Your search keyword '"Jessica C Pickles"' showing total 29 results

1. Recurrent adamantinomatous craniopharyngiomas show MAPK pathway activation, clonal evolution and rare TP53-loss-mediated malignant progression

Author

John R. Apps, Jose Mario Gonzalez-Meljem, Romain Guiho, Jessica C. Pickles, Eric Prince, Edward Schwalbe, Nikhil Joshi, Thomas J. Stone, Olumide Ogunbiyi, Jane Chalker, Akang Bassey, Georg Otto, Rosalind Davies, Debbie Hughes, Sebastian Brandner, Enrica Tan, Victoria Lee, Caroline Hayhurst, Cassie Kline, Sergi Castellano, Todd Hankinson, Timo Deutschbein, Thomas S. Jacques, and Juan Pedro Martinez-Barbera

Subjects

Craniopharyngioma, MAPK signalling pathway, MEK inhibitor, Macrophage/microglia, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract The two types of craniopharyngioma, adamantinomatous (ACP) and papillary (PCP), are clinically relevant tumours in children and adults. Although the biology of primary craniopharyngioma is starting to be unravelled, little is known about the biology of recurrence. To fill this gap in knowledge, we have analysed through methylation array, RNA sequencing and pERK1/2 immunohistochemistry a cohort of paired primary and recurrent samples (32 samples from 14 cases of ACP and 4 cases of PCP). We show the presence of copy number alterations and clonal evolution across recurrence in 6 cases of ACP, and analysis of additional whole genome sequencing data from the Children’s Brain Tumour Network confirms chromosomal arm copy number changes in at least 7/67 ACP cases. The activation of the MAPK/ERK pathway, a feature previously shown in primary ACP, is observed in all but one recurrent cases of ACP. The only ACP without MAPK activation is an aggressive case of recurrent malignant human craniopharyngioma harbouring a CTNNB1 mutation and loss of TP53. Providing support for a functional role of this TP53 mutation, we show that Trp53 loss in a murine model of ACP results in aggressive tumours and reduced mouse survival. Finally, we characterise the tumour immune infiltrate showing differences in the cellular composition and spatial distribution between ACP and PCP. Together, these analyses have revealed novel insights into recurrent craniopharyngioma and provided preclinical evidence supporting the evaluation of MAPK pathway inhibitors and immunomodulatory approaches in clinical trials in against recurrent ACP.

Published

2024

2. Pediatric pan-central nervous system tumor analysis of immune-cell infiltration identifies correlates of antitumor immunity

Author

Yura Grabovska, Alan Mackay, Patricia O’Hare, Stephen Crosier, Martina Finetti, Edward C. Schwalbe, Jessica C. Pickles, Amy R. Fairchild, Aimee Avery, Julia Cockle, Rebecca Hill, Janet Lindsey, Debbie Hicks, Mark Kristiansen, Jane Chalker, John Anderson, Darren Hargrave, Thomas S. Jacques, Karin Straathof, Simon Bailey, Chris Jones, Steven C. Clifford, and Daniel Williamson

Subjects

Science

Abstract

Here, using methylCIBERSORT, the authors characterize the tumour-immune microenvironment of paediatric central nervous system (CNS) tumours and its association with tumour type and prognosis. These findings suggest that immuno-methylomic profiling may inform immunotherapy approaches in paediatric patients with CNS tumour.

Published

2020

3. Supplementary Table S1 from Infant High-Grade Gliomas Comprise Multiple Subgroups Characterized by Novel Targetable Gene Fusions and Favorable Outcomes

Author

Chris Jones, David T.W. Jones, Thomas S. Jacques, David W. Ellison, Sergey Popov, David Capper, Maria Vinci, Andrea Carai, Angela Mastronuzzi, Suzanne J. Baker, Felix Sahm, Stefan M. Pfister, Christof M. Kramm, Andreas von Deimling, Lynley V. Marshall, Fernando Carceller, Darren R. Hargrave, Kristian Aquilina, Matthias A. Karajannis, David S. Ziegler, Mark J. Cowley, Maria Tsoli, Stephen P. Lowis, Timothy E.G. Hassall, Andrew S. Moore, Simon Bailey, Francesca Diomedi-Camassei, Giovanna Stefania Colafati, Evelina Miele, Clare Mitchell, Tabitha Bloom, Olaf Witt, Marc Zuckermann, Dominik Sturm, Barbara C. Worst, Lotte Hiddingh, Andrey Korshunov, Pablo Hernáiz Driever, Felipe Andreiuolo, Torsten Pietsch, Simone Hettmer, Kornelius Kerl, Winand N.M. Dinjens, Martin Ebinger, Martin U. Schuhmann, Jens Schittenhelm, Michael Karremann, Michael Capra, Jane B. Cryan, Michael Farrell, Petter Brandal, Thale Kristin Olsen, David A. Solomon, Monika Ashok Davare, Lissa Baird, Matthew D. Wood, Barbara Faganel Kotnik, Mara Popović, Shani Caspi, Ho-Keung Ng, Roger Packer, Irene Slavc, Christine Haberler, Matthias Preusser, Tobey J. Macdonald, Paula Z. Proszek, Debbie Hughes, Marc K. Rosenblum, Stephen W. Gilheeney, Ira J. Dunkel, Martin Sill, Simon P. Robinson, Jessica K.R. Boult, Rachael Natrajan, Claire Cairns, Bassel Zebian, Christopher Chandler, Safa Al-Sarraj, Lawrence J. Doey, Andrew J. Martin, Leslie Bridges, Matija Snuderl, David E. Kram, Uwe Kordes, Ulrich Schüller, Jeffrey Knipstein, Stephen Crosier, Mellissa Maybury, Catherine Rowe, Kathreena M. Kurian, Michael Hubank, Ji Wen, Wilda Orisme, James D. Dalton, Kelly Haupfear, Mark Kristiansen, Jane Chalker, Aimee Avery, Amy R. Fairchild, Alex Virasami, Louise Howell, Anna Burford, Valeria Molinari, Diana M. Carvalho, Sara Temelso, Elisa Izquierdo, Iris Stoler, Tejus A. Bale, Scott Newman, Ruth G. Tatevossian, Jessica C. Pickles, Britta Ismer, Alan Mackay, and Matthew Clarke

Abstract

Supplementary Table S1

Published

2023

4. Supplementary Data from Infant High-Grade Gliomas Comprise Multiple Subgroups Characterized by Novel Targetable Gene Fusions and Favorable Outcomes

