Comprehensive Molecular Characterization of Muscle-Invasive Bladder Cancer

Robertson, A. Gordon; Kim, Jaegil; Al‐Ahmadie, Hikmat; Bellmunt, Joaquim; Guo, Guangwu; Cherniack, Andrew D.; Hinoue, Toshinori; Laird, Peter W.; Hoadley, Katherine A.; Akbani, Rehan; Castro, Mauro A. A.; Gibb, Ewan A.; Kanchi, Rupa S.; Gordenin, Dmitry A.; Shukla, Sachet A.; Sanchez‐Vega, Francisco; Hansel, Donna E.; Czerniak, Bogdan; Reuter, Victor E.; Su, Xiaoping; Carvalho, Benílton de Sá; Chagas, Vinicius S.; Mungall, Karen; Sadeghi, Sara; Pedamallu, Chandra Sekhar; Lu, Yiling; Klimczak, Leszek J.; Zhang, Jiexin; Choo, Caleb; Ojesina, Akinyemi I.; Bullman, Susan; Leraas, Kristen; Lichtenberg, Tara M.; Wu, Catherine J.; Schultz, Nicholaus; Getz, Gad; Meyerson, Matthew; Mills, Gordon B.; McConkey, David J.; Albert, Monique; Alexopoulou, Iakovina; Ally, Adrian; Antic, Tatjana; Aron, Manju; Balasundaram, Miruna; Bartlett, John M.S.; Baylin, Stephen B.; Beaver, Allison; Birol, İnanç; Boice, Lori; Bootwalla, Moiz S.; Bowen, Jay; Bowlby, Reanne; Brooks, Denise; Broom, Bradley M.; Bshara, Wiam; Burks, Eric; Cárcano, Flavio Mavignier; Carlsen, Rebecca; Carvalho, André Lopes; Castle, Eric; Castro, Patricia; Catto, James W.F.; Chesla, David; Chuah, Eric; Chudamani, Sudha; Cortessis, Victoria K.; Cottingham, Sandra; Crain, Daniel; Curley, Erin; Daneshmand, Siamak; Demchok, John A.; Dhalla, Noreen; Djaladat, Hooman; Eckman, John; Egea, Sophie C.; Engel, Jay; Felau, Ina; Ferguson, Martin L.; Gardner, Johanna; Gastier‐Foster, Julie M.; Gerken, Mark; Gomez‐Fernandez, Carmen; Harr, Jodi; Hartmann, Arndt; Herbert, Lynn M.; Ho, Thai H.; Holt, Robert A.; Hutter, Carolyn M.; Jones, Steven J.M.; Jordà, Mercè; Kahnoski, Richard J.; Kasaian, Katayoon; Kwiatkowski, David J.; Lai, Phillip H.; Lane, Brian R.; Lerner, Seth P.; Liu, Jia; Lolla, Laxmi; Lotan, Yair; Lucchesi, Fabiano Rubião; Ma, Yussanne; Machado, Roberto Días; Maglinte, Dennis T.; Mallery, David; Marra, Marco A.; Martin, Sue Ellen; Mayo, Michael; Meraney, Anoop; Moinzadeh, Alireza; Moore, Richard A.; Pinero, Edna M. Mora; Morris, Scott; Morrison, Carl; Mungall, Andrew J.; Myers, Jerome; Naresh, Rashi; O’Donnell, Peter H.; Parekh, Dipen J.; Parfitt, Jeremy; Paulauskis, Joseph; Penny, Robert; Pihl, Todd; Porten, Sima P.; Quintero-Aguilo, Mario; Ramirez, Nilsa C.; Rathmell, W. Kimryn; Rieger-Christ, Kimberly; Saller, Charles; Salner, Andrew L.; Sandusky, George E.; Scapulatempo‐Neto, Cristovam; Schein, Jacqueline E.; Schuckman, Anne; Shelton, Candace; Shelton, Troy; Simko, Jeff; Singh, Parminder; Sipahimalani, Payal; Smith, Norm D.; Sofia, Heidi J.; Sorcini, Andrea; Stanton, Melissa L.; Steinberg, Gary D.; Stoehr, Robert; Sullivan, Travis; Sun, Qiang; Tam, Angela; Tarnuzzer, Roy; Tarvin, Katherine; Täubert, Helge; Thiessen, Nina; Thorne, Leigh B.; Tse, Kane; Tucker, Kelinda; Berg, David J. Van Den; Kessel, Kim E. van; Wach, Sven; Wan, Yunhu; Wang, Zhining; Weinstein, John N.; Weisenberger, Daniel J.; Wise, Lisa; Wong, Tina; Wu, Ye; Yang, Liming; Zach, Leigh Anne; Zenklusen, Jean C.; Zhang, Jiashan; Zmuda, Erik; Zwarthoff, Ellen C.

doi:10.1016/j.cell.2017.09.007

Cited by 1,770 publications

(1,845 citation statements)

References 117 publications

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“…Notably, the ASC signature performed better than other stem cell signatures tested (Figure 4D). A recent characterization of muscle invasive bladder cancers included a minor fraction of samples (~ 1%) histologically defined as small cell neuroendocrine or a mixed phenotype with a small cell neuroendocrine component (Robertson et al, 2017). Comparing the ASC signature scores between the SCN and non-SCN bladder cancers revealed that the SCN bladder cancers were significantly more adult stem cell-like (Figure 4E).…”

Section: Resultsmentioning

confidence: 99%

A Human Adult Stem Cell Signature Marks Aggressive Variants across Epithelial Cancers

et al. 2018

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Cancer progression to an aggressive phenotype often co-opts aspects of stem cell biology. Here, we developed gene signatures for normal human stem cell populations to understand the relationship between epithelial cancers and stem cell transcriptional programs. Using a pan-cancer approach, we reveal that aggressive epithelial cancers are enriched for a transcriptional signature shared by epithelial adult stem cells. The adult stem cell signature selected for epithelial cancers with worse overall survival and alterations of oncogenic drivers. Lethal small cell neuroendocrine lung, prostate, and bladder cancers transcriptionally converged onto the adult stem cell signature and not other stem cell signatures tested. We found that DNA methyltransferase expression correlated with adult stem cell signature status and was enriched in small cell neuroendocrine cancers. DNA methylation analysis uncovered a shared epigenomic profile between small cell neuroendocrine cancers. These pan-cancer findings establish a molecular link between human adult stem cells and aggressive epithelial cancers.

