A genome-wide approach for the discovery of novel repeat expansion disorders in the Undiagnosed Diseases Network cohort

Undiagnosed Diseases Network

doi:10.1016/j.gim.2025.101462

A genome-wide approach for the discovery of novel repeat expansion disorders in the Undiagnosed Diseases Network cohort

Undiagnosed Diseases Network

Research output: Contribution to journal › Article › peer-review

Abstract

Purpose: The Undiagnosed Diseases Network is a National Institutes of Health funded research study that aims to solve a broad clinical spectrum of challenging rare disease cases. Participants receive care from multiple clinical specialists, who collaborate to perform deep phenotyping and state-of-the-art multiomics analyses. As bioinformatics of short-read sequencing has matured, the discovery of repeat expansion disorders (REDs) is accelerating. REDs comprise approximately 60 characterized disorders, which exhibit a broad spectrum of phenotypes. Thus, a largely unbiased genome-wide approach in a phenotypically diverse sample will add to the diagnostic depth, explore the limits of short-read genome analysis, and establish novel candidate RED loci. Methods: Here, we present a genome-wide analysis of repeat expansions conducted on 1018 genomes from the Undiagnosed Diseases Network. By leveraging 2 distinct bioinformatics tools, ExpansionHunter Denovo and STRling, we showed that repeat expansions can be accurately detected in short-read genomes. Results: We demonstrated that a genotype-first approach can diagnose atypical cases of known REDs and provide valuable clinical insights. We present clinical details on participants with expansions in ATXN7, DMPK, FMR1, GLS, HTT, RFC1, AFF3, and MARCH6. Importantly, we highlight 2 cases of juvenile Huntington disease that were discovered through our analysis. Finally, we present a list of novel candidate short tandem repeats (TR) that could potentially be pathogenic if expanded. Conclusion: Importantly, our approach showcases the bioinformatic advancements in genome analysis for RED detection and highlights its practical applications.

Original language	English
Article number	101462
Journal	Genetics in Medicine
Volume	27
Issue number	8
DOIs	https://doi.org/10.1016/j.gim.2025.101462
State	Published - Aug 2025

Keywords

Bioinformatics
Rare disease
Rare diseases
Short tandem repeats
Tandem repeat expansion disorders

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10.1016/j.gim.2025.101462

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@article{ca4872860313415680ffd5f6fa025496,

title = "A genome-wide approach for the discovery of novel repeat expansion disorders in the Undiagnosed Diseases Network cohort",

abstract = "Purpose: The Undiagnosed Diseases Network is a National Institutes of Health funded research study that aims to solve a broad clinical spectrum of challenging rare disease cases. Participants receive care from multiple clinical specialists, who collaborate to perform deep phenotyping and state-of-the-art multiomics analyses. As bioinformatics of short-read sequencing has matured, the discovery of repeat expansion disorders (REDs) is accelerating. REDs comprise approximately 60 characterized disorders, which exhibit a broad spectrum of phenotypes. Thus, a largely unbiased genome-wide approach in a phenotypically diverse sample will add to the diagnostic depth, explore the limits of short-read genome analysis, and establish novel candidate RED loci. Methods: Here, we present a genome-wide analysis of repeat expansions conducted on 1018 genomes from the Undiagnosed Diseases Network. By leveraging 2 distinct bioinformatics tools, ExpansionHunter Denovo and STRling, we showed that repeat expansions can be accurately detected in short-read genomes. Results: We demonstrated that a genotype-first approach can diagnose atypical cases of known REDs and provide valuable clinical insights. We present clinical details on participants with expansions in ATXN7, DMPK, FMR1, GLS, HTT, RFC1, AFF3, and MARCH6. Importantly, we highlight 2 cases of juvenile Huntington disease that were discovered through our analysis. Finally, we present a list of novel candidate short tandem repeats (TR) that could potentially be pathogenic if expanded. Conclusion: Importantly, our approach showcases the bioinformatic advancements in genome analysis for RED detection and highlights its practical applications.",

keywords = "Bioinformatics, Rare disease, Rare diseases, Short tandem repeats, Tandem repeat expansion disorders",