Author

Chris Jones, David T.W. Jones, Thomas S. Jacques, David W. Ellison, Sergey Popov, David Capper, Maria Vinci, Andrea Carai, Angela Mastronuzzi, Suzanne J. Baker, Felix Sahm, Stefan M. Pfister, Christof M. Kramm, Andreas von Deimling, Lynley V. Marshall, Fernando Carceller, Darren R. Hargrave, Kristian Aquilina, Matthias A. Karajannis, David S. Ziegler, Mark J. Cowley, Maria Tsoli, Stephen P. Lowis, Timothy E.G. Hassall, Andrew S. Moore, Simon Bailey, Francesca Diomedi-Camassei, Giovanna Stefania Colafati, Evelina Miele, Clare Mitchell, Tabitha Bloom, Olaf Witt, Marc Zuckermann, Dominik Sturm, Barbara C. Worst, Lotte Hiddingh, Andrey Korshunov, Pablo Hernáiz Driever, Felipe Andreiuolo, Torsten Pietsch, Simone Hettmer, Kornelius Kerl, Winand N.M. Dinjens, Martin Ebinger, Martin U. Schuhmann, Jens Schittenhelm, Michael Karremann, Michael Capra, Jane B. Cryan, Michael Farrell, Petter Brandal, Thale Kristin Olsen, David A. Solomon, Monika Ashok Davare, Lissa Baird, Matthew D. Wood, Barbara Faganel Kotnik, Mara Popović, Shani Caspi, Ho-Keung Ng, Roger Packer, Irene Slavc, Christine Haberler, Matthias Preusser, Tobey J. Macdonald, Paula Z. Proszek, Debbie Hughes, Marc K. Rosenblum, Stephen W. Gilheeney, Ira J. Dunkel, Martin Sill, Simon P. Robinson, Jessica K.R. Boult, Rachael Natrajan, Claire Cairns, Bassel Zebian, Christopher Chandler, Safa Al-Sarraj, Lawrence J. Doey, Andrew J. Martin, Leslie Bridges, Matija Snuderl, David E. Kram, Uwe Kordes, Ulrich Schüller, Jeffrey Knipstein, Stephen Crosier, Mellissa Maybury, Catherine Rowe, Kathreena M. Kurian, Michael Hubank, Ji Wen, Wilda Orisme, James D. Dalton, Kelly Haupfear, Mark Kristiansen, Jane Chalker, Aimee Avery, Amy R. Fairchild, Alex Virasami, Louise Howell, Anna Burford, Valeria Molinari, Diana M. Carvalho, Sara Temelso, Elisa Izquierdo, Iris Stoler, Tejus A. Bale, Scott Newman, Ruth G. Tatevossian, Jessica C. Pickles, Britta Ismer, Alan Mackay, and Matthew Clarke

Abstract

Supplementary Figures and Legends

Published

2023

5. Data from Infant High-Grade Gliomas Comprise Multiple Subgroups Characterized by Novel Targetable Gene Fusions and Favorable Outcomes

Author

Chris Jones, David T.W. Jones, Thomas S. Jacques, David W. Ellison, Sergey Popov, David Capper, Maria Vinci, Andrea Carai, Angela Mastronuzzi, Suzanne J. Baker, Felix Sahm, Stefan M. Pfister, Christof M. Kramm, Andreas von Deimling, Lynley V. Marshall, Fernando Carceller, Darren R. Hargrave, Kristian Aquilina, Matthias A. Karajannis, David S. Ziegler, Mark J. Cowley, Maria Tsoli, Stephen P. Lowis, Timothy E.G. Hassall, Andrew S. Moore, Simon Bailey, Francesca Diomedi-Camassei, Giovanna Stefania Colafati, Evelina Miele, Clare Mitchell, Tabitha Bloom, Olaf Witt, Marc Zuckermann, Dominik Sturm, Barbara C. Worst, Lotte Hiddingh, Andrey Korshunov, Pablo Hernáiz Driever, Felipe Andreiuolo, Torsten Pietsch, Simone Hettmer, Kornelius Kerl, Winand N.M. Dinjens, Martin Ebinger, Martin U. Schuhmann, Jens Schittenhelm, Michael Karremann, Michael Capra, Jane B. Cryan, Michael Farrell, Petter Brandal, Thale Kristin Olsen, David A. Solomon, Monika Ashok Davare, Lissa Baird, Matthew D. Wood, Barbara Faganel Kotnik, Mara Popović, Shani Caspi, Ho-Keung Ng, Roger Packer, Irene Slavc, Christine Haberler, Matthias Preusser, Tobey J. Macdonald, Paula Z. Proszek, Debbie Hughes, Marc K. Rosenblum, Stephen W. Gilheeney, Ira J. Dunkel, Martin Sill, Simon P. Robinson, Jessica K.R. Boult, Rachael Natrajan, Claire Cairns, Bassel Zebian, Christopher Chandler, Safa Al-Sarraj, Lawrence J. Doey, Andrew J. Martin, Leslie Bridges, Matija Snuderl, David E. Kram, Uwe Kordes, Ulrich Schüller, Jeffrey Knipstein, Stephen Crosier, Mellissa Maybury, Catherine Rowe, Kathreena M. Kurian, Michael Hubank, Ji Wen, Wilda Orisme, James D. Dalton, Kelly Haupfear, Mark Kristiansen, Jane Chalker, Aimee Avery, Amy R. Fairchild, Alex Virasami, Louise Howell, Anna Burford, Valeria Molinari, Diana M. Carvalho, Sara Temelso, Elisa Izquierdo, Iris Stoler, Tejus A. Bale, Scott Newman, Ruth G. Tatevossian, Jessica C. Pickles, Britta Ismer, Alan Mackay, and Matthew Clarke

Abstract

Infant high-grade gliomas appear clinically distinct from their counterparts in older children, indicating that histopathologic grading may not accurately reflect the biology of these tumors. We have collected 241 cases under 4 years of age, and carried out histologic review, methylation profiling, and custom panel, genome, or exome sequencing. After excluding tumors representing other established entities or subgroups, we identified 130 cases to be part of an “intrinsic” spectrum of disease specific to the infant population. These included those with targetable MAPK alterations, and a large proportion of remaining cases harboring gene fusions targeting ALK (n = 31), NTRK1/2/3 (n = 21), ROS1 (n = 9), and MET (n = 4) as their driving alterations, with evidence of efficacy of targeted agents in the clinic. These data strongly support the concept that infant gliomas require a change in diagnostic practice and management.Significance:Infant high-grade gliomas in the cerebral hemispheres comprise novel subgroups, with a prevalence of ALK, NTRK1/2/3, ROS1, or MET gene fusions. Kinase fusion–positive tumors have better outcome and respond to targeted therapy clinically. Other subgroups have poor outcome, with fusion-negative cases possibly representing an epigenetically driven pluripotent stem cell phenotype.See related video: https://vimeo.com/438254885See related commentary by Szulzewsky and Cimino, p. 904.This article is highlighted in the In This Issue feature, p. 890

