An analysis of a multiple biomarker panel to better predict prostate cancer metastasis after radical prostatectomy

Zhang, Alison; Chiam, Karen; Haupt, Ygal; Fox, Stephen B.; Birch, Simone; Tilley, Wayne D.; Butler, Lisa M.; Knudsen, Karen E.; Comstock, Clay E.S.; Rasiah, K.; Grogan, Judith; Mahon, Kate; Bianco‐Miotto, Tina; Ricciardelli, Carmela; Böhm, Maret; Henshall, Susan M.; Delprado, Warick; Stricker, Phillip D.; Horvath, Lisa G.; Kench, James G.

doi:10.1002/ijc.31906

Cited by 15 publications

(12 citation statements)

References 60 publications

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“… 10 Recent work from our own group has shown that markers clearly associated with biochemical recurrence do not necessarily translate into markers of MR with more mature follow-up. 11 In this cohort, p53 nuclear accumulation correlates with biochemical recurrence after radical prostatectomy (RP) as described by our group more than 15 years ago. 12 With longer follow-up, we aimed to examine whether p53 could also predict MR and PC specific survival.…”

Section: Introductionmentioning

confidence: 59%

“…Work from our group and others has shown that assessing p53 mutations on IHC from tissue microarrays (TMA) has not delivered the same results. 11 While TMA analysis is convenient and with appropriate sampling technique is suitable for most prostate cancer biomarkers, 21 our study has shown that p53 is an unusual biomarker that requires analysis of whole tissue sections and may be dismissed by the TMA method. The prognostic significance of the ‘clustering’ of p53-positive tumour nuclei is particularly relevant to the method of analysis.…”

Section: Discussionmentioning

confidence: 89%

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p53 nuclear accumulation as an early indicator of lethal prostate cancer

et al. 2019

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Background After radical prostatectomy (RP) for prostate cancer (PC), p53 alterations predict biochemical relapse (BCR), however, recent evidence suggests that metastatic relapse (MR) not BCR is a surrogate for PC specific mortality (PCSM). This updated analysis of a previously published study investigated the association between p53 aberrations, MR and PCSM in men with localised PC. Methods Two hundred and seventy-one men with localised PC treated with RP were included. RP specimens stained for p53 by immunohistochemistry were scored as (a) percentage of p53-positive tumour nuclei; and (b) clustering, where ≥12 p53-positive cells within a ×200 power field was deemed ‘cluster positive’. Associations between p53 status and clinical outcomes (BCR, MR and PCSM) were evaluated. Results Increasing percentage of p53-positive nuclei was significantly associated with shorter time to BCR, MR and PCSM (All p < 0.001). Half of the patients were p53 cluster positive. p53 cluster positivity was significantly associated with poorer outcomes at all clinical endpoints (BCR: HR 2.0, 95% CI 1.51–2.65, p < 0.001; MR: HR 4.1, 95% CI 2.02–8.14, p < 0.001; PCSM: HR 12.2, 95% CI 1.6–93; p = 0.016). These associations were independent of other established prognostic variables. Conclusions p53 aberrations in radical prostatectomy tissue predict clinically relevant endpoints of MR and PCSM.

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Section: Introductionmentioning

confidence: 59%

Section: Discussionmentioning

confidence: 89%

p53 nuclear accumulation as an early indicator of lethal prostate cancer

et al. 2019

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“…While this may reflect limitations in the sample size of our cohorts, it also raises the possibility that lipidomic profiling may provide independent information regarding tumor biology and prognosis. Moreover, the associations we detected between lipid profiles and the TMPRSS2-ERG molecular subtype and Ki67 proliferative index are interesting observations that warrant further investigation in larger independent tissue cohorts, particularly in light of our recent report of Ki67 status in localized prostate cancer being a significant predictive biomarker of subsequent metastatic relapse(21).Despite differences in the breadth and scope of lipid classes measured, certain key cancerrelated changes in PL profile reported here support the findings of previous imaging-based studies, notably for altered abundance and/or elongation of PC and PI-based lipids and ceramides (reviewed in (2,22)). While the functional consequences of individual lipid changes remain to be elucidated, PI lipids are of fundamental importance in cancer cells as they form the membrane scaffold for kinase and phosphatase activity that supports oncogenic signaling.…”

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confidence: 58%

Lipidomic profiling of clinical prostate cancer reveals targetable alterations in membrane lipid composition

Butler

Mah

Machiels

et al. 2020

Preprint

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Dysregulated lipid metabolism is a prominent feature of prostate cancer that is driven by androgen receptor (AR) signaling. Herein, we used quantitative mass spectrometry to define the "lipidome" in prostate tumors with matched benign tissues (n=21), independent tissues (n=47), and primary prostate explants cultured with a clinical AR antagonist, enzalutamide (n=43). Significant differences in lipid composition were evident and spatially visualized in tumors compared to matched benign samples. Notably, tumors featured higher proportions of monounsaturated lipids overall and elongated fatty acid chains in phosphatidylinositol and phosphatidylserine lipids. Significant associations between lipid profile and malignancy were detected, and PL composition was characteristically altered in patient tissues that responded to AR inhibition. Importantly, targeting of tumor-related lipid features, via inhibition of acetyl CoA carboxylase 1, significantly reduced cellular proliferation in tissue explants (n=13). This first characterization of the prostate cancer lipidome in clinical tissues revealed enhanced fatty acid synthesis, elongation and desaturation as tumor-defining features, with potential for therapeutic targeting.

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“…Importantly, the clinical outcome most often studied is BCR, defined by an increase in serum PSA levels post-RP. However, there is increasing evidence that BCR is not a sufficient indicator of progression to aggressive lethal disease, with metastatic relapse instead being the clinically relevant endpoint for predicting survival [ 72 , 73 ]. This requires long-term follow-up (≥15 years) for metastatic relapse and PCa death to manifest [ 16 ], which many study populations lack, thus reducing their ability to fully evaluate and assess molecular biomarkers of PCa prognosis.…”

Section: Current State Of Prognostic Methylated Biomarkersmentioning

confidence: 99%

Advances in Prognostic Methylation Biomarkers for Prostate Cancer

Lam

Clark

Stirzaker

et al. 2020

Cancers

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There is a major clinical need for accurate biomarkers for prostate cancer prognosis, to better inform treatment strategies and disease monitoring. Current clinically recognised prognostic factors, including prostate-specific antigen (PSA) levels, lack sensitivity and specificity in distinguishing aggressive from indolent disease, particularly in patients with localised intermediate grade prostate cancer. There has therefore been a major focus on identifying molecular biomarkers that can add prognostic value to existing markers, including investigation of DNA methylation, which has a known role in tumorigenesis. In this review, we will provide a comprehensive overview of the current state of DNA methylation biomarker studies in prostate cancer prognosis, and highlight the advances that have been made in this field. We cover the numerous studies into well-established candidate genes, and explore the technological transition that has enabled hypothesis-free genome-wide studies and the subsequent discovery of novel prognostic genes.

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An analysis of a multiple biomarker panel to better predict prostate cancer metastasis after radical prostatectomy

Cited by 15 publications

References 60 publications

p53 nuclear accumulation as an early indicator of lethal prostate cancer

p53 nuclear accumulation as an early indicator of lethal prostate cancer

Lipidomic profiling of clinical prostate cancer reveals targetable alterations in membrane lipid composition

Advances in Prognostic Methylation Biomarkers for Prostate Cancer

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