, genome, Pediatrics, RJ1-570

Abstract

Technological advances and decreasing costs of genomic sequencing have paved the way for the increased incorporation of genomics into newborn screening (NBS). Genomic sequencing may complement current NBS laboratory analyses or may be used as a first-tier screening tool to identify disorders not detected by current approaches. As a large proportion of infant deaths occur in children with an underlying genetic disorder, earlier diagnosis of these disorders may improve neonatal and infant mortality rates. This lends an additional layer of ethical consideration regarding genomic newborn screening. We review the current understanding of genomic contributions to infant mortality and explore the potential implications of expanded access to genomic screening for infant mortality rates.

Published

2023

9. Genome sequencing identifies a homozygous inversion disrupting QDPR as a cause for dihydropteridine reductase deficiency

Author

Hardo Lilleväli, Sander Pajusalu, Monica H. Wojcik, Julia Goodrich, Ryan L. Collins, Ülle Murumets, Pille Tammur, Nenad Blau, Kersti Lilleväli, and Katrin Õunap

Subjects

dihydropteridine reductase deficiency, genome sequencing, inversion, QDPR gene, tetrahydrobiopterin deficiencies, Genetics, QH426-470

Abstract

Abstract Background Dihydropteridine reductase (DHPR) is one of the key enzymes for maintaining in the organism the supply of tetrahydrobiopterin (BH4), an essential cofactor for aromatic amino acid hydroxylases. Its dysfunction causes the condition of hyperphenylalaninemia together with the lack of neurotransmitters. Methods We report a patient with biochemically diagnosed DHPR deficiency, with extensive molecular investigations undertaken to detect variations in quinoid dihydropteridine reductase (QDPR) gene. Sanger sequencing of QDPR coding regions, exome sequencing, QDPR mRNA PCR, and karyotyping were followed by trio genome sequencing. Results Short‐read genome sequencing revealed a homozygous 9‐Mb inversion disrupting QDPR. Structural variant breakpoints in chromosome 4 were located to intron 2 of QDPR at Chr4(GRCh38):g.17505522 and in intron 8 of the ACOX3 gene, Chr4(GRCh38):g.8398067). Both nonrelated parents carried the variant in heterozygous state. The inversion was not present in gnomAD structural variant database. Conclusion Identification of the exact breakpoints now allows further straightforward molecular genetic testing of potential carriers of the inversion. This study extends the pathogenic variant spectrum of DHPR deficiency and highlights the role of structural variants in recessive metabolic disorders. To our knowledge, this is the first report on a large, canonical (rather than complex) homozygous pathogenic inversion detected by genome sequencing.

Published

2020

10. Trisomy 13: Survival beyond the NICU

Author

Rachel S, Hu, Jody, Heffernan, Jessica, Sims, and Monica H, Wojcik

Subjects

Pediatrics, Perinatology and Child Health

Published

2023

11. Re: 'Next generation sequencing in neonatology: what does it mean for the next generation?'

Author

Monica H. Wojcik, Kristen P. Fishler, and Bimal P. Chaudhari

Subjects

Genetics, Genetics (clinical)

Published

2022

12. Rare diseases, common barriers: disparities in pediatric clinical genetics outcomes

Author

Monica H. Wojcik, Mairead Bresnahan, Maya C. del Rosario, Mayra Martinez Ojeda, Amy Kritzer, and Yarden S. Fraiman

Subjects

Pediatrics, Perinatology and Child Health

Published

2022

13. Ethical implications of early genetic diagnosis in an infant with <scp>Lesch–Nyhan</scp> syndrome

Author

Tian Zhang, Julie M. Briere, Kristen T. Leeman, Monica H. Wojcik, and Pankaj B. Agrawal

Subjects

Genetics (clinical)

Published

2022

14. Perspectives of United States neonatologists on genetic testing practices

Author

Monica H. Wojcik, Maya C. del Rosario, and Pankaj B. Agrawal

Subjects

Neonatologists, Intensive Care Units, Neonatal, Surveys and Questionnaires, Exome Sequencing, Infant, Newborn, Humans, Genetic Testing, Article, United States, Genetics (clinical)

Abstract

PURPOSE: Genetic disorders often present in the neonatal intensive care unit (NICU), and detecting or confirming these diagnoses has been shown to impact care. However, the availability and usage of genetic testing, particularly exome or genome sequencing, among NICUs varies widely. We therefore sought to investigate practice patterns related to genetic testing in NICUs around the country in order to identify and quantify potential discrepancies. METHODS: We designed a survey that was distributed to neonatologists via email. The survey contained questions related to test availability and desirability, the process of test ordering in the NICU, and general comfort with ordering and interpreting genetic testing. Demographic data related to the survey participant and characteristics of their NICU were also obtained. RESULTS: 162 neonatologists completed the survey, representing 40 states and 112 distinct NICUs. While nearly all (93.2%) attributed a high level of importance to identifying a genetic diagnosis for their patients, genetic consultations were only available at 78% of NICUs and exome or genome sequencing was not available on a regular basis (69% of NICUs). CONCLUSIONS: Among U.S. neonatologists surveyed, although most feel that genetic tests are indicated for their patients, they are not always clinically available. Further research into implementation barriers is warranted.

Published

2022

15. Untargeted metabolomics profiling in pediatric patients and adult populations indicates a connection between lipid imbalance and epilepsy

Author

Kaisa Teele Oja, Mihkel Ilisson, Karit Reinson, Kai Muru, Tiia Reimand, Hedi Peterson, Dmytro Fishman, Tõnu Esko, Toomas Haller, Jaanika Kronberg, Monica H. Wojcik, Adam Kennedy, Gregory Michelotti, Anne O’Donnell-Luria, Eve Õiglane-Šlik, Sander Pajusalu, and Katrin Õunap

Subjects

Article

Abstract

IntroductionEpilepsy is a common central nervous system disorder characterized by abnormal brain electrical activity. We aimed to compare the metabolic profiles of plasma from patients with epilepsy across different etiologies, seizure frequency, seizure type, and patient age to try to identify common disrupted pathways.Material and methodsWe used data from three separate cohorts. The first cohort (PED-C) consisted of 31 pediatric patients with suspicion of a genetic disorder with unclear etiology; the second cohort (AD-C) consisted of 250 adults from the Estonian Biobank (EstBB), and the third cohort consisted of 583 adults ≥ 69 years of age from the EstBB (ELD-C). We compared untargeted metabolomics and lipidomics data between individuals with and without epilepsy in each cohort.ResultsIn the PED-C, significant alterations (p-value ConclusionOur results suggest that cell membrane fluidity may have a significant role in the mechanism of epilepsy, and changes in lipid balance may indicate epilepsy. However, further studies are needed to evaluate whether untargeted metabolomics analysis could prove helpful in diagnosing epilepsy earlier.

Published

2023

16. Advancing Understanding of Inequities in Rare Disease Genomics

Author

Jillian G Serrano, Melanie O’Leary, Grace VanNoy, Ingrid A Holm, Yarden S Fraiman, Heidi L Rehm, Anne O’Donnell-Luria, and Monica H Wojcik

Subjects

Article

Abstract

PurposeAdvances in genomic research have led to the diagnosis of rare, early-onset diseases for thousands of individuals. Unfortunately, the benefits of advanced genetic diagnostic technology are not distributed equitably among the population, as has been seen in many other healthcare contexts. Even quantifying and describing inequities in genetic diagnostic yield is challenging due to variation in referrals to clinical genetics practices and other barriers to clinical genetic testing.MethodsThe Rare Genomes Project (RGP) at the Broad Institute of MIT and Harvard offers research genome sequencing to individuals with rare disease who remain genetically undiagnosed through direct interaction with the individual or family. This presents an opportunity for diagnosis beyond the clinical context, thus eliminating many barriers to access.FindingsAn initial goal of RGP was to equalize access to genomic sequencing by decoupling testing access from proximity to a major medical center and physician referral. However, our study participants are overwhelmingly non-disadvantaged, as evidenced by their access to specialist care and genetic testing prior to RGP enrollment, and are also predominantly white.ImplicationsWe therefore describe our novel initiative to diversify RGP enrollment in order to advance equity in rare disease genetic diagnosis and research. In addition to the moral imperative of medical equity, this is also critical in order to fully understand the genomic underpinnings of rare disease. We utilize a mixed methods approach to understand the priorities and values of underrepresented communities, existing disparities, and the obstacles to addressing them: all of which is necessary to promote equity in future genomic medicine initiatives.