Published

2023

6. DNA methylation‐based classification of glioneuronal tumours synergises with histology and radiology to refine accurate molecular stratification

Author

Thomas J. Stone, Kshitij Mankad, Ai Peng Tan, Wajanat Jan, Jessica C. Pickles, Maria Gogou, Jane Chalker, Iwona Slodkowska, Emily Pang, Mark Kristiansen, Gaganjit K. Madhan, Leysa Forrest, Deborah Hughes, Eleni Koutroumanidou, Talisa Mistry, Olumide Ogunbiyi, Saira W. Ahmed, J. Helen Cross, Mike Hubank, Darren Hargrave, and Thomas S. Jacques

Subjects

Histology, Neurology, Physiology (medical), Neurology (clinical), Pathology and Forensic Medicine

Published

2023

7. Identifying cellular signalling molecules in developmental disorders of the brain: Evidence from focal cortical dysplasia and tuberous sclerosis

Author

Amy R Fairchild, Jessica C Pickles, François Guillemot, Martin Tisdall, Darren Hargrave, Dale Moulding, Simon M. L. Paine, Fatma Scerif, SA Yasin, Thomas S. Jacques, Simon R. Picker, Aimee Avery, Thomas J Stone, Yao-Feng Li, J. Helen Cross, Alex Virasami, and William Harkness

Subjects

0301 basic medicine, Cell type, Chemokine, Histology, Developmental Disabilities, Population, Cell, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Tuberous Sclerosis, Physiology (medical), Gene expression, medicine, Humans, education, PI3K/AKT/mTOR pathway, education.field_of_study, biology, Brain, Cortical dysplasia, medicine.disease, Immunohistochemistry, Hedgehog signaling pathway, Cell biology, Malformations of Cortical Development, 030104 developmental biology, medicine.anatomical_structure, Neurology, Malformations of Cortical Development, Group I, biology.protein, Neurology (clinical), 030217 neurology & neurosurgery, Signal Transduction

Abstract

Aims We understand little of the pathogenesis of developmental cortical lesions, because we understand little of the diversity of the cell types that contribute to the diseases or how those cells interact. We tested the hypothesis that cellular diversity and cell-cell interactions play an important role in these disorders by investigating the signalling molecules in the commonest cortical malformations that lead to childhood epilepsy, focal cortical dysplasia (FCD) and tuberous sclerosis (TS). Methods Transcriptional profiling clustered cases into molecularly distinct groups. Using gene expression data, we identified the secretory signalling molecules in FCD/TS and characterised the cell types expressing these molecules. We developed a functional model using organotypic cultures. Results We identified 113 up-regulated secretory molecules in FCDIIB/TS. The top 12 differentially expressed genes (DEGs) were validated by immunohistochemistry. This highlighted two molecules, Chitinase 3-like protein 1 (CHI3L1) and C-C motif chemokine ligand 2 (CCL2) (MCP1) that were expressed in a unique population of small cells in close proximity to balloon cells (BC). We then characterised these cells and developed a functional model in organotypic slice cultures. We found that the number of CHI3L1 and CCL2 expressing cells decreased following inhibition of mTOR, the main aberrant signalling pathway in TS and FCD. Conclusions Our findings highlight previously uncharacterised small cell populations in FCD and TS which express specific signalling molecules. These findings indicate a new level of diversity and cellular interactions in cortical malformations and provide a generalisable approach to understanding cell-cell interactions and cellular heterogeneity in developmental neuropathology.

Published

2021

8. DNA methylation changes from primary cultures through senescence-bypass in Syrian hamster fetal cells initially exposed to benzo[a]pyrene

Author

Daniel Desaulniers, Cathy Cummings-Lorbetskie, Karen Leingartner, Matthew J. Meier, Jessica C. Pickles, and Carole L. Yauk

Subjects

Toxicology

Published

2023

9. A rare case of paediatric astroblastoma with concomitant MN1 ‐ GTSE1 and EWSR1 ‐ PATZ1 gene fusions altering management

Author

Daniel Scoffings, Jessica C Pickles, Patrick S. Tarpey, Jamie Trotman, Thomas S. Jacques, Karan R Chadda, Sam Behjati, Andrew F. Dean, Kieren Allinson, Matthew J. Murray, and Katherine Holland

Subjects

0301 basic medicine, Unpredictable behaviour, Histology, business.industry, Astroblastoma, PATZ1 gene, Bioinformatics, medicine.disease, Pathology and Forensic Medicine, 03 medical and health sciences, Childhood Neoplasm, 030104 developmental biology, 0302 clinical medicine, Neurology, Paediatric cancer, Physiology (medical), Concomitant, Rare case, Medicine, Neurology (clinical), business, Who classification, 030217 neurology & neurosurgery

Abstract

Brain tumours are the commonest childhood neoplasm, with a worldwide incidence of 29.9-47.1/million (1). Childhood brain tumours carry substantial morbidity/mortality and are the largest cause of paediatric cancer deaths (2). Historically, classification was largely based on histological features. In recent years, expansion of high-resolution genomic, epigenetic and transcriptomic profiling has led to improved molecular understanding and categorisation, as well as targeted therapies (3). Consequently, the 2016 WHO classification incorporated molecular features in some brain tumour entities (4). According to this classification, astroblastomas are extremely rare, not formally graded, and listed under 'other gliomas'. Astroblastomas are generally treated by surgery alone but can display intermediate behaviour with high recurrence rates and unpredictable behaviour (5, 6). Controversy exists as to whether astroblastomas are a truly distinct entity as they have histological features in common with both astrocytomas and ependymomas (7-9). Diagnosing astroblastomas is therefore challenging and misclassification can alter subsequent management (8). The present case demonstrates how recent molecular advances identified a novel gene fusion for this patient, confirmed a more precise tumour diagnosis and guided subsequent management decisions. The findings here have general importance to other rare paediatric brain tumour entities.

