Your search keyword '"Katia Nones"' showing total 8 results

1. Multi-omic features of oesophageal adenocarcinoma in patients treated with preoperative neoadjuvant therapy

Author

Marjan M. Naeini, Felicity Newell, Lauren G. Aoude, Vanessa F. Bonazzi, Kalpana Patel, Guy Lampe, Lambros T. Koufariotis, Vanessa Lakis, Venkateswar Addala, Olga Kondrashova, Rebecca L. Johnston, Sowmya Sharma, Sandra Brosda, Oliver Holmes, Conrad Leonard, Scott Wood, Qinying Xu, Janine Thomas, Euan Walpole, G. Tao Mai, Stephen P. Ackland, Jarad Martin, Matthew Burge, Robert Finch, Christos S. Karapetis, Jenny Shannon, Louise Nott, Robert Bohmer, Kate Wilson, Elizabeth Barnes, John R. Zalcberg, B. Mark Smithers, John Simes, Timothy Price, Val Gebski, Katia Nones, David I. Watson, John V. Pearson, Andrew P. Barbour, and Nicola Waddell

Subjects

Multidisciplinary, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Abstract

Oesophageal adenocarcinoma is a poor prognosis cancer and the molecular features underpinning response to treatment remain unclear. We investigate whole genome, transcriptomic and methylation data from 115 oesophageal adenocarcinoma patients mostly from the DOCTOR phase II clinical trial (Australian New Zealand Clinical Trials Registry-ACTRN12609000665235), with exploratory analysis pre-specified in the study protocol of the trial. We report genomic features associated with poorer overall survival, such as the APOBEC mutational and RS3-like rearrangement signatures. We also show that positron emission tomography non-responders have more sub-clonal genomic copy number alterations. Transcriptomic analysis categorises patients into four immune clusters correlated with survival. The immune suppressed cluster is associated with worse survival, enriched with myeloid-derived cells, and an epithelial-mesenchymal transition signature. The immune hot cluster is associated with better survival, enriched with lymphocytes, myeloid-derived cells, and an immune signature including CCL5, CD8A, and NKG7. The immune clusters highlight patients who may respond to immunotherapy and thus may guide future clinical trials.

Published

2023

2. Comprehensive genomic and tumour immune profiling reveals potential therapeutic targets in malignant pleural mesothelioma

Author

Jenette Creaney, Ann-Marie Patch, Venkateswar Addala, Sophie A. Sneddon, Katia Nones, Ian M. Dick, Y. C. Gary Lee, Felicity Newell, Ebony J. Rouse, Marjan M. Naeini, Olga Kondrashova, Vanessa Lakis, Apostolos Nakas, David Waller, Annabel Sharkey, Pamela Mukhopadhyay, Stephen H. Kazakoff, Lambros T. Koufariotis, Aimee L. Davidson, Priya Ramarao-Milne, Oliver Holmes, Qinying Xu, Conrad Leonard, Scott Wood, Sean M. Grimmond, Raphael Bueno, Dean A. Fennell, John V. Pearson, Bruce W. Robinson, and Nicola Waddell

Subjects

Mesothelioma, Lung Neoplasms, Pleural Neoplasms, Mesothelioma, Malignant, Tumor Microenvironment, Genetics, Humans, Molecular Medicine, Genomics, Molecular Biology, Genetics (clinical)

Abstract

Background Malignant pleural mesothelioma (MPM) has a poor overall survival with few treatment options. Whole genome sequencing (WGS) combined with the immune features of MPM offers the prospect of identifying changes that could inform future clinical trials. Methods We analysed somatic mutations from 229 MPM samples, including previously published data and 58 samples that had undergone WGS within this study. This was combined with RNA-seq analysis to characterize the tumour immune environment. Results The comprehensive genome analysis identified 12 driver genes, including new candidate genes. Whole genome doubling was a frequent event that correlated with shorter survival. Mutational signature analysis revealed SBS5/40 were dominant in 93% of samples, and defects in homologous recombination repair were infrequent in our cohort. The tumour immune environment contained high M2 macrophage infiltrate linked with MMP2, MMP14, TGFB1 and CCL2 expression, representing an immune suppressive environment. The expression of TGFB1 was associated with overall survival. A small subset of samples (less than 10%) had a higher proportion of CD8 T cells and a high cytolytic score, suggesting a ‘hot’ immune environment independent of the somatic mutations. Conclusions We propose accounting for genomic and immune microenvironment status may influence therapeutic planning in the future.