Published

2023

17. Centers for Mendelian Genomics: A decade of facilitating gene discovery

Author

Samantha M. Baxter, Jennifer E. Posey, Nicole J. Lake, Nara Sobreira, Jessica X. Chong, Steven Buyske, Elizabeth E. Blue, Lisa H. Chadwick, Zeynep H. Coban-Akdemir, Kimberly F. Doheny, Colleen P. Davis, Monkol Lek, Christopher Wellington, Shalini N. Jhangiani, Mark Gerstein, Richard A. Gibbs, Richard P. Lifton, Daniel G. MacArthur, Tara C. Matise, James R. Lupski, David Valle, Michael J. Bamshad, Ada Hamosh, Shrikant Mane, Deborah A. Nickerson, Heidi L. Rehm, Anne O’Donnell-Luria, Marcia Adams, François Aguet, Gulsen Akay, Peter Anderson, Corina Antonescu, Harindra M. Arachchi, Mehmed M. Atik, Christina A. Austin-Tse, Larry Babb, Tamara J. Bacus, Vahid Bahrambeigi, Suganthi Balasubramanian, Yavuz Bayram, Arthur L. Beaudet, Christine R. Beck, John W. Belmont, Jennifer E. Below, Kaya Bilguvar, Corinne D. Boehm, Eric Boerwinkle, Philip M. Boone, Sara J. Bowne, Harrison Brand, Kati J. Buckingham, Alicia B. Byrne, Daniel Calame, Ian M. Campbell, Xiaolong Cao, Claudia Carvalho, Varuna Chander, Jaime Chang, Katherine R. Chao, Ivan K. Chinn, Declan Clarke, Ryan L. Collins, Beryl Cummings, Zain Dardas, Moez Dawood, Kayla Delano, Stephanie P. DiTroia, Harshavardhan Doddapaneni, Haowei Du, Renqian Du, Ruizhi Duan, Mohammad Eldomery, Christine M. Eng, Eleina England, Emily Evangelista, Selin Everett, Jawid Fatih, Adam Felsenfeld, Laurent C. Francioli, Christian D. Frazar, Jack Fu, Emmanuel Gamarra, Tomasz Gambin, Weiniu Gan, Mira Gandhi, Vijay S. Ganesh, Kiran V. Garimella, Laura D. Gauthier, Danielle Giroux, Claudia Gonzaga-Jauregui, Julia K. Goodrich, William W. Gordon, Sean Griffith, Christopher M. Grochowski, Shen Gu, Sanna Gudmundsson, Stacey J. Hall, Adam Hansen, Tamar Harel, Arif O. Harmanci, Isabella Herman, Kurt Hetrick, Hadia Hijazi, Martha Horike-Pyne, Elvin Hsu, Jianhong Hu, Yongqing Huang, Jameson R. Hurless, Steve Jahl, Gail P. Jarvik, Yunyun Jiang, Eric Johanson, Angad Jolly, Ender Karaca, Michael Khayat, James Knight, J. Thomas Kolar, Sushant Kumar, Seema Lalani, Kristen M. Laricchia, Kathryn E. Larkin, Suzanne M. Leal, Gabrielle Lemire, Richard A. Lewis, He Li, Hua Ling, Rachel B. Lipson, Pengfei Liu, Alysia Kern Lovgren, Francesc López-Giráldez, Melissa P. MacMillan, Brian E. Mangilog, Stacy Mano, Dana Marafi, Beth Marosy, Jamie L. Marshall, Renan Martin, Colby T. Marvin, Michelle Mawhinney, Sean McGee, Daniel J. McGoldrick, Michelle Mehaffey, Betselote Mekonnen, Xiaolu Meng, Tadahiro Mitani, Christina Y. Miyake, David Mohr, Shaine Morris, Thomas E. Mullen, David R. Murdock, Mullai Murugan, Donna M. Muzny, Ben Myers, Juanita Neira, Kevin K. Nguyen, Patrick M. Nielsen, Natalie Nudelman, Emily O’Heir, Melanie C. O’Leary, Chrissie Ongaco, Jordan Orange, Ikeoluwa A. Osei-Owusu, Ingrid S. Paine, Lynn S. Pais, Justin Paschall, Karynne Patterson, Davut Pehlivan, Benjamin Pelle, Samantha Penney, Jorge Perez de Acha Chavez, Emma Pierce-Hoffman, Cecilia M. Poli, Jaya Punetha, Aparna Radhakrishnan, Matthew A. Richardson, Eliete Rodrigues, Gwendolin T. Roote, Jill A. Rosenfeld, Erica L. Ryke, Aniko Sabo, Alice Sanchez, Isabelle Schrauwen, Daryl A. Scott, Fritz Sedlazeck, Jillian Serrano, Chad A. Shaw, Tameka Shelford, Kathryn M. Shively, Moriel Singer-Berk, Joshua D. Smith, Hana Snow, Grace Snyder, Matthew Solomonson, Rachel G. Son, Xiaofei Song, Pawel Stankiewicz, Taylorlyn Stephan, V. Reid Sutton, Abigail Sveden, Diana Cornejo Sánchez, Monica Tackett, Michael Talkowski, Machiko S. Threlkeld, Grace Tiao, Miriam S. Udler, Laura Vail, Zaheer Valivullah, Elise Valkanas, Grace E. VanNoy, Qingbo S. Wang, Gao Wang, Lu Wang, Michael F. Wangler, Nicholas A. Watts, Ben Weisburd, Jeffrey M. Weiss, Marsha M. Wheeler, Janson J. White, Clara E. Williamson, Michael W. Wilson, Wojciech Wiszniewski, Marjorie A. Withers, Dane Witmer, Lauren Witzgall, Elizabeth Wohler, Monica H. Wojcik, Isaac Wong, Jordan C. Wood, Nan Wu, Jinchuan Xing, Yaping Yang, Qian Yi, Bo Yuan, Jordan E. Zeiger, Chaofan Zhang, Peng Zhang, Yan Zhang, Xiaohong Zhang, Yeting Zhang, Shifa Zhang, Huda Zoghbi, and Igna van den Veyver

Subjects

Phenotype, Exome Sequencing, Humans, Exome, Genomics, Article, Genetic Association Studies, Genetics (clinical)

Abstract

PURPOSE: Mendelian disease genomic research has undergone a massive transformation over the past decade. With increasing availability of exome and genome sequencing, the role of Mendelian research has expanded beyond data collection, sequencing, and analysis to worldwide data sharing and collaboration. METHODS: Over the past 10 years, the National Institutes of Health–supported Centers for Mendelian Genomics (CMGs) have played a major role in this research and clinical evolution. RESULTS: We highlight the cumulative gene discoveries facilitated by the program, biomedical research leveraged by the approach, and the larger impact on the research community. Beyond generating a list of gene-phenotype relationships and participating in widespread data sharing, the CMGs have created resources, tools, and training for the larger community to foster understanding of genes and genome variation. The CMGs have participated in a wide range of data sharing activities, including deposition of all eligible CMG data into the Analysis, Visualization, and Informatics Lab-space (AnVIL), sharing candidate genes through the Matchmaker Exchange and the CMG website, and sharing variants in Genotypes to Mendelian Phenotypes (Geno2MP) and VariantMatcher. CONCLUSION: The work is far from complete; strengthening communication between research and clinical realms, continued development and sharing of knowledge and tools, and improving access to richly characterized data sets are all required to diagnose the remaining molecularly undiagnosed patients.

Published

2022

18. Delayed diagnosis and racial bias in children with genetic conditions

Author

Jacklyn Omorodion, Leah Dowsett, Robin D. Clark, Jamie Fraser, Aya Abu‐El‐Haija, Alanna Strong, Monica H. Wojcik, Allison S. Bryant, and Nina B. Gold

Subjects

Delayed Diagnosis, Racism, Racial Groups, Genetics, Humans, Minority Health, Child, Health Services Accessibility, Minority Groups, United States, Article, Genetics (clinical)

Abstract

As more therapeutics for genetic conditions become available, the need for timely and equitable genetic diagnosis has become urgent. Using clinical cases, we consider the health system-, provider-, and patient-level factors that contribute to the delayed diagnosis of genetic conditions in pediatric patients from minority populations, leading to health disparities between racial groups. We then provide suggestions to address these factors, with the aim of improving minority health and access to genetic care for all children.

Published

2022

19. Follow-up for a Preterm Infant with Beckwith-Wiedemann Syndrome

Author

Mairead, Bresnahan and Monica H, Wojcik

Subjects

Beckwith-Wiedemann Syndrome, Pediatrics, Perinatology and Child Health, Infant, Newborn, Humans, Infant, Infant, Newborn, Diseases, Infant, Premature, Follow-Up Studies

Published

2022

20. Alternative polyadenylation alters protein dosage by switching between intronic and 3′UTR sites

Author

Nicola de Prisco, Caitlin Ford, Nathan D. Elrod, Winston Lee, Lauren C. Tang, Kai-Lieh Huang, Ai Lin, Ping Ji, Venkata S. Jonnakuti, Lia Boyle, Maximilian Cabaj, Salvatore Botta, Katrin Õunap, Karit Reinson, Monica H. Wojcik, Jill A. Rosenfeld, Weimin Bi, Kristian Tveten, Trine Prescott, Thorsten Gerstner, Audrey Schroeder, Chin-To Fong, Jaya K. George-Abraham, Catherine A. Buchanan, Andrea Hanson-Khan, Jonathan A. Bernstein, Aikaterini A. Nella, Wendy K. Chung, Vicky Brandt, Marko Jovanovic, Kimara L. Targoff, Hari Krishna Yalamanchili, Eric J. Wagner, and Vincenzo A. Gennarino

Subjects

Multidisciplinary

Abstract

Alternative polyadenylation (APA) creates distinct transcripts from the same gene by cleaving the pre-mRNA at poly(A) sites that can lie within the 3′ untranslated region (3′UTR), introns, or exons. Most studies focus on APA within the 3′UTR; however, here, we show that CPSF6 insufficiency alters protein levels and causes a developmental syndrome by deregulating APA throughout the transcript. In neonatal humans and zebrafish larvae, CPSF6 insufficiency shifts poly(A) site usage between the 3′UTR and internal sites in a pathway-specific manner. Genes associated with neuronal function undergo mostly intronic APA, reducing their expression, while genes associated with heart and skeletal function mostly undergo 3′UTR APA and are up-regulated. This suggests that, under healthy conditions, cells toggle between internal and 3′UTR APA to modulate protein expression.

Published

2023

21. Jansen-de Vries syndrome: Expansion of the PPM1D clinical and phenotypic spectrum in 34 families

Author

Monica H. Wojcik, Siddharth Srivastava, Pankaj B. Agrawal, Tugce B. Balci, Bert Callewaert, Pier Luigi Calvo, Diana Carli, Michelle Caudle, Samantha Colaiacovo, Laura Cross, Kalliope Demetriou, Katy Drazba, Marina Dutra‐Clarke, Matthew Edwards, Casie A. Genetti, Dorothy K. Grange, Scott E. Hickey, Bertrand Isidor, Sébastien Küry, Herbert M. Lachman, Alinoe Lavillaureix, Michael J. Lyons, Carlo Marcelis, Elysa J. Marco, Julian A. Martinez‐Agosto, Catherine Nowak, Antonio Pizzol, Marc Planes, Eloise J. Prijoles, Evelise Riberi, Eric T. Rush, Bianca E. Russell, Rani Sachdev, Betsy Schmalz, Deborah Shears, David A. Stevenson, Kate Wilson, Sandra Jansen, Bert B. A. de Vries, and Cynthia J. Curry

Subjects

All institutes and research themes of the Radboud University Medical Center, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Genetics, Genetics (clinical)

Abstract

Item does not contain fulltext Jansen-de Vries syndrome (JdVS) is a neurodevelopmental condition attributed to pathogenic variants in Exons 5 and 6 of PPM1D. As the full phenotypic spectrum and natural history remain to be defined, we describe a large cohort of children and adults with JdVS. This is a retrospective cohort study of 37 individuals from 34 families with disease-causing variants in PPM1D leading to JdVS. Clinical data were provided by treating physicians and/or families. Of the 37 individuals, 27 were male and 10 female, with median age 8.75 years (range 8 months to 62 years). Four families document autosomal dominant transmission, and 32/34 probands were diagnosed via exome sequencing. The facial gestalt, including a broad forehead and broad mouth with a thin and tented upper lip, was most recognizable between 18 and 48 months of age. Common manifestations included global developmental delay (35/36, 97%), hypotonia (25/34, 74%), short stature (14/33, 42%), constipation (22/31, 71%), and cyclic vomiting (6/35, 17%). Distinctive personality traits include a hypersocial affect (21/31, 68%) and moderate-to-severe anxiety (18/28, 64%). In conclusion, JdVS is a clinically recognizable neurodevelopmental syndrome with a characteristic personality and distinctive facial features. The association of pathogenic variants in PPM1D with cyclic vomiting bears not only medical attention but also further pathogenic and mechanistic evaluation. 01 juli 2023

Published

2023

22. Hospital-Level Variation in Genetic Testing in Children's Hospitals Neonatal Intensive Care Units from 2016 to 2021

Author

Katharine Press Callahan, Joshua Radack, Monica H. Wojcik, Sabrina Malone Jenkins, Russell T. Nye, Cara Skraban, Katherine Taylor Wild, and Chris Feudtner

Subjects

Genetics (clinical)

Abstract

To examine variation in genetic testing between neonatal intensive care units (NICUs) across hospitals over time.We performed a multicenter large-scale retrospective cohort study using NICU discharge data from the Pediatric Hospital Information System Database between 2016 and 2021. We analyzed variation in the percentage of NICU patients who had any genetic testing between hospitals and over time. We used a multivariable multilevel logistic regression model to investigate the potential association of patient characteristics and genetic testing.The final analysis included 207,228 neonates from 38 hospitals. Overall, 13% of patients had at least one genetic test sent, though this varied from 4% to 50% across hospitals. Over the study period, the proportion of patients tested increased, with the increase disproportionately borne by hospitals already testing high proportions of patients. On average, patients who received genetic testing had higher illness severity. Controlling for severity, however, only minimally reduced the degree of hospital-level variation in genetic testing.The percentage of NICU patients who undergo genetic testing varies among hospitals, and increasingly so over time. Variation is largely unexplained by differences in severity between hospitals. The degree of variation suggests that clearer guidelines for NICU genetic testing are warranted.