Published

2021

10. DNA methylation-based profiling for paediatric CNS tumour diagnosis and treatment: a population-based study

Author

Martin Sill, Jessica C Pickles, Abigail F Peary, Mark Kristiansen, David T.W. Jones, Steven C. Clifford, Dariusz Ladon, David A Hilton, Darren Hargrave, SA Yasin, David Capper, Nitika Rathi, Aimee Avery, Olumide Ogunbiyi, Amy R Fairchild, Marie Edwards, Lawrence Doey, Kathreena M Kurian, G. Alistair Lammie, Chris Jones, Antonia Torgersen, Ashirwad Merve, Lorelle Brownlee, Rebecca M Hill, James A. R. Nicoll, Yura Grabovska, Azzam Ismail, Frances Rae, Thomas S. Jacques, Daniel Williamson, Aruna Chakrabarty, Clara Limback-Stanic, Tabitha Bloom, Safa Al-Sarraj, Jamie Gonzalez Zapata, Catherine Rowe, Leslie R. Bridges, Stefan M. Pfister, Carryl Dryden, Saira W. Ahmed, Khaja Syed, Lisa Wilkhu, Colin Smith, Thomas J Stone, Paul N Johns, Andreas von Deimling, Matthew Clarke, Clare Mitchell, and Jane Chalker

Subjects

Oncology, medicine.medical_specialty, Population, MEDLINE, Neuropathology, real world evidence, Central Nervous System Neoplasms, 03 medical and health sciences, 0302 clinical medicine, molecular pathology, 030225 pediatrics, Internal medicine, Biomarkers, Tumor, Developmental and Educational Psychology, Humans, Medicine, Molecular Targeted Therapy, 030212 general & internal medicine, Child, education, Telomerase, Retrospective Studies, neuropathology, education.field_of_study, business.industry, Molecular pathology, Neuropathologist, methylation array, DNA Methylation, Subtyping, paediatric brain tumours, Gene Expression Regulation, Neoplastic, methylation classifier, Pediatrics, Perinatology and Child Health, DNA methylation, Cohort, business, World Health Organisation

Abstract

Summary Background Marked variation exists in the use of genomic data in tumour diagnosis, and optimal integration with conventional diagnostic technology remains uncertain despite several studies reporting improved diagnostic accuracy, selection for targeted treatments, and stratification for trials. Our aim was to assess the added value of molecular profiling in routine clinical practice and the impact on conventional and experimental treatments. Methods This population-based study assessed the diagnostic and clinical use of DNA methylation-based profiling in childhood CNS tumours using two large national cohorts in the UK. In the diagnostic cohort—which included routinely diagnosed CNS tumours between Sept 1, 2016, and Sept 1, 2018—we assessed how the methylation profile altered or refined diagnosis in routine clinical practice and estimated how this would affect standard patient management. For the archival cohort of diagnostically difficult cases, we established how many cases could be solved using modern standard pathology, how many could only be solved using the methylation profile, and how many remained unsolvable. Findings Of 484 patients younger than 20 years with CNS tumours, 306 had DNA methylation arrays requested by the neuropathologist and were included in the diagnostic cohort. Molecular profiling added a unique contribution to clinical diagnosis in 107 (35%; 95% CI 30–40) of 306 cases in routine diagnostic practice—providing additional molecular subtyping data in 99 cases, amended the final diagnosis in five cases, and making potentially significant predictions in three cases. We estimated that it could change conventional management in 11 (4%; 95% CI 2–6) of 306 patients. Among 195 historically difficult-to-diagnose tumours in the archival cohort, 99 (51%) could be diagnosed using standard methods, with the addition of methylation profiling solving a further 34 (17%) cases. The remaining 62 (32%) cases were unresolved despite specialist pathology and methylation profiling. Interpretation Together, these data provide estimates of the impact that could be expected from routine implementation of genomic profiling into clinical practice, and indicate limitations where additional techniques will be required. We conclude that DNA methylation arrays are a useful diagnostic adjunct for childhood CNS tumours. Funding The Brain Tumour Charity, Children with Cancer UK, Great Ormond Street Hospital Children's Charity, Olivia Hodson Cancer Fund, Cancer Research UK, and the National Institute of Health Research.

Published

2020

11. Infant High-Grade Gliomas Comprise Multiple Subgroups Characterized by Novel Targetable Gene Fusions and Favorable Outcomes

Author

Michael Karremann, Olaf Witt, Tabitha Bloom, Winand N.M. Dinjens, Felipe Andreiuolo, Michael Farrell, Scott Newman, Simone Hettmer, James Dalton, Leslie R. Bridges, Jens Schittenhelm, Martin Ebinger, Thomas S. Jacques, Francesca Diomedi-Camassei, Dominik Sturm, Jane Chalker, Matija Snuderl, David W. Ellison, Paula Proszek, Irene Slavc, Matthias A. Karajannis, Giovanna Stefania Colafati, Louise Howell, Christine Haberler, Simon Bailey, Barbara C. Worst, David A. Solomon, Andrew J. Martin, Stefan M. Pfister, Maria Vinci, Ho Keung Ng, Kelly Haupfear, Mellissa Maybury, Stephen Gilheeney, Bassel Zebian, Martin Sill, David T.W. Jones, Pablo Hernáiz Driever, Martin U. Schuhmann, Angela Mastronuzzi, Jessica K.R. Boult, Matthew Clarke, Rachael Natrajan, Kornelius Kerl, Lawrence Doey, Alex Virasami, Andrey Korshunov, Christof M. Kramm, Jane Cryan, David E. Kram, Timothy E.G. Hassall, Debbie Hughes, Claire Mitchell, Chris Jones, Monika A. Davare, Evelina Miele, Safa Al-Sarraj, Sara Temelso, Catherine Rowe, Suzanne J. Baker, Sergey Popov, Torsten Pietsch, Matthew D. Wood, Roger J. Packer, Lynley V. Marshall, Michael Capra, Valeria Molinari, Diana Carvalho, Marc Zuckermann, Andreas von Deimling, Uwe Kordes, Kathreena M Kurian, Shani Caspi, Ira J. Dunkel, Wilda Orisme, Ulrich Schüller, Claire Cairns, Matthias Preusser, Kristian Aquilina, Petter Brandal, Stephen Lowis, Iris Stoler, Christopher Chandler, Lissa C. Baird, Marc K. Rosenblum, Ji Wen, Felix Sahm, Barbara Faganel Kotnik, Stephen Crosier, Mara Popović, Andrea Carai, Lotte Hiddingh, Thale Kristin Olsen, Fernando Carceller, Simon P. Robinson, Maria Tsoli, Ruth G. Tatevossian, Anna Burford, Mike Hubank, Elisa Izquierdo, Tejus Bale, David Capper, Andrew S. Moore, David S. Ziegler, Amy R Fairchild, Aimee Avery, Alan Mackay, Jessica C Pickles, Mark Kristiansen, Jeffrey Knipstein, Darren Hargrave, Mark J. Cowley, Tobey J. MacDonald, Britta Ismer, and Pathology