Published

2022

3. Pathogenic germline variants are associated with poor survival in stage III/IV melanoma patients

Author

Vanessa F. Bonazzi, Sandra Brosda, Katia Nones, John V. Pearson, Scott Wood, Kalpana Patel, Nicola Waddell, Andrew Barbour, Melissa Arneil, James M. Lonie, Victoria Atkinson, B. Mark Smithers, Lauren G. Aoude, Harald Oey, and Lambros T. Koufariotis

Subjects

Adult, Male, Proto-Oncogene Proteins B-raf, Oncology, medicine.medical_specialty, Skin Neoplasms, lcsh:Medicine, Article, Germline, Tumour biomarkers, Germline mutation, CDKN2A, Internal medicine, Cancer genomics, Biomarkers, Tumor, medicine, Humans, Prospective Studies, lcsh:Science, Adverse effect, Cancer genetics, Melanoma, Germ-Line Mutation, Aged, Aged, 80 and over, Multidisciplinary, business.industry, lcsh:R, Middle Aged, Prognosis, medicine.disease, Survival Analysis, MRE11A, Cohort, Cutaneous melanoma, Female, lcsh:Q, business

Abstract

Patients with late stage resected cutaneous melanoma have poor overall survival (OS) and experience irreversible adverse events from systemic therapy. There is a clinical need to identify biomarkers to predict outcome. Performing germline/tumour whole-exome sequencing of 44 stage III/IV melanoma patients we identified pathogenic germline mutations in CDKN2A, CDK4, ATM, POLH, MRE11A, RECQL4 and XPC, affecting 7/44 patients. These mutations were associated with poor OS (p = 0.0082). We confirmed our findings in The Cancer Genome Atlas (TCGA) human skin cutaneous melanoma cohort where we identified pathogenic variants in 40/455 patients (p = 0.0203). Combining these cohorts (n = 499) further strengthened these findings showing germline carriers had worse OS (p = 0.0009). Additionally, we determined whether tumour mutation burden (TMB) or BRAF status were prognostic markers of survival. Low TMB rate (p = 0.0034) and BRAF p.V600 mutation (p = 0.0355) were associated with worse progression-free survival. Combining these biomarkers indicated that V600 mutant patients had significantly lower TMB (p = 0.0155). This was confirmed in the TCGA (n = 443, p = 0.0007). Integrative analysis showed germline mutation status conferred the highest risk (HR 5.2, 95% CI 1.72–15.7). Stage IV (HR 2.5, 0.74–8.6) and low TMB (HR 2.3, 0.57–9.4) were similar, whereas BRAF V600 status was the weakest prognostic biomarker (HR 1.5, 95% CI 0.44–5.2).

Published

2020

4. Characterization of a novel breast cancer cell line derived from a metastatic bone lesion of a breast cancer patient

Author

Sarah Song, Fares Al-Ejeh, Cameron N. Johnstone, Stephen H. Kazakoff, Chanel E. Smart, Victorian Cancer BioBank, Rebecca L. Johnston, Julie Johnson, Nicola Waddell, Peter T. Simpson, Ana Christina Vargas, Georgia Chenevix-Trench, Jodi M. Saunus, Sibylle Cocciardi, Darrell C. Bessette, Sunil R. Lakhani, Kum Kum Khanna, Katia Nones, and E Rozali

