Your search keyword '"Katia Nones"' showing total 4 results

1. Phenotypic and molecular dissection of metaplastic breast cancer and the prognostic implications

Author

Amy Ellen, McCart Reed, Emarene, Kalaw, Katia, Nones, Mark, Bettington, Malcolm, Lim, James, Bennett, Kate, Johnstone, Jamie Rose, Kutasovic, Jodi Marie, Saunus, Stephen, Kazakoff, Qinying, Xu, Scott, Wood, Oliver, Holmes, Conrad, Leonard, Lynne Estelle, Reid, Debra, Black, Colleen, Niland, Kaltin, Ferguson, Irma, Gresshoff, Ashwini, Raghavendra, Kate, Harvey, Caroline, Cooper, Cheng, Liu, Lauren, Kalinowski, Andrew Scott, Reid, Morgan, Davidson, John V, Pearson, Nirmala, Pathmanathan, Gary, Tse, David, Papadimos, Rajadurai, Pathmanathan, Gavin, Harris, Rin, Yamaguchi, Puay Hoon, Tan, Stephen B, Fox, Sandra A, O'Toole, Peter Thomas, Simpson, Nicola, Waddell, and Sunil R, Lakhani

Subjects

Epithelial-Mesenchymal Transition, Class I Phosphatidylinositol 3-Kinases, Breast Neoplasms, breast cancer, Antigens, CD, molecular pathology, Biomarkers, Tumor, genomics, Humans, Genetic Predisposition to Disease, skin and connective tissue diseases, Metaplasia, Neurofibromin 1, metaplastic, PTEN Phosphohydrolase, Middle Aged, Cadherins, Neoplasms, Complex and Mixed, Tumor Burden, ErbB Receptors, Cross-Sectional Studies, Phenotype, NF1, Mutation, Keratins, Female, Neoplasm Grading, Tumor Suppressor Protein p53, Article Commentary

Abstract

Metaplastic breast carcinoma (MBC) is relatively rare but accounts for a significant proportion of global breast cancer mortality. This group is extremely heterogeneous and by definition exhibits metaplastic change to squamous and/or mesenchymal elements, including spindle, squamous, chondroid, osseous, and rhabdomyoid features. Clinically, patients are more likely to present with large primary tumours (higher stage), distant metastases, and overall, have shorter 5-year survival compared to invasive carcinomas of no special type. The current World Health Organisation (WHO) diagnostic classification for this cancer type is based purely on morphology - the biological basis and clinical relevance of its seven sub-categories are currently unclear. By establishing the Asia-Pacific MBC (AP-MBC) Consortium, we amassed a large series of MBCs (n = 347) and analysed the mutation profile of a subset, expression of 14 breast cancer biomarkers, and clinicopathological correlates, contextualising our findings within the WHO guidelines. The most significant indicators of poor prognosis were large tumour size (T3; p = 0.004), loss of cytokeratin expression (lack of staining with pan-cytokeratin AE1/3 antibody; p = 0.007), EGFR overexpression (p = 0.01), and for 'mixed' MBC, the presence of more than three distinct morphological entities (p = 0.007). Conversely, fewer morphological components and EGFR negativity were favourable indicators. Exome sequencing of 30 cases confirmed enrichment of TP53 and PTEN mutations, and intriguingly, concurrent mutations of TP53, PTEN, and PIK3CA. Mutations in neurofibromatosis-1 (NF1) were also overrepresented [16.7% MBCs compared to ∼5% of breast cancers overall; enrichment p = 0.028; mutation significance p = 0.006 (OncodriveFM)], consistent with published case reports implicating germline NF1 mutations in MBC risk. Taken together, we propose a practically minor but clinically significant modification to the guidelines: all WHO_1 mixed-type tumours should have the number of morphologies present recorded, as a mechanism for refining prognosis, and that EGFR and pan-cytokeratin expression are important prognostic markers. Copyright © 2018 Pathological Society of Great Britain and Ireland. Published by John WileySons, Ltd.

Published

2018

2. Integrated genomic and transcriptomic analysis of human brain metastases identifies alterations of potential clinical significance

Author

Mythily Mariasegaram, Ann-Marie Patch, Conrad Leonard, Admire Matsika, Sean M. Grimmond, Fares Al-Ejeh, Margaret C. Cummings, Rosalind L. Jeffree, Georgia Chenevix-Trench, Oliver Holmes, Leonard Da Silva, Nur Aishah Taib, Adrienne M. Flanagan, Teresa K. Withers, Matthew J. Anderson, Vairavan Narayanan, Ehsan Nourbakhsh, Queenie Lau, Sunil R. Lakhani, J. Lynn Fink, kConFab, Felicity Newell, Katia Nones, Stephen H. Kazakoff, Colleen Niland, Parmjit S. Jat, Ivon Harliwong, Peter T. Simpson, Lynne Reid, Nicola Waddell, Soo Hwang Teo, Karin S. Kassahn, Sebastian Brandner, John V. Pearson, Nick Waddell, Qinying Xu, Scott Wood, Darrin Taylor, Senel Idrisoglu, Peter Wilson, Timothy J. C. Bruxner, Kum Kum Khanna, Craig Nourse, Shivangi Wani, Angelika N. Christ, David Miller, Amy E. McCart Reed, Michael C.J. Quinn, Yock Ping Chow, Jodi M. Saunus, Suzanne Manning, and Peter Bailey