Subjects

0301 basic medicine, Oncology, Disease specific, medicine.medical_specialty, Population, Genome, Article, 03 medical and health sciences, 0302 clinical medicine, Text mining, Proto-Oncogene Proteins, Internal medicine, ROS1, medicine, Humans, education, Grading (tumors), Gene, Exome sequencing, education.field_of_study, business.industry, Receptor Protein-Tyrosine Kinases, Infant, Glioma, Protein-Tyrosine Kinases, Prognosis, 030104 developmental biology, Treatment Outcome, 030220 oncology & carcinogenesis, Gene Fusion, Neoplasm Grading, business

Abstract

Infant high-grade gliomas appear clinically distinct from their counterparts in older children, indicating that histopathologic grading may not accurately reflect the biology of these tumors. We have collected 241 cases under 4 years of age, and carried out histologic review, methylation profiling, and custom panel, genome, or exome sequencing. After excluding tumors representing other established entities or subgroups, we identified 130 cases to be part of an “intrinsic” spectrum of disease specific to the infant population. These included those with targetable MAPK alterations, and a large proportion of remaining cases harboring gene fusions targeting ALK (n = 31), NTRK1/2/3 (n = 21), ROS1 (n = 9), and MET (n = 4) as their driving alterations, with evidence of efficacy of targeted agents in the clinic. These data strongly support the concept that infant gliomas require a change in diagnostic practice and management. Significance: Infant high-grade gliomas in the cerebral hemispheres comprise novel subgroups, with a prevalence of ALK, NTRK1/2/3, ROS1, or MET gene fusions. Kinase fusion–positive tumors have better outcome and respond to targeted therapy clinically. Other subgroups have poor outcome, with fusion-negative cases possibly representing an epigenetically driven pluripotent stem cell phenotype. See related video: https://vimeo.com/438254885 See related commentary by Szulzewsky and Cimino, p. 904. This article is highlighted in the In This Issue feature, p. 890

Published

2020

12. Clinical outcomes, Kadish-INSICA staging and therapeutic targeting of somatostatin receptor 2 in olfactory neuroblastoma

Author

Matt Lechner, Yoko Takahashi, Mario Turri-Zanoni, Jacklyn Liu, Nicholas Counsell, Mario Hermsen, Raman Preet Kaur, Tianna Zhao, Murugappan Ramanathan, Volker H. Schartinger, Oscar Emanuel, Sam Helman, Jordan Varghese, Jozsef Dudas, Herbert Riechelmann, Susanne Sprung, Johannes Haybaeck, David Howard, Nils Wolfgang Engel, Sarah Stewart, Laura Brooks, Jessica C. Pickles, Thomas S. Jacques, Tim R. Fenton, Luke Williams, Francis M. Vaz, Paul O'Flynn, Paul Stimpson, Simon Wang, S. Alam Hannan, Samit Unadkat, Jonathan Hughes, Raghav Dwivedi, Cillian T. Forde, Premjit Randhawa, Simon Gane, Jonathan Joseph, Peter J. Andrews, Gary Royle, Alessandro Franchi, Roberta Maragliano, Simonetta Battocchio, Helen Bewicke-Copley, Christodoulos Pipinikas, Amy Webster, Chrissie Thirlwell, Debbie Ho, Andrew Teschendorff, Tianyu Zhu, Christopher D. Steele, Nischalan Pillay, Bart Vanhaesebroeck, Ahmed Mohyeldin, Juan Fernandez-Miranda, Ki Wan Park, Quynh-Thu Le, Robert B. West, Rami Saade, R. Peter Manes, Sacit Bulent Omay, Eugenia M. Vining, Benjamin L. Judson, Wendell G. Yarbrough, Maddalena Sansovini, Nicolini Silvia, Ilaria Grassi, Alberto Bongiovanni, David Capper, Ulrich Schüller, Selvam Thavaraj, Ann Sandison, Pavol Surda, Claire Hopkins, Marco Ferrari, Davide Mattavelli, Vittorio Rampinelli, Fabio Facchetti, Piero Nicolai, Paolo Bossi, Oswaldo A. Henriquez, Kelly Magliocca, C. Arturo Solares, Sarah K. Wise, Jose L. Llorente, Zara M. Patel, Jayakar V. Nayak, Peter H. Hwang, Peter D. Lacy, Robbie Woods, James P. O'Neill, Amrita Jay, Dawn Carnell, Martin D. Forster, Masaru Ishii, Nyall R. London, Diana M. Bell, Gary L. Gallia, Paolo Castelnuovo, Stefano Severi, Valerie J. Lund, and Ehab Y. Hanna

Subjects

Radioisotopes, Cancer Research, Radiotherapy, Nose Neoplasms, Esthesioneuroblastoma, Olfactory, Esthesioneuroblastoma, Prognosis, Article, Neuroblastoma, Oncology, Adjuvant, Diagnostic imaging, Human, Olfactory, Receptors, Somatostatin, SSTR2 protein, Positron-Emission Tomography, Humans, Receptors, Somatostatin, Nasal Cavity, Radionuclide Imaging, Retrospective Studies

Abstract

Introduction: olfactory neuroblastoma (ONB) is a rare cancer of the sinonasal region. We provide a comprehensive analysis of this malignancy with molecular and clinical trial data on a subset of our cohort to report on the potential efficacy of somatostatin receptor 2 (SSTR2)-targeting imaging and therapy.Methods: we conducted a retrospective analysis of 404 primary, locally recurrent, and metastatic olfactory neuroblastoma (ONB) patients from 12 institutions in the United States of America, United Kingdom and Europe. Clinicopathological characteristics and treatment approach were evaluated. SSTR2 expression, SSTR2-targeted imaging and the efficacy of peptide receptor radionuclide therapy [PRRT](177Lu-DOTATATE) were reported in a subset of our cohort (LUTHREE trial; NCT03454763).Results: dural infiltration at presentation was a significant predictor of overall survival (OS) and disease-free survival (DFS) in primary cases (n = 278). Kadish-Morita staging and Dulguerov T-stage both had limitations regarding their prognostic value. Multivariable survival analysis demonstrated improved outcomes with lower stage and receipt of adjuvant radiotherapy. Prophylactic neck irradiation significantly reduces the rate of nodal recurrence. 82.4% of the cohort were positive for SSTR2; treatment of three metastatic cases with SSTR2-targeted peptide-radionuclide receptor therapy (PRRT) in the LUTHREE trial was well-tolerated and resulted in stable disease (SD).Conclusions: this study presents pertinent clinical data from the largest dataset, to date, on ONB. We identify key prognostic markers and integrate these into an updated staging system, highlight the importance of adjuvant radiotherapy across all disease stages, the utility of prophylactic neck irradiation and the potential efficacy of targeting SSTR2 to manage disease.