Subjects

0301 basic medicine, Cancer Research, DNA Copy Number Variations, Somatic cell, Bone Neoplasms, Triple Negative Breast Neoplasms, Metastasis, Mice, 03 medical and health sciences, Breast cancer, CDKN2A, Cell Line, Tumor, medicine, Animals, Humans, Exome, Breast, biology, CD44, Bone metastasis, medicine.disease, Primary tumor, Neoplasm Proteins, 3. Good health, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, Mutation, MCF-7 Cells, biology.protein, Cancer research, Female, Estrogen receptor alpha

Abstract

We aimed to generate and characterize a novel cell line from a breast cancer bone metastasis to better study the progression of the disease. The cell line, P7731, was derived from a metastatic bone lesion of a breast cancer patient and assessed for marker expression. P7731 was analyzed for DNA copy number variation, somatic mutations, and gene expression and was compared with the primary tumor. P7731 cells are negative for estrogen receptor alpha (ERα), progesterone receptor (PR), and HER2 (triple-negative); strongly express vimentin (100% of cells positive) and also express cytokeratins 8/18 and 19 but at lower frequencies. Flow cytometry indicates P7731 cells are predominantly CD44+/CD49f+/EpCAM−, consistent with a primitive, mesenchymal-like phenotype. The cell line is tumorigenic in immunocompromised mice. Exome sequencing identified a total of 45 and 76 somatic mutations in the primary tumor and cell line, respectively, of which 32 were identified in both samples and included mutations in known driver genes PIK3CA, TP53, and ARID1A. P7731 retains the DNA copy number alterations present in the matching primary tumor. Homozygous deletions detected in the cell line and in the primary tumor were found in regions containing three known (CDKN2A, CDKN2B, and CDKN1B) and 23 putative tumor suppressor genes. Cell line-specific gene amplification coupled with mRNA expression analysis revealed genes and pathways with potential pro-metastatic functions. This novel human breast cancer-bone metastasis cell line will be a useful model to study aspects of breast cancer biology, particularly metastasis-related changes from breast to bone.

Published

2018

5. Whole-genome landscapes of major melanoma subtypes

Author

Anna Fitzgerald, John V. Pearson, Andrew J. Spillane, Loretta Lau, Nuria Lopez-Bigas, Peter Johansson, Catherine A. Shang, Richard A. Scolyer, John F. Thompson, Scott Wood, Valerie Jakrot, Peter Hersey, Katia Nones, Rebecca A. Dagg, Antonia L. Pritchard, Conrad Leonard, Andreas Behren, Varsha Tembe, Robyn P. M. Saw, Loris Mularoni, Nick Waddell, Mark Shackleton, Hojabr Kakavand, Ping Shang, Jean Y. Yang, Graham J. Mann, Radhakrishnan Sabarinathan, Gulietta M. Pupo, Ricardo De Paoli-Iseppi, Jonathan Cebon, Richard F. Kefford, Ricardo E. Vilain, Hilda A. Pickett, Stephen H. Kazakoff, Ludmil B. Alexandrov, Oliver Holmes, Nicholas K. Hayward, Nicola Waddell, Ken Dutton-Regester, Jonathan R. Stretch, Sean M. Grimmond, Felicity Newell, Qinying Xu, James S. Wilmott, Hazel Burke, Georgina V. Long, Sarah-Jane Schramm, Matthew A. Field, and Ann-Marie Patch

Subjects

Proto-Oncogene Proteins B-raf, 0301 basic medicine, Neuroblastoma RAS viral oncogene homolog, X-linked Nuclear Protein, Neurofibromatosis 1, Ultraviolet Rays, Biology, medicine.disease_cause, GTP Phosphohydrolases, 03 medical and health sciences, 0302 clinical medicine, CDKN2A, medicine, Humans, Càncer, skin and connective tissue diseases, Melanoma, Telomerase, neoplasms, ATRX, Cancer, Genetics, Mutation, Multidisciplinary, Genome, Human, Genes, p16, DNA Helicases, Mucosal melanoma, Membrane Proteins, Nuclear Proteins, Telomere, Phosphoproteins, medicine.disease, 3. Good health, 030104 developmental biology, 030220 oncology & carcinogenesis, Cutaneous melanoma, Cancer research, RNA Splicing Factors, Mitogen-Activated Protein Kinases, Tumor Suppressor Protein p53, Signal Transduction