Published

2022

23. Neuroimaging in Kabuki syndrome and another<scp>KMT2D</scp>‐related disorder

Author

Pankaj B. Agrawal, Thomas E. Mullen, Monica H. Wojcik, Margaret A. Kenna, Rachel Stadelmaier, Olaf Bodamer, Caroline D. Robson, and Devon Barrett

Subjects

Male, Pathology, medicine.medical_specialty, Neuroimaging, Article, CHARGE syndrome, Exon, Temporal bone, Genetics, medicine, Humans, Missense mutation, Abnormalities, Multiple, Genetic Predisposition to Disease, Allele, Genetics (clinical), Retrospective Studies, Genetic testing, Histone Demethylases, medicine.diagnostic_test, business.industry, DNA Helicases, Infant, Newborn, Infant, medicine.disease, Hematologic Diseases, Neoplasm Proteins, DNA-Binding Proteins, Phenotype, Vestibular Diseases, Face, Mutation, Female, CHARGE Syndrome, business, Kabuki syndrome

Abstract

Recognition of distinct phenotypic features is an important component of genetic diagnosis. Although CHARGE syndrome, Kabuki syndrome, and a recently delineated KMT2D Ex 38/39 allelic disorder exhibit significant overlap, differences on neuroimaging may help distinguish these conditions and guide genetic testing and variant interpretation. We present an infant clinically diagnosed with CHARGE syndrome but subsequently found to have a de novo missense variant in exon 38 of KMT2D, the gene implicated in both Kabuki syndrome and a distinct KMT2D allelic disorder. We compare her brain and inner ear morphology to a retrospective cohort of 21 patients with classic Kabuki syndrome and to typical CHARGE syndrome findings described in the literature. Thirteen of the 21 Kabuki syndrome patients had temporal bone imaging (5/13 CT, 12/13 MRI) and/or brain MRI (12/13) which revealed findings distinct from both CHARGE syndrome and the KMT2D allelic disorder. Our findings further elucidate the spectrum of inner ear dysmorphology distinguishing Kabuki syndrome and the KMT2D allelic disorder from CHARGE syndrome, suggesting that these three disorders may be differentiated at least in part by their inner ear anomalies.

Published

2021

24. Loss-of-function and missense variants in NSD2 cause decreased methylation activity and are associated with a distinct developmental phenotype

Author

Newell Belnap, Bert B.A. de Vries, Austin Larson, Rolph Pfundt, Marijke R. Wevers, Valérie Benoit, Markus Zweier, Pascal Joset, Anita Rauch, Angela Bahr, Jeroen Mourmans, Patricia G Wheeler, Or Gozani, Marisa V. Andrews, Monica H. Wojcik, Didier Lacombe, Sarah Grotto, Marwan Shinawi, Lot Snijders Blok, Conny M. A. van Ravenswaaij-Arts, Keri Ramsey, Deepanwita Sengupta, Mariarosaria Lang-Muritano, Isabelle Maystadt, Katharina Steindl, Paolo Zanoni, Antonio Vitobello, Geoffroy Delplancq, Katrin Õunap, Tania Attié-Bitach, Heinrich Sticht, Giulia Petrilli, Laurence Faivre, Vassilis Tsatsaris, and Clinical Cognitive Neuropsychiatry Research Program (CCNP)

Subjects

0301 basic medicine, In silico, Biology, Article, REGION, 03 medical and health sciences, ROGERS-DANKS-SYNDROME, 0302 clinical medicine, Missense mutation, HISTONE H3, Gene, Genetics (clinical), Loss function, Genetics, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], DELETION, DEFECTS, Methylation, Phenotype, LYSINE 36, 030104 developmental biology, Molecular mechanism, WOLF-HIRSCHHORN-SYNDROME, 030217 neurology & neurosurgery, Function (biology), Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

Purpose Despite a few recent reports of patients harboring truncating variants in NSD2, a gene considered critical for the Wolf–Hirschhorn syndrome (WHS) phenotype, the clinical spectrum associated with NSD2 pathogenic variants remains poorly understood. Methods We collected a comprehensive series of 18 unpublished patients carrying heterozygous missense, elongating, or truncating NSD2 variants; compared their clinical data to the typical WHS phenotype after pooling them with ten previously described patients; and assessed the underlying molecular mechanism by structural modeling and measuring methylation activity in vitro. Results The core NSD2-associated phenotype includes mostly mild developmental delay, prenatal-onset growth retardation, low body mass index, and characteristic facial features distinct from WHS. Patients carrying missense variants were significantly taller and had more frequent behavioral/psychological issues compared with those harboring truncating variants. Structural in silico modeling suggested interference with NSD2’s folding and function for all missense variants in known structures. In vitro testing showed reduced methylation activity and failure to reconstitute H3K36me2 in NSD2 knockout cells for most missense variants. Conclusion NSD2 loss-of-function variants lead to a distinct, rather mild phenotype partially overlapping with WHS. To avoid confusion for patients, NSD2 deficiency may be named Rauch–Steindl syndrome after the delineators of this phenotype., Genetics in Medicine, 23 (8)

Published

2021

25. The Unrecognized Mortality Burden of Genetic Disorders in Infancy

Author

Dominique Heinke, Wen-Hann Tan, Monica H. Wojcik, Ingrid A. Holm, Rachel Stadelmaier, and Pankaj B. Agrawal

Subjects

Male, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Research & ANALYSIS, 030105 genetics & heredity, Congenital Abnormalities, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Cause of Death, 030225 pediatrics, Infant Mortality, medicine, Humans, Retrospective Studies, business.industry, Genetic Diseases, Inborn, Infant, Newborn, Public Health, Environmental and Occupational Health, Infant, Mortality statistics, Retrospective cohort study, United States, Vital Statistics, Mortality data, Female, business, Forecasting

Abstract

Objectives. To determine how deaths of infants with genetic diagnoses are described in national mortality statistics. Methods. We present a retrospective cohort study of mortality data, obtained from the National Death Index (NDI), and clinical data for 517 infants born from 2011 to 2017 who died before 1 year of age in the United States. Results. Although 115 of 517 deceased infants (22%) had a confirmed diagnosis of a genetic disorder, only 61 of 115 deaths (53%) were attributed to International Classification of Diseases, 10th Revision codes representing congenital anomalies or genetic disorders (Q00-Q99) as the underlying cause of death because of inconsistencies in death reporting. Infants with genetic diagnoses whose underlying causes of death were coded as Q00-Q99 were more likely to have chromosomal disorders than monogenic conditions (43/61 [70%] vs 18/61 [30%]; P Conclusions. Genetic disorders, although a leading cause of infant mortality, are not accurately captured by vital statistics. Public Health Implications. Expanded access to genetic testing and further clarity in death reporting are needed to describe properly the contribution of genetic disorders to infant mortality.

Published

2021

26. POLRMT mutations impair mitochondrial transcription causing neurological disease

Author

Kimia Kahrizi, Tomáš Mráček, Hector Diaz-Maldonado, Maria Falkenberg, Safoora B. Syeda, Penelope E. Bonnen, Stanislav Kmoch, Peter B. Kang, Zuzana Korandová, Emily Hoberg, Bradley Peter, Lauren Brady, K. Nicole Weaver, Louis M. Kunkel, Alena Pecinová, Mark A. Tarnopolsky, Zsolt Szilagyi, Hossein Najmabadi, Meenakshi Singh, Ewen W. Sommerville, Sasigarn A. Bowden, Elicia Estrella, Kim L. McBride, Hans-Hilger Ropers, Grainne S. Gorman, Emma L. Blakely, Claes M. Gustafsson, Viktor Stránecký, Christine C. Bruels, Monika Oláhová, Sander Pajusalu, Carlos E. Prada, Jack J Collier, Katrin Õunap, Lynn Pais, Hana Hartmannová, Monica H. Wojcik, Robert W. Taylor, and Anthony J. Bleyer

Subjects

Adult, Male, 0301 basic medicine, Mitochondrial DNA, Adolescent, Transcription, Genetic, POLRMT, Science, General Physics and Astronomy, Biology, DNA, Mitochondrial, Article, Oxidative Phosphorylation, General Biochemistry, Genetics and Molecular Biology, Young Adult, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Protein Domains, Transcription (biology), RNA polymerase, Genetics, Humans, RNA, Messenger, Child, Polymerase, Multidisciplinary, Massive parallel sequencing, Molecular medicine, Infant, DNA-Directed RNA Polymerases, General Chemistry, Fibroblasts, Phenotype, Mitochondria, Pedigree, Protein Subunits, 030104 developmental biology, Neurology, chemistry, Mutation, biology.protein, Female, Nervous System Diseases, 030217 neurology & neurosurgery, DNA, Neuroscience

Abstract

While >300 disease-causing variants have been identified in the mitochondrial DNA (mtDNA) polymerase γ, no mitochondrial phenotypes have been associated with POLRMT, the RNA polymerase responsible for transcription of the mitochondrial genome. Here, we characterise the clinical and molecular nature of POLRMT variants in eight individuals from seven unrelated families. Patients present with global developmental delay, hypotonia, short stature, and speech/intellectual disability in childhood; one subject displayed an indolent progressive external ophthalmoplegia phenotype. Massive parallel sequencing of all subjects identifies recessive and dominant variants in the POLRMT gene. Patient fibroblasts have a defect in mitochondrial mRNA synthesis, but no mtDNA deletions or copy number abnormalities. The in vitro characterisation of the recombinant POLRMT mutants reveals variable, but deleterious effects on mitochondrial transcription. Together, our in vivo and in vitro functional studies of POLRMT variants establish defective mitochondrial transcription as an important disease mechanism., POLRMT is key for transcription of the mitochondrial genome, yet has not been implicated in mitochondrial disease to date. Here, the authors identify mutations in POLRMT in individuals with mitochondrial disease-related phenotypes and characterise underlying defects in mitochondrial transcription.

