TY - JOUR T1 - Current clinical criteria for Lynch syndrome are not sensitive enough to identify <em>MSH6</em> mutation carriers JF - Journal of Medical Genetics JO - J Med Genet SP - 579 LP - 585 DO - 10.1136/jmg.2010.077677 VL - 47 IS - 9 AU - Wenche Sjursen AU - Bjørn Ivar Haukanes AU - Eli Marie Grindedal AU - Harald Aarset AU - Astrid Stormorken AU - Lars F Engebretsen AU - Christoffer Jonsrud AU - Inga Bjørnevoll AU - Per Arne Andresen AU - Sarah Ariansen AU - Liss Anne S Lavik AU - Bodil Gilde AU - Inger Marie Bowitz-Lothe AU - Lovise Mæhle AU - Pål Møller Y1 - 2010/09/01 UR - http://jmg.bmj.com/content/47/9/579.abstract N2 - Background Reported prevalence, penetrance and expression of deleterious mutations in the mismatch repair (MMR) genes, MLH1, MSH2, MSH6 and PMS2, may reflect differences in the clinical criteria used to select families for DNA testing. The authors have previously reported that clinical criteria are not sensitive enough to identify MMR mutation carriers among incident colorectal cancer cases.Objective To describe the sensitivity of the criteria when applied to families with a demonstrated MMR mutation.Methods Families with an aggregation of colorectal cancers were examined for deleterious MMR mutations according to the Mallorca guidelines. All families with a detected MMR mutation as of November 2009 were reclassified according to the Amsterdam and Bethesda criteria.Results Sixty-nine different DNA variants were identified in a total of 129 families. The original Amsterdam clinical criteria were met by 38%, 12%, 78% and 25% of families with mutations in MSH2, MSH6, MLH1 and PMS2, respectively. Corresponding numbers for the revised Amsterdam criteria were 62%, 48%, 87% and 38%. Similarly, each of the four clinical Bethesda criteria had low sensitivity for identifying MSH6 or PMS2 mutations.Conclusion Amsterdam criteria and each of the Bethesda criteria were inadequate for identifying MSH6 mutation-carrying kindreds. MSH6 mutations may be more common than currently assumed, and the penetrance/expression of MSH6 mutations, as derived from families meeting current clinical criteria, may be misleading. To increase detection rate of MMR mutation carriers, all cancers in the Lynch syndrome tumour spectrum should be subjected to immunohistochemical analysis and/or analysis for microsatellite instability. ER -