Leveraging cancer mutation data to inform the pathogenicity classification of germline missense variants

Bushra Haque; David Cheerie; Amy Pan; Meredith Curtis; Thomas Nalpathamkalam; Jimmy Nguyen; Celine Salhab; Bhooma Thiruvahindrapuram; Jade Zhang; Madeline Couse; Taila Hartley; Michelle M Morrow; E Magda Price; Susan Walker; David Malkin; Frederick P Roth; Gregory Costain

doi:10.1371/journal.pgen.1011540

Leveraging cancer mutation data to inform the pathogenicity classification of germline missense variants

PLoS Genet. 2025 Jan 6;21(1):e1011540. doi: 10.1371/journal.pgen.1011540. Online ahead of print.

Authors

Bushra Haque^{1

2}, David Cheerie^{1

2}, Amy Pan², Meredith Curtis^{1

2}, Thomas Nalpathamkalam³, Jimmy Nguyen^{1

2}, Celine Salhab^{1

2}, Bhooma Thiruvahindrapuram³, Jade Zhang⁴, Madeline Couse⁵, Taila Hartley⁶, Michelle M Morrow⁷, E Magda Price⁶, Susan Walker⁸, David Malkin⁹, Frederick P Roth^{2

10

11

12

13}, Gregory Costain^{1

2

3

14}

Affiliations

¹ Program in Genetics and Genome Biology, SickKids Research Institute, Toronto, Ontario, Canada.
² Department of Molecular Genetics, University of Toronto, Toronto, Ontario, Canada.
³ The Centre for Applied Genomics, The Hospital for Sick Children, Toronto, Ontario, Canada.
⁴ Human Biology Program, University of Toronto, Toronto, Ontario, Canada.
⁵ Centre for Computational Medicine, Hospital for Sick Children, Toronto, Ontario, Canada.
⁶ Children's Hospital of Eastern Ontario Research Institute, University of Ottawa, Ottawa, Ontario, Canada.
⁷ GeneDx, Gaithersburg, Maryland, United States of America.
⁸ Genomics England, London, United Kingdom.
⁹ Division of Haematology/Oncology, The Hospital for Sick Children, Department of Pediatrics, University of Toronto, Toronto, Ontario, Canada.
¹⁰ Donnelly Centre for Cellular and Biomolecular Research (CCBR), University of Toronto, Toronto, Ontario, Canada.
¹¹ Lunenfeld-Tanenbaum Research Institute (LTRI), Sinai Health System, Toronto, Ontario, Canada.
¹² Center for Cancer Systems Biology (CCSB), Dana-Farber Cancer Institute, Boston, Massachusetts, United States of America.
¹³ Department of Computer Science, University of Toronto, Toronto, Ontario, Canada.
¹⁴ Division of Clinical and Metabolic Genetics, The Hospital for Sick Children, and Department of Paediatrics, University of Toronto, Toronto, Ontario, Canada.

PMID: 39761285
DOI: 10.1371/journal.pgen.1011540

Abstract

Innovative and easy-to-implement strategies are needed to improve the pathogenicity assessment of rare germline missense variants. Somatic cancer driver mutations identified through large-scale tumor sequencing studies often impact genes that are also associated with rare Mendelian disorders. The use of cancer mutation data to aid in the interpretation of germline missense variants, regardless of whether the gene is associated with a hereditary cancer predisposition syndrome or a non-cancer-related developmental disorder, has not been systematically assessed. We extracted putative cancer driver missense mutations from the Cancer Hotspots database and annotated them as germline variants, including presence/absence and classification in ClinVar. We trained two supervised learning models (logistic regression and random forest) to predict variant classifications of germline missense variants in ClinVar using Cancer Hotspot data (training dataset). The performance of each model was evaluated with an independent test dataset generated in part from searching public and private genome-wide sequencing datasets from ~1.5 million individuals. Of the 2,447 cancer mutations, 691 corresponding germline variants had been previously classified in ClinVar: 426 (61.6%) as likely pathogenic/pathogenic, 261 (37.8%) as uncertain significance, and 4 (0.6%) as likely benign/benign. The odds ratio for a likely pathogenic/pathogenic classification in ClinVar was 28.3 (95% confidence interval: 24.2-33.1, p < 0.001), compared with all other germline missense variants in the same 216 genes. Both supervised learning models showed high correlation with pathogenicity assessments in the training dataset. There was high area under precision-recall curve values (0.847 and 0.829) and area under the receiver-operating characteristic curve values (0.821 and 0.774) for logistic regression and random forest models, respectively, when applied to the test dataset. With the use of cancer and germline datasets and supervised learning techniques, our study shows that cancer mutation data can be leveraged to improve the interpretation of germline missense variation potentially causing rare Mendelian disorders.

Copyright: © 2025 Haque et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.