Published

2022

13. Emergence and maintenance of actionable genetic drivers at medulloblastoma relapse

Author

Krzysztof Zakrzewski, Matthew Bashton, Louise Pease, Stacey Richardson, Yura Grabovksa, Maria Lastowska, Thomas S. Jacques, Rebecca M Hill, Nicolas André, Maria Vinci, Abhijit Joshi, Jordan R. Hansford, Christopher Kui, Stephen B. Wharton, Debbie Hicks, Jessica C Pickles, Edward C. Schwalbe, Vijay Ramaswamy, Mette Jorgensen, Steven C. Clifford, Claire Keeling, Stefan M. Pfister, Daniel Williamson, Dominique Figarella-Branger, Antony Michalski, Simon Bailey, Barry Pizer, Stephen Crosier, Michael D. Taylor, Janet C. Lindsey, Institut de neurophysiopathologie (INP), and Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Oncology, Cancer Research, medicine.medical_specialty, DNA Copy Number Variations, Selective maintenance, [SDV]Life Sciences [q-bio], Genomics, Biology, Gene mutation, medulloblastoma, subgroups, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, genomics, medicine, AcademicSubjects/MED00300, Humans, Copy-number variation, Cerebellar Neoplasms, 030304 developmental biology, relapse, Medulloblastoma, 0303 health sciences, C100, Wnt signaling pathway, drivers, A300, C400, medicine.disease, 3. Good health, Genetic divergence, 030220 oncology & carcinogenesis, Basic and Translational Investigations, Mutation, Cohort, AcademicSubjects/MED00310, Neurology (clinical), Neoplasm Recurrence, Local

Abstract

Background Less than 5% of medulloblastoma (MB) patients survive following failure of contemporary radiation-based therapies. Understanding the molecular drivers of medulloblastoma relapse (rMB) will be essential to improve outcomes. Initial genome-wide investigations have suggested significant genetic divergence of the relapsed disease. Methods We undertook large-scale integrated characterization of the molecular features of rMB—molecular subgroup, novel subtypes, copy number variation (CNV), and driver gene mutation. 119 rMBs were assessed in comparison with their paired diagnostic samples (n = 107), alongside an independent reference cohort sampled at diagnosis (n = 282). rMB events were investigated for association with outcome post-relapse in clinically annotated patients (n = 54). Results Significant genetic evolution occurred over disease-course; 40% of putative rMB drivers emerged at relapse and differed significantly between molecular subgroups. Non-infant MBSHH displayed significantly more chromosomal CNVs at relapse (TP53 mutation-associated). Relapsed MBGroup4 demonstrated the greatest genetic divergence, enriched for targetable (eg, CDK amplifications) and novel (eg, USH2A mutations) events. Importantly, many hallmark features of MB were stable over time; novel subtypes (>90% of tumors) and established genetic drivers (eg, SHH/WNT/P53 mutations; 60% of rMB events) were maintained from diagnosis. Critically, acquired and maintained rMB events converged on targetable pathways which were significantly enriched at relapse (eg, DNA damage signaling) and specific events (eg, 3p loss) predicted survival post-relapse. Conclusions rMB is characterised by the emergence of novel events and pathways, in concert with selective maintenance of established genetic drivers. Together, these define the actionable genetic landscape of rMB and provide a basis for improved clinical management and development of stratified therapeutics, across disease-course.

Published

2022

14. ATRT-20. Novel prognostic molecular signatures for improved risk-classification of Atypical Teratoid Rhabdoid Tumours

Author

Claire Keeling, Yura Grabovska, Patricia O'Hare, Stephen Crosier, Jessica C Pickles, Martina A Finetti, Amy R Fairchild, John Anderson, Darren Hargrave, Bernadette Brennan, Thomas S Jacques, Steven C Clifford, Simon Bailey, and Daniel Williamson

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

Malignant Rhabdoid Tumours (MRT) are aggressive paediatric malignancies seen in the central nervous system (Atypical Teratoid Rhabdoid Tumours (ATRT)), and kidney and other soft tissues (Extra-cranial Rhabdoid Tumours (ECRT)). With current therapies often proving ineffective and a lack of clear prognostic associations with consensus subgroups, we explored the possibility of using prognostic molecular signatures to further identify the biological characteristics of high risk ATRT patients. By employing a cross-validated feature selection method the methylation profiles of 121 MRT patients were analysed with clinical data to obtain meta-CpG signatures associated with prognosis for ATRT, ECRT and MRT. The relationship between these meta-CpG signatures and the consensus subgroups were further explored, along with the correlation of meta-CpGs with gene expression to establish biological significance. By selecting CpGs for their ability to predict survival this method obtained three novel prognostic methylation signatures which predict MRT outcome (ATRT-5, ECRT-14 and MRT-42). These signatures are independent of molecular subgroup and each signature was significantly associated with overall survival (OS) and event free survival (EFS) in their respective cohorts (p

Published

2022

15. A case series of Diffuse Glioneuronal Tumours with Oligodendroglioma-like features and Nuclear Clusters (DGONC)

Author

Leslie R. Bridges, David T.W. Jones, Darren Hargrave, Jane Chalker, Alice Rolland, Thomas S. Jacques, Talisa Mistry, Kshitij Mankad, Carryl Dryden, Felix Sahm, Simon M. L. Paine, Thomas J Stone, Amy R Fairchild, Fernando Carceller, Elisa Garimberti, Elwira Szychot, Mark Walker, Miren Aizpurua, Jessica C Pickles, Dilys Addy, and Olumide Ogunbiyi

Subjects

Male, 0301 basic medicine, DNA methylation classification, Pathology, medicine.medical_specialty, paediatric, glioneuronal tumour, Histology, Oligodendroglioma, monosomy 14, Biology, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Physiology (medical), medicine, Humans, brain tumour, Child, neoplasms, Ganglioglioma, Series (stratigraphy), Brain Neoplasms, medicine.disease, nervous system diseases, 030104 developmental biology, Neurology, Neurology (clinical), Monosomy 14, Scientific Correspondence, 030217 neurology & neurosurgery

Abstract

In this study, we report three paediatric cases of Diffuse Glioneuronal Tumours with Oligodendroglioma-like features and Nuclear Clusters (DGONC).

