Sir Peter MacCallum Department of Oncology - Research Publications

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Author: Bowtell, David × Author: Etemadmoghadam, Dariush × Author: Fereday, Julie × Start date: 1990 ×

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    Driver mutations in TP53 are ubiquitous in high grade serous carcinoma of the ovary
    Ahmed, AA ; Etemadmoghadam, D ; Temple, J ; Lynch, AG ; Riad, M ; Sharma, R ; Stewart, C ; Fereday, S ; Caldas, C ; DeFazio, A ; Bowtell, D ; Brenton, JD (WILEY, 2010-05)
    Numerous studies have tested the association between TP53 mutations in ovarian cancer and prognosis but these have been consistently confounded by limitations in study design, methodology, and/or heterogeneity in the sample cohort. High-grade serous (HGS) carcinoma is the most clinically important histological subtype of ovarian cancer. As these tumours may arise from the ovary, Fallopian tube or peritoneum, they are collectively referred to as high-grade pelvic serous carcinoma (HGPSC). To identify the true prevalence of TP53 mutations in HGPSC, we sequenced exons 2-11 and intron-exon boundaries in tumour DNA from 145 patients. HGPSC cases were defined as having histological grade 2 or 3 and FIGO stage III or IV. Surprisingly, pathogenic TP53 mutations were identified in 96.7% (n = 119/123) of HGPSC cases. Molecular and pathological review of mutation-negative cases showed evidence of p53 dysfunction associated with copy number gain of MDM2 or MDM4, or indicated the exclusion of samples as being low-grade serous tumours or carcinoma of uncertain primary site. Overall, p53 dysfunction rate approached 100% of confirmed HGPSCs. No association between TP53 mutation and progression-free or overall survival was found. From this first comprehensive mapping of TP53 mutation rate in a homogeneous group of HGPSC patients, we conclude that mutant TP53 is a driver mutation in the pathogenesis of HGPSC cancers. Because TP53 mutation is almost invariably present in HGPSC, it is not of substantial prognostic or predictive significance.
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    Genomic footprints of activated telomere maintenance mechanisms in cancer
    Sieverling, L ; Hong, C ; Koser, SD ; Ginsbach, P ; Kleinheinz, K ; Hutter, B ; Braun, DM ; Cortes-Ciriano, I ; Xi, R ; Kabbe, R ; Park, PJ ; Eils, R ; Schlesner, M ; Brors, B ; Rippe, K ; Jones, DTW ; Feuerbach, L (NATURE PORTFOLIO, 2020-02-05)
    Cancers require telomere maintenance mechanisms for unlimited replicative potential. They achieve this through TERT activation or alternative telomere lengthening associated with ATRX or DAXX loss. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, we dissect whole-genome sequencing data of over 2500 matched tumor-control samples from 36 different tumor types aggregated within the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium to characterize the genomic footprints of these mechanisms. While the telomere content of tumors with ATRX or DAXX mutations (ATRX/DAXXtrunc) is increased, tumors with TERT modifications show a moderate decrease of telomere content. One quarter of all tumor samples contain somatic integrations of telomeric sequences into non-telomeric DNA. This fraction is increased to 80% prevalence in ATRX/DAXXtrunc tumors, which carry an aberrant telomere variant repeat (TVR) distribution as another genomic marker. The latter feature includes enrichment or depletion of the previously undescribed singleton TVRs TTCGGG and TTTGGG, respectively. Our systematic analysis provides new insight into the recurrent genomic alterations associated with telomere maintenance mechanisms in cancer.
