Functional Evaluation of p53 and PTEN Gene Mutations in Gliomas
We screened mutations of two major tumor suppressor genes, p53 and PTEN , in 66 human brain tumors using a yeast-based functional assay and cDNA-based direct sequencing, respectively. The frequency of p53 mutations was 28.8% (19 of 66) and was higher in anaplastic astrocytoma (9 of 14, 64.3%,) than...
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Veröffentlicht in: | Clinical cancer research 2000-10, Vol.6 (10), p.3937-3943 |
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Sprache: | eng |
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Zusammenfassung: | We
screened mutations of two major tumor suppressor genes,
p53 and PTEN , in 66 human brain tumors
using a yeast-based functional assay and cDNA-based direct sequencing,
respectively. The frequency of p53 mutations was 28.8%
(19 of 66) and was higher in anaplastic astrocytoma (9 of 14, 64.3%,)
than in glioblastoma multiforme (GBM; 7 of 27, 25.9%,), supporting
previous speculation that there are at least two genetic pathways
leading to GBM, a de novo pathway without
p53 mutation and a “progressive” pathway with
p53 mutation. PTEN mutation was observed
in 8 of 64 tumors (12.5%), mainly GBMs (7 of 26, 26.9%), both with
and without p53 mutation. These results suggest that
mutation of the PTEN gene is a later event than that of
the p53 gene in glioma progression and is associated
with both the genetic pathways. All of the detected PTEN
missense mutations and an in-frame small deletion inactivated PTEN
phosphoinositide phosphatase activity in vitro . Because
the tumors containing PTEN mutations also showed loss of
heterozygosity in the chromosome 10q23 region flanking the
PTEN gene, our data clearly indicate that inactivation
of both PTEN alleles occurs in a subset of high-grade
gliomas, therefore confirming the previous idea that
PTEN acts as a tumor suppressor gene. |
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ISSN: | 1078-0432 1557-3265 |