Abstract
Since the first novel gene discovery for a Mendelian condition was made via exome sequencing, the rapid increase in the number of genes known to underlie Mendelian conditions coupled with the adoption of exome (and more recently, genome) sequencing by diagnostic testing labs has changed the landscape of genomic testing for rare diseases. Specifically, many individuals suspected to have a Mendelian condition are now routinely offered clinical ES. This commonly results in a precise genetic diagnosis but frequently overlooks the identification of novel candidate genes. Such candidates are also less likely to be identified in the absence of large-scale gene discovery research programs. Accordingly, clinical laboratories have both the opportunity, and some might argue a responsibility, to contribute to novel gene discovery, which should, in turn, increase the diagnostic yield for many conditions. However, clinical diagnostic laboratories must necessarily balance priorities for throughput, turnaround time, cost efficiency, clinician preferences, and regulatory constraints and often do not have the infrastructure or resources to effectively participate in either clinical translational or basic genome science research efforts. For these and other reasons, many laboratories have historically refrained from broadly sharing potentially pathogenic variants in novel genes via networks such as Matchmaker Exchange, much less reporting such results to ordering providers. Efforts to report such results are further complicated by a lack of guidelines for clinical reporting and interpretation of variants in novel candidate genes. Nevertheless, there are myriad benefits for many stakeholders, including patients/families, clinicians, and researchers, if clinical laboratories systematically and routinely identify, share, and report novel candidate genes. To facilitate this change in practice, we developed criteria for triaging, sharing, and reporting novel candidate genes that are most likely to be promptly validated as underlying a Mendelian condition and translated to use in clinical settings.
Original language | English (US) |
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Article number | 101199 |
Journal | Genetics in Medicine |
Volume | 26 |
Issue number | 10 |
DOIs | |
State | Published - Oct 2024 |
Funding
The GREGoR Consortium is funded by the National Human Genome Research Institute of the National Institutes of Health , through the following grants: U01HG011758, U01HG011755, U01HG011745, U01HG011762, U01HG011744, and U24HG011746. All authors of this manuscript are funded by the NIH. Erica Smith is a current employee of Ambry Genetics and a stockholder of Invitae genetics. Megan H. Hawley is an employee of Invitae and own stock in the company. Michael J. Bamshad is the chair of the Scientific Advisory Board of GeneDx and receives funding from the American Society of Human Genetics as the Editor-in-Chief of HGG Advances. Jessica X. Chong receives funding from the American Society of Human Genetics as the Deputy Editor of HGG Advances. Heidi L. Rehm has received rare-disease research funding from Microsoft and Illumina and compensation as a past member of the scientific advisory board of Genome Medical.The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. We thank Anthony J. Marcello for assistance in data retrieval for Supplemental Table 1. The GREGoR Consortium is funded by the National Human Genome Research Institute of the National Institutes of Health, through the following grants: U01HG011758, U01HG011755, U01HG011745, U01HG011762, U01HG011744, and U24HG011746. Conceptualization: J.X.C. S.Berger, S.Baxter, E.S. C.X. S.D.; Data curation: J.X.C. H.L.R.; Investigation: J.X.C. S.Berger, S.Baxter, E.S. C.X. D.C. M.H. E.A.R.-M. S.D. H.L.R.; Methodology: J.X.C. S.Berger, S.Baxter, E.S. C.X. D.C. M.H. E.A.R.-M. S.D. H.L.R.; Project administration: S.Baxter; Visualization: S.Berger. C.X.; Writing-original draft: J.X.C. S.Berger, S. Baxter, E.S. C.X. D.C. M.H. E.A.R.