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    High-coverage whole-genome analysis of 1220 cancers reveals hundreds of genes deregulated by rearrangement-mediated cis-regulatory alterations
    Zhang, Y ; Chen, F ; Fonseca, NA ; He, Y ; Fujita, M ; Nakagawa, H ; Zhang, Z ; Brazma, A ; Creighton, CJ (NATURE PUBLISHING GROUP, 2020-02-05)
    The impact of somatic structural variants (SVs) on gene expression in cancer is largely unknown. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole-genome sequencing data and RNA sequencing from a common set of 1220 cancer cases, we report hundreds of genes for which the presence within 100 kb of an SV breakpoint associates with altered expression. For the majority of these genes, expression increases rather than decreases with corresponding breakpoint events. Up-regulated cancer-associated genes impacted by this phenomenon include TERT, MDM2, CDK4, ERBB2, CD274, PDCD1LG2, and IGF2. TERT-associated breakpoints involve ~3% of cases, most frequently in liver biliary, melanoma, sarcoma, stomach, and kidney cancers. SVs associated with up-regulation of PD1 and PDL1 genes involve ~1% of non-amplified cases. For many genes, SVs are significantly associated with increased numbers or greater proximity of enhancer regulatory elements near the gene. DNA methylation near the promoter is often increased with nearby SV breakpoint, which may involve inactivation of repressor elements.
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    Comprehensive analysis of chromothripsis in 2,658 human cancers using whole-genome sequencing
    Cortes-Ciriano, I ; Lee, JJ-K ; Xi, R ; Jain, D ; Jung, YL ; Yang, L ; Gordenin, D ; Klimczak, LJ ; Zhang, C-Z ; Pellman, DS ; Park, PJ ; Akdemir, KC ; Alvarez, EG ; Baez-Ortega, A ; Beroukhim, R ; Boutros, PC ; Bowtell, DDL ; Brors, B ; Burns, KH ; Campbell, PJ ; Chan, K ; Chen, K ; Dueso-Barroso, A ; Dunford, AJ ; Edwards, PA ; Estivill, X ; Etemadmoghadam, D ; Feuerbach, L ; Fink, JL ; Frenkel-Morgenstern, M ; Garsed, DW ; Gerstein, M ; Gordenin, DA ; Haan, D ; Haber, JE ; Hess, JM ; Hutter, B ; Imielinski, M ; Jones, DTW ; Ju, YS ; Kazanov, MD ; Koh, Y ; Korbel, JO ; Kumar, K ; Lee, EA ; Li, Y ; Lynch, AG ; Macintyre, G ; Markowetz, F ; Martincorena, I ; Martinez-Fundichely, A ; Miyano, S ; Nakagawa, H ; Navarro, FCP ; Ossowski, S ; Pearson, J ; Puiggros, M ; Rippe, K ; Roberts, ND ; Roberts, SA ; Rodriguez-Martin, B ; Schumacher, SE ; Scully, R ; Shackleton, M ; Sidiropoulos, N ; Sieverling, L ; Stewart, C ; Torrents, D ; Tubio, JMC ; Villasante, I ; Waddell, N ; Wala, JA ; Weischenfeldt, J ; Yao, X ; Yoon, S-S ; Zamora, J ; Alsop, K ; Christie, EL ; Fereday, S ; Mileshkin, L ; Mitchell, C ; Thorne, H ; Traficante, N ; Cmero, M ; Cowin, PA ; Hamilton, A ; Mir Arnau, G ; Vedururu, R ; Grimmond, SM ; Hofmann, O ; Morrison, C ; Oien, KA ; Pairojkul, C ; Waring, PM ; van de Vijver, MJ ; Behren, A (Nature Research, 2020-03)
    Chromothripsis is a mutational phenomenon characterized by massive, clustered genomic rearrangements that occurs in cancer and other diseases. Recent studies in selected cancer types have suggested that chromothripsis may be more common than initially inferred from low-resolution copy-number data. Here, as part of the Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium of the International Cancer Genome Consortium (ICGC) and The Cancer Genome Atlas (TCGA), we analyze patterns of chromothripsis across 2,658 tumors from 38 cancer types using whole-genome sequencing data. We find that chromothripsis events are pervasive across cancers, with a frequency of more than 50% in several cancer types. Whereas canonical chromothripsis profiles display oscillations between two copy-number states, a considerable fraction of events involve multiple chromosomes and additional structural alterations. In addition to non-homologous end joining, we detect signatures of replication-associated processes and templated insertions. Chromothripsis contributes to oncogene amplification and to inactivation of genes such as mismatch-repair-related genes. These findings show that chromothripsis is a major process that drives genome evolution in human cancer.