Published

2021

27. Heterozygous Variants in KDM4B Lead to Global Developmental Delay and Neuroanatomical Defects

Author

Cyril Goizet, Arthur Sorlin, Antonio Novelli, Christophe Philippe, Mathilde Nizon, Joan M. Stoler, Maria J. Guillen Sacoto, Marielle Alders, Grace Yoon, Binnaz Yalcin, Aurélien Trimouille, Anna R. Duncan, Valerie E. Vancollie, Emanuele Agolini, Lance H. Rodan, Monica H. Wojcik, Christopher J. Lelliott, Saskia M. Maas, Antonio Vitobello, Pankaj B. Agrawal, Ange Line Bruel, Laurence Faivre, Paolo Prontera, Stephan C. Collins, Teresa Santiago-Sim, Casie A. Genetti, Ann Seman, Jiahai Shi, Marieke F. van Dooren, Patricia Ellen Grant, Clinical Genetics, Boston Children's Hospital, Unité fonctionnelle d' Innovation en Diagnostic Génomique des Maladies Rares (CHU Dijon) (UF6254), Centre Hospitalier Universitaire de Dijon - Hôpital François Mitterrand (CHU Dijon), Equipe GAD (LNC - U1231), Lipides - Nutrition - Cancer [Dijon - U1231] (LNC), Université de Bourgogne (UB)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Agro Dijon, Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro)-Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro)-Université de Bourgogne (UB)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Agro Dijon, Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro)-Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro), Centre de génétique - Centre de référence des maladies rares, anomalies du développement et syndromes malformatifs (CHU de Dijon), FHU TRANSLAD (CHU de Dijon), The Wellcome Trust Sanger Institute [Cambridge], City University of Hong Kong [Hong Kong] (CUHK), Bambino Gesù Children’s Hospital [Rome, Italy], Università degli Studi di Perugia = University of Perugia (UNIPG), GeneDx [Gaithersburg, MD, USA], Service de génétique médicale, Université de Bordeaux (UB)-CHU Bordeaux [Bordeaux]-Groupe hospitalier Pellegrin, Centre hospitalier universitaire de Nantes (CHU Nantes), Erasmus University Medical Center [Rotterdam] (Erasmus MC), Amsterdam UMC - Amsterdam University Medical Center, Centre de référence des maladies rares des déficiences intellectuelles de causes rares (CHU Dijon) (CRMR des déficiences intellectuelles de causes rares), The Hospital for sick children [Toronto] (SickKids), Dupuis, Christine, Human Genetics, Amsterdam Neuroscience - Cellular & Molecular Mechanisms, ACS - Pulmonary hypertension & thrombosis, Amsterdam Reproduction & Development (AR&D), Lelliott, Christopher [0000-0001-8087-4530], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Male, Jumonji Domain-Containing Histone Demethylases, [SDV]Life Sciences [q-bio], Developmental Disabilities, Corpus callosum, Hippocampus, Epigenesis, Genetic, Histones, Mice, 0302 clinical medicine, Neurodevelopmental disorder, Polymicrogyria, Global developmental delay, Agenesis of the corpus callosum, Genetics (clinical), Brain, Magnetic Resonance Imaging, [SDV] Life Sciences [q-bio], intellectual disability, Brain size, Female, dysmorphic hippocampi, Signal Transduction, Heterozygote, heterozygous variant, global developmental delay, Biology, Nervous System Malformations, Methylation, 03 medical and health sciences, Seizures, Report, KDM4B, Genetics, medicine, Animals, Humans, neurodevelopmental disorder, Dentate gyrus, Genetic Variation, JMJD2B, medicine.disease, 030104 developmental biology, agenesis of the corpus callosum, Neuroscience, Protein Processing, Post-Translational, 030217 neurology & neurosurgery, Ventriculomegaly

Abstract

International audience; KDM4B is a lysine-specific demethylase with a preferential activity on H3K9 tri/di-methylation (H3K9me3/2)-modified histones. H3K9 tri/di-demethylation is an important epigenetic mechanism responsible for silencing of gene expression in animal development and cancer. However, the role of KDM4B on human development is still poorly characterized. Through international data sharing, we gathered a cohort of nine individuals with mono-allelic de novo or inherited variants in KDM4B. All individuals presented with dysmorphic features and global developmental delay (GDD) with language and motor skills most affected. Three individuals had a history of seizures, and four had anomalies on brain imaging ranging from agenesis of the corpus callosum with hydrocephalus to cystic formations, abnormal hippocampi, and polymicrogyria. In mice, lysine demethylase 4B is expressed during brain development with high levels in the hippocampus, a region important for learning and memory. To understand how KDM4B variants can lead to GDD in humans, we assessed the effect of KDM4B disruption on brain anatomy and behavior through an in vivo heterozygous mouse model (Kdm4b þ/À), focusing on neuroanatomical changes. In mutant mice, the total brain volume was significantly reduced with decreased size of the hippocampal dentate gyrus, partial agenesis of the corpus callosum, and ventriculomegaly. This report demonstrates that variants in KDM4B are associated with GDD/ intellectual disability and neuroanatomical defects. Our findings suggest that KDM4B variation leads to a chromatinopathy, broadening the spectrum of this group of Mendelian disorders caused by alterations in epigenetic machinery.

Published

2020

28. A model to implement genomic medicine in the neonatal intensive care unit

Author

Monica H. Wojcik, Alissa M. D’Gama, and Pankaj B. Agrawal

Subjects

Pediatrics, Perinatology and Child Health, Obstetrics and Gynecology

Abstract

Rapid genomic sequencing has been shown to have a high diagnostic yield for critically ill infants, with multiple research studies demonstrating both diagnostic and clinical utility. However, clinical implementation of rapid sequencing in the neonatal intensive care unit (NICU), as well as other aspects of genomic medicine such as precision therapy, may be challenging. We describe the Neonatal Genomics Program, developed at our institution as a multidisciplinary approach to improve clinical genetic diagnosis and outcomes for infants in our NICU through genomic medicine. The creation of a dedicated program implementing genomic medicine to improve care in the NICU allows not only for improved access to genomic sequencing for rapid diagnosis, but also advancement of rare disease research and precision therapeutics. Ongoing efforts will help to define an optimal approach to genomic medicine in the NICU context.

Published

2022

29. Multicenter Consensus Approach to Evaluation of Neonatal Hypotonia in the Genomic Era: A Review

Author

Sarah U. Morton, John Christodoulou, Gregory Costain, Francesco Muntoni, Emma Wakeling, Monica H. Wojcik, Courtney E. French, Anna Szuto, James J. Dowling, Ronald D. Cohn, F. Lucy Raymond, Basil T. Darras, David A. Williams, Sebastian Lunke, Zornitza Stark, David H. Rowitch, and Pankaj B. Agrawal

Subjects

Consensus, Intensive Care Units, Neonatal, Exome Sequencing, Infant, Newborn, Humans, Infant, Multicenter Studies as Topic, Muscle Hypotonia, Neurology (clinical), Genetic Testing, Child, Article

Abstract

IMPORTANCE: Infants with hypotonia can present with a variety of potentially severe clinical signs and symptoms and often require invasive testing and multiple procedures. The wide range of clinical presentations and potential etiologies leaves diagnosis and prognosis uncertain, underscoring the need for rapid elucidation of the underlying genetic cause of disease. OBSERVATIONS: The clinical application of exome sequencing or genome sequencing has dramatically improved the timely yield of diagnostic testing for neonatal hypotonia, with diagnostic rates of greater than 50% in academic neonatal intensive care units (NICUs) across Australia, Canada, the UK, and the US, which compose the International Precision Child Health Partnership (IPCHiP). A total of 74% (17 of 23) of patients had a change in clinical care in response to genetic diagnosis, including 2 patients who received targeted therapy. This narrative review discusses the common causes of neonatal hypotonia, the relative benefits and limitations of available testing modalities used in NICUs, and hypotonia management recommendations. CONCLUSIONS AND RELEVANCE: This narrative review summarizes the causes of neonatal hypotonia and the benefits of prompt genetic diagnosis, including improved prognostication and identification of targeted treatments which can improve the short-term and long-term outcomes. Institutional resources can vary among different NICUs; as a result, consideration should be given to rule out a small number of relatively unique conditions for which rapid targeted genetic testing is available. Nevertheless, the consensus recommendation is to use rapid genome or exome sequencing as a first-line testing option for NICU patients with unexplained hypotonia. As part of the IPCHiP, this diagnostic experience will be collected in a central database with the goal of advancing knowledge of neonatal hypotonia and improving evidence-based practice.

Published

2022

30. Exome sequencing identifies novel missense and deletion variants in <scp> RTN4IP1 </scp> associated with optic atrophy, global developmental delay, epilepsy, ataxia, and choreoathetosis

Author

Katherine R. Chao, Eleina M. England, Pankaj B. Agrawal, Gerard T. Berry, Alcy Torres, Sanjay P. Prabhu, Jiahai Shi, Monica H. Wojcik, Wen-Hann Tan, Alissa M. D'Gama, and Jill A. Madden

Subjects

Genetics, Proband, Ataxia, medicine.diagnostic_test, Choreoathetosis, Biology, Compound heterozygosity, medicine.disease, Article, Atrophy, medicine, Global developmental delay, medicine.symptom, Genetics (clinical), Exome sequencing, Genetic testing

Abstract

Inherited optic neuropathies (IONs) are neurodegenerative disorders characterized by optic atrophy with or without extra-ocular manifestations. Optic atrophy-10 (OPA10) is an autosomal recessive ION recently reported to be caused by mutations in RTN4IP1, which encodes reticulon 4 interacting protein 1 (RTN4IP1), a mitochondrial ubiquinol oxydo-reductase. Here we report novel compound heterozygous mutations in RTN4IP1 in a male proband with developmental delay, epilepsy, optic atrophy, ataxia, and choreoathetosis. Workup was notable for transiently elevated lactate and lactate-to-pyruvate ratio, brain magnetic resonance imaging with optic atrophy and T2 signal abnormalities, and a non-diagnostic initial genetic workup, including chromosomal microarray and mitochondrial panel testing. Exome sequencing identified a paternally inherited missense variant (c.263T>G, p.Val88Gly) predicted to be deleterious and a maternally inherited deletion encompassing RTN4IP1. To our knowledge, this is the first report of a non-single nucleotide pathogenic variant associated with OPA10. This case highlights the expanding phenotypic spectrum of OPA10, the association between “syndromic” cases and severe RTN4IP1 mutations, and the importance of non-biased genetic testing, such as ES, to analyze multiple genes and variants types, in patients suspected of having genetic disease.

Published

2020

31. The influence of social determinants of health on the genetic diagnostic odyssey: who remains undiagnosed, why, and to what effect?

