Fluorescence in situ hybridization study shows association of PTEN deletion with ERG rearrangement during prostate cancer progression
The link between ERG rearrangement and PTEN (phosphatase and tensin homolog deleted on chromosome 10) deletion is unclear in prostate cancer progression. Using fluorescence in situ hybridization, we systematically validated the frequency and distribution of ERG and PTEN aberrations in a cohort of 73...
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Veröffentlicht in: | Modern pathology 2009-08, Vol.22 (8), p.1083-1093 |
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Zusammenfassung: | The link between
ERG
rearrangement and
PTEN
(phosphatase and tensin homolog deleted on chromosome 10) deletion is unclear in prostate cancer progression. Using fluorescence
in situ
hybridization, we systematically validated the frequency and distribution of
ERG
and
PTEN
aberrations in a cohort of 73 benign prostate tissues, 59 high-grade prostatic intraepithelial neoplasia (HGPIN) foci, 281 localized prostate cancer and 47 androgen-independent metastatic prostate cancer patients. Overall,
ERG
rearrangement was present in 15% (5/33) of HGPIN, 45% (121/267) of localized cancers and 35% (15/43) of metastases. By contrast,
PTEN
deletion was identified in 9% (3/33) of HGPIN, 17% (42/251) of localized cancers and 54% (22/41) of metastases, of which 0%, 40% (17/42) and 45% (10/22) were homozygous, respectively. Concomitance of
ERG
rearrangement and
PTEN
deletion was observed in a subset of HGPIN. Significantly, association between
PTEN
deletion and
ERG
rearrangement was present both in localized cancers (
P
=0.0008) and metastases (
P
=0.02). Further, immunohistochemistry revealed significant correlation of decreased PTEN protein expression with
PTEN
genomic deletion both in localized and metastatic cancer. Of note,
ERG
aberration, but not
PTEN
deletion, was consistently identical both in localized cancer and adjacent HGPIN. Similarly, whereas all metastases (41/41, 100%) shared the same
ERG
status across multiple sites from the same patient, 5% (2/41) of cases showed discordance for
PTEN
deletion status across multiple sites. Collectively, our data support
PTEN
deletion as a late genetic event in human prostate cancer, presumably a ‘second hit’ after
ERG
rearrangement.
PTEN
deletion and
ERG
rearrangement may cooperate, but contribute at different stages, in prostate cancer progression. |
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ISSN: | 0893-3952 1530-0285 |
DOI: | 10.1038/modpathol.2009.69 |