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    Cancer LncRNA Census reveals evidence for deep functional conservation of long noncoding RNAs in tumorigenesis
    Carlevaro-Fita, J ; Lanzos, A ; Feuerbach, L ; Hong, C ; Mas-Ponte, D ; Pedersen, JS ; Johnson, R ; Abascal, F ; Amin, SB ; Bader, GD ; Barenboim, J ; Beroukhim, R ; Bertl, J ; Boroevich, KA ; Brunak, S ; Campbell, PJ ; Carlevaro-Fita, J ; Chakravarty, D ; Chan, CWY ; Chen, K ; Choi, JK ; Deu-Pons, J ; Dhingra, P ; Diamanti, K ; Feuerbach, L ; Fink, JL ; Fonseca, NA ; Frigola, J ; Gambacorti-Passerini, C ; Garsed, DW ; Gerstein, M ; Getz, G ; Gonzalez-Perez, A ; Guo, Q ; Gut, IG ; Haan, D ; Hamilton, MP ; Haradhvala, NJ ; Harmanci, AO ; Helmy, M ; Herrmann, C ; Hess, JM ; Hobolth, A ; Hodzic, E ; Hong, C ; Hornshoj, H ; Isaev, K ; Izarzugaza, JMG ; Johnson, TA ; Juul, M ; Juul, RI ; Kahles, A ; Kahraman, A ; Kellis, M ; Khurana, E ; Kim, J ; Kim, JK ; Kim, Y ; Komorowski, J ; Korbel, JO ; Kumar, S ; Lanzos, A ; Larsson, E ; Lawrence, MS ; Lee, D ; Lehmann, K-V ; Li, S ; Li, X ; Lin, Z ; Liu, EM ; Lochovsky, L ; Lou, S ; Madsen, T ; Marchal, K ; Martincorena, I ; Martinez-Fundichely, A ; Maruvka, YE ; McGillivray, PD ; Meyerson, W ; Muinos, F ; Mularoni, L ; Nakagawa, H ; Nielsen, MM ; Paczkowska, M ; Park, K ; Park, K ; Pedersen, JS ; Pich, O ; Pons, T ; Pulido-Tamayo, S ; Raphael, BJ ; Reimand, J ; Reyes-Salazar, I ; Reyna, MA ; Rheinbay, E ; Rubin, MA ; Rubio-Perez, C ; Sabarinathan, R ; Sahinalp, SC ; Saksena, G ; Salichos, L ; Sander, C ; Schumacher, SE ; Shackleton, M ; Shapira, O ; Shen, C ; Shrestha, R ; Shuai, S ; Sidiropoulos, N ; Sieverling, L ; Sinnott-Armstrong, N ; Stein, LD ; Stuart, JM ; Tamborero, D ; Tiao, G ; Tsunoda, T ; Umer, HM ; Uuskula-Reimand, L ; Valencia, A ; Vazquez, M ; Verbeke, LPC ; Wadelius, C ; Wadi, L ; Wang, J ; Warrell, J ; Waszak, SM ; Weischenfeldt, J ; Wheeler, DA ; Wu, G ; Yu, J ; Zhang, J ; Zhang, X ; Zhang, Y ; Zhao, Z ; Zou, L ; von Mering, C (NATURE PUBLISHING GROUP, 2020-02-05)
    Long non-coding RNAs (lncRNAs) are a growing focus of cancer genomics studies, creating the need for a resource of lncRNAs with validated cancer roles. Furthermore, it remains debated whether mutated lncRNAs can drive tumorigenesis, and whether such functions could be conserved during evolution. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, we introduce the Cancer LncRNA Census (CLC), a compilation of 122 GENCODE lncRNAs with causal roles in cancer phenotypes. In contrast to existing databases, CLC requires strong functional or genetic evidence. CLC genes are enriched amongst driver genes predicted from somatic mutations, and display characteristic genomic features. Strikingly, CLC genes are enriched for driver mutations from unbiased, genome-wide transposon-mutagenesis screens in mice. We identified 10 tumour-causing mutations in orthologues of 8 lncRNAs, including LINC-PINT and NEAT1, but not MALAT1. Thus CLC represents a dataset of high-confidence cancer lncRNAs. Mutagenesis maps are a novel means for identifying deeply-conserved roles of lncRNAs in tumorigenesis.
