Discovery and Validation of a Prostate Cancer Genomic Classifier that Predicts Early Metastasis Following Radical Prostatectomy

Erho, Nicholas; Crisan, Anamaria; Vergara, Ismael A.; Mitra, Anirban P.; Ghadessi, Mercedeh; Buerki, Christine; Bergstralh, Eric J.; Kollmeyer, Thomas M.; Fink, Stephanie; Haddad, Zaid; Zimmermann, B.; Sierocinski, Thomas; Ballman, Karla V.; Triche, Timothy J.; Black, Peter C.; Karnes, R. Jeffrey; Klee, George G.; Davicioni, Elai; Jenkins, Robert B.

doi:10.1371/journal.pone.0066855

Cited by 546 publications

(643 citation statements)

References 69 publications

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“…The TAI showed a strong decreasing trend with Gleason score, in both the TCGA (Fig. 1E) and an independent dataset (18), and similar results were obtained using the grade of LIHC and STAD tumors (SI Appendix, Figs. S10 and S11).…”

Section: Significancesupporting

confidence: 78%

Altered interactions between unicellular and multicellular genes drive hallmarks of transformation in a diverse range of solid tumors

Trigos

Pearson

Papenfuss

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

176

217

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Tumors of distinct tissues of origin and genetic makeup display common hallmark cellular phenotypes, including sustained proliferation, suppression of cell death, and altered metabolism. These phenotypic commonalities have been proposed to stem from disruption of conserved regulatory mechanisms evolved during the transition to multicellularity to control fundamental cellular processes such as growth and replication. Dating the evolutionary emergence of human genes through phylostratigraphy uncovered close association between gene age and expression level in RNA sequencing data from The Cancer Genome Atlas for seven solid cancers. Genes conserved with unicellular organisms were strongly up-regulated, whereas genes of metazoan origin were primarily inactivated. These patterns were most consistent for processes known to be important in cancer, implicating both selection and active regulation during malignant transformation. The coordinated expression of strongly interacting multicellularity and unicellularity processes was lost in tumors. This separation of unicellular and multicellular functions appeared to be mediated by 12 highly connected genes, marking them as important general drivers of tumorigenesis. Our findings suggest common principles closely tied to the evolutionary history of genes underlie convergent changes at the cellular process level across a range of solid cancers. We propose altered activity of genes at the interfaces between multicellular and unicellular regions of human gene regulatory networks activate primitive transcriptional programs, driving common hallmark features of cancer. Manipulation of cross-talk between biological processes of different evolutionary origins may thus present powerful and broadly applicable treatment strategies for cancer.

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Section: Significancesupporting

confidence: 78%

Altered interactions between unicellular and multicellular genes drive hallmarks of transformation in a diverse range of solid tumors

Trigos

Pearson

Papenfuss

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

176

217

View full text Add to dashboard Cite

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“…The normalization and summarization of the microarray samples were done with the Single Channel Array Normalization algorithm with quality control performed as described previously. [16][17][18][19] Gene expression for each gene was calculated using the Affymetrix Core level summaries for annotated genes. Microarray data are available on the NCBI Gene Expression Omnibus as accession numbers GSE46691 (MCI), GSE62116 (MCII) and GSE62667 (CC).…”

Section: Study Design and Tissue Samplesmentioning

confidence: 99%

High-Throughput Transcriptomic Analysis Nominates Proteasomal Genes As Age Specific Biomarkers and Therapeutic Targets in Prostate Cancer

Zhao

Jackson

Kothari

et al. 2015

International Journal of Radiation Oncology*Biology*Physics

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BACKGROUND: Although prostate cancer (PCa) is hypothesized to differ in nature between younger versus older patients, the underlying molecular distinctions are poorly understood. We hypothesized that high-throughput transcriptomic analysis would elucidate biological differences in PCas arising in younger versus older men, and would nominate potential age-specific biomarkers and therapeutic targets. METHODS: The high-density Affymetrix GeneChip platform, encompassing 41 million genomic loci, was utilized to assess gene expression in 1090 radical prostatectomy samples from patients with long-term follow-up. We identified genes associated with metastatic progression by 10 years post-treatment in younger (ageo65) versus older (age ⩾ 65) patients, and ranked these genes by their prognostic value. We performed Gene Set Enrichment Analysis (GSEA) to nominate biological concepts that demonstrated agespecific effects, and validated a target by treating with a clinically available drug in three PCa cell lines derived from younger men. RESULTS: Over 80% of the top 1000 prognostic genes in younger and older men were specific to that age group. GSEA nominated the proteasome pathway as the most differentially prognostic in younger versus older patients. High expression of proteasomal genes conferred worse prognosis in younger but not older men on univariate and multivariate analysis. Bortezomib, a Food and Drug Administration approved proteasome inhibitor, decreased proliferation in three PCa cell lines derived from younger patients. CONCLUSIONS: Our data show significant global differences in prognostic genes between older versus younger men. We nominate proteasomeal gene expression as an age-specific biomarker and potential therapeutic target specifically in younger men. Limitations of our study include clinical differences between cohorts, and increased comorbidities and lower survival in older patients. These intriguing findings suggest that current models of PCa biology do not adequately represent genetic heterogeneity of PCa related to age, and future clinical trials would benefit from stratification based on age.

