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. 2024 Nov;56(11):2422-2433.
doi: 10.1038/s41588-024-01966-6. Epub 2024 Oct 29.

Gene-based burden tests of rare germline variants identify six cancer susceptibility genes

Erna V Ivarsdottir #  1 Julius Gudmundsson #  2 Vinicius Tragante  2 Gardar Sveinbjornsson  2 Snaedis Kristmundsdottir  2 Simon N Stacey  2 Gisli H Halldorsson  2 Magnus I Magnusson  2 Asmundur Oddsson  2 G Bragi Walters  2 Asgeir Sigurdsson  2 Saedis Saevarsdottir  2   3   4 Doruk Beyter  2 Gudmar Thorleifsson  2 Bjarni V Halldorsson  2   5 Pall Melsted  2   6 Hreinn Stefansson  2 Ingileif Jonsdottir  2   3   7 Erik Sørensen  8 Ole B Pedersen  9   10 Christian Erikstrup  11   12 Martin Bøgsted  13 Mette Pøhl  14 Andreas Røder  9   15 Hein Vincent Stroomberg  9   15 Ismail Gögenur  9   16 Jens Hillingsø  17 Stig E Bojesen  9   18 Ulrik Lassen  9   14 Estrid Høgdall  9   19 Henrik Ullum  20 Søren Brunak  21 Sisse R Ostrowski  8   9 DBDS Genomic ConsortiumIda Elken Sonderby  22   23   24 Oleksandr Frei  24   25   26 Srdjan Djurovic  22   23   24 Alexandra Havdahl  27   28   29 Pal Moller  30 Mev Dominguez-Valentin  30 Jan Haavik  31   32 Ole A Andreassen  23   24   25 Eivind Hovig  26   30 Bjarni A Agnarsson  3   33 Rafn Hilmarsson  34 Oskar Th Johannsson  35 Trausti Valdimarsson  36   37 Steinn Jonsson  3   4 Pall H Moller  3   34 Jon H Olafsson  3   38 Bardur Sigurgeirsson  3   38 Jon G Jonasson  3   33 Geir Tryggvason  3   39 Hilma Holm  2 Patrick Sulem  2 Thorunn Rafnar  2 Daniel F Gudbjartsson  2   6 Kari Stefansson  40   41
Collaborators, Affiliations

Gene-based burden tests of rare germline variants identify six cancer susceptibility genes

Erna V Ivarsdottir et al. Nat Genet. 2024 Nov.

Abstract

Discovery of cancer risk variants in the sequence of the germline genome can shed light on carcinogenesis. Here we describe gene burden association analyses, aggregating rare missense and loss of function variants, at 22 cancer sites, including 130,991 cancer cases and 733,486 controls from Iceland, Norway and the United Kingdom. We identified four genes associated with increased cancer risk; the pro-apoptotic BIK for prostate cancer, the autophagy involved ATG12 for colorectal cancer, TG for thyroid cancer and CMTR2 for both lung cancer and cutaneous melanoma. Further, we found genes with rare variants that associate with decreased risk of cancer; AURKB for any cancer, irrespective of site, and PPP1R15A for breast cancer, suggesting that inhibition of PPP1R15A may be a preventive strategy for breast cancer. Our findings pinpoint several new cancer risk genes and emphasize autophagy, apoptosis and cell stress response as a focus point for developing new therapeutics.

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