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Section: Resultsmentioning

confidence: 99%

A Human Adult Stem Cell Signature Marks Aggressive Variants across Epithelial Cancers

et al. 2018

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“…Thus molecular biomarkers are needed to improve prediction of treatment response or even for clinical decision-making in the sense of preemptive biomarkers (Youssef and Lotan 2011; Kluth et al 2015). Based on recent data, the most promising results were provided by gene expression signatures of TURB samples and by liquid biopsies from urine or blood (Contreras-Sanz et al 2017; Robertson et al 2017). The elucidation of valuable invasive or non-invasive biomarkers or drug targets is still at its beginning.…”

Section: Introductionmentioning

confidence: 99%

“…We have recently shown that FOXM1 is a predictor for overall and disease-specific survival in muscle invasive bladder cancer (MIBC) superior to the TNM staging system and MKI67 (Rinaldetti et al 2017). A recent TCGA study further underlined the role of FOXM1 as regulator in MIBC (Robertson et al 2017). As MKI67 is considered as the gold standard biomarker for proliferation and prognosis, the impact of FOXM1 needs yet again to be compared with the later (Rodríguez-Alonso et al 2002).…”

Section: Introductionmentioning

confidence: 99%

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FOXM1 predicts disease progression in non-muscle invasive bladder cancer

Rinaldetti

Wirtz²,

Worst

et al. 2018

J Cancer Res Clin Oncol

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PurposeThe proto-oncogene forkhead box M1 (FOXM1) is associated with poor survival in many cancers. The impact of FOXM1 expression on progression-free survival (PFS) of non-muscle invasive bladder cancer (NMIBC) has not yet been investigated. The differential expression of FOXM1 between the different molecular NMIBC subtypes has further been assessed.MethodsTranscript levels of FOXM1 and MKI67 were determined in 460 NMIBC patients (UROMOL cohort) by RNA-Seq and validated in silico by the Chungbuk and Lund cohort (n = 277). FOXM1 and MKI67 cutoffs were identified by the minimal p value method. Variables were evaluated by multivariable Cox regression analyses in order to identify independent predictors.ResultsFOXM1 is an independent predictor for PFS superior to current histological, clinical and molecular staging methods. Patients with high FOXM1 expression have a 6- to 8-fold higher risk of progression in multivariable analysis (p < 0.03). Highest transcript levels were found in the Class 2 and genomically unstable molecular NMIBC subtype (p < 0.03). The proto-oncogene further positively correlated with tumor grade and stage. NMIBCs with high FOXM1 expression showed a PFS advantage when treated with intravesical BCG instillation.ConclusionFOXM1 is a highly prognostic marker for disease progression of NMIBC superior to current histological, clinical and molecular staging methods and MKI67. It is mainly expressed in the Class 2 and genomically unstable molecular bladder cancer subtypes. Its role in drug resistance development makes FOXM1 valuable biomarker for NMIBC risk stratification.

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“…These data move the field considerably closer to a comprehensive catalogue of molecular features and have enabled the influence of molecular subtype on patient outcomes to be examined at a much greater level of detail. The rich dataset includes whole-exome, mRNA, long non-coding RNA (lncRNA), and microRNA sequencing data, DNA copy number variation and methylation data, and reverse-phase protein array data 1 . The tumours analysed were chemotherapy naive and the majority (86%) were pure urothelial carcinomas.…”

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confidence: 99%

Multi-omic profiling refines the molecular view

Hurst

Knowles

2017

Nat Rev Clin Oncol

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Standfirst |Muscle-invasive bladder cancer (MIBC) is a heterogeneous disease for which treatment has, historically, lagged behind that of many other solid tumour types. A more detailed understanding of the biology of individual tumours and the identification of molecular features that provide prognostic and predictive information is key to the application of personalized care for patients with this disease. The recent publication of the complete TCGA study of 412 MIBC samples 1 now provides such data. Estimates suggest that >400,000 new cases of bladder cancer and 165,000 bladder-cancer-related deaths occur worldwide each year 2 . Approximately 25% of cases are muscle-invasive bladder cancers (MIBC). These comprise a heterogeneous group of tumours, and for patients with metastatic disease, the prognosis is generally poor. Until the recent approval of immune-checkpoint inhibitors for use in some patients with advanced MIBC, no new drugs had been approved for the treatment of bladder cancer in more than two decades and no significant changes in survival outcomes had been recorded 3 . Refers to Robertson

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Comprehensive Molecular Characterization of Muscle-Invasive Bladder Cancer

Cited by 1,770 publications

References 117 publications

A Human Adult Stem Cell Signature Marks Aggressive Variants across Epithelial Cancers

A Human Adult Stem Cell Signature Marks Aggressive Variants across Epithelial Cancers

FOXM1 predicts disease progression in non-muscle invasive bladder cancer

Multi-omic profiling refines the molecular view

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