No association between MUTYH and MSH6 germline mutations in 64 HNPCC patients

Research output: Contribution to journalResearch articleContributedpeer-review

Contributors

  • Verena Steinke - , University of Bonn (Author)
  • Nils Rahner - , University of Bonn (Author)
  • Monika Morak - , Ludwig Maximilian University of Munich, Center for Medical Genetics and Primary Health Care (Author)
  • Gisela Keller - , Technical University of Munich (Author)
  • Hans K. Schackert - , Department of Surgical Research (Author)
  • Heike Görgens - , Department of Surgical Research (Author)
  • Wolff Schmiegel - , Ruhr University Bochum (Author)
  • Brigitte Royer-Pokora - , Heinrich Heine University Düsseldorf (Author)
  • Wolfgang Dietmaier - , University of Regensburg (Author)
  • Matthias Kloor - , Heidelberg University  (Author)
  • Christoph Engel - , Leipzig University (Author)
  • Peter Propping - , University of Bonn (Author)
  • Stefan Aretz - , University of Bonn (Author)

Abstract

Hereditary non-polyposis colorectal cancer (HNPCC) is an autosomal dominant tumour predisposition syndrome caused by germline mutations in mismatch repair (MMR) genes. In contrast to MLH1 and MSH2, germline mutations in MSH6 are associated with a milder and particularly variable phenotype. Based on the reported interaction of the MMR complex and the base excision repair protein MUTYH, it was hypothesised that MUTYH mutations serve as phenotypical modifiers in HNPCC families. Recently, a significantly higher frequency of heterozygosity for MUTYH mutations among MSH6 mutation carriers was reported. We examined 64 MSH6 mutation carriers (42 truncating mutations, 19 missense mutations and 3 silent mutations) of the German HNPCC Consortium for MUTYH mutations by sequencing the whole coding region of the gene. Monoallelic MUTYH mutations were identified in 2 of the 64 patients (3.1%), no biallelic MUTYH mutation carrier was found. The frequency of MUTYH mutations was not significantly higher than that in healthy controls, neither in the whole patient group (P = 0.30) nor in different subgroups regarding mutation type. Our results do not support the association between MSH6 mutations and heterozygosity for MUTYH mutations.

Details

Original languageEnglish
Pages (from-to)587-592
Number of pages6
JournalEuropean journal of human genetics
Volume16
Issue number5
Publication statusPublished - May 2008
Peer-reviewedYes

External IDs

PubMed 18301448

Keywords

Sustainable Development Goals

ASJC Scopus subject areas