TRIM24 as an independent prognostic biomarker for prostate cancer

•Risk stratification of prostate cancer urgently needs independent prognostic biomarkers.•Expression of TRIM24 on primary tumors predicts disease recurrence after surgery.•The prognostic value of TRIM24 is independent from established parameters.•TRIM24 is validated as prognostic marker on biopsies...

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Bibliographic Details
Published in:Urologic oncology 2019-09, Vol.37 (9), p.576.e1-576.e10
Main Authors: Offermann, Anne, Roth, Doris, Hupe, Marie Christine, Hohensteiner, Silke, Becker, Finn, Joerg, Vincent, Carlsson, Jessica, Kuempers, Christiane, Ribbat-Idel, Julika, Tharun, Lars, Sailer, Verena, Kirfel, Jutta, Svensson, Maria, Andren, Ove, Lubczyk, Verena, Kuefer, Rainer, Merseburger, Axel S., Perner, Sven
Format: Article
Language:English
Subjects:
Biomarker
Disease recurrence
Immunohistochemical test
Prostate cancer
TRIM24
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Summary:•Risk stratification of prostate cancer urgently needs independent prognostic biomarkers.•Expression of TRIM24 on primary tumors predicts disease recurrence after surgery.•The prognostic value of TRIM24 is independent from established parameters.•TRIM24 is validated as prognostic marker on biopsies from time of initial diagnosis. [Display omitted] Simply applicable biomarkers for prostate cancer patients predicting the clinical course are urgently needed. Recently, TRIM24 has been identified to promote androgen receptor signaling and to correlate with an aggressive prostate cancer phenotype. Based on these data, we proofed TRIM24 as a prognostic biomarker for risk stratification. We performed TRIM24 immunohistochemistry on 2 independent cohorts including a total of 806 primary tumors, 26 locally advanced/recurrent tumors, 30 lymph node metastases, 30 distant metastases, and 129 benign prostatic samples from 497 patients as well as on 246 prostate needle biopsies. Expression data were correlated with clinic-pathological data including biochemical recurrence-free survival (bRFS) as endpoint. Benign samples show no or low TRIM24 expression in 94%, while tumor tissues demonstrate significant higher levels. Strongest expression is observed in advanced and metastatic tumors. In multivariate analyses, TRIM24 up-regulation on radical prostatectomy specimens correlates with shorter bRFS independent of other prognostic parameters. 5-(10-) year bRFS rates for TRIM24 negative, low, medium and high expressing tumors are 93.1(93.1)%, 75.4(68.5)%, 54.9(47.5)% and 43.1(32.3)%, respectively. Of interest, tumors diagnosed as indolent disease, TRIM24 expression stratifies patients into specific risk groups. Increased TRIM24 expression associates with higher grade group, positive nodal status and extraprostatic tumor growth. TRIM24 assessment on prostate needle biopsies taken prior to treatment decision at time of initial diagnosis significantly correlates with recurrence after surgery. Using 2 large independent radical prostatectomy specimen cohorts, we found that TRIM24 expression predicts patients’ risk to develop disease recurrence with high accuracy and independent from other established biomarkers. Further, this is the first study exploring TRIM24 expression on prostate needle biopsies which represents the clinically relevant tissue type on which biomarkers guide treatment decisions. Thus, we strongly suggest introducing TRIM24 evaluation in prostate needle biopsies in
ISSN:1078-1439
1873-2496
1873-2496
DOI:10.1016/j.urolonc.2019.05.006