Abstract

Melanoma of the skin is a common cancer only in Europeans, whereas it arises in internal body surfaces (mucosal sites) and on the hands and feet (acral sites) in people throughout the world. Here we report analysis of whole-genome sequences from cutaneous, acral and mucosal subtypes of melanoma. The heavily mutated landscape of coding and non-coding mutations in cutaneous melanoma resolved novel signatures of mutagenesis attributable to ultraviolet radiation. However, acral and mucosal melanomas were dominated by structural changes and mutation signatures of unknown aetiology, not previously identified in melanoma. The number of genes affected by recurrent mutations disrupting non-coding sequences was similar to that affected by recurrent mutations to coding sequences. Significantly mutated genes included BRAF, CDKN2A, NRAS and TP53 in cutaneous melanoma, BRAF, NRAS and NF1 in acral melanoma and SF3B1 in mucosal melanoma. Mutations affecting the TERT promoter were the most frequent of all; however, neither they nor ATRX mutations, which correlate with alternative telomere lengthening, were associated with greater telomere length. Most melanomas had potentially actionable mutations, most in components of the mitogen-activated protein kinase and phosphoinositol kinase pathways. The whole-genome mutation landscape of melanoma reveals diverse carcinogenic processes across its subtypes, some unrelated to sun exposure, and extends potential involvement of the non-coding genome in its pathogenesis.

Published

2017

6. Pancreatic cancer genomes reveal aberrations in axon guidance pathway genes

Author

Conrad Leonard, Stefano Serra, Jeremy L. Humphris, J. Lynn Fink, Vincenzo Corbo, Deepa Pai, Ami Panchal, Jennifer Drummond, Anirban Maitra, Katia Nones, Mark J. Cowley, Nam Q. Nguyen, Marc D. Jones, David A. Largaespada, Karen M. Mann, Ralph H. Hruban, Nicole Cloonan, Timothy Beck, Marie-Claude Gingras, Sally E. Hodges, Darrin Taylor, Andrew V. Biankin, Angela Chou, Craig Nourse, Marina Pajic, Gloria M. Petersen, Kimberly Begley, Richard A. Morgan, Rita T. Lawlor, Senel Idrisoglu, Jessica A. Lovell, Lincoln Stein, Christina K. Yung, Lee Timms, Adnan Nagrial, Giampaolo Tortora, Shivangi Wani, Mark Pinese, Angelika N. Christ, Amanda Mawson, Neil D. Merrett, Maria Scardoni, Min Wang, Ann-Marie Patch, Steven Gallinger, Huyen Dinh, Richard A. Gibbs, John Douglas Mcpherson, Amber L. Johns, Nipun Kakkar, David A. Wheeler, Andrew Barbour, Patricia Shaw, Milena Gongora, Emily S. Humphrey, Christopher J. Scarlett, Matthew J. Anderson, Lodewyk F. A. Wessels, Andrew M.K. Brown, Christopher W. Toon, Felicity Newell, Margaret A. Tempero, Fengmei Zhao, Richard D. Schulick, Paola Capelli, Timothy J. C. Bruxner, Christine A. Iacobuzio-Donahue, Ivon Harliwong, Richard de Borja, Pedro A. Perez-Mancera, Jianmin Wu, Emily K. Colvin, Michelle Sam, Warren Kaplan, Debabrata Mukhopadhyay, John V. Pearson, Gabriel Kolle, Oliver Holmes, Lorraine A. Chantrill, Lora Lewis, Jaswinder S. Samra, Scott Wood, Lakshmi Muthuswamy, James R. Eshleman, Neal G. Copeland, Peter Wilson, David Miller, Anthony J. Gill, Qinying Xu, Nicola Waddell, Ming-Sound Tsao, Karin S. Kassahn, Venessa T. Chin, James G. Kench, David K. Chang, William E. Fisher, Kyle Chang, Aldo Scarpa, Christopher L. Wolfgang, Roger J. Daly, Alistair G. Rust, Ehsan Nourbakhsh, Jeffrey G. Reid, Nikolajs Zeps, Nicole Onetto, Donna M. Muzny, Brooke Gardiner, Robert E. Denroche, Yuan Qing Wu, Nancy A. Jenkins, Sean M. Grimmond, R. Scott Mead, David A. Tuveson, David J. Adams, Yi Han, F. Charles Brunicardi, Andreia V. Pinho, Elizabeth A. Musgrove, Sarah Song, Ilse Rooman, Thomas J. Hudson, Christian J. Buhay, Robert L. Sutherland, Suzanne Manning, Nicholas Buchner, Krishna Epari, Basic (bio-) Medical Sciences, and Laboratory for Medical and Molecular Oncology

