The Barrett-associated variants at GDF7 and TBX5 also increase esophageal adenocarcinoma risk.

Jéssica Becker ,Katharina Weise,Josef Weismüller,Timo Hess,Lothar Veits,Andrea May,Brigitte Schumacher,Michael Vieth,Katja Ott,Thomas Schmidt,Michael Knapp,Hauke Lang,Markus Moehler,Jakob R Izbicki,Johannes Schumacher,Nils Kosiol,Sophie K M Heinrichs,Markus M Nöthen,Claudia Schmidt,Christian Gerges,Mario Anders,Peter Malfertheiner,Oliver Pech,Michael Arras,Horst Neuhaus,Hendrik Manner,Jan‐Hinnerk Hofer,Tania Noder,Andreas Hackelsberger,Rupert Mayershofer,Arnulf H Hölscher,Ines Gockel,Christian Ell,Anne C Böhmer,Thomas Rösch,Elfriede Bollschweiler,Marino Venerito,Nicole Kreuser,Orestis Lyros,Yogesh K Vashist ,D Lorenz ,Constantin Johannes Ahlbrand ,Sebastian J Hofer ,Ralf Kießlich

doi:10.1002/cam4.641

Abstract

Barrett's esophagus (BE) and esophageal adenocarcinoma (EAC) represent two stages within the esophagitis‐metaplasia‐dysplasia‐adenocarcinoma sequence. Previously genetic risk factors have been identified that confer risk to BE and EAC development. However, to which extent the genetic variants confer risk to different stages of the BE/EAC sequence remains mainly unknown. In this study we analyzed three most recently identified BE variants at the genes GDF7 (rs3072), TBX5 (rs2701108), and ALDH1A2 (rs3784262) separately in BE and EAC samples in order to determine their risk effects during BE/EAC sequence. Our data show that rs3072 at GDF7 and rs2701108 at TBX5 are also associated with EAC and conclude that both loci confer disease risk also at later stages of the BE/EAC sequence. In contrast, rs3784262 at ALDH1A2 was highly significantly associated with BE, but showed no association with EAC. Our data do not provide evidence that the ALDH1A2 locus confers equal risk in early and late stages of BE/EAC sequence.

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