-M. S.D. M.B. H.L.R.; Writing-review & editing: J.X.C. S.Berger, S. Baxter, E.S. C.X. D.C. M.H. E.A.R.-M. S.D. M.B. H.L.R. This manuscript does not report studies on human subjects; therefore, no IRB approval was necessary. Siwaar Abouhala, Jessica Albert, Miguel Almalvez, Raquel Alvarez, Mutaz Amin, Peter Anderson, Swaroop Aradhya, Euan Ashley, Themistocles Assimes, Light Auriga, Christina Austin-Tse, Mike Bamshad, Hayk Barseghyan, Samantha Baxter, Sairam Behera, Shaghayegh Beheshti, Gill Bejerano, Seth Berger, Jon Bernstein, Sabrina Best, Benjamin Blankenmeister, Elizabeth Blue, Eric Boerwinkle, Emily Bonkowski, Devon Bonner, Philip Boone, Miriam Bornhorst, Harrison Brand, Kati Buckingham, Daniel Calame, Jennefer Carter, Silvia Casadei, Lisa Chadwick, Clarisa Chavez, Ziwei Chen, Ivan Chinn, Jessica Chong, Zeynep Coban-Akdemir, Andrea J. Cohen, Sarah Conner, Matthew Conomos, Karen Coveler, Ya Allen Cui, Sara Currin, Robert Daber, Zain Dardas, Colleen Davis, Moez Dawood, Ivan de Dios, Celine de Esch, Meghan Delaney, Emmanuele Delot, Stephanie DiTroia, Harsha Doddapaneni, Haowei Du, Ruizhi Duan, Shannon Dugan-Perez, Nhat Duong, Michael Duyzend, Evan Eichler, Sara Emami, Jamie Fraser, Vincent Fusaro, Miranda Galey, Vijay Ganesh, Brandon Garcia, Kiran Garimella, Richard Gibbs, Casey Gifford, Amy Ginsburg, Page Goddard, Stephanie Gogarten, Nikhita Gogate, William Gordon, John E. Gorzynski, William Greenleaf, Christopher Grochowski, Emily Groopman, Rodrigo Guarischi Sousa, Sanna Gudmundsson, Ashima Gulati, Stacey Hall, William Harvey, Megan Hawley, Ben Heavner, Martha Horike-Pyne, Jianhong Hu, Yongqing Huang, James Hwang, Gail Jarvik, Tanner Jensen, Shalini Jhangiani, David Jimenez-Morales, Christopher Jin, Ahmed K. Saad, Amanda Kahn-Kirby, Jessica Kain, Parneet Kaur, Laura Keehan, Susan Knoblach, Arthur Ko, Anshul Kundaje, Soumya Kundu, Samuel M. Lancaster, Katie Larsson, Arthur Lee, Gabrielle Lemire, Richard Lewis, Wei Li, Yidan Li, Pengfei Liu, Jonathan LoTempio, James (Jim) Lupski, Jialan Ma, Daniel MacArthur, Medhat Mahmoud, Nirav Malani, Brian Mangilog, Dana Marafi, Sofia Marmolejos, Daniel Marten, Eva Martinez, Colby Marvin, Shruti Marwaha, Francesco Kumara Mastrorosa, Dena Matalon, Susanne May, Sean McGee, Lauren Meador, Heather Mefford, Hector Rodrigo Mendez, Alexander Miller, Danny E. Miller, Tadahiro Mitani, Stephen Montgomery, Mariana Moyses, Chloe Munderloh, Donna Muzny, Sarah Nelson, Thuy-mi P. Nguyen, Jonathan Nguyen, Robert Nussbaum, Keith Nykamp, William O'Callaghan, Emily O'Heir, Melanie O'Leary, Jeren Olsen, Ikeoluwa Osei-Owusu, Anne O'Donnell-Luria, Evin Padhi, Lynn Pais, Miao Pan, Piyush Panchal, Karynne Patterson, Sheryl Payne, Davut Pehlivan, Paul Petrowski, Alicia Pham, Georgia Pitsava, Astaria \u2018Sara\u2019 Podesta, Sarah Ponce, Elizabeth Porter, Jennifer Posey, Jaime Prosser, Thomas Quertermous, Archana Rai, Arun Ramani, Heidi Rehm, Chloe Reuter, Jason Reuter, Matthew Richardson, Andres Rivera-Munoz, Oriane Rubio, Aniko Sabo, Monica Salani, Kaitlin Samocha, Alba Sanchis-Juan, Sarah Savage, Evette Scott, Stuart Scott, Fritz Sedlazeck, Gulalai Shah, Ali Shojaie, Mugdha Singh, Kevin Smith, Josh Smith, Hana Snow, Michael Snyder, Kayla Socarras, Lea Starita, Brigitte Stark, Sarah Stenton, Andrew Stergachis, Adrienne Stilp, V. Reid Sutton, Jui-Cheng Tai, Michael (Mike) Talkowski, Christina Tise, Catherine (Cat) Tong, Philip Tsao, Rachel Ungar, Grace VanNoy, Eric Vilain, Isabella Voutos, Kim Walker, Chia-Lin Wei, Ben Weisburd, Jeff Weiss, Chris Wellington, Ziming Weng, Emily Westheimer, Marsha Wheeler, Matthew Wheeler, Laurens Wiel, Michael Wilson, Monica Wojcik, Quenna Wong, Changrui Xiao, Rachita Yadav, Qian Yi, Bo Yuan, Jianhua Zhao, Jimmy Zhen, Harry Zhou
Keywords
- Candidate gene
- Diagnostics
- Gene discovery
- Mendelian disorder
- Rare disease
ASJC Scopus subject areas
- Genetics(clinical)