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“…Both the 17‐gene Oncotype DX and the 31‐gene Prolaris improve risk stratification of patients with high risk of PC recurrence at time of diagnosis (Albala et al ., 2016; Cuzick et al ., 2011; Klein et al ., 2014; Knezevic et al ., 2013; Oderda et al ., 2017) and after radical prostatectomy (RP) (Cooperberg et al ., 2013; Cullen et al ., 2015). The 22‐gene Decipher predicts metastasis following RP (Erho et al ., 2013; Karnes et al ., 2013; Klein et al ., 2016). While these and other biomarkers assist decision making and thus improve patient management, their clinical application requires further validation (Lamy et al ., 2017; Martin, 2016; McGrath et al ., 2016; Patel and Gnanapragasam, 2016; Ross et al ., 2016; Zhuang and Johnson, 2016).…”

Section: Introductionmentioning

confidence: 99%

Construction of a set of novel and robust gene expression signatures predicting prostate cancer recurrence

Jiang

Mei

et al. 2018

Molecular Oncology

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We report here numerous novel genes and multiple new signatures which robustly predict prostate cancer (PC) recurrence. We extracted 696 differentially expressed genes relative to a reported PC signature from the TCGA dataset (n = 492) and built a 15‐gene signature (SigMuc1NW) using Elastic‐net with 10‐fold cross‐validation through analyzing their expressions at 1.5 standard deviation/SD below and 2 SD above a population mean. SigMuc1NW predicts biochemical recurrence (BCR) following surgery with 56.4% sensitivity, 72.6% specificity, and 63.24 median months disease free (MMDF) (P = 1.12e‐12). The prediction accuracy is improved with the use of SigMuc1NW's cutpoint (P = 3e‐15) and is further enhanced (sensitivity 67%, specificity 75.7%, MMDF 45.2, P = 0) when all 15 genes were analyzed through their cutpoints instead of their SDs. These genes individually associate with BCR using either SD or cutpoint as the cutoff points. Eight of 15 genes are individual risk factors after adjusting for age at diagnosis, Gleason score, surgical margin, and tumor stage. Eleven of 15 genes are novel to PC. SigMuc1NW discriminates BCR with time‐dependent AUC (tAUC) values of 76.6% at 11.5 months (76.6%–11.5 m), 73.8%‐22.3 m, 78.5%‐32.1 m, and 76.4%–48.4 m. SigMuc1NW is correlated with adverse features of PC, high Gleason scores (odds ratio/OR 1.48, P < 2e‐16), and advanced tumor stages (OR 1.33, P = 4.37e‐13). SigMuc1NW remains an independent risk factor of BCR (HR 2.44, 95% CI 1.53–3.87, P = 1.62e‐4) after adjusting for age at diagnosis, Gleason score, surgical margin, and tumor stage. In an independent PC (MSKCC) cohort (n = 140), these 15 genes were altered in PC vs normal tissue, metastatic PCs vs primary PCs, and recurrent PCs vs nonrecurrent PCs. Importantly, a 10‐gene subsignature SigMuc1NW1 predicts BCR in MSKCC (P = 3.11e‐15) and TCGA (P = 3.13e‐12); SigMuc1NW1 discriminates BCR at 18.4 m with tAUC as 82.5%. Collectively, our analyses support SigMuc1NW as a novel and robust signature in predicting BCR of PC.

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Discovery and Validation of a Prostate Cancer Genomic Classifier that Predicts Early Metastasis Following Radical Prostatectomy

Cited by 546 publications

References 69 publications

Altered interactions between unicellular and multicellular genes drive hallmarks of transformation in a diverse range of solid tumors

Altered interactions between unicellular and multicellular genes drive hallmarks of transformation in a diverse range of solid tumors

High-Throughput Transcriptomic Analysis Nominates Proteasomal Genes As Age Specific Biomarkers and Therapeutic Targets in Prostate Cancer

Construction of a set of novel and robust gene expression signatures predicting prostate cancer recurrence

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