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      Loss or Somatic Mutations of hMSH2 Occur in Hereditary Nonpolyposis Colorectal Cancers with hMSH2 Germline Mutations

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          Abstract

          Hereditary nonpolyposis colorectal cancer (HNPCC) is a major cancer susceptibility syndrome known to be caused by the inheritance of mutations in DNA mismatch repair genes, such as hMSH2, hMLH1, hPMS1 and hPMS2. To investigate the role of genetic alterations of hMSH2 in HNPCC tumorigenesis, we analyzed 36 Japanese HNPCC kindreds as to hMSH2 germline mutations. Moreover, we also examined somatic mutations of hMSH2 or loss of heterozygosity at or near the hMSH2 locus in the tumors from the hMSH2‐related kindreds. Germline mutations were detected in five HNPCC kindreds (5/36, 14%). Among them, three were nonsense mutations, one was a frameshift mutation and the other was a mutation in an intron where the mutation affected splicing. Loss of heterozygosity in four and somatic mutations in one were detected among the eight tumors with hMSH2 germline mutations. All these alterations were only detected in genomic instability(+) tumors, i.e., not in genomic instability(‐) ones, indicating that mutations of hMSH2 were responsible for at least some of the tumors with genomic instability. These data establish a basis for the presymptomatic diagnosis of HNPCC patients, and constitute further evidence that both DNA mismatch repair genes and tumor suppressor genes may share the same requirement, i.e., two hits are necessary to inactivate the gene function.

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          Mutation and cancer: statistical study of retinoblastoma.

          A Knudson (1971)
          Based upon observations on 48 cases of retinoblastoma and published reports, the hypothesis is developed that retinoblastoma is a cancer caused by two mutational events. In the dominantly inherited form, one mutation is inherited via the germinal cells and the second occurs in somatic cells. In the nonhereditary form, both mutations occur in somatic cells. The second mutation produces an average of three retinoblastomas per individual inheriting the first mutation. Using Poisson statistics, one can calculate that this number (three) can explain the occasional gene carrier who gets no tumor, those who develop only unilateral tumors, and those who develop bilateral tumors, as well as explaining instances of multiple tumors in one eye. This value for the mean number of tumors occurring in genetic carriers may be used to estimate the mutation rate for each mutation. The germinal and somatic rates for the first, and the somatic rate for the second, mutation, are approximately equal. The germinal mutation may arise in some instances from a delayed mutation.
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            Ubiquitous somatic mutations in simple repeated sequences reveal a new mechanism for colonic carcinogenesis.

            Y Ionov, M A Peinado, S Malkhosyan (1993)
            Spontaneous errors in DNA replication have been suggested to play a significant role in neoplastic transformation and to explain the chromosomal alterations seen in cancer cells. A defective replication factor could increase the mutation rate in clonal variants arising during tumour progression, but despite intensive efforts, increases in tumour cell mutation rates have not been unambiguously shown. Here we use an unbiased genomic fingerprinting technique to show that 12 per cent of colorectal carcinomas carry somatic deletions in poly(dA.dT) sequences and other simple repeats. We estimate that cells from these tumours can carry more than 100,000 such mutations. Only tumours with affected poly(dA.dT) sequences carry mutations in the other simple repeats examined, and such mutations can be found in all neoplastic regions of multiple tumours from the same patient, including adenomas. Tumours with these mutations show distinctive genotypic and phenotypic features. We conclude that these mutations reflect a previously undescribed form of carcinogenesis in the colon (predisposition to which may be inherited) mediated by a mutation in a DNA replication factor resulting in reduced fidelity for replication or repair (a 'mutator mutation').
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              Mutation in the DNA mismatch repair gene homologue hMLH1 is associated with hereditary non-polyposis colon cancer.

              C Bronner, S. M. Baker, P T Morrison (1994)
              The human DNA mismatch repair gene homologue hMSH2, on chromosome 2p is involved in hereditary non-polyposis colon cancer (HNPCC). On the basis of linkage data, a second HNPCC locus was assigned to chromosome 3p21-23 (ref. 3). Here we report that a human gene encoding a protein, hMLH1 (human MutL homologue), homologous to the bacterial DNA mismatch repair protein MutL, is located on human chromosome 3p21.3-23. We propose that hMLH1 is the HNPCC gene located on 3p because of the similarity of the hMLH1 gene product to the yeast DNA mismatch repair protein, MLH1, the coincident location of the hMLH1 gene and the HNPCC locus on chromosome 3, and hMLH1 missense mutations in affected individuals from a chromosome 3-linked HNPCC family.
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                Author and article information

                Journal
                Journal ID (nlm-ta): Jpn J Cancer Res
                Journal ID (iso-abbrev): Jpn. J. Cancer Res
                Journal ID (doi): 10.1111/(ISSN)1349-7006a
                Journal ID (publisher-id): CAS
                Title: Japanese Journal of Cancer Research : Gann
                Publisher: Blackwell Publishing Ltd (Oxford, UK )
                ISSN (Print): 0910-5050
                ISSN (Electronic): 1876-4673
                Publication date (Print): March 1996
                Volume: 87
                Issue: 3 ( doiID: 10.1111/cas.1996.87.issue-3 )
                Pages: 279-287
                Affiliations
                [ 1 ]Department of Hygiene and Oncology, Tokyo Medical and Dental University School of Medicine, 1‐5‐45 Yushima, Bunkyo‐ku, Tokyo 113
                [ 2 ]Department of Surgery, Hoshi General Hospital, 2‐1‐16 Daimachi, Koriyama, Fukushima 963
                [ 3 ]Department of Surgery, Yamagata Prefectural Central Hospital, 7‐17 Sakura‐cho, Yamagata, Yamagata 990
                [ 4 ]Department of Surgery, Hamamatsu University School of Medicine, 3600 Handa‐cho, Hamamatsu, Shizuoka 431‐31
                [ 5 ]Department of Radiological Diagnosis, National Cancer Center, 5‐1‐1 Tsukiji, Chuo‐ku, Tokyo 104
                [ 6 ]Department of Surgery, Tokyo Medical and Dental University School of Medicine, 1‐5‐45 Yushinia, Bunkyo‐ku, Tokyo 113
                Author notes
                [*] [* ]To whom all correspondence should be addressed.
                Article
                Publisher ID: CAE279
                DOI: 10.1111/j.1349-7006.1996.tb00218.x
                PMC ID: 5921088
                PubMed ID: 8613431
                SO-VID: 57d496b0-c1fc-446e-8e72-4b442045ba87
                History
                Page count
                References: 35, Pages: 9
                Categories
                Subject: Article
                Custom metadata
                source-schema-version-number 2.0
                cover-date March 1996
                details-of-publishers-convertor Converter:WILEY_ML3GV2_TO_NLMPMC version:4.6.9 mode:remove_FC converted:04.11.2015

                Keywords: hereditary nonpolyposis colorectal cancer,hmsh2,germline mutation,somatic mutation,loss of heterozygosity
                Data availability:
                Keywords: hereditary nonpolyposis colorectal cancer, hmsh2, germline mutation, somatic mutation, loss of heterozygosity

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