Estrogen receptors α and β and aromatase as independent predictors for prostate cancer outcome
Permanent link
https://hdl.handle.net/10037/10365Date
2016-09-09Type
Journal articleTidsskriftartikkel
Peer reviewed
Author
Grindstad, Thea; Skjefstad, Kaja; Andersen, Sigve; Ness, Nora; Nordby, Yngve; Al-Saad, Samer; Fismen, Silje; Dønnem, Tom; Rakaee, Mehrdad; Busund, Lill-Tove; Bremnes, Roy M.; Richardsen, ElinAbstract
Androgens are considered important in normal prostate physiology and prostate cancer (PCa)
pathogenesis. However, androgen-targeted treatment preventing PCa recurrence is still lacking.
This indicates additional mediators contributing to cancer development. We sought to determine the
prognostic significance of estrogen receptors, ERα and -β, and the aromatase enzyme in PCa. Tissue
microarrays were created from 535 PCa patients treated with radical prostatectomy. Expression of ERα,
ERβ and aromatase were evaluated using immunohistochemistry. Representative tumor epithelial (TE)
and tumor stromal (TS) areas were investigated separately. Survival analyses were used to evaluate
the markers correlation to PCa outcome. In univariate analyses, ERα in TS was associated with delayed
time to clinical failure (CF) (p = 0.042) and PCa death (p = 0.019), while ERβ was associated with reduced
time to biochemical failure (BF) (p = 0.002). Aromatase in TS and TE was associated with increased time
to BF and CF respectively (p = 0.016, p = 0.046). Multivariate analyses supported these observations,
indicating an independent prognostic impact of all markers. When stratifying the analysis according to
different surgical centers the results were unchanged. In conclusion, significant prognostic roles of ERα,
ERβ and aromatase were discovered in the in PCa specimens of our large multicenter cohort.
Description
Published version. Source at http://dx.doi.org/10.1038/srep33114
Publisher
Nature Publishing GroupCitation
Grindstad, T. et al. Estrogen receptors α and β and aromatase as independent predictors for prostate cancer outcome. Sci. Rep. 6, 33114; doi: 10.1038/srep33114 (2016).Metadata
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