Published

2021

16. Therapeutic Implications of Improved Molecular Diagnostics for Rare CNS-Embryonal Tumor Entities: Results of an International, Retrospective, Observational Study

Author

Katja von Hoff, Christine Haberler, Felix Schmitt-Hoffner, Elizabeth Schepke, Teresa de Rojas, Sandra Jacobs, Michal Zapotocky, David Sumerauer, Marta Perek-Polnik, Christelle Dufour, Dannis von Vuurden, Irene Slavc, Johannes Gojo, Jessica C. Pickles, Nicolas U. Gerber, Maura Massimino, Maria Joao Gil-da-Costa, Miklos Garami, Ella Kumirova, Astrid Sehested, David Scheie, Ofelia Cruz, Lucas Moreno, Jaeho Cho, Bernward Zeller, Niels Bovenschen, Michael Grotzer, Daniel Alderete, Matija Snuderl, Olga Zheludkova, Andrey Golanov, Konstantin Okonechnikov, Martin Mynarek, B. Ole Juhnke, Stefan Rutkowski, Ulrich Schüller, Barry Pizer, Barbara von Zezschwitz, Robert Kwiecien, Maximilian Wechsung, Frank Konietschke, Eugene I. Hwang, Dominik Sturm, Stefan M. Pfister, Andreas von Deimling, Elisabeth J. Rushing, Marina Ryzhova, Peter Hauser, Maria Lastowska, Pieter Wesseling, Felice Giangaspero, Cynthia Hawkins, Dominique Figarella-Branger, Charles Eberhardt, Peter Burger, Marco Gessi, Andrey Korshunov, Tom S. Jacques, David Capper, Torsten Pietsch, and Marcel Kool

Published

2021

17. Therapeutic implications of improved molecular diagnostics for rare CNS embryonal tumor entities: results of an international, retrospective study

Author

Christelle Dufour, Johannes Gojo, Sandra Jacobs, Barry Pizer, Dominik Sturm, Torsten Pietsch, Stefan Rutkowski, Christine Haberler, Nicolas U. Gerber, Teresa de Rojas, Peter Hauser, Ulrich Schüller, Peter C. Burger, Marta Perek-Polnik, Martin Mynarek, Jaeho Cho, Matija Snuderl, Bernward Zeller, Michal Zapotocky, Maura Massimino, Robert Kwiecien, Dominique Figarella-Branger, Andrey Golanov, Charles G. Eberhart, Stefan M. Pfister, Daniel Alderete, Thomas S. Jacques, Ella Kumirova, Konstantin Okonechnikov, Astrid Sehested, Ofelia Cruz, Andrey Korshunov, Björn Ole Juhnke, Niels Bovenschen, Jessica C Pickles, David Sumerauer, Cynthia Hawkins, David Scheie, Eugene Hwang, Pieter Wesseling, Barbara von Zezschwitz, Felice Giangaspero, Marcel Kool, Elizabeth Schepke, Andreas von Deimling, Marco Gessi, Dannis G. van Vuurden, Maximilian Wechsung, Miklós Garami, David Capper, Katja von Hoff, Maria Joao Gil-da-Costa, Maria Łastowska, Felix Schmitt-Hoffner, Olga Zheludkova, Lucas Moreno, Michael A. Grotzer, Frank Konietschke, Marina Ryzhova, Elisabeth J. Rushing, Irene Slavc, Institut de neurophysiopathologie (INP), Centre National de la Recherche Scientifique (CNRS)-Aix Marseille Université (AMU), Laboratoire d'Anatomie Pathologique-Neuropathologique [AP-HM Hôpital La Timone], Hôpital de la Timone [CHU - APHM] (TIMONE), Pediatric surgery, CCA - Imaging and biomarkers, CCA - Cancer Treatment and quality of life, Pathology, and Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Oncology, Cancer Research, genetics [Central Nervous System Neoplasms], medicine.medical_treatment, [SDV]Life Sciences [q-bio], diagnosis [Central Nervous System Neoplasms], Central Nervous System Neoplasms, 0302 clinical medicine, CNS-PNET, Medicine, Neuroectodermal Tumors, Primitive, genetics [Neoplasms, Germ Cell and Embryonal], Pathology, Molecular, diagnosis [Brain Neoplasms], Brain Neoplasms, genetics [Neuroectodermal Tumors, Primitive], CNS embryonal tumor, Forkhead Transcription Factors, Neoplasms, Germ Cell and Embryonal, 3. Good health, therapy [Brain Neoplasms], therapy [Neoplasms, Germ Cell and Embryonal], 030220 oncology & carcinogenesis, DNA methylation, DNA methylation profiling, therapy [Central Nervous System Neoplasms], medicine.medical_specialty, CNS NB-FOXR2, ETMR, FOXR2 protein, human, 03 medical and health sciences, Glioma, Internal medicine, Neuroblastoma, Humans, ddc:610, diagnosis [Neuroectodermal Tumors, Primitive], Retrospective Studies, Chemotherapy, business.industry, Retrospective cohort study, medicine.disease, Molecular diagnostics, therapy [Neuroectodermal Tumors, Primitive], genetics [Brain Neoplasms], CNS Embryonal Tumor, Regimen, diagnosis [Neoplasms, Germ Cell and Embryonal], Neurology (clinical), business, Pediatric Neuro-Oncology, 030217 neurology & neurosurgery

Abstract

Background Only few data are available on treatment-associated behavior of distinct rare CNS embryonal tumor entities previously treated as “CNS-primitive neuroectodermal tumors” (CNS-PNET). Respective data on specific entities, including CNS neuroblastoma, FOXR2 activated (CNS NB-FOXR2), and embryonal tumors with multilayered rosettes (ETMR) are needed for development of differentiated treatment strategies. Methods Within this retrospective, international study, tumor samples of clinically well-annotated patients with the original diagnosis of CNS-PNET were analyzed using DNA methylation arrays (n = 307). Additional cases (n = 66) with DNA methylation pattern of CNS NB-FOXR2 were included irrespective of initial histological diagnosis. Pooled clinical data (n = 292) were descriptively analyzed. Results DNA methylation profiling of “CNS-PNET” classified 58 (19%) cases as ETMR, 57 (19%) as high-grade glioma (HGG), 36 (12%) as CNS NB-FOXR2, and 89(29%) cases were classified into 18 other entities. Sixty-seven (22%) cases did not show DNA methylation patterns similar to established CNS tumor reference classes. Best treatment results were achieved for CNS NB-FOXR2 patients (5-year PFS: 63% ± 7%, OS: 85% ± 5%, n = 63), with 35/42 progression-free survivors after upfront craniospinal irradiation (CSI) and chemotherapy. The worst outcome was seen for ETMR and HGG patients with 5-year PFS of 18% ± 6% and 22% ± 7%, and 5-year OS of 24% ± 6% and 25% ± 7%, respectively. Conclusion The historically reported poor outcome of CNS-PNET patients becomes highly variable when tumors are molecularly classified based on DNA methylation profiling. Patients with CNS NB-FOXR2 responded well to current treatments and a standard-risk CSI-based regimen may be prospectively evaluated. The poor outcome of ETMR across applied treatment strategies substantiates the necessity for evaluation of novel treatments.

