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Gut 2000;47:262-267 doi:10.1136/gut.47.2.262
  • Cancer

The E-cadherin gene (CDH1) variants T340A and L599V in gastric and colorectal cancer patients in Korea

  1. H C Kima,
  2. J M D Wheelera,
  3. J C Kimb,
  4. M Ilyasa,
  5. N E Becka,
  6. B S Kimb,
  7. K C Parkb,
  8. W F Bodmera
  1. aCancer and Immunogenetics Laboratory, Imperial Cancer Research Fund, Institute of Molecular Medicine, John Radcliffe Hospital, Oxford OX3 9DS, UK, bDepartment of Surgery, University of Ulsan College of Medicine and Asan Medical Centre 388–1, Seoul, Korea
  1. J M D Wheeler.
  • Accepted 1 February 2000

Abstract

INTRODUCTION Germline mutations in E-cadherin (CDH1) have been reported in families with early onset, diffuse gastric cancer. More recently, mutations in CDH1 have been described in colorectal cancer cell lines.

AIMS We have investigated if germline mutations in CDH1occur among different groups of Korean gastric and colorectal cancer patients, with and without a positive family history.

METHODS We studied 131 patients and 168 normal controls (88 Korean and 80 non-Korean). Patients were divided into five groups: group I, 20 gastric cancer patients with a family history; group II, 26 colorectal cancer patients with a family history of gastric cancer (those from familial adenomatous polyposis (FAP) and hereditary non-polyposis colorectal cancer (HNPCC) kindred were excluded); group III, 16 HNPCC patients without identified germline mutations inhMLH1 and hMSH2; group IV, 35 gastric cancer patients without a family history; and group V, 34 colorectal cancer patients without a family history. Polymerase chain reaction, single strand conformational polymorphism analysis, direct sequencing, and genotyping for identified variants were performed.

RESULTS Several germline changes in CDH1 were found. In addition to previously described polymorphisms, we found three novel changes, two of which were missense changes (T340A and L599V). T340A was present in one patient in group III and one in group V. L599V was present in one patient in group II, in two in group III, and in one in group IV. T340A was not found in normal controls while L599V was present in two of 88 Korean controls. Patients with these variants may appear to have a tendency to early onset cancer with a positive family history, although differences in frequencies did not reach statistical significance. Genotyping results suggest that these variants might have a common origin, particularly T340A.

CONCLUSION We have described two new missense germline variants inCDH1 in various groups of Korean gastrointestinal cancer patients. Further work is required to assess if these variants increase the risk of gastrointestinal cancer.

Footnotes

  • Abbreviations used in this paper:
    HNPCC
    hereditary non-polyposis colorectal cancer
    FAP
    familial adenomatous polyposis
    APC
    adenomatous polyposis coli

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