Subjects

Exome sequencing, Gene Dosage, Copy number analysis, PDAC, KRAS, Kaplan-Meier Estimate, Biology, medicine.disease_cause, Mice, CDKN2A, Pancreatic cancer, medicine, Animals, Humans, Genetics, Mutation, Genome, Multidisciplinary, Proteins, Cancer, medicine.disease, Axons, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, Cancer research, Carcinogenesis, Carcinoma, Pancreatic Ductal, Signal Transduction

Abstract

Pancreatic cancer is a highly lethal malignancy with few effective therapies. We performed exome sequencing and copy number analysis to define genomic aberrations in a prospectively accrued clinical cohort (n = 142) of early (stage I and II) sporadic pancreatic ductal adenocarcinoma. Detailed analysis of 99 informative tumours identified substantial heterogeneity with 2,016 non-silent mutations and 1,628 copy-number variations. We define 16 significantly mutated genes, reaffirming known mutations (KRAS, TP53, CDKN2A, SMAD4, MLL3, TGFBR2, ARID1A and SF3B1), and uncover novel mutated genes including additional genes involved in chromatin modification (EPC1 and ARID2), DNA damage repair (ATM) and other mechanisms (ZIM2, MAP2K4, NALCN, SLC16A4 and MAGEA6). Integrative analysis with in vitro functional data and animal models provided supportive evidence for potential roles for these genetic aberrations in carcinogenesis. Pathway-based analysis of recurrently mutated genes recapitulated clustering in core signalling pathways in pancreatic ductal adenocarcinoma, and identified new mutated genes in each pathway. We also identified frequent and diverse somatic aberrations in genes described traditionally as embryonic regulators of axon guidance, particularly SLIT/ROBO signalling, which was also evident in murine Sleeping Beauty transposon-mediated somatic mutagenesis models of pancreatic cancer, providing further supportive evidence for the potential involvement of axon guidance genes in pancreatic carcinogenesis.