author = "\{Undiagnosed Diseases Network\} and Sarah Fazal and Harriet Dashnow and Dohrn, \{Maike F.\} and Jacquelyn Raposo and Laurel Hiatt and Danzi, \{Matt C.\} and Xu, \{Isaac R.L.\} and Camilo Toro and Adams, \{David R.\} and Karen Usdin and Bruce Hayward and Kobren, \{Shilpa Nadimpalli\} and Sunyaev, \{Shamil R.\} and Spillmann, \{Rebecca C.\} and Vandana Shashi and Adriana Rebelo and Guney Bademci and Aaron Quinlan and Abdul Elkadri and Adeline Vanderver and Adriana Rebelo and Beggs, \{Alan H.\} and \{La Spada\}, \{Albert R.\} and Alden Huang and Alex Paul and Alexander Miller and Ali Al-Beshri and Alistair Ward and Allen Bale and Allyn McConkie-Rosell and Tran, \{Alyssa A.\} and Andrea Gropman and Andres Vargas and Crouse, \{Andrew B.\} and Andrew Stergachis and Anna Hurst and Anna Raper and Arjun Tarakad and Ashley Andrews and Ashley McMinn and Ashok Balasubramanyam and \{Pusey Swerdzewski\}, \{Barbara N.\} and Beatriz Anguiano and Ben Afzali and Ben Solomon and Martin, \{Beth A.\} and Russell, \{Bianca E.\} and Wilk, \{Brandon M.\} and Breanna Mitchell and Lanpher, \{Brendan C.\} and Lee, \{Brendan H.\} and Fogel, \{Brent L.\} and Brett Bordini and Graham, \{Brett H.\} and Brian Corner and Brianna Tucker and Bruce Korf and MacRae, \{Calum A.\} and Camilo Toro and Cara Skraban and Bacino, \{Carlos A.\} and Carol Oladele and Caroline Hendry and Smith, \{Carson A.\} and Cecilia Esteves and Changrui Xiao and Reuter, \{Chloe M.\} and Eng, \{Christine M.\} and Chan, \{Chun Hung\} and Wahl, \{Colleen E.\} and Welt, \{Corrine K.\} and Tifft, \{Cynthia J.\} and Dana Kiley and Rader, \{Daniel J.\} and Daniel Wegner and Danny Miller and Scott, \{Daryl A.\} and Dave Viskochil and Sweetser, \{David A.\} and Adams, \{David R.\} and Deborah Barbouth and Rao, \{Deepak A.\} and Devin Oglesbee and Devon Bonner and Donald Basel and Donna Novacic and \{Bustos velasq\}, Francisco and Dustin Baldridge and Edward Behrens and Silverman, \{Edwin K.\} and Elaine Seto and Elijah Kravets and Elisabeth Rosenthal and Worthey, \{Elizabeth A.\} and Burke, \{Elizabeth A.\} and Elizabeth Blue and Chao, \{Elizabeth C.\} and Fieg, \{Elizabeth L.\} and Macnamara, \{Ellen F.\} and Elsa Balton and Emily Glanton and Emily Shelkowitz and Emily Wang and Eric Allenspach and Eric Klee and Eric Vilain and Erin Conboy and Baldwin, \{Erin E.\} and Erin McRoy and Dell'Angelica, \{Esteban C.\} and Ashley, \{Euan A.\} and Cole, \{F. Sessions\} and \{Pinto e Vairo\}, Filippo and Frances High and Francesco Vetrini and Francis Rossignol and Hisama, \{Fuki M.\} and Gabor Marth and Jarvik, \{Gail P.\} and Clark, \{Gary D.\} and George Carvalho and Berry, \{Gerard T.\} and Ghayda Mirzaa and Giorgio Sirugo and Gonench Kilich and Guney Bademci and Mendez, \{Hector Rodrigo\} and Heidi Wood and Herman Taylor and Tabor, \{Holly K.\} and Hongzheng Dai and Chao, \{Hsiao Tuan\} and Hua Xu and Bellen, \{Hugo J.\} and Hui Zhang and Ian Glass and Lanza, \{Ian R.\} and Holm, \{Ingrid A.\} and Kohane, \{Isaac S.\} and Isum Ward and Ivan Chinn and Pallais, \{J. Carl\} and Sampson, \{Jacinda B.\} and Orengo, \{James P.\} and James Verbsky and Jared Sninsky and Jason Hom and Jason Schend and Kohler, \{Jennefer N.\} and Posey, \{Jennifer E.\} and Jennifer Morgan and Jennifer Schymick and Jennifer Wambach and Jessica Douglas and Jiayu Fu and Rosenfeld, \{Jill A.\} and Jimann Shin and Stoler, \{Joan M.\} and Gonzalez, \{Joanna M.\} and Phillips, \{John A.\} and John Carey and Gorzynski, \{John E.\} and Mulvihill, \{John J.\} and Joie Davis and Bernstein, \{Jonathan A.\} and Jordan Whitlock and Jose Abdenur and Joseph Loscalzo and Cogan, \{Joy D.\} and Mart{\'i}nez-Agosto, \{Julian A.\} and Julie McCarrier and Justin Alvey and Kahlen Darr and Kaitlin Callaway and Leppig, \{Kathleen A.\} and Kathleen Sullivan and Kathy Sisco and Kathyrn Singh and Katrina Dipple and Treat, \{Kayla M.\} and Kelly Hassey and Kelly Schoch and Smith, \{Kevin S.\} and Khurram Liaqat and Kim Worley and Kimberly Ezell and Kimberly LeBlanc and Kumarie Latchman and Rodan, \{Lance H.\} and Laura Keehan and Laura Pace and Cobban, \{Laurel A.\} and Lauren Blieden and Briere, \{Lauren C.\} and Lauren Jeffries and Laurens Wiel and Lilianna Solnica-Krezel and Patricia Dickson and Stephen Pak and Timothy Schedl",

