Association of germline variants with KRAS-mutation status in colorectal cancer

NP Tjader; J Ramroop; T Gandhi; C Dauch; O Meadows; P Stevens; R Pearlman; H Hampel; EK Aglago; SI Berndt; A Bloomer; H Brenner; DD Buchanan; PT Campbell; Y Cao; AT Chan; I Cheng; N Dimou; DA Drew; AJ French; P Georgeson; M Giannakis; GG Giles; M Gomez; SB Gruber; M Hoffmeister; WY Huang; MAJ Hullar; JR Huyghe; N Loroña; V Moreno; CC Newton; JA Nowak; M Obón-Santacana; S Ogino; A Pellatt; AR Peoples; JB Permuth; SL Schmit; RE Schoen; EM Siegel; RS Steinfelder; W Sun; JK Teer; CE Thomas; QM Trinh; K Tsilidis; T Ugai; CY Um; B Van Guelpen; SH Zaidi; J Figueiredo; U Peters; AI Phipps; JP McElroy; AE Toland

Journal article

Association of germline variants with KRAS-mutation status in colorectal cancer

NP Tjader, J Ramroop, T Gandhi, C Dauch, O Meadows, P Stevens, R Pearlman, H Hampel, EK Aglago, SI Berndt, A Bloomer, H Brenner, DD Buchanan, PT Campbell, Y Cao, AT Chan, I Cheng, N Dimou, DA Drew, AJ French Show all

Scientific Reports | Springer Science and Business Media LLC | Published : 2026

DOI: 10.1038/s41598-026-39644-8

Abstract

Somatic mutations in KRAS are a common driver of colorectal cancer (CRC) and present at different frequencies by race, sex, tumor site, ethnicity, and genetic similarity. Inherited germline variants may influence tumor somatic mutation frequency by altering mutation or DNA repair processes or altering cellular, immunological and/or microenvironmental responses after a mutation. We hypothesized that the germline genetic background modifies somatic KRAS mutation frequency in CRC. To test this, we performed a genome-wide association study (GWAS) in 7071 individuals with CRC, using KRAS mutation status as the phenotype. Single-nucleotide variants were chosen for validation analyses based on P va..

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