Janos Papp1, Marietta E Kovacs, Edith Olah. 1. Department Molecular Genetics, National Institute of Oncology, Rath Gy. u. 7-9, H-1122 Budapest, Hungary.
Abstract
AIM: To analyze the prevalence of germline MLH1 and MSH2 gene mutations and evaluate the clinical characteristics of Hungarian hereditary non-polyposis colorectal cancer (HNPCC) families. METHODS: Thirty-six kindreds were tested for mutations using conformation sensitive gel electrophoreses, direct sequencing and also screening for genomic rearrangements applying multiplex ligation-dependent probe amplification (MLPA). RESULTS: Eighteen germline mutations (50%) were identified, 9 in MLH1 and 9 in MSH2. Sixteen of these sequence alterations were considered pathogenic, the remaining two were non-conservative missense alterations occurring at highly conserved functional motifs. The majority of the definite pathogenic mutations (81%, 13/16) were found in families fulfilling the stringent Amsterdam I/II criteria, including three rearrangements revealed by MLPA (two in MSH2 and one in MLH1). However, in three out of sixteen HNPCC-suspected families (19%), a disease-causing alteration could be revealed. Furthermore, nine mutations described here are novel, and none of the sequence changes were found in more than one family. CONCLUSION: Our study describes for the first time the prevalence and spectrum of germline mismatch repair gene mutations in Hungarian HNPCC and suspected-HNPCC families. The results presented here suggest that clinical selection criteria should be relaxed and detection of genomic rearrangements should be included in genetic screening in this population.
AIM: To analyze the prevalence of germline MLH1 and MSH2 gene mutations and evaluate the clinical characteristics of Hungarian hereditary non-polyposis colorectal cancer (HNPCC) families. METHODS: Thirty-six kindreds were tested for mutations using conformation sensitive gel electrophoreses, direct sequencing and also screening for genomic rearrangements applying multiplex ligation-dependent probe amplification (MLPA). RESULTS: Eighteen germline mutations (50%) were identified, 9 in MLH1 and 9 in MSH2. Sixteen of these sequence alterations were considered pathogenic, the remaining two were non-conservative missense alterations occurring at highly conserved functional motifs. The majority of the definite pathogenic mutations (81%, 13/16) were found in families fulfilling the stringent Amsterdam I/II criteria, including three rearrangements revealed by MLPA (two in MSH2 and one in MLH1). However, in three out of sixteen HNPCC-suspected families (19%), a disease-causing alteration could be revealed. Furthermore, nine mutations described here are novel, and none of the sequence changes were found in more than one family. CONCLUSION: Our study describes for the first time the prevalence and spectrum of germline mismatch repair gene mutations in Hungarian HNPCC and suspected-HNPCC families. The results presented here suggest that clinical selection criteria should be relaxed and detection of genomic rearrangements should be included in genetic screening in this population.
Authors: Jan P Schouten; Cathal J McElgunn; Raymond Waaijer; Danny Zwijnenburg; Filip Diepvens; Gerard Pals Journal: Nucleic Acids Res Date: 2002-06-15 Impact factor: 16.971
Authors: G Kurzawski; J Suchy; J Kładny; K Safranow; A Jakubowska; P Elsakov; V Kucinskas; J Gardovski; A Irmejs; H Sibul; T Huzarski; T Byrski; T Debniak; C Cybulski; J Gronwald; O Oszurek; J Clark; S Góźdź; S Niepsuj; R Słomski; A Pławski; A Łacka-Wojciechowska; A Rozmiarek; Ł Fiszer-Maliszewska; M Bebenek; D Sorokin; M Stawicka; D Godlewski; P Richter; I Brozek; B Wysocka; A Jawień; Z Banaszkiewicz; J Kowalczyk; D Czudowska; P E Goretzki; G Moeslein; J Lubiński Journal: J Med Genet Date: 2002-10 Impact factor: 6.318
Authors: T Liu; P Tannergård; P Hackman; C Rubio; U Kressner; G Lindmark; D Hellgren; B Lambert; A Lindblom Journal: Hum Genet Date: 1999-11 Impact factor: 4.132
Authors: Trinidad Caldes; Javier Godino; Miguel de la Hoya; Iciar Garcia Carbonero; Pedro Perez Segura; Charis Eng; Manuel Benito; Eduardo Diaz-Rubio Journal: Int J Cancer Date: 2002-04-10 Impact factor: 7.396
Authors: Miklós Tanyi; Judit Olasz; Janos L Tanyi; László Tóth; Péter Antal-Szalmás; Tamás Bubán; Csilla András; Hilda Urbancsek; Zoltán Garami; Orsolya Csuka; László Damjanovich Journal: Fam Cancer Date: 2012-09 Impact factor: 2.375