note = "Publisher Copyright: {\textcopyright} 2025 American College of Medical Genetics and Genomics",

year = "2025",

month = aug,

doi = "10.1016/j.gim.2025.101462",

language = "English",

volume = "27",

journal = "Genetics in Medicine",

issn = "1098-3600",

number = "8",

}

TY - JOUR

T1 - A genome-wide approach for the discovery of novel repeat expansion disorders in the Undiagnosed Diseases Network cohort

AU - Undiagnosed Diseases Network

AU - Fazal, Sarah

AU - Dashnow, Harriet

AU - Dohrn, Maike F.

AU - Raposo, Jacquelyn

AU - Hiatt, Laurel

AU - Danzi, Matt C.

AU - Xu, Isaac R.L.

AU - Toro, Camilo

AU - Adams, David R.

AU - Usdin, Karen

AU - Hayward, Bruce

AU - Kobren, Shilpa Nadimpalli

AU - Sunyaev, Shamil R.

AU - Spillmann, Rebecca C.

AU - Shashi, Vandana

AU - Rebelo, Adriana

AU - Bademci, Guney

AU - Quinlan, Aaron

AU - Elkadri, Abdul

AU - Vanderver, Adeline

AU - Rebelo, Adriana

AU - Beggs, Alan H.

AU - La Spada, Albert R.

AU - Huang, Alden

AU - Paul, Alex

AU - Miller, Alexander

AU - Al-Beshri, Ali

AU - Ward, Alistair

AU - Bale, Allen

AU - McConkie-Rosell, Allyn

AU - Tran, Alyssa A.

AU - Gropman, Andrea

AU - Vargas, Andres

AU - Crouse, Andrew B.

AU - Stergachis, Andrew

AU - Hurst, Anna

AU - Raper, Anna

AU - Tarakad, Arjun

AU - Andrews, Ashley

AU - McMinn, Ashley

AU - Balasubramanyam, Ashok

AU - Pusey Swerdzewski, Barbara N.

AU - Anguiano, Beatriz

AU - Afzali, Ben

AU - Solomon, Ben

AU - Martin, Beth A.

AU - Russell, Bianca E.

AU - Wilk, Brandon M.

AU - Mitchell, Breanna

AU - Lanpher, Brendan C.

AU - Lee, Brendan H.

AU - Fogel, Brent L.

AU - Bordini, Brett

AU - Graham, Brett H.

AU - Corner, Brian

AU - Tucker, Brianna

AU - Korf, Bruce

AU - MacRae, Calum A.

AU - Toro, Camilo

AU - Skraban, Cara

AU - Bacino, Carlos A.

AU - Oladele, Carol

AU - Hendry, Caroline

AU - Smith, Carson A.