Author

Yarden S. Fraiman and Monica H. Wojcik

Subjects

medicine.medical_specialty, Social Determinants of Health, Population, Risk Assessment, Health Services Accessibility, Article, 03 medical and health sciences, 0302 clinical medicine, Quality of life (healthcare), Predictive Value of Tests, Risk Factors, 030225 pediatrics, Health care, medicine, Genetic predisposition, Humans, Genetic Predisposition to Disease, Genetic Testing, Social determinants of health, Healthcare Disparities, Intensive care medicine, education, Genetic testing, education.field_of_study, medicine.diagnostic_test, business.industry, Genetic Diseases, Inborn, Genetic Variation, Health Status Disparities, Precision medicine, Race Factors, Pediatrics, Perinatology and Child Health, business, 030217 neurology & neurosurgery, Rare disease

Abstract

Although Mendelian genetic disorders are individually rare, they are collectively more common and contribute disproportionately to pediatric morbidity and mortality. Remarkable advances in the past decade have led to identification of the precise genetic variants responsible for many of these conditions. Confirming the molecular diagnosis through genetic testing allows for individualized treatment plans in addition to ending the diagnostic odyssey, which not only halts further unnecessary testing but may also result in immense psychological benefit, leading to improved quality of life. However, ensuring equitable application of these advances in genomic technology has been challenging. Though prior studies have revealed disparities in testing for genetic predisposition to cancer in adults, little is known about the prevalence and nature of disparities in diagnostic testing in the pediatric rare disease population. While it seems logical that those with impaired access to healthcare would be less likely to receive the genetic testing needed to end their odyssey, few studies have addressed this question directly and the potential impact on health outcomes. This review synthesizes the available evidence regarding disparities in pediatric genetic diagnosis, defining the need for further, prospective studies with the ultimate goal of delivering precision medicine to all who stand to benefit. IMPACT: Social determinants of health are known to contribute to inequality in outcomes, though the impact on pediatric rare disease patients is not fully understood. Diagnostic genetic testing is a powerful tool, though it may not be available to all in need. This article represents the first effort, to our knowledge, to evaluate the existing literature regarding disparities in genetic testing for pediatric rare disease diagnosis and identify gaps in care.

Published

2020

32. Reconsidering Genetic Testing for Neonatal Polycystic Kidney Disease

Author

Pankaj B. Agrawal, Casie A. Genetti, Thomas E. Mullen, Monica H. Wojcik, Grace E. VanNoy, and Deborah R. Stein

Subjects

medicine.medical_specialty, medicine.diagnostic_test, Nephrology, business.industry, Internal medicine, medicine, MEDLINE, Polycystic kidney disease, Research Letter, medicine.disease, business, Genetic testing

Published

2020

33. Genetic diagnosis in the fetus

Author

Monica H. Wojcik, Tabitha Poorvu, Pankaj B. Agrawal, and Rebecca M. Reimers

Subjects

medicine.medical_specialty, Aneuploidy, Disease, Article, 03 medical and health sciences, Fetus, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, 030225 pediatrics, Humans, Medicine, Genetic Testing, 030212 general & internal medicine, Family history, Intensive care medicine, Genetic testing, Modalities, medicine.diagnostic_test, business.industry, Obstetrics and Gynecology, medicine.disease, Pediatrics, Perinatology and Child Health, Amniocentesis, Female, business

Abstract

Many genetic disorders are detectable in the prenatal period, and the capacity to identify them has increased remarkably as molecular genetic testing techniques continue to improve and become incorporated into clinical practice. The indications for prenatal genetic testing vary widely, including follow-up of an anomaly found by routine ultrasound or maternal aneuploidy screening, a family history of genetic disease, advanced maternal or paternal age, or evaluation of a low-risk pregnancy due to parental concern. The interpretation of genetic variants identified in the prenatal period poses unique challenges due to the lack of ability for deep phenotyping as well as the option to make critical decisions regarding pregnancy continuation and perinatal management. In this review, we address the various modalities currently available and commonly used for genetic testing, including pre-implantation genetic testing of embryos, cell-free DNA testing, and diagnostic procedures such as chorionic villous sampling, amniocentesis, or percutaneous umbilical blood sampling, from which samples may be sent for a wide variety of genetic tests. We discuss the difference between these modalities for the genetic diagnosis of a fetus, their strengths and weaknesses, and strategies for their optimal use in order to direct perinatal care.

Published

2020

34. A neurodevelopmental disorder caused by a novel de novo SVA insertion in exon 13 of the SRCAP gene

Author

Boxun Zhao, Jill A. Madden, Jasmine Lin, Gerard T. Berry, Monica H. Wojcik, Xuefang Zhao, Harrison Brand, Michael Talkowski, Eunjung Alice Lee, and Pankaj B. Agrawal

Subjects

Adenosine Triphosphatases, Adult, Craniofacial Abnormalities, Heart Septal Defects, Ventricular, Male, Neurodevelopmental Disorders, Genetics, Humans, Abnormalities, Multiple, Female, Exons, Genetics (clinical)

Abstract

Pathogenic variants in the SRCAP (SNF2-related CREBBP activator protein) gene, which encodes a chromatin-remodeling ATPase, cause neurodevelopmental disorders including Floating Harbor syndrome (FLHS). Here, we report the discovery of a de novo transposon insertion in SRCAP exon 13 from trio genome sequencing in a 28-year-old female with failure to thrive, developmental delay, mood disorder and seizure disorder. The insertion was a full-length (~2.8 kb), antisense-oriented SVA insertion relative to the SRCAP transcript, bearing a 5' transduction and hallmarks of target-primed reverse transcription. The 20-bp 5' transduction allowed us to trace the source SVA element to an intron of a long non-coding RNA on chromosome 12, which is highly expressed in testis. RNA sequencing and qRT-PCR confirmed significant depletion of SRCAP expression and low-level exon skipping in the proband. This case highlights a novel disease-causing structural variant and the importance of transposon analysis in a clinical diagnostic setting.

Published

2022

35. Delineation of a novel neurodevelopmental syndrome associated with PAX5 haploinsufficiency

Author

Yoel Gofin, Tianyun Wang, Madelyn A. Gillentine, Tiana M. Scott, Aliska M. Berry, Mahshid S. Azamian, Casie Genetti, Pankaj B. Agrawal, Jonathan Picker, Monica H. Wojcik, Mauricio R. Delgado, Sally A. Lynch, Stephen W. Scherer, Jennifer L. Howe, Carlos A. Bacino, Stephanie DiTroia, Grace E. VanNoy, Anne O'Donnell‐Luria, Seema R. Lalani, William D. Graf, Jill A. Rosenfeld, Evan E. Eichler, Rachel K. Earl, and Daryl A. Scott

Subjects

Mice, Phenotype, Autism Spectrum Disorder, Neurodevelopmental Disorders, Intellectual Disability, Genetics, PAX5 Transcription Factor, Animals, Humans, Haploinsufficiency, Genetics (clinical), Article

Abstract

PAX5 is a transcription factor associated with abnormal posterior midbrain and cerebellum development in mice. PAX5 is highly loss-of-function intolerant and missense constrained, and has been identified as a candidate gene for autism spectrum disorder (ASD). We describe 16 individuals from 12 families who carry deletions involving PAX5 and surrounding genes, de novo frameshift variants that are likely to trigger nonsense-mediated mRNA decay, a rare stop-gain variant, or missense variants that affect conserved amino acid residues. Four of these individuals were published previously but without detailed clinical descriptions. All these individuals have been diagnosed with one or more neurodevelopmental phenotypes including delayed developmental milestones (DD), intellectual disability (ID), and/or ASD. Seizures were documented in four individuals. No recurrent patterns of brain magnetic resonance imaging (MRI) findings, structural birth defects, or dysmorphic features were observed. Our findings suggest that PAX5 haploinsufficiency causes a neurodevelopmental disorder whose cardinal features include DD, variable ID, and/or ASD.

Published

2021

36. Mortality in the Neonatal Intensive Care Unit: Improving the Accuracy of Death Reporting

Author

Jenny Chan Yuen, Monica H. Wojcik, Anne Hansen, and Kristen T. Leeman

Subjects

medicine.medical_specialty, 2019-20 coronavirus outbreak, Neonatal intensive care unit, Quality management, Ongoing review, business.industry, Public health, Psychological intervention, Infant, Newborn, Obstetrics and Gynecology, Infant, Infant, Low Birth Weight, Quality Improvement, Infant mortality, Article, Infant, Newborn, Diseases, Intensive Care Units, Neonatal, Pediatrics, Perinatology and Child Health, Emergency medicine, Infant Mortality, Medicine, Humans, business, PDCA

Abstract

OBJECTIVE: Death certificates commonly contain errors, which hinders understanding of infant mortality. We, therefore, undertook a quality improvement (QI) initiative to improve death reporting in our neonatal intensive care unit (NICU). STUDY DESIGN: After our baseline assessment (January 1, 2015 to June 30, 2017), we implemented our QI initiatives using Plan, Do, Study, Act (PDSA) tests of change. We prospectively reviewed death certificates (July 1, 2017 to December 31, 2019) to evaluate the impact of our interventions. RESULTS: The overall proportion of incorrect death certificates significantly decreased from 71 to 22% with special cause variation noted after the second PDSA cycle. The most common errors involved inaccurate or incomplete reporting of prematurity and errors in the sequence of events. CONCLUSION: Through a series of PDSA cycles focused on formal provider education and ongoing review, we significantly reduced inaccurate death reporting. These interventions are generalizable across NICUs and important to improve public health reporting accuracy.

Published

2021

37. A missense mutation in the catalytic domain of O ‐GlcNAc transferase links perturbations in protein O ‐GlcNAcylation to X‐linked intellectual disability

Author

Marios P. Stavridis, Mehmet Gundogdu, Sergio G. Bartual, Daan M. F. van Aalten, Andrew T. Ferenbach, Riina Žordania, Katrin Õunap, Veronica M. Pravata, Monica H. Wojcik, and Sander Pajusalu

Subjects

Models, Molecular, Glycosylation, X-linked intellectual disability, Mutation, Missense, Glycobiology, Biophysics, OGlcNAC transferase, Biology, N-Acetylglucosaminyltransferases, medicine.disease_cause, Biochemistry, Cell Line, Mice, 03 medical and health sciences, Structural Biology, Catalytic Domain, Research Letter, Genetics, medicine, Animals, Humans, Transferase, Missense mutation, Molecular Biology, Gene, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Mutation, neurodevelopment, XLID, 030302 biochemistry & molecular biology, Cell Biology, medicine.disease, Phenotype, Research Letters, 3. Good health, Enzyme, chemistry, intellectual disability, Cytoplasm, OGT, O‐GlcNAc

Abstract

X‐linked intellectual disabilities (XLID) are common developmental disorders. The enzyme O‐GlcNAc transferase encoded by OGT, a recently discovered XLID gene, attaches O‐GlcNAc to nuclear and cytoplasmic proteins. As few missense mutations have been described, it is unclear what the aetiology of the patient phenotypes is. Here, we report the discovery of a missense mutation in the catalytic domain of OGT in an XLID patient. X‐ray crystallography reveals that this variant leads to structural rearrangements in the catalytic domain. The mutation reduces in vitro OGT activity on substrate peptides/protein. Mouse embryonic stem cells carrying the mutation reveal reduced O‐GlcNAcase (OGA) and global O‐GlcNAc levels. These data suggest a direct link between changes in the O‐GlcNAcome and intellectual disability observed in patients carrying OGT mutations.

