Germline loss-of-function variants in the base-excision repair gene MBD4 cause a Mendelian recessive syndrome of adenomatous colorectal polyposis and acute myeloid leukaemia

Author:

Palles Claire,Chew Edward,Grolleman Judith E.,Galavotti Sara,Flensburg Christoffer,Jansen Erik A.M.,Curley Helen,Chegwidden Laura,Barnes Edward Arbe,Bajel Ashish,Sherwood Kitty,Martin Lynn,Thomas Huw,Georgiou Demetra,Fostira Florentia,Goldberg Yael,Adams David J.,van der Biezen Simone A.M.,Christie Michael,Clendenning Mark,Deltas Constantinos,Dimovski Aleksandar J.,Dymerska Dagmara,Lubinski Jan,Mahmood Khalid,van der Post Rachel S.,Sanders Mathijs,Weitz Jürgen,Taylor Jenny C.,Turnbull Clare,Vreede Lilian,van Wezel Tom,Whalley Celina,Pac Claudia Arnedo,Caravagna Gulio,Cross William,Chubb Daniel,Frangou Anna,Gruber Andreas,Kinnersley Ben,Noyvert Boris,Church David,Graham Trevor,Houlston Richard,Lopez-Bigas Nuria,Sottoriva Andrea,Wedge David,Jenkins Mark A.,Kuiper Roland P.,Roberts Andrew W.,Ligtenberg Marjolijn J.L.,Hoogerbrugge Nicoline,Koelzer Viktor H.,Rivas Andres Dacal,Winship Ingrid M.,Ponte Clara Ruiz,Buchanan Daniel D.,Tomlinson Ian P.M.,Majewski Ian J.,de Voer Richarda M.ORCID, , ,

Abstract

ABSTRACTInherited defects in base-excision repair (BER) predispose to adenomatous polyposis and colorectal cancer (CRC), yet our understanding of this important DNA repair pathway remains incomplete. By combining detailed clinical, histological and molecular profiling, we reveal biallelic germline loss-of-function (LOF) variants in the BER gene MBD4 to predispose to adenomatous polyposis and –uniquely amongst CRC predisposition syndromes– to myeloid neoplasms. Neoplasms from MBD4-deficient patients almost exclusively accumulate somatic CpG>TpG mutations, resembling mutational signature SBS1. MBD4-deficient adenomas harbour mutations in known CRC driver genes, although AMER1 mutations were more common and KRAS mutations less frequent. We did not find an increased risk for colorectal tumours in individuals with a monoallelic MBD4 LOF variant. We suggest that this condition should be termed MBD4-associated neoplasia syndrome (MANS) and that MBD4 is included in testing for the genetic diagnosis of polyposis and/or early-onset AML.

Publisher

Cold Spring Harbor Laboratory

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