Subjects

medicine.medical_treatment, Cancer, Genomic signature, Biology, medicine.disease, Bioinformatics, Pathology and Forensic Medicine, Targeted therapy, Gene expression profiling, Breast cancer, ErbB, medicine, Cancer research, skin and connective tissue diseases, Exome, Brain metastasis

Abstract

Treatment options for patients with brain metastases (BMs) have limited efficacy and the mortality rate is virtually 100%. Targeted therapy is critically under-utilized, and our understanding of mechanisms underpinning metastatic outgrowth in the brain is limited. To address these deficiencies, we investigated the genomic and transcriptomic landscapes of 36 BMs from breast, lung, melanoma and oesophageal cancers, using DNA copy-number analysis and exome- and RNA-sequencing. The key findings were as follows. (a) Identification of novel candidates with possible roles in BM development, including the significantly mutated genes DSC2, ST7, PIK3R1 and SMC5, and the DNA repair, ERBB-HER signalling, axon guidance and protein kinase-A signalling pathways. (b) Mutational signature analysis was applied to successfully identify the primary cancer type for two BMs with unknown origins. (c) Actionable genomic alterations were identified in 31/36 BMs (86%); in one case we retrospectively identified ERBB2 amplification representing apparent HER2 status conversion, then confirmed progressive enrichment for HER2-positivity across four consecutive metastatic deposits by IHC and SISH, resulting in the deployment of HER2-targeted therapy for the patient. (d) In the ERBB/HER pathway, ERBB2 expression correlated with ERBB3 (r(2) = 0.496; p < 0.0001) and HER3 and HER4 were frequently activated in an independent cohort of 167 archival BM from seven primary cancer types: 57.6% and 52.6% of cases were phospho-HER3(Y1222) or phospho-HER4(Y1162) membrane-positive, respectively. The HER3 ligands NRG1/2 were barely detectable by RNAseq, with NRG1 (8p12) genomic loss in 63.6% breast cancer-BMs, suggesting a microenvironmental source of ligand. In summary, this is the first study to characterize the genomic landscapes of BM. The data revealed novel candidates, potential clinical applications for genomic profiling of resectable BMs, and highlighted the possibility of therapeutically targeting HER3, which is broadly over-expressed and activated in BMs, independent of primary site and systemic therapy.

Published

2015

3. Mixed ductal-lobular carcinomas: evidence for progression from ductal to lobular morphology

Author

Amy E, McCart Reed, Jamie R, Kutasovic, Katia, Nones, Jodi M, Saunus, Leonard, Da Silva, Felicity, Newell, Stephen, Kazakoff, Lewis, Melville, Janani, Jayanthan, Ana Cristina, Vargas, Lynne E, Reid, Jonathan, Beesley, Xiao Qing, Chen, Anne-Marie, Patch, David, Clouston, Alan, Porter, Elizabeth, Evans, John V, Pearson, Georgia, Chenevix-Trench, Margaret C, Cummings, Nicola, Waddell, Sunil R, Lakhani, and Peter T, Simpson

Subjects

Adult, DNA Mutational Analysis, Breast Neoplasms, clonality, breast cancer, Antigens, CD, Exome Sequencing, invasive lobular carcinoma, morphology, Biomarkers, Tumor, Humans, Genetic Predisposition to Disease, skin and connective tissue diseases, Aged, Aged, 80 and over, Comparative Genomic Hybridization, Original Paper, E‐cadherin, Middle Aged, Cadherins, Immunohistochemistry, Neoplasms, Complex and Mixed, Original Papers, body regions, Carcinoma, Intraductal, Noninfiltrating, Phenotype, Mutation, Disease Progression, Female, pathology, tumour heterogeneity, Breast Carcinoma In Situ, mixed ductal–lobular carcinoma

Abstract

Mixed ductal–lobular carcinomas (MDLs) show both ductal and lobular morphology, and constitute an archetypal example of intratumoural morphological heterogeneity. The mechanisms underlying the coexistence of these different morphological entities are poorly understood, although theories include that these components either represent ‘collision’ of independent tumours or evolve from a common ancestor. We performed comprehensive clinicopathological analysis of a cohort of 82 MDLs, and found that: (1) MDLs more frequently coexist with ductal carcinoma in situ (DCIS) than with lobular carcinoma in situ (LCIS); (2) the E‐cadherin–catenin complex was normal in the ductal component in 77.6% of tumours; and (3) in the lobular component, E‐cadherin was almost always aberrantly located in the cytoplasm, in contrast to invasive lobular carcinoma (ILC), where E‐cadherin is typically absent. Comparative genomic hybridization and multiregion whole exome sequencing of four representative cases revealed that all morphologically distinct components within an individual case were clonally related. The mutations identified varied between cases; those associated with a common clonal ancestry included BRCA2, TBX3, and TP53, whereas those associated with clonal divergence included CDH1 and ESR1. Together, these data support a model in which separate morphological components of MDLs arise from a common ancestor, and lobular morphology can arise via a ductal pathway of tumour progression. In MDLs that present with LCIS and DCIS, the clonal divergence probably occurs early, and is frequently associated with complete loss of E‐cadherin expression, as in ILC, whereas, in the majority of MDLs, which present with DCIS but not LCIS, direct clonal divergence from the ductal to the lobular phenotype occurs late in tumour evolution, and is associated with aberrant expression of E‐cadherin. The mechanisms driving the phenotypic change may involve E‐cadherin–catenin complex deregulation, but are yet to be fully elucidated, as there is significant intertumoural heterogeneity, and each case may have a unique molecular mechanism. © 2018 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.

