Literature DB >> 1682292

Frequent loss of heterozygosity at the MCC locus on chromosome 5q21-22 in sporadic colorectal carcinomas.

Y Miki1, I Nishisho, Y Miyoshi, A Horii, H Ando, T Nakajima, J Utsunomiya, Y Nakamura.   

Abstract

Recent studies have identified a gene on chromosome 5q, designated MCC (mutated in colorectal cancers), as a candidate for the putative colorectal tumor suppressor gene that is located at 5q21. We examined loss of heterozygosity (LOH) at the MCC locus and its vicinity in sporadic colorectal carcinomas, using 12 RFLP (restriction fragment length polymorphism) markers. One clone, L5.71, had been used to identify the MCC gene; all 12 markers also had tight linkage to the gene responsible for adenomatous polyposis coli. All 40 cases studied were informative with at least one marker, and 22 of them (55%) showed LOH at one or more loci. LOH in the tumors was more frequent in the immediate vicinity of L5.71 than in distant parts of the chromosome, and a common region of deletion was detected between markers L5.62 and 15A6. In one case, alleles were retained at L5.71 and at loci proximal to L5.71, but alleles were lost at loci distal to L5.71. In another case, both alleles were retained at L5.71 but alleles were lost at loci proximal and distal to L5.71. These results support the conclusion that a tumor suppressor gene for colorectal carcinoma is located within or around locus L5.71.

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Year:  1991        PMID: 1682292      PMCID: PMC5918609          DOI: 10.1111/j.1349-7006.1991.tb01935.x

Source DB:  PubMed          Journal:  Jpn J Cancer Res        ISSN: 0910-5050


  20 in total

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3.  Localization of the gene for familial adenomatous polyposis on chromosome 5.

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5.  The gene for familial polyposis coli maps to the long arm of chromosome 5.

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6.  Identification of a chromosome 18q gene that is altered in colorectal cancers.

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8.  Genetic changes and histopathological types in colorectal tumors from patients with familial adenomatous polyposis.

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10.  High frequency of APC loss in sporadic colorectal carcinoma due to breaks clustered in 5q21-22.

Authors:  P G Ashton-Rickardt; M G Dunlop; Y Nakamura; R G Morris; C A Purdie; C M Steel; H J Evans; C C Bird; A H Wyllie
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Review 3.  Development and progression of colorectal neoplasia.

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6.  Allele loss from 5q21 (APC/MCC) and 18q21 (DCC) and DCC mRNA expression in breast cancer.

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Review 7.  Involvement of DNA damage response pathways in hepatocellular carcinoma.

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8.  Contribution of APC and MUTYH mutations to familial adenomatous polyposis susceptibility in Hungary.

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9.  Insertion/deletion polymorphism and other restriction fragment length polymorphisms in the MCC gene.

Authors:  Y Miyoshi; I Nishisho; Y Miki; T Mori; K W Kinzler; B Vogelstein; Y Nakamura
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  9 in total

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