Published

2021

18. Author response for 'A case series of Diffuse Glioneuronal Tumours with Oligodendroglioma-like features and Nuclear Clusters (DGONC)'

Author

Simon M. L. Paine, Miren Aizpurua, Thomas S. Jacques, Elisa Garimberti, David T. W. Jones, Mark Walker, Thomas J Stone, Felix Sahm, Alice Rolland, Olumide Ogunbiyi, Jessica C Pickles, Dilys Addy, Jane Chalker, Elwira Szychot, Carryl Dryden, Kshitij Mankad, Amy R Fairchild, Talisa Mistry, Fernando Carceller, Darren Hargrave, and Leslie R. Bridges

Subjects

Physics, Nuclear magnetic resonance, Series (mathematics), medicine, Oligodendroglioma, medicine.disease

Published

2020

19. Pediatric pan-central nervous system tumor analysis of immune-cell infiltration identifies correlates of antitumor immunity

Author

Janet C. Lindsey, Amy R Fairchild, Jane Chalker, Julia V. Cockle, Chris Jones, Aimee Avery, Darren Hargrave, Simon Bailey, Yura Grabovska, Martina Finetti, Alan Mackay, Edward C. Schwalbe, Karin Straathof, Stephen Crosier, Debbie Hicks, Thomas S. Jacques, Patricia O’Hare, Daniel Williamson, Jessica C Pickles, Rebecca M Hill, Mark Kristiansen, John Anderson, and Steven C. Clifford

Subjects

0301 basic medicine, Oncology, medicine.medical_treatment, General Physics and Astronomy, 02 engineering and technology, Central Nervous System Neoplasms, Cohort Studies, Histones, Cancer genomics, Leukocytes, Tumor Microenvironment, lcsh:Science, Child, Multidisciplinary, Glioma, 021001 nanoscience & nanotechnology, Prognosis, Phenotype, medicine.anatomical_structure, Child, Preschool, Cohort, Immunotherapy, 0210 nano-technology, Cell type, medicine.medical_specialty, Adolescent, Science, Central nervous system, General Biochemistry, Genetics and Molecular Biology, Article, Paediatric cancer, 03 medical and health sciences, Therapeutic approach, Immune system, Internal medicine, medicine, Humans, Rhabdoid Tumor, business.industry, General Chemistry, medicine.disease, B900, 030104 developmental biology, Mutation, lcsh:Q, business, Medulloblastoma

Abstract

Immune-therapy is an attractive alternative therapeutic approach for targeting central nervous system (CNS) tumors and the constituency of the Tumor Immune Microenvironment (TIME) likely to predict patient response. Here, we describe the TIME of >6000 primarily pediatric CNS tumors using a deconvolution approach (methylCIBERSORT). We produce and validate a custom reference signature defining 11 non-cancer cell types to estimate relative proportions of infiltration in a panCNS tumor cohort spanning 80 subtypes. We group patients into three broad immune clusters associated with CNS tumor types/subtypes. In cohorts of medulloblastomas (n = 2325), malignant rhabdoid tumors (n = 229) and pediatric high-grade gliomas (n = 401), we show significant associations with molecular subgroups/subtypes, mutations, and prognosis. We further identify tumor-specific immune clusters with phenotypic characteristics relevant to immunotherapy response (i.e. Cytolytic score, PDL1 expression). Our analysis provides an indication of the potential future therapeutic and prognostic possibilities of immuno-methylomic profiling in pediatric CNS tumor patients that may ultimately inform approach to immune-therapy., Here, using methylCIBERSORT, the authors characterize the tumour-immune microenvironment of paediatric central nervous system (CNS) tumours and its association with tumour type and prognosis. These findings suggest that immuno-methylomic profiling may inform immunotherapy approaches in paediatric patients with CNS tumour.

Published

2020

20. Methylation-based algorithms for diagnosis: experience from neuro-oncology

Author

Thomas J Stone, Jessica C Pickles, and Thomas S. Jacques

Subjects

0301 basic medicine, Molecular pathology, Neuro oncology, Astrocytoma, Methylation, DNA Methylation, medicine.disease, Pathology and Forensic Medicine, Dna methylation profiling, Central Nervous System Neoplasms, Gene Expression Regulation, Neoplastic, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, Biomarkers, Tumor, Profiling (information science), Humans, Pathology, Molecular, Algorithm, Pathological, Algorithms, Cause of death

Abstract

Brain tumours are the most common tumour-related cause of death in young people. Survivors are at risk of significant disability, at least in part related to the effects of treatment. Therefore, there is a need for a precise diagnosis that stratifies patients for the most suitable treatment, matched to the underlying biology of their tumour. Although traditional histopathology has been accurate in predicting treatment responses in many cases, molecular profiling has revealed a remarkable, previously unappreciated, level of biological complexity in the classification of these tumours. Among different molecular technologies, DNA methylation profiling has had the most pronounced impact on brain tumour classification. Furthermore, using machine learning-based algorithms, DNA methylation profiling is changing diagnostic practice. This can be regarded as an exemplar for how molecular pathology can influence diagnostic practice and illustrates some of the unanticipated benefits and risks. © 2020 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Published

2020

21. CNS embryonal tumours: WHO 2016 and beyond

Author

Cynthia Hawkins, Thomas S. Jacques, Torsten Pietsch, and Jessica C Pickles

Subjects

Oncology, medicine.medical_specialty, Pathology, Histology, Tumour heterogeneity, Central nervous system, Biology, World Health Organization, Pathology and Forensic Medicine, Central Nervous System Neoplasms, 03 medical and health sciences, 0302 clinical medicine, Physiology (medical), Internal medicine, medicine, Humans, Medulloblastoma, High mortality, Diagnostic test, Neoplasms, Germ Cell and Embryonal, medicine.disease, medicine.anatomical_structure, Atypical teratoid/rhabdoid tumour, Neurology, 030220 oncology & carcinogenesis, Neurology (clinical), Who classification, 030217 neurology & neurosurgery

Abstract

Embryonal tumours of the central nervous system (CNS) present a significant clinical challenge. Many of these neoplasms affect young children, have a very high mortality and therapeutic strategies are often aggressive with poor long-term outcomes. There is a great need to accurately diagnose embryonal tumours, predict their outcome and adapt therapy to the individual patient's risk. For the first time in 2016, the WHO classification took into account molecular characteristics for the diagnosis of CNS tumours. This integration of histological features with genetic information has significantly changed the diagnostic work-up and reporting of tumours of the CNS. However, this remains challenging in embryonal tumours due to their previously unaccounted tumour heterogeneity. We describe the recent