Published

2017

4. Integrated genomic and transcriptomic analysis of human brain metastases identifies alterations of potential clinical significance

Author

Jodi M, Saunus, Michael C J, Quinn, Ann-Marie, Patch, John V, Pearson, Peter J, Bailey, Katia, Nones, Amy E, McCart Reed, David, Miller, Peter J, Wilson, Fares, Al-Ejeh, Mythily, Mariasegaram, Queenie, Lau, Teresa, Withers, Rosalind L, Jeffree, Lynne E, Reid, Leonard, Da Silva, Admire, Matsika, Colleen M, Niland, Margaret C, Cummings, Timothy J C, Bruxner, Angelika N, Christ, Ivon, Harliwong, Senel, Idrisoglu, Suzanne, Manning, Craig, Nourse, Ehsan, Nourbakhsh, Shivangi, Wani, Matthew J, Anderson, J Lynn, Fink, Oliver, Holmes, Stephen, Kazakoff, Conrad, Leonard, Felicity, Newell, Darrin, Taylor, Nick, Waddell, Scott, Wood, Qinying, Xu, Karin S, Kassahn, Vairavan, Narayanan, Nur Aishah, Taib, Soo-Hwang, Teo, Yock Ping, Chow, kConFab, Parmjit S, Jat, Sebastian, Brandner, Adrienne M, Flanagan, Kum Kum, Khanna, Georgia, Chenevix-Trench, Sean M, Grimmond, Peter T, Simpson, Nicola, Waddell, and Sunil R, Lakhani

Subjects

Receptor, ErbB-4, Receptor, ErbB-3, Brain Neoplasms, Receptor, ErbB-2, Gene Expression Profiling, DNA Mutational Analysis, Gene Amplification, Gene Dosage, Genomics, Ligands, Immunohistochemistry, Enzyme Activation, Gene Expression Regulation, Neoplastic, Phenotype, Predictive Value of Tests, Mutation, Biomarkers, Tumor, Tumor Microenvironment, Humans, Genetic Predisposition to Disease, Molecular Targeted Therapy, Phosphorylation, Precision Medicine, Protein Kinase Inhibitors, Genetic Association Studies

Abstract

Treatment options for patients with brain metastases (BMs) have limited efficacy and the mortality rate is virtually 100%. Targeted therapy is critically under-utilized, and our understanding of mechanisms underpinning metastatic outgrowth in the brain is limited. To address these deficiencies, we investigated the genomic and transcriptomic landscapes of 36 BMs from breast, lung, melanoma and oesophageal cancers, using DNA copy-number analysis and exome- and RNA-sequencing. The key findings were as follows. (a) Identification of novel candidates with possible roles in BM development, including the significantly mutated genes DSC2, ST7, PIK3R1 and SMC5, and the DNA repair, ERBB-HER signalling, axon guidance and protein kinase-A signalling pathways. (b) Mutational signature analysis was applied to successfully identify the primary cancer type for two BMs with unknown origins. (c) Actionable genomic alterations were identified in 31/36 BMs (86%); in one case we retrospectively identified ERBB2 amplification representing apparent HER2 status conversion, then confirmed progressive enrichment for HER2-positivity across four consecutive metastatic deposits by IHC and SISH, resulting in the deployment of HER2-targeted therapy for the patient. (d) In the ERBB/HER pathway, ERBB2 expression correlated with ERBB3 (r(2) = 0.496; p0.0001) and HER3 and HER4 were frequently activated in an independent cohort of 167 archival BM from seven primary cancer types: 57.6% and 52.6% of cases were phospho-HER3(Y1222) or phospho-HER4(Y1162) membrane-positive, respectively. The HER3 ligands NRG1/2 were barely detectable by RNAseq, with NRG1 (8p12) genomic loss in 63.6% breast cancer-BMs, suggesting a microenvironmental source of ligand. In summary, this is the first study to characterize the genomic landscapes of BM. The data revealed novel candidates, potential clinical applications for genomic profiling of resectable BMs, and highlighted the possibility of therapeutically targeting HER3, which is broadly over-expressed and activated in BMs, independent of primary site and systemic therapy.

Published

2015