Published

2019

38. Infant mortality: the contribution of genetic disorders

Author

Heather Paterson, Casie A. Genetti, Pankaj B. Agrawal, Monica H. Wojcik, Grace E. VanNoy, Timothy W. Yu, Rachel Stadelmaier, Cynthia S. Gubbels, Katri Thiele, Thomas E. Mullen, Wen-Hann Tan, Jill A. Madden, and Talia S. Schwartz

Subjects

Male, Pediatrics, medicine.medical_specialty, MEDLINE, Chromosome Disorders, Infant Death, Article, 03 medical and health sciences, 0302 clinical medicine, 030225 pediatrics, Infant Mortality, Prevalence, medicine, Humans, 030212 general & internal medicine, Medical diagnosis, Exome sequencing, Retrospective Studies, business.industry, Medical record, Genetic Diseases, Inborn, Infant, Newborn, Genetic disorder, Infant, Obstetrics and Gynecology, Retrospective cohort study, medicine.disease, United States, Infant mortality, 3. Good health, Pediatrics, Perinatology and Child Health, Cohort, Female, business

Abstract

To determine the proportion of infant deaths occurring in the setting of a confirmed genetic disorder. A retrospective analysis of the electronic medical records of infants born from 1 January, 2011 to 1 June, 2017, who died prior to 1 year of age. Five hundred and seventy three deceased infants were identified. One hundred and seventeen were confirmed to have a molecular or cytogenetic diagnosis in a clinical diagnostic laboratory and an additional seven were diagnosed by research testing for a total of 124/573 (22%) diagnosed infants. A total of 67/124 (54%) had chromosomal disorders and 58/124 (47%) had single gene disorders (one infant had both). The proportion of diagnoses made by sequencing technologies, such as exome sequencing, increased over the years. The prevalence of confirmed genetic disorders within our cohort of infant deaths is higher than that previously reported. Increased efforts are needed to further understand the mortality burden of genetic disorders in infancy.

Published

2019

39. De Novo Variants Disturbing the Transactivation Capacity of POU3F3 Cause a Characteristic Neurodevelopmental Disorder

Author

Christopher Cunniff, Laurence Faivre, Simon E. Fisher, Hester Y. Kroes, Catherine Au, Rolph Pfundt, Jacqueline Leonard, Ahmad N. Abou Tayoun, Kosuke Izumi, Katherine Bergstrom, Deepali N. Shinde, Pelagia Deriziotis, Saskia M. Maas, Marcello Niceta, Antonio Vitobello, Sha Tang, Hanka Venselaar, Christophe Philippe, Christian Gilissen, Tjitske Kleefstra, Marco Tartaglia, Helen V. Firth, Nobuhiko Okamoto, Laurens Wiel, Lot Snijders Blok, Naomichi Matsumoto, Maria Lisa Dentici, Han G. Brunner, Samuel W. Baker, Susan Tomkins, Augusta M. A. Lachmeijer, Simon Bodek, Alejandro D. Iglesias, Monica H. Wojcik, Katrin Õunap, Noriko Miyake, Koen L.I. van Gassen, Zöe Powis, The DDD Study, Human Genetics, ANS - Complex Trait Genetics, MUMC+: DA Klinische Genetica (5), Klinische Genetica, and RS: GROW - R4 - Reproductive and Perinatal Medicine

Subjects

0301 basic medicine, Male, Protein Conformation, Sequence Homology, Language in Interaction, Transactivation, 0302 clinical medicine, Neurodevelopmental disorder, BINDING, Transcriptional regulation, Missense mutation, Genetics(clinical), speech/language disorder, BRET assay, Child, de novo variants, luciferase reporter, Genetics (clinical), Genetics, TRANSCRIPTIONAL REGULATION, POU3F3, FOXP2, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], POU3F2, SPEECH, Brain-1, intellectual disability, Female, Neuroinformatics, Transcriptional Activation, EXPRESSION, GENES, Genotype, PROTEINS, Biology, BRN-2, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, Report, medicine, Humans, Amino Acid Sequence, Allele, Gene, Transcription factor, Genetic Association Studies, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], medicine.disease, 030104 developmental biology, Gene Expression Regulation, Neurodevelopmental Disorders, Mutation, POU Domain Factors, HOMODIMERIZATION, Nanomedicine Radboud Institute for Molecular Life Sciences [Radboudumc 19], 030217 neurology & neurosurgery

Abstract

POU3F3, also referred to as Brain-1, is a well-known transcription factor involved in the development of the central nervous system, but it has not previously been associated with a neurodevelopmental disorder. Here, we report the identification of 19 individuals with heterozygous POU3F3 disruptions, most of which are de novo variants. All individuals had developmental delays and/or intellectual disability and impairments in speech and language skills. Thirteen individuals had characteristic low-set, prominent, and/or cupped ears. Brain abnormalities were observed in seven of eleven MRI reports. POU3F3 is an intronless gene, insensitive to nonsense-mediated decay, and 13 individuals carried protein-truncating variants. All truncating variants that we tested in cellular models led to aberrant subcellular localization of the encoded protein. Luciferase assays demonstrated negative effects of these alleles on transcriptional activation of a reporter with a FOXP2-derived binding motif. In addition to the loss-of-function variants, five individuals had missense variants that clustered at specific positions within the functional domains, and one small in-frame deletion was identified. Two missense variants showed reduced transactivation capacity in our assays, whereas one variant displayed gain-of-function effects, suggesting a distinct pathophysiological mechanism. In bioluminescence resonance energy transfer (BRET) interaction assays, all the truncated POU3F3 versions that we tested had significantly impaired dimerization capacities, whereas all missense variants showed unaffected dimerization with wild-type POU3F3. Taken together, our identification and functional cell-based analyses of pathogenic variants in POU3F3, coupled with a clinical characterization, implicate disruptions of this gene in a characteristic neurodevelopmental disorder.

Published

2019

40. A retrospective analysis of the prevalence of imprinting disorders in Estonia from 1998 to 2016

Author

Vallo Tillmann, Karit Reinson, Pille Mee, Rita Teek, Mari-Anne Vals, Tiina Kahre, Sander Pajusalu, Ülle Murumets, Eve Õiglane-Shlik, Riina Žordania, Katrin Õunap, Aleksandr Peet, Maria Yakoreva, and Monica H. Wojcik

Subjects

Adult, Estonia, Pediatrics, medicine.medical_specialty, Beckwith-Wiedemann Syndrome, Adolescent, Prevalence, Chromosome Disorders, Article, Genomic Imprinting, Young Adult, 03 medical and health sciences, Angelman syndrome, Epidemiology, Genetics, medicine, Humans, Prospective Studies, Child, Prospective cohort study, Cyclin-Dependent Kinase Inhibitor p57, Genetics (clinical), Aged, Retrospective Studies, Aged, 80 and over, 0303 health sciences, business.industry, 030305 genetics & heredity, Infant, Newborn, Infant, Retrospective cohort study, DNA Methylation, Middle Aged, medicine.disease, Silver-Russell Syndrome, Transient neonatal diabetes mellitus, Child, Preschool, Pseudopseudohypoparathyroidism, Angelman Syndrome, Live birth, business, Prader-Willi Syndrome

Abstract

Imprinting disorders (ImpDis) represent a small group of rare congenital diseases primarily affecting growth, development, and the hormonal and metabolic systems. The aim of present study was to identify the prevalence of the ImpDis in Estonia, to describe trends in the live birth prevalence of these disorders between 1998 and 2016, and to compare the results with previously published data. We retrospectively reviewed the records of all Estonian patients since 1998 with both molecularly and clinically diagnosed ImpDis. A prospective study was also conducted, in which all patients with clinical suspicion for an ImpDis were molecularly analyzed. Eighty-seven individuals with ImpDis were identified. Twenty-seven (31%) of them had Prader–Willi syndrome (PWS), 15 (17%) had Angelman syndrome (AS), 15 (17%) had Silver–Russell syndrome (SRS), 12 (14%) had Beckwith–Wiedemann syndrome (BWS), 10 (11%) had pseudo- or pseudopseudohypoparathyroidism, four had central precocious puberty, two had Temple syndrome, one had transient neonatal diabetes mellitus, and one had myoclonus-dystonia syndrome. One third of SRS and BWS cases fulfilled the diagnostic criteria for these disorders, but tested negative for genetic abnormalities. Seventy-six individuals were alive as of January 1, 2018, indicating the total prevalence of ImpDis in Estonia is 5.8/100,000 (95% CI 4.6/100,000–7.2/100,000). The minimum live birth prevalence of all ImpDis in Estonia in 2004–2016 was 1/3,462, PWS 1/13,599, AS 1/27,198, BWS 1/21,154, SRS 1/15,866, and PHP/PPHP 1/27,198. Our results are only partially consistent with previously published data. The worldwide prevalence of SRS and GNAS-gene-related ImpDis is likely underestimated and may be at least three times higher than expected.

Published

2019

41. Commentary on Clinicians at Crossroads for a Dangerous Interference in Neonatal Bilirubin Determination at the Point-of-Care

Author

Monica H Wojcik

Subjects

Biochemistry (medical), Clinical Biochemistry

Published

2022

42. Medical and surgical interventions and outcomes for infants with trisomy 18 (T18) or trisomy 13 (T13) at children's hospitals neonatal intensive care units (NICUs)

Author

Jessica T. Fry, Carl H. Coghill, Isabella Zaniletti, Anita R. Shah, Con Yee Ling, Krishna Acharya, Narendra Dereddy, Robert DiGeronimo, Ankur Datta, Julie Weiner, Laura E. Jackson, Nana Matoba, Christine E Bishop, Helen O. Williams, Girija Natarajan, Amy B. Schlegel, Steven R. Leuthner, Monica H. Wojcik, Jamie Seale, Jason Z Niehaus, Sujir Pritha Nayak, Palliative Care, and Kevin L. Sullivan

Subjects

Pediatrics, medicine.medical_specialty, Trisomy 13 Syndrome, MEDLINE, Article, 03 medical and health sciences, 0302 clinical medicine, 030225 pediatrics, Intensive care, Intensive Care Units, Neonatal, medicine, Humans, 030212 general & internal medicine, Child, Retrospective Studies, Ethics, business.industry, Intensive treatment, Infant, Newborn, Obstetrics and Gynecology, Infant, Retrospective cohort study, medicine.disease, Hospitals, Pediatric, Aneuploidy, Outcomes research, Pediatrics, Perinatology and Child Health, Trisomy, business, Surgical interventions, Trisomy 18 Syndrome

Abstract

Objectives To examine characteristics and outcomes of T18 and T13 infants receiving intensive surgical and medical treatment compared to those receiving non-intensive treatment in NICUs. Study design Retrospective cohort of infants in the Children’s Hospitals National Consortium (CHNC) from 2010 to 2016 categorized into three groups by treatment received: surgical, intensive medical, or non-intensive. Results Among 467 infants admitted, 62% received intensive medical treatment; 27% received surgical treatment. The most common surgery was a gastrostomy tube. Survival in infants who received surgeries was 51%; intensive medical treatment was 30%, and non-intensive treatment was 72%. Infants receiving surgeries spent more time in the NICU and were more likely to receive oxygen and feeding support at discharge. Conclusions Infants with T13 or T18 at CHNC NICUs represent a select group for whom parents may have desired more intensive treatment. Survival to NICU discharge was possible, and surviving infants had a longer hospital stay and needed more discharge supports.

