Clinically relevant combined effect of polygenic background, rare pathogenic germline variants, and family history on colorectal cancer incidence

HASSANIN, Emadeldin Saeed Fathy Sayed; Spier, Isabel; BOBBILI, Dheeraj Reddy; Aldisi, Rana; Klinkhammer, Hannah; David, Friederike; Dueñas, Nuria; Hüneburg, Robert; Perne, Claudia; Brunet, Joan; Capella, Gabriel; Nöthen, Markus M.; Forstner, Andreas J.; Mayr, Andreas; Krawitz, Peter; MAY, Patrick; Aretz, Stefan; Maj, Carlo

doi:10.1186/s12920-023-01469-z

Article (Périodiques scientifiques)

Clinically relevant combined effect of polygenic background, rare pathogenic germline variants, and family history on colorectal cancer incidence

HASSANIN, Emadeldin Saeed Fathy Sayed; Spier, Isabel; BOBBILI, Dheeraj Reddy et al.

2023 • In BMC Medical Genomics, 16 (1), p. 42

Peer reviewed vérifié par ORBi

Permalien
https://hdl.handle.net/10993/54800

DOI
10.1186/s12920-023-01469-z

PubMed
36872334

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Résumé :

[en] Background and aims: Summarised in polygenic risk scores (PRS), the effect of common, low penetrant genetic variants associated with colorectal cancer (CRC), can be used for risk stratification. Methods: To assess the combined impact of the PRS and other main factors on CRC risk, 163,516 individuals from the UK Biobank were stratified as follows: 1. carriers status for germline pathogenic variants (PV) in CRC susceptibility genes ( APC, MLH1, MSH2, MSH6, PMS2) , 2. low (\textless 20\%), intermediate (20–80\%), or high PRS (\textgreater 80\%), and 3. family history (FH) of CRC. Multivariable logistic regression and Cox proportional hazards models were applied to compare odds ratios and to compute the lifetime incidence, respectively. Results: Depending on the PRS, the CRC lifetime incidence for non-carriers ranges between 6 and 22\%, compared to 40 and 74 for carriers. A suspicious FH is associated with a further increase of the cumulative incidence reaching 26 for non-carriers and 98 for carriers. In non-carriers without FH, but high PRS, the CRC risk is doubled, whereas a low PRS even in the context of a FH results in a decreased risk. The full model including PRS, carrier status, and FH improved the area under the curve in risk prediction (0.704). Conclusion: The findings demonstrate that CRC risks are strongly influenced by the PRS for both a sporadic and monogenic background. FH, PV, and common variants complementary contribute to CRC risk. The implementation of PRS in routine care will likely improve personalized risk stratification, which will in turn guide tailored preventive surveillance strategies in high, intermediate, and low risk groups.

Centre de recherche :

- Luxembourg Centre for Systems Biomedicine (LCSB): Bioinformatics Core (R. Schneider Group)

Disciplines :

Oncologie
Génétique & processus génétiques

Auteur, co-auteur :

HASSANIN, Emadeldin Saeed Fathy Sayed ; University of Luxembourg > Luxembourg Centre for Systems Biomedicine (LCSB) > Bioinformatics Core

Spier, Isabel

BOBBILI, Dheeraj Reddy ; University of Luxembourg > Luxembourg Centre for Systems Biomedicine (LCSB) > Bioinformatics Core

Aldisi, Rana

Klinkhammer, Hannah

David, Friederike

Dueñas, Nuria

Hüneburg, Robert

Perne, Claudia

Brunet, Joan

Plus d'auteurs (8 en +)

Co-auteurs externes :

yes

Langue du document :

Anglais

Titre :

Clinically relevant combined effect of polygenic background, rare pathogenic germline variants, and family history on colorectal cancer incidence

Date de publication/diffusion :

23 mars 2023

Titre du périodique :

BMC Medical Genomics

eISSN :

1755-8794

Maison d'édition :

BioMed Central, London, Royaume-Uni

Volume/Tome :

Fascicule/Saison :

Pagination :

Peer reviewed :

Peer reviewed vérifié par ORBi

Focus Area :

Systems Biomedicine

URL complémentaire :

https://bmcmedgenomics.biomedcentral.com/articles/10.1186/s12920-023-01469-z

Disponible sur ORBilu :

depuis le 06 avril 2023

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Bibliographie

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