Effect of a polygenic risk score in patients with late-onset, early-onset, familial, or hereditary colorectal cancer.

Klinkhammer, Hannah; Franke, Marcus; Engel, Christoph; Steinke-Lange, Verena; Möslein, Gabriela; Schmidt, Börge; Vangala, Deepak; Forstner, Andreas J; Büttner, Reinhard; Maj, Carlo; Perne, Claudia; Hüneburg, Robert; Holinski-Feder, Elke; Kloor, Matthias; Nguyen, Huu Phuc; Jahn, Arne; Hoffmann, Per; Mayr, Andreas; Aretz, Stefan; Redler, Silke; Spier, Isabel; Schröck, Evelin

doi:10.1093/jncics/pkag041

Journal Article

DKFZ-2026-00868

Effect of a polygenic risk score in patients with late-onset, early-onset, familial, or hereditary colorectal cancer.

Klinkhammer, H. ; Spier, I. ; Perne, C. ; Hoffmann, P. ; Büttner, R. ; Schröck, E.DKFZ* ; Redler, S. ; Jahn, A.DKFZ* ; Franke, M.DKFZ* ; Möslein, G. ; Kloor, M. ; Schmidt, B. ; Vangala, D. ; Nguyen, H. P. ; Forstner, A. J. ; Steinke-Lange, V. ; Holinski-Feder, E. ; Hüneburg, R. ; Maj, C. ; Engel, C. ; Mayr, A. ; Aretz, S.

2026
Oxford University Press Oxford

JNCI cancer spectrum nn, nn (2026) [10.1093/jncics/pkag041]

Abstract: This study investigates how a polygenic risk score (PRS) influences colorectal cancer (CRC) risk across clinically and molecularly defined risk groups.1,839 European-descendant individuals were stratified according to low (<20%), intermediate (20 to 80%), or high (>80%) PRS, based on 93 CRC-associated SNPs, for four high risk groups: (i) Lynch syndrome [LS; with CRC: n = 679, CRC-free carriers: n = 422]; (ii) early-onset sporadic CRC [EOS-CRC; n = 518], (iii) positive family history for CRC [F-CRC; n = 220]; and, in EOS-CRC and F-CRC patients (iv) MSI/dMMR CRC [n = 144] vs MSS/pMMR CRC [n = 485]. CRC risk was compared to population-based controls [n = 3,119] and late-onset sporadic CRC patients from UK Biobank [LOS-CRC; n = 781] using multivariable logistic regression and Cox models.PRS was significantly increased in all risk groups compared to population controls. Being in the high PRS category doubled CRC risk in EOS-CRC and F-CRC corresponding to cumulative incidences before 50 and 75 years of 24% and 13%, respectively. PRS was significantly higher in EOS-CRC than LOS-CRC. In LS, PRS in non-CRC carriers lay between CRC-LS and population controls. Non-LS individuals with MSI/dMMR tumors showed significantly lower PRS than those with pMMR/MSS tumors, but no difference compared to LS CRC individuals.PRS most strongly influences CRC risk in unexplained EOS- and F-CRC. The effect in LS individuals strongly depends on the penetrance of the altered gene and study design. Non-significant trends can partly be explained by the sample size of subgroups. Larger collaborative, prospective studies are needed to validate PRS for personalized CRC risk stratification.

Keyword(s): Family History ; Lynch syndrome ; Polygenic Risk ; Risk Stratification ; Risk assessment ; hereditary tumor syndromes

Classification:

ddc:610

Note: epub

Contributing Institute(s):

DKTK Koordinierungsstelle Dresden (DD01)

Research Program(s):

899 - ohne Topic (POF4-899) (POF4-899)

Appears in the scientific report 2026

Database coverage:
Medline

;

; Article Processing Charges ; Clarivate Analytics Master Journal List ; DOAJ Seal ; Emerging Sources Citation Index ; Fees ; IF < 5 ; JCR ; SCOPUS ; Web of Science Core Collection

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Record created 2026-04-14, last modified 2026-04-14

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