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Cancer risk in families with hereditary nonpolyposis colorectal cancer diagnosed by mutation analysis

被引:602
作者
Vasen, HFA
Wijnen, JT
Menko, FH
Kleibeuker, JH
Taal, BG
Griffioen, G
Nagengast, FM
MeijersHeijboer, EH
Bertario, L
Varesco, L
Bisgaard, ML
Mohr, J
Fodde, R
Khan, PM
机构
[1] STATE UNIV LEIDEN HOSP,DEPT GASTROENTEROL,LEIDEN,NETHERLANDS
[2] UNIV UTRECHT HOSP,DEPT INTERNAL MED,UTRECHT,NETHERLANDS
[3] LEIDEN UNIV,DEPT HUMAN GENET,CTR MED GENET,2300 RA LEIDEN,NETHERLANDS
[4] FREE UNIV AMSTERDAM HOSP,DEPT CLIN GENET,AMSTERDAM,NETHERLANDS
[5] UNIV GRONINGEN HOSP,DEPT GASTROENTEROL,GRONINGEN,NETHERLANDS
[6] NETHERLANDS CANC INST,DEPT GASTROENTEROL,AMSTERDAM,NETHERLANDS
[7] UNIV NIJMEGEN HOSP,DEPT GASTROENTEROL,6500 HB NIJMEGEN,NETHERLANDS
[8] ERASMUS UNIV ROTTERDAM,DEPT CLIN GENET,3000 DR ROTTERDAM,NETHERLANDS
[9] IST NAZL STUDIO & CURA TUMORI,I-20133 MILAN,ITALY
[10] IST NAZL RIC CANC,CHEM CANCEROGENESIS LAB,I-16132 GENOA,ITALY
[11] UNIV COPENHAGEN,NATL HOSP,COPENHAGEN,DENMARK
[12] DANISH HEREDITARY NONPOLYPOSIS COLORECTAL CANC RE,COPENHAGEN,DENMARK
[13] UNIV COPENHAGEN,PANUM INST,INST MED BIOCHEM & GENET,DK-2200 COPENHAGEN,DENMARK
来源
GASTROENTEROLOGY | 1996年 / 110卷 / 04期
关键词
D O I
10.1053/gast.1996.v110.pm8612988
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
Background & Aims: Hereditary nonpolyposis colorectal cancer is characterized by early-onset colorectal cancer and the occurrence of various other cancers, The recent isolation of four mismatch repair genes responsible for hereditary nonpolyposis colorectal cancer allows for the identification of carriers within affected families. The purpose of this study was to assess the age-specific cancer risk in a large series of gene carriers, Methods: Thirty-four families were studied by mutation analysis. In 19 of these families, pathogenic mutations were found at hMSH2 or hMLH1. Of 382 relatives, 124 had a mutation in hMLH1 and 86 in hMSH2, Results: The lifetime risk of colorectal cancer was the same in both groups of gene carriers (80%), The risk of endometrial cancer was greater in hMSH2 gene carriers compared with hMLH1 gene carriers (61% vs. 42%), but the difference was not statistically significant. A very high relative risk of cancer of the small bowel (relative risk of >100) was observed in carriers of either gene, Only the carriers of hMSH2 mutations had a significantly increased relative risk of cancer of the urinary tract (kidney and ureter) (relative risk of 75.3), stomach (relative risk of 19.3), and ovaries (relative risk of 8.0). Conclusions: This study provides estimates of cancer risk that may contribute to the appropriate management of gene carriers within families with hereditary nonpolyposisis colorectal cancer.
引用
收藏
页码:1020 / 1027
页数:8
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