Missed diagnoses: Clinically relevant lessons learned through medical mysteries solved by the Undiagnosed Diseases Network

Heidi Cope; Rebecca Spillmann; Jill A. Rosenfeld; Elly Brokamp; Rebecca Signer; Kelly Schoch; Emily G. Kelley; Jennifer A. Sullivan; Ellen Macnamara; Sharyn Lincoln; Katie Golden‐Grant; Undiagnosed Diseases Network; James P. Orengo; Gary Clark; Lindsay C. Burrage; Jennifer E. Posey; Jaya Punetha; Amy Robertson; Joy Cogan; John A. Phillips III; Julian Martinez‐Agosto; Vandana Shashi

doi:10.1002/mgg3.1397

Molecular Genetics & Genomic Medicine (Oct 2020)

Missed diagnoses: Clinically relevant lessons learned through medical mysteries solved by the Undiagnosed Diseases Network

Heidi Cope,
Rebecca Spillmann,
Jill A. Rosenfeld,
Elly Brokamp,
Rebecca Signer,
Kelly Schoch,
Emily G. Kelley,
Jennifer A. Sullivan,
Ellen Macnamara,
Sharyn Lincoln,
Katie Golden‐Grant,
Undiagnosed Diseases Network,
James P. Orengo,
Gary Clark,
Lindsay C. Burrage,
Jennifer E. Posey,
Jaya Punetha,
Amy Robertson,
Joy Cogan,
John A. Phillips III,
Julian Martinez‐Agosto,
Vandana Shashi

Affiliations

Heidi Cope: Division of Medical Genetics Department of Pediatrics Duke University Medical Center Durham NC USA
Rebecca Spillmann: Division of Medical Genetics Department of Pediatrics Duke University Medical Center Durham NC USA
Jill A. Rosenfeld: Department of Molecular and Human Genetics Baylor College of Medicine Houston TX USA
Elly Brokamp: Division of Medical Genetics and Genomic Medicine Vanderbilt University Medical Center Nashville TN USA
Rebecca Signer: Department of Human Genetics University of California Los Angeles CA USA
Kelly Schoch: Division of Medical Genetics Department of Pediatrics Duke University Medical Center Durham NC USA
Emily G. Kelley: Department of Biomedical Informatics Harvard Medical School Boston MA USA
Jennifer A. Sullivan: Division of Medical Genetics Department of Pediatrics Duke University Medical Center Durham NC USA
Ellen Macnamara: Undiagnosed Diseases Program Common Fund Office of the Director National Institutes of HealthNIH Bethesda MD USA
Sharyn Lincoln: Division of Genetics and Genomics Department of Pediatrics Boston Children’s Hospital Boston MA USA
Katie Golden‐Grant: Division of Medical Genetics University of Washington Seattle WA USA
Undiagnosed Diseases Network: Undiagnosed Diseases Program Common Fund Office of the Director National Institutes of HealthNIH Bethesda MD USA
James P. Orengo: Department of Neurology Baylor College of Medicine Houston TX USA
Gary Clark: Department of Neurology Baylor College of Medicine Houston TX USA
Lindsay C. Burrage: Department of Molecular and Human Genetics Baylor College of Medicine Houston TX USA
Jennifer E. Posey: Department of Molecular and Human Genetics Baylor College of Medicine Houston TX USA
Jaya Punetha: Department of Molecular and Human Genetics Baylor College of Medicine Houston TX USA
Amy Robertson: Division of Medical Genetics and Genomic Medicine Vanderbilt University Medical Center Nashville TN USA
Joy Cogan: Division of Medical Genetics and Genomic Medicine Vanderbilt University Medical Center Nashville TN USA
John A. Phillips III: Division of Medical Genetics and Genomic Medicine Vanderbilt University Medical Center Nashville TN USA
Julian Martinez‐Agosto: Department of Human Genetics University of California Los Angeles CA USA
Vandana Shashi: Division of Medical Genetics Department of Pediatrics Duke University Medical Center Durham NC USA

DOI: https://doi.org/10.1002/mgg3.1397
Journal volume & issue: Vol. 8, no. 10
pp. n/a – n/a

Abstract

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Abstract Background Resources within the Undiagnosed Diseases Network (UDN), such as genome sequencing (GS) and model organisms aid in diagnosis and identification of new disease genes, but are currently difficult to access by clinical providers. While these resources do contribute to diagnoses in many cases, they are not always necessary to reach diagnostic resolution. The UDN experience has been that participants can also receive diagnoses through the thoughtful and customized application of approaches and resources that are readily available in clinical settings. Methods The UDN Genetic Counseling and Testing Working Group collected case vignettes that illustrated how clinically available methods resulted in diagnoses. The case vignettes were classified into three themes; phenotypic considerations, selection of genetic testing, and evaluating exome/GS variants and data. Results We present 12 participants that illustrate how clinical practices such as phenotype‐driven genomic investigations, consideration of variable expressivity, selecting the relevant tissue of interest for testing, utilizing updated testing platforms, and recognition of alternate transcript nomenclature resulted in diagnoses. Conclusion These examples demonstrate that when a diagnosis is elusive, an iterative patient‐specific approach utilizing assessment options available to clinical providers may solve a portion of cases. However, this does require increased provider time commitment, a particular challenge in the current practice of genomics.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

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