AU - Esteves, Cecilia

AU - Xiao, Changrui

AU - Reuter, Chloe M.

AU - Eng, Christine M.

AU - Chan, Chun Hung

AU - Wahl, Colleen E.

AU - Welt, Corrine K.

AU - Tifft, Cynthia J.

AU - Kiley, Dana

AU - Rader, Daniel J.

AU - Wegner, Daniel

AU - Miller, Danny

AU - Scott, Daryl A.

AU - Viskochil, Dave

AU - Sweetser, David A.

AU - Adams, David R.

AU - Barbouth, Deborah

AU - Rao, Deepak A.

AU - Oglesbee, Devin

AU - Bonner, Devon

AU - Basel, Donald

AU - Novacic, Donna

AU - Bustos velasq, Francisco

AU - Baldridge, Dustin

AU - Behrens, Edward

AU - Silverman, Edwin K.

AU - Seto, Elaine

AU - Kravets, Elijah

AU - Rosenthal, Elisabeth

AU - Worthey, Elizabeth A.

AU - Burke, Elizabeth A.

AU - Blue, Elizabeth

AU - Chao, Elizabeth C.

AU - Fieg, Elizabeth L.

AU - Macnamara, Ellen F.

AU - Balton, Elsa

AU - Glanton, Emily

AU - Shelkowitz, Emily

AU - Wang, Emily

AU - Allenspach, Eric

AU - Klee, Eric

AU - Vilain, Eric

AU - Conboy, Erin

AU - Baldwin, Erin E.

AU - McRoy, Erin

AU - Dell'Angelica, Esteban C.

AU - Ashley, Euan A.

AU - Cole, F. Sessions

AU - Pinto e Vairo, Filippo

AU - High, Frances

AU - Vetrini, Francesco

AU - Rossignol, Francis

AU - Hisama, Fuki M.

AU - Marth, Gabor

AU - Jarvik, Gail P.

AU - Clark, Gary D.

AU - Carvalho, George

AU - Berry, Gerard T.

AU - Mirzaa, Ghayda

AU - Sirugo, Giorgio

AU - Kilich, Gonench

AU - Bademci, Guney

AU - Mendez, Hector Rodrigo

AU - Wood, Heidi

AU - Taylor, Herman

AU - Tabor, Holly K.

AU - Dai, Hongzheng

AU - Chao, Hsiao Tuan

AU - Xu, Hua

AU - Bellen, Hugo J.

AU - Zhang, Hui

AU - Glass, Ian

AU - Lanza, Ian R.

AU - Holm, Ingrid A.

AU - Kohane, Isaac S.

AU - Ward, Isum

AU - Chinn, Ivan

AU - Pallais, J. Carl

AU - Sampson, Jacinda B.

AU - Orengo, James P.

AU - Verbsky, James

AU - Sninsky, Jared

AU - Hom, Jason

AU - Schend, Jason

AU - Kohler, Jennefer N.

AU - Posey, Jennifer E.

AU - Morgan, Jennifer

AU - Schymick, Jennifer

AU - Wambach, Jennifer

AU - Douglas, Jessica

AU - Fu, Jiayu

AU - Rosenfeld, Jill A.

AU - Shin, Jimann

AU - Stoler, Joan M.

AU - Gonzalez, Joanna M.

AU - Phillips, John A.

AU - Carey, John

AU - Gorzynski, John E.

AU - Mulvihill, John J.

AU - Davis, Joie

AU - Bernstein, Jonathan A.

AU - Whitlock, Jordan

AU - Abdenur, Jose

AU - Loscalzo, Joseph

AU - Cogan, Joy D.

AU - Martínez-Agosto, Julian A.

AU - McCarrier, Julie

AU - Alvey, Justin

AU - Darr, Kahlen

AU - Callaway, Kaitlin

AU - Leppig, Kathleen A.

AU - Sullivan, Kathleen

AU - Sisco, Kathy

AU - Singh, Kathyrn

AU - Dipple, Katrina

AU - Treat, Kayla M.

AU - Hassey, Kelly

AU - Schoch, Kelly

AU - Smith, Kevin S.