Published

2012

7. Erratum: Corrigendum: Whole-genome landscape of pancreatic neuroendocrine tumours

Author

Irene Dalai, Conrad Leonard, Eliana Amato, Andrew B. Barbour, Marc D. Jones, Rita T. Lawlor, Andreia V. Pinho, Amanda Mawson, Neil D. Merrett, Caterina Vicentini, Matteo Fassan, Ivon Harliwong, J. Lynn Fink, Giovanni Butturini, Anthony J. Gill, David Miller, Senel Idrisoglu, James G. Kench, Andrew V. Biankin, Ilse Rooman, Angela Chou, Marie-Claude Gingras, Katia Nones, Venessa T. Chin, Marco Miotto, Davide Antonello, Borislav Rusev, Paola Capelli, Rebecca A. Dagg, Christopher W. Toon, Jeremy L. Humphris, Samantha Bersani, David K. Chang, Nigel B. Jamieson, George Van Buren, Vincenzo Corbo, Jaswinder S. Samra, Stephen H. Kazakoff, Scott Wood, Claudio Bassi, Emily K. Colvin, Stefano Barbi, Amber L. Johns, Christopher J. Scarlett, Nicola Waddell, Jianmin Wu, Michael Lee, Michele Simbolo, Luca Landoni, Katarzyna O. Sikora, Michael C.J. Quinn, John V. Pearson, Nam Q. Nguyen, Angelo Paolo Dei Tos, Mark J. Cowley, Adnan Nagrial, Peter Bailey, Roger R. Reddel, Sean M. Grimmond, Peter Wilson, Skye McKay, Richard A. Gibbs, Jessica A. Lovell, Nikolajs Zeps, Kum Kum Khanna, Stefano Partelli, Timothy J. C. Bruxner, Janelle L. Harris, Andrea Mafficini, Barbara A. Leggett, Angelika N. Christ, Oliver Holmes, Craig Nourse, Krishna Epari, Felicity Newell, Ivana Cataldo, Paolo Pederzoli, Vicki L. J. Whitehall, Matthew J. Anderson, William E. Fisher, Maria Scardoni, Loretta Lau, Massimo Falconi, Ann-Marie Patch, Aldo Scarpa, Lorraine A. Chantrill, Shivashankar H. Nagaraj, Giampaolo Tortora, Sara Cingarlini, Elizabeth A. Musgrove, Ehsan Nourbakhsh, Maria Vittoria Davì, David A. Wheeler, Suzanne McLean, Fraser Duthie, Qinying Xu, Mark Pinese, Anna Malpaga, Nick Waddell, Emily S. Humphrey, Jonathan M. Harris, Marina Pajic, and Hilda A. Pickett

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, Multidisciplinary, Breakpoint, RNA splicing, Computational biology, Biology, Genome

Abstract

Nature 543, 65–71 (2017); doi:10.1038/nature21063 It has been brought to our attention that in Fig. 2d of this Article, an incorrect Sanger trace was used to represent the breakpoint of the EWSR1 and FLI1 type 2 fusion. This was due to an error during manuscript preparation, when we inadvertently inserted the electrophoretic trace referring to EWSR1 splicing variants.

Published

2017

8. Imperfect centered miRNA binding sites are common and can mediate repression of target mRNAs

Author

Hilary C. Martin, Nicole Cloonan, Anita L Steptoe, Shivangi Wani, Sean M. Grimmond, Alexander V. Vlassov, Keerthana Krishnan, Katia Nones, and Ehsan Nourbakhsh

Subjects

Genetics, 0303 health sciences, Binding Sites, Genome, Human, Research, HEK 293 cells, RNA, MiRNA binding, Computational biology, Biology, Genome, MicroRNAs, 03 medical and health sciences, HEK293 Cells, 0302 clinical medicine, 030220 oncology & carcinogenesis, microRNA, Humans, Human genome, RNA, Messenger, RNA Processing, Post-Transcriptional, Binding site, Psychological repression, 030304 developmental biology

Abstract

Background\ud MicroRNAs (miRNAs) bind to mRNAs and target them for translational inhibition or transcriptional degradation. It is thought that most miRNA-mRNA interactions involve the seed region at the 5′ end of the miRNA. The importance of seed sites is supported by experimental evidence, although there is growing interest in interactions mediated by the central region of the miRNA, termed centered sites. To investigate the prevalence of these interactions, we apply a biotin pull-down method to determine the direct targets of ten human miRNAs, including four isomiRs that share centered sites, but not seeds, with their canonical partner miRNAs.\ud \ud Results\ud We confirm that miRNAs and their isomiRs can interact with hundreds of mRNAs, and that imperfect centered sites are common mediators of miRNA-mRNA interactions. We experimentally demonstrate that these sites can repress mRNA activity, typically through translational repression, and are enriched in regions of the transcriptome bound by AGO. Finally, we show that the identification of imperfect centered sites is unlikely to be an artifact of our protocol caused by the biotinylation of the miRNA. However, the fact that there was a slight bias against seed sites in our protocol may have inflated the apparent prevalence of centered site-mediated interactions.\ud \ud Conclusions\ud Our results suggest that centered site-mediated interactions are much more frequent than previously thought. This may explain the evolutionary conservation of the central region of miRNAs, and has significant implications for decoding miRNA-regulated genetic networks, and for predicting the functional effect of variants that do not alter protein sequence.

Published

2014