Published

2021

43. Discordant results between conventional newborn screening and genomic sequencing in the BabySeq Project

Author

Monica H. Wojcik, Tian Zhang, Ozge Ceyhan-Birsoy, Casie A. Genetti, Matthew S. Lebo, Timothy W. Yu, Richard B. Parad, Ingrid A. Holm, Heidi L. Rehm, Alan H. Beggs, Robert C. Green, Pankaj B. Agrawal, Wendi N. Betting, Kurt D. Christensen, Dmitry Dukhovny, Shawn Fayer, Leslie A. Frankel, Chet Graham, Amanda M. Guiterrez, Maegan Harden, Joel B. Krier, Harvey L. Levy, Xingquan Lu, Kalotina Machini, Amy L. McGuire, Jaclyn B. Murry, Medha Naik, Tiffany T. Nguyen, Hayley A. Peoples, Stacey Pereira, Devan Petersen, Uma Ramamurthy, Vivek Ramanathan, Amy Roberts, Jill O. Robinson, Serguei Roumiantsev, Talia S. Schwartz, Tina K. Truong, Grace E. VanNoy, and Susan E. Waisbren

Subjects

0301 basic medicine, Pediatrics, medicine.medical_specialty, Population, 030105 genetics & heredity, Monogenic disease, Article, 03 medical and health sciences, Neonatal Screening, Risk Factors, Exome Sequencing, False positive paradox, Medicine, Humans, education, Genetics (clinical), Exome sequencing, Newborn screening, education.field_of_study, business.industry, Genomic sequencing, Infant, Newborn, food and beverages, Chromosome Mapping, Infant, Hearing screen, Genomics, 030104 developmental biology, embryonic structures, business, Genetic diagnosis

Abstract

Purpose Newborn screening (NBS) is performed to identify neonates at risk for actionable, severe, early-onset disorders, many of which are genetic. The BabySeq Project randomized neonates to receive conventional NBS or NBS plus exome sequencing (ES) capable of detecting sequence variants that may also diagnose monogenic disease or indicate genetic disease risk. We therefore evaluated how ES and conventional NBS results differ in this population. Methods We compared results of NBS (including hearing screens) and ES for 159 infants in the BabySeq Project. Infants were considered "NBS positive" if any abnormal result was found indicating disease risk and "ES positive" if ES identified a monogenic disease risk or a genetic diagnosis. Results Most infants (132/159, 84%) were NBS and ES negative. Only one infant was positive for the same disorder by both modalities. Nine infants were NBS positive/ES negative, though seven of these were subsequently determined to be false positives. Fifteen infants were ES positive/NBS negative, all of which represented risk of genetic conditions that are not included in NBS programs. No genetic explanation was identified for eight infants referred on the hearing screen. Conclusion These differences highlight the complementarity of information that may be gleaned from NBS and ES in the newborn period.

Published

2021

44. Further Considerations on the Value of Whole-Genome Sequencing in Critically Ill Infants

Author

Monica H. Wojcik and Yarden S. Fraiman

Subjects

Whole Genome Sequencing, Critical Illness, Exome Sequencing, Pediatrics, Perinatology and Child Health, Humans, Infant, Article

Published

2022

45. Deciphering congenital anomalies for the next generation

Author

Monica H. Wojcik and Pankaj B. Agrawal

Subjects

Pediatrics, medicine.medical_specialty, Pregnancy, Family Characteristics, business.industry, Extramural, Family characteristics, MEDLINE, Infant, Congenital malformations, General Medicine, medicine.disease, Infant mortality, Congenital Abnormalities, Commentary, Medicine, Humans, Female, business, Sequence (medicine)

Abstract

Congenital anomalies are common, with 2%–3% of infants estimated to have at least one major congenital malformation and countless others with minor malformations of lesser cosmetic or medical importance. As congenital malformations are major drivers of morbidity and mortality, representing the leading cause of infant mortality in the United States, there is substantial interest in understanding the underlying etiologies—particularly if modifiable causes may be identified or pre- or postnatal treatments can be offered. Recent research has begun to reveal the spectrum of monogenic disorders that commonly result in birth defects, and newer approaches have revealed non-Mendelian genetic contributions including gene–environment interactions. Our experience suggests that increased efforts to sequence and analyze cases of perinatal death, as well as continued global collaboration, will be essential in understanding the genomic landscape of structural anomalies.

Published

2020

46. Histone H3.3 beyond cancer: Germline mutations in

Author

Laura, Bryant, Dong, Li, Samuel G, Cox, Dylan, Marchione, Evan F, Joiner, Khadija, Wilson, Kevin, Janssen, Pearl, Lee, Michael E, March, Divya, Nair, Elliott, Sherr, Brieana, Fregeau, Klaas J, Wierenga, Alexandrea, Wadley, Grazia M S, Mancini, Nina, Powell-Hamilton, Jiddeke, van de Kamp, Theresa, Grebe, John, Dean, Alison, Ross, Heather P, Crawford, Zoe, Powis, Megan T, Cho, Marcia C, Willing, Linda, Manwaring, Rachel, Schot, Caroline, Nava, Alexandra, Afenjar, Davor, Lessel, Matias, Wagner, Thomas, Klopstock, Juliane, Winkelmann, Claudia B, Catarino, Kyle, Retterer, Jane L, Schuette, Jeffrey W, Innis, Amy, Pizzino, Sabine, Lüttgen, Jonas, Denecke, Tim M, Strom, Kristin G, Monaghan, Zuo-Fei, Yuan, Holly, Dubbs, Renee, Bend, Jennifer A, Lee, Michael J, Lyons, Julia, Hoefele, Roman, Günthner, Heiko, Reutter, Boris, Keren, Kelly, Radtke, Omar, Sherbini, Cameron, Mrokse, Katherine L, Helbig, Sylvie, Odent, Benjamin, Cogne, Sandra, Mercier, Stephane, Bezieau, Thomas, Besnard, Sebastien, Kury, Richard, Redon, Karit, Reinson, Monica H, Wojcik, Katrin, Õunap, Pilvi, Ilves, A Micheil, Innes, Kristin D, Kernohan, Gregory, Costain, M Stephen, Meyn, David, Chitayat, Elaine, Zackai, Anna, Lehman, Hilary, Kitson, Martin G, Martin, Julian A, Martinez-Agosto, Stan F, Nelson, Christina G S, Palmer, Jeanette C, Papp, Neil H, Parker, Janet S, Sinsheimer, Eric, Vilain, Jijun, Wan, Amanda J, Yoon, Allison, Zheng, Elise, Brimble, Giovanni Battista, Ferrero, Francesca Clementina, Radio, Diana, Carli, Sabina, Barresi, Alfredo, Brusco, Marco, Tartaglia, Jennifer Muncy, Thomas, Luis, Umana, Marjan M, Weiss, Garrett, Gotway, K E, Stuurman, Michelle L, Thompson, Kirsty, McWalter, Constance T R M, Stumpel, Servi J C, Stevens, Alexander P A, Stegmann, Kristian, Tveten, Arve, Vøllo, Trine, Prescott, Christina, Fagerberg, Lone Walentin, Laulund, Martin J, Larsen, Melissa, Byler, Robert Roger, Lebel, Anna C, Hurst, Joy, Dean, Samantha A, Schrier Vergano, Jennifer, Norman, Saadet, Mercimek-Andrews, Juanita, Neira, Margot I, Van Allen, Nicola, Longo, Elizabeth, Sellars, Raymond J, Louie, Sara S, Cathey, Elly, Brokamp, Delphine, Heron, Molly, Snyder, Adeline, Vanderver, Celeste, Simon, Xavier, de la Cruz, Natália, Padilla, J Gage, Crump, Wendy, Chung, Benjamin, Garcia, Hakon H, Hakonarson, and Elizabeth J, Bhoj

Subjects

endocrine system, SciAdv r-articles, Forkhead Transcription Factors, Neurodegenerative Diseases, Zebrafish Proteins, Histones, fluids and secretions, mental disorders, Genetics, Animals, Humans, Molecular Biology, reproductive and urinary physiology, Germ-Line Mutation, Zebrafish, Research Articles, Research Article

Abstract

Germ line mutations in H3F3A and H3F3B cause a previously unidentified neurodevelopmental syndrome., Although somatic mutations in Histone 3.3 (H3.3) are well-studied drivers of oncogenesis, the role of germline mutations remains unreported. We analyze 46 patients bearing de novo germline mutations in histone 3 family 3A (H3F3A) or H3F3B with progressive neurologic dysfunction and congenital anomalies without malignancies. Molecular modeling of all 37 variants demonstrated clear disruptions in interactions with DNA, other histones, and histone chaperone proteins. Patient histone posttranslational modifications (PTMs) analysis revealed notably aberrant local PTM patterns distinct from the somatic lysine mutations that cause global PTM dysregulation. RNA sequencing on patient cells demonstrated up-regulated gene expression related to mitosis and cell division, and cellular assays confirmed an increased proliferative capacity. A zebrafish model showed craniofacial anomalies and a defect in Foxd3-derived glia. These data suggest that the mechanism of germline mutations are distinct from cancer-associated somatic histone mutations but may converge on control of cell proliferation.