AU - Liaqat, Khurram

AU - Worley, Kim

AU - Ezell, Kimberly

AU - LeBlanc, Kimberly

AU - Latchman, Kumarie

AU - Rodan, Lance H.

AU - Keehan, Laura

AU - Pace, Laura

AU - Cobban, Laurel A.

AU - Blieden, Lauren

AU - Briere, Lauren C.

AU - Jeffries, Lauren

AU - Wiel, Laurens

AU - Solnica-Krezel, Lilianna

AU - Dickson, Patricia

AU - Pak, Stephen

AU - Schedl, Timothy

PY - 2025/8

Y1 - 2025/8

N2 - Purpose: The Undiagnosed Diseases Network is a National Institutes of Health funded research study that aims to solve a broad clinical spectrum of challenging rare disease cases. Participants receive care from multiple clinical specialists, who collaborate to perform deep phenotyping and state-of-the-art multiomics analyses. As bioinformatics of short-read sequencing has matured, the discovery of repeat expansion disorders (REDs) is accelerating. REDs comprise approximately 60 characterized disorders, which exhibit a broad spectrum of phenotypes. Thus, a largely unbiased genome-wide approach in a phenotypically diverse sample will add to the diagnostic depth, explore the limits of short-read genome analysis, and establish novel candidate RED loci. Methods: Here, we present a genome-wide analysis of repeat expansions conducted on 1018 genomes from the Undiagnosed Diseases Network. By leveraging 2 distinct bioinformatics tools, ExpansionHunter Denovo and STRling, we showed that repeat expansions can be accurately detected in short-read genomes. Results: We demonstrated that a genotype-first approach can diagnose atypical cases of known REDs and provide valuable clinical insights. We present clinical details on participants with expansions in ATXN7, DMPK, FMR1, GLS, HTT, RFC1, AFF3, and MARCH6. Importantly, we highlight 2 cases of juvenile Huntington disease that were discovered through our analysis. Finally, we present a list of novel candidate short tandem repeats (TR) that could potentially be pathogenic if expanded. Conclusion: Importantly, our approach showcases the bioinformatic advancements in genome analysis for RED detection and highlights its practical applications.

AB - Purpose: The Undiagnosed Diseases Network is a National Institutes of Health funded research study that aims to solve a broad clinical spectrum of challenging rare disease cases. Participants receive care from multiple clinical specialists, who collaborate to perform deep phenotyping and state-of-the-art multiomics analyses. As bioinformatics of short-read sequencing has matured, the discovery of repeat expansion disorders (REDs) is accelerating. REDs comprise approximately 60 characterized disorders, which exhibit a broad spectrum of phenotypes. Thus, a largely unbiased genome-wide approach in a phenotypically diverse sample will add to the diagnostic depth, explore the limits of short-read genome analysis, and establish novel candidate RED loci. Methods: Here, we present a genome-wide analysis of repeat expansions conducted on 1018 genomes from the Undiagnosed Diseases Network. By leveraging 2 distinct bioinformatics tools, ExpansionHunter Denovo and STRling, we showed that repeat expansions can be accurately detected in short-read genomes. Results: We demonstrated that a genotype-first approach can diagnose atypical cases of known REDs and provide valuable clinical insights. We present clinical details on participants with expansions in ATXN7, DMPK, FMR1, GLS, HTT, RFC1, AFF3, and MARCH6. Importantly, we highlight 2 cases of juvenile Huntington disease that were discovered through our analysis. Finally, we present a list of novel candidate short tandem repeats (TR) that could potentially be pathogenic if expanded. Conclusion: Importantly, our approach showcases the bioinformatic advancements in genome analysis for RED detection and highlights its practical applications.

KW - Bioinformatics

KW - Rare disease

KW - Rare diseases

KW - Short tandem repeats

KW - Tandem repeat expansion disorders

UR - https://www.scopus.com/pages/publications/105009588600

U2 - 10.1016/j.gim.2025.101462

DO - 10.1016/j.gim.2025.101462

M3 - Article

C2 - 40417743

AN - SCOPUS:105009588600

SN - 1098-3600

VL - 27

JO - Genetics in Medicine

JF - Genetics in Medicine

IS - 8

M1 - 101462

ER -

A genome-wide approach for the discovery of novel repeat expansion disorders in the Undiagnosed Diseases Network cohort

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