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Analysis of p53 tumor
suppressor gene in families with multiple glioma patients
Paunu N, Syrjakoski K,
Sankila R, Simola KO, Helen P, Niemela M, Matikainen M, Isola J, Haapasalo H
Department of Pathology, Tampere University Hospital and
University of Tampere, Finland. niina.paunu@uta.fi
The high incidence of gliomas in Li-Fraumeni families and the high
frequency of somatic p53 mutations in sporadic glial tumors have raised the
possibility that germline p53 mutations could play an important role in familial
aggregation of gliomas.
In the present study, 18 families with two or more
gliomas were screened for germline p53 mutation.
The families were identified
through questionnaires sent to 369 consecutive glioma patients operated at
Tampere University Hospital during 1983-1994.
In these families, a family
history of cancer was verified through the Finnish Cancer Registry.
Interestingly, the questionnaires reveled only 15 of 57 cancers (index gliomas
excluded) retrieved through the Cancer Registry.
None of the 18 families
fufilled the criteria for classic Li-Fraumeni syndrome.
Immunostaining analysis
of p53 protein accumulation suggested that alterations of the p53 gene are as
common in familial as in sporadic gliomas.
Sequencing analysis of exons 4-10 of
the p53 gene revealed no germline mutations in any of the 18 families.
Thus,
although occasional glioma families carrying germline p53 mutations have been
identified in earlier studies, systematic evaluation of familial glioma patients
suggests that the p53 gene is not a common susceptibility gene in case of
familial gliomas.
The p53 tumor suppressor gene seems to have a similar role in
the tumorigenesis of most familial and sporadic gliomas.
PMID: 11859970, UI: 21848706
Source: http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=pubmed&dopt=Abstract&list_uids=11859970
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