Published

2020

47. Distinct effects on mRNA export factor GANP underlie neurological disease phenotypes and alter gene expression depending on intron content

Author

Monique M. Ryan, Roberto T. Zori, Diana Bharucha-Goebel, Matthew White, Carsten G. Bönnemann, Henry Houlden, Reza Maroofian, Jemeen Sreedharan, Karit Reinson, Noora Andersson, Mariëtte J.V. Hoffer, Monica H. Wojcik, Maie Walsh, Olli Carpén, Emilia K. Bijlsma, Marie-José H. van den Boogaard, Rosa Woldegebriel, Fang Zhao, Sara Winchester, Emil Ylikallio, Inge Cuppen, Zornitza Stark, Murray Stewart, Jouni Kvist, Henna Tyynismaa, Emer O'Connor, Sandra Donkervoort, Katrin Õunap, Centre of Excellence in Stem Cell Metabolism, STEMM - Stem Cells and Metabolism Research Program, Research Programs Unit, University of Helsinki, HUS Children and Adolescents, Department of Pathology, Helsinki University Hospital Area, Research Program in Systems Oncology, HUSLAB, Precision Cancer Pathology, Olli Mikael Carpen / Principal Investigator, Clinicum, HUS Neurocenter, Department of Neurosciences, Neurologian yksikkö, Department of Medical and Clinical Genetics, Staff Services, Henna Tyynismaa / Principal Investigator, Neuroscience Center, and Helsinki Institute of Life Science HiLIFE

Subjects

AcademicSubjects/SCI01140, Male, PROMOTES, Protein Conformation, SAGA, RNA Transport, Transcriptome, INITIATION, 0302 clinical medicine, Transcription (biology), Gene expression, TRANSCRIPTION, Age of Onset, Child, Genetics (clinical), SAC3, Regulation of gene expression, Genetics, 0303 health sciences, TREX-2 COMPLEX, 1184 Genetics, developmental biology, physiology, Intracellular Signaling Peptides and Proteins, Nuclear Proteins, Peripheral Nervous System Diseases, General Medicine, Phenotype, Child, Preschool, Antigens, Surface, Female, General Article, MCM3AP, Biology, REGION, 03 medical and health sciences, Acetyltransferases, Intellectual Disability, Humans, RNA, Messenger, Molecular Biology, Transcription factor, Gene, 030304 developmental biology, Glycoproteins, Cell Nucleus, Flavoproteins, Intron, PATHWAYS, Phosphoproteins, Introns, Phosphoric Monoester Hydrolases, Exodeoxyribonucleases, Gene Expression Regulation, REPLICATION, 1182 Biochemistry, cell and molecular biology, 3111 Biomedicine, Nervous System Diseases, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Defects in the mRNA export scaffold protein GANP, encoded by the MCM3AP gene, cause autosomal recessive early-onset peripheral neuropathy with or without intellectual disability. We extend here the phenotypic range associated with MCM3AP variants, by describing a severely hypotonic child and a sibling pair with a progressive encephalopathic syndrome. In addition, our analysis of skin fibroblasts from affected individuals from seven unrelated families indicates that disease variants result in depletion of GANP except when they alter critical residues in the Sac3 mRNA binding domain. GANP depletion was associated with more severe phenotypes compared with the Sac3 variants. Patient fibroblasts showed transcriptome alterations that suggested intron content-dependent regulation of gene expression. For example, all differentially expressed intronless genes were downregulated, including ATXN7L3B, which couples mRNA export to transcription activation by association with the TREX-2 and SAGA complexes. Our results provide insight into the molecular basis behind genotype-phenotype correlations in MCM3AP-associated disease and suggest mechanisms by which GANP defects might alter RNA metabolism.

Published

2020

48. Developmental Support for Infants With Genetic Disorders

Author

Susan E. Waisbren, Jonathan S. Litt, Monica H. Wojcik, and Jane E. Stewart

Subjects

Pediatrics, medicine.medical_specialty, Developmental Disabilities, Psychological intervention, MEDLINE, Context (language use), Infant, Premature, Diseases, 03 medical and health sciences, 0302 clinical medicine, 030225 pediatrics, Intervention (counseling), Intellectual disability, Early Intervention, Educational, medicine, Humans, Medical diagnosis, business.industry, Incidence (epidemiology), Genetic Diseases, Inborn, Infant, Newborn, Genetic disorder, medicine.disease, State-of-the-Art Review, Pediatrics, Perinatology and Child Health, business, Infant, Premature

Abstract

As the technical ability for genetic diagnosis continues to improve, an increasing number of diagnoses are made in infancy or as early as the neonatal period. Many of these diagnoses are known to be associated with developmental delay and intellectual disability, features that would not be clinically detectable at the time of diagnosis. Others may be associated with cognitive impairment, but the incidence and severity are yet to be fully described. These neonates and infants with genetic diagnoses therefore represent an emerging group of patients who are at high risk for neurodevelopmental disabilities. Although there are well-established developmental supports for high-risk infants, particularly preterm infants, after discharge from the NICU, programs specifically for infants with genetic diagnoses are rare. And although previous research has demonstrated the positive effect of early developmental interventions on outcomes among preterm infants, the impact of such supports for infants with genetic disorders who may be born term, remains to be understood. We therefore review the literature regarding existing developmental assessment and intervention approaches for children with genetic disorders, evaluating these in the context of current developmental supports postdischarge for preterm infants. Further research into the role of developmental support programs for early assessment and intervention in high-risk neonates diagnosed with rare genetic disorders is needed.

Published

2020

49. Prenatal Diagnosis of a Ventral Abdominal Wall Defect

Author

Kristyn S. Beam, Judy A. Estroff, Charles J. Smithers, Pankaj B. Agrawal, and Monica H. Wojcik

Subjects

medicine.medical_specialty, Palliative care, Article, Ultrasonography, Prenatal, 03 medical and health sciences, 0302 clinical medicine, Fatal Outcome, Pregnancy, 030225 pediatrics, Prenatal Diagnosis, medicine, Vaginal septum, Humans, Diaphragmatic hernia, Abnormalities, Multiple, 030212 general & internal medicine, Uterine septum, Hernia, Diaphragmatic, medicine.diagnostic_test, business.industry, Gastroschisis, Abdominal wall defect, Infant, Newborn, Ectopia cordis, medicine.disease, Magnetic Resonance Imaging, Hernia, Ventral, Hernia, Abdominal, Echocardiography, Pediatrics, Perinatology and Child Health, Female, Radiology, business, Fetal echocardiography

Abstract

* Abbreviations: MFCC: : Maternal Fetal Care Center MRI: : magnetic resonance imaging VSD: : ventricular septal defect A 12-week fetal sonogram in a 22-year-old gravida 1 para 0 pregnant woman was suggestive of multiple anomalies. She had previously been known to have a congenital uterine anomaly with both a vaginal septum and uterine septum that were removed 3 years before the current pregnancy. She had 2 cervices with 1 uterine cavity and normal bilateral fallopian tubes at the time of this spontaneous pregnancy. Her initial course was uncomplicated, but fetal ultrasonography at 12 weeks’ gestation showed a large anterior wall defect spanning both the chest and abdomen, with concern for possible ectopia cordis. The fetus was noted to have restricted movement within a subjectively small amniotic sac. Cell-free fetal DNA screening was low risk and amniocentesis was not performed. She was referred to the Maternal Fetal Care Center (MFCC) at 17 weeks’ gestation for further evaluation and counseling. Imaging at the MFCC at 17 weeks and 3 days of gestation included fetal ultrasonography, magnetic resonance imaging (MRI), and fetal echocardiography. Imaging findings included the following: a small portion of the cardiac apex was outside the chest, a small anterior diaphragmatic hernia, a large abdominal wall defect with liver and bowel herniation, and significant thoracic kyphosis (Fig 1). In addition, a complete amnion-chorion separation was noted (Fig 2, ultrasound scan; Fig 3, MRI). Fetal echocardiography showed a ventricular septal defect (VSD) with a mildly hypoplastic pulmonary valve and partial ectopia cordis with a small sternal defect with left cardiac ventricle herniation. Figure 1. Prenatal T2 magnetic resonance imaging at 17 weeks’ gestation demonstrating herniated liver (solid green arrow) and small herniation of the apex of the heart (dashed green arrow) through a diaphragmatic defect. Evisceration of the small bowel (solid yellow arrow) and colon (dashed yellow arrow) are also visualized. Demonstration of kyphoscoliosis (red arrow). Figure 2. Ultrasound image demonstrating …

Published

2020

50. Genome sequencing identifies a homozygous inversion disrupting QDPR as a cause for dihydropteridine reductase deficiency

Author

Katrin Õunap, Ülle Murumets, Hardo Lilleväli, Ryan L. Collins, Kersti Lilleväli, Nenad Blau, Monica H. Wojcik, Julia K. Goodrich, Sander Pajusalu, Pille Tammur, University of Zurich, and Õunap, Katrin

Subjects

0301 basic medicine, 2716 Genetics (clinical), lcsh:QH426-470, 610 Medicine & health, 030105 genetics & heredity, Biology, tetrahydrobiopterin deficiencies, DNA sequencing, Chromosome Breakpoints, inversion, 03 medical and health sciences, symbols.namesake, dihydropteridine reductase deficiency, 1311 Genetics, Phenylketonurias, Exome Sequencing, Genetics, 1312 Molecular Biology, Humans, Coding region, Genetic Testing, Child, Molecular Biology, Gene, Genetics (clinical), Exome sequencing, Sanger sequencing, Homozygote, Original Articles, QDPR gene, Dihydropteridine Reductase, genome sequencing, lcsh:Genetics, QDPR, 030104 developmental biology, Chromosome 4, 10036 Medical Clinic, Chromosome Inversion, symbols, Female, Original Article, Acyl-CoA Oxidase, Chromosomes, Human, Pair 4

Abstract

Background Dihydropteridine reductase (DHPR) is one of the key enzymes for maintaining in the organism the supply of tetrahydrobiopterin (BH4), an essential cofactor for aromatic amino acid hydroxylases. Its dysfunction causes the condition of hyperphenylalaninemia together with the lack of neurotransmitters. Methods We report a patient with biochemically diagnosed DHPR deficiency, with extensive molecular investigations undertaken to detect variations in quinoid dihydropteridine reductase (QDPR) gene. Sanger sequencing of QDPR coding regions, exome sequencing, QDPR mRNA PCR, and karyotyping were followed by trio genome sequencing. Results Short‐read genome sequencing revealed a homozygous 9‐Mb inversion disrupting QDPR. Structural variant breakpoints in chromosome 4 were located to intron 2 of QDPR at Chr4(GRCh38):g.17505522 and in intron 8 of the ACOX3 gene, Chr4(GRCh38):g.8398067). Both nonrelated parents carried the variant in heterozygous state. The inversion was not present in gnomAD structural variant database. Conclusion Identification of the exact breakpoints now allows further straightforward molecular genetic testing of potential carriers of the inversion. This study extends the pathogenic variant spectrum of DHPR deficiency and highlights the role of structural variants in recessive metabolic disorders. To our knowledge, this is the first report on a large, canonical (rather than complex) homozygous pathogenic inversion detected by genome sequencing., We present a case in whom genome sequencing revealed a homozygous 9‐Mb inversion disrupting QDPR, not previously detected by Sanger sequencing of QDPR coding regions, exome sequencing, QDPR mRNA PCR, or karyotyping. This case is very good example how genome sequencing is giving an additional diagnostic yield to more common molecular methods. To our knowledge, this is the first report on a large, canonical homozygous pathogenic inversion detected by genome sequencing.

Published

2020