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    Integrative pathway enrichment analysis of multivariate omics data
    Paczkowska, M ; Barenboim, J ; Sintupisut, N ; Fox, NS ; Zhu, H ; Abd-Rabbo, D ; Mee, MW ; Boutros, PC ; Reimand, J (NATURE PUBLISHING GROUP, 2020-02-05)
    Multi-omics datasets represent distinct aspects of the central dogma of molecular biology. Such high-dimensional molecular profiles pose challenges to data interpretation and hypothesis generation. ActivePathways is an integrative method that discovers significantly enriched pathways across multiple datasets using statistical data fusion, rationalizes contributing evidence and highlights associated genes. As part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole genome sequencing data from 2658 cancers across 38 tumor types, we integrated genes with coding and non-coding mutations and revealed frequently mutated pathways and additional cancer genes with infrequent mutations. We also analyzed prognostic molecular pathways by integrating genomic and transcriptomic features of 1780 breast cancers and highlighted associations with immune response and anti-apoptotic signaling. Integration of ChIP-seq and RNA-seq data for master regulators of the Hippo pathway across normal human tissues identified processes of tissue regeneration and stem cell regulation. ActivePathways is a versatile method that improves systems-level understanding of cellular organization in health and disease through integration of multiple molecular datasets and pathway annotations.
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    Combined burden and functional impact tests for cancer driver discovery using DriverPower
    Shuai, S ; Gallinger, S ; Stein, L (NATURE PORTFOLIO, 2020-02-05)
    The discovery of driver mutations is one of the key motivations for cancer genome sequencing. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole genome sequencing data from 2658 cancers across 38 tumour types, we describe DriverPower, a software package that uses mutational burden and functional impact evidence to identify driver mutations in coding and non-coding sites within cancer whole genomes. Using a total of 1373 genomic features derived from public sources, DriverPower's background mutation model explains up to 93% of the regional variance in the mutation rate across multiple tumour types. By incorporating functional impact scores, we are able to further increase the accuracy of driver discovery. Testing across a collection of 2583 cancer genomes from the PCAWG project, DriverPower identifies 217 coding and 95 non-coding driver candidates. Comparing to six published methods used by the PCAWG Drivers and Functional Interpretation Working Group, DriverPower has the highest F1 score for both coding and non-coding driver discovery. This demonstrates that DriverPower is an effective framework for computational driver discovery.
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    Pathway and network analysis of more than 2500 whole cancer genomes
    Reyna, MA ; Haan, D ; Paczkowska, M ; Verbeke, LPC ; Vazquez, M ; Kahraman, A ; Pulido-Tamayo, S ; Barenboim, J ; Wadi, L ; Dhingra, P ; Shrestha, R ; Getz, G ; Lawrence, MS ; Pedersen, JS ; Rubin, MA ; Wheeler, DA ; Brunak, S ; Izarzugaza, JMG ; Khurana, E ; Marchal, K ; von Mering, C ; Sahinalp, SC ; Valencia, A ; Reimand, J ; Stuart, JM ; Raphael, BJ (NATURE RESEARCH, 2020-02-05)
    The catalog of cancer driver mutations in protein-coding genes has greatly expanded in the past decade. However, non-coding cancer driver mutations are less well-characterized and only a handful of recurrent non-coding mutations, most notably TERT promoter mutations, have been reported. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole genome sequencing data from 2658 cancer across 38 tumor types, we perform multi-faceted pathway and network analyses of non-coding mutations across 2583 whole cancer genomes from 27 tumor types compiled by the ICGC/TCGA PCAWG project that was motivated by the success of pathway and network analyses in prioritizing rare mutations in protein-coding genes. While few non-coding genomic elements are recurrently mutated in this cohort, we identify 93 genes harboring non-coding mutations that cluster into several modules of interacting proteins. Among these are promoter mutations associated with reduced mRNA expression in TP53, TLE4, and TCF4. We find that biological processes had variable proportions of coding and non-coding mutations, with chromatin remodeling and proliferation pathways altered primarily by coding mutations, while developmental pathways, including Wnt and Notch, altered by both coding and non-coding mutations. RNA splicing is primarily altered by non-coding mutations in this cohort, and samples containing non-coding mutations in well-known RNA splicing factors exhibit similar gene expression signatures as samples with coding mutations in these genes. These analyses contribute a new repertoire of possible cancer genes and mechanisms that are altered by non-coding mutations and offer insights into additional cancer vulnerabilities that can be investigated for potential therapeutic treatments.
