Cancer Risk Associated with Germline DNA Mismatch Repair Gene Mutations

The autosomal dominant syndrome of Hereditary Nonpolyposis Colorectal Cancer (HNPCC) is due to germline DNA mismatch repair gene mutations in most cases. However, the penetrance of such mutations outwith classical HNPCC kindreds is unknown because families studied to date have been specifically sele...

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Bibliographic Details
Published in:Human molecular genetics 1997-01, Vol.6 (1), p.105-110
Main Authors: Dunlop, Malcolm G., Farrington, Susan M., Carothers, Andrew D., Wyllie, Andrew H., Sharp, Linda, Burn, John, Liu, Bo, Kinzler, Kenneth W., Vogelstein, Bert
Format: Article
Language:English
Subjects:
Biological and medical sciences
Colorectal Neoplasms, Hereditary Nonpolyposis - genetics
DNA Repair
Gastroenterology. Liver. Pancreas. Abdomen
Germ Cells
Heterozygote
Humans
Medical sciences
Mutagenesis
Pedigree
Risk Factors
Stomach. Duodenum. Small intestine. Colon. Rectum. Anus
Tumors
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Summary:The autosomal dominant syndrome of Hereditary Nonpolyposis Colorectal Cancer (HNPCC) is due to germline DNA mismatch repair gene mutations in most cases. However, the penetrance of such mutations outwith classical HNPCC kindreds is unknown because families studied to date have been specifically selected for research purposes. Using a population-based strategy, we have calculated the lifetime cancer risk associated with germline DNA mismatch repair gene mutations, irrespective of their family history. We identified 67 gene carriers whose risk to age 70 for all cancers was 91% for males and 69% for females. The risk of developing colorectal cancer was significantly greater for males than for females (74% versus 30%, P = 0.006). The risk of uterine cancer (42%) exceeded that for colorectal cancer in females, emphasising the need for uterine screening. Our findings give further insight into the biological effect of defective DNA mismatch repair. We have demonstrated a systematic approach to identifying individuals at high risk of cancer but who may not be part of classical HNPCC families. The risk estimates derived from these analyses provide a rational basis on which to guide genetic counselling and to tailor clinical surveillance.
ISSN:0964-6906
1460-2083
1460-2083
DOI:10.1093/hmg/6.1.105