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    Sex differences in oncogenic mutational processes
    Li, CH ; Prokopec, SD ; Sun, RX ; Yousif, F ; Schmitz, N ; Boutros, PC (NATURE PORTFOLIO, 2020-08-28)
    Sex differences have been observed in multiple facets of cancer epidemiology, treatment and biology, and in most cancers outside the sex organs. Efforts to link these clinical differences to specific molecular features have focused on somatic mutations within the coding regions of the genome. Here we report a pan-cancer analysis of sex differences in whole genomes of 1983 tumours of 28 subtypes as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium. We both confirm the results of exome studies, and also uncover previously undescribed sex differences. These include sex-biases in coding and non-coding cancer drivers, mutation prevalence and strikingly, in mutational signatures related to underlying mutational processes. These results underline the pervasiveness of molecular sex differences and strengthen the call for increased consideration of sex in molecular cancer research.
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    LRP1B Deletion in High-Grade Serous Ovarian Cancers Is Associated with Acquired Chemotherapy Resistance to Liposomal Doxorubicin
    Cowin, PA ; George, J ; Fereday, S ; Loehrer, E ; Van Loo, P ; Cullinane, C ; Etemadmoghadam, D ; Ftouni, S ; Galletta, L ; Anglesio, MS ; Hendley, J ; Bowes, L ; Sheppard, KE ; Christie, EL ; Pearson, RB ; Harnett, PR ; Heinzelmann-Schwarz, V ; Friedlander, M ; McNally, O ; Quinn, M ; Campbell, P ; deFazio, A ; Bowtell, DDL (AMER ASSOC CANCER RESEARCH, 2012-08-15)
    High-grade serous cancer (HGSC), the most common subtype of ovarian cancer, often becomes resistant to chemotherapy, leading to poor patient outcomes. Intratumoral heterogeneity occurs in nearly all solid cancers, including ovarian cancer, contributing to the development of resistance mechanisms. In this study, we examined the spatial and temporal genomic variation in HGSC using high-resolution single-nucleotide polymorphism arrays. Multiple metastatic lesions from individual patients were analyzed along with 22 paired pretreatment and posttreatment samples. We documented regions of differential DNA copy number between multiple tumor biopsies that correlated with altered expression of genes involved in cell polarity and adhesion. In the paired primary and relapse cohort, we observed a greater degree of genomic change in tumors from patients that were initially sensitive to chemotherapy and had longer progression-free interval compared with tumors from patients that were resistant to primary chemotherapy. Notably, deletion or downregulation of the lipid transporter LRP1B emerged as a significant correlate of acquired resistance in our analysis. Functional studies showed that reducing LRP1B expression was sufficient to reduce the sensitivity of HGSC cell lines to liposomal doxorubicin, but not to doxorubicin, whereas LRP1B overexpression was sufficient to increase sensitivity to liposomal doxorubicin. Together, our findings underscore the large degree of variation in DNA copy number in spatially and temporally separated tumors in HGSC patients, and they define LRP1B as a potential contributor to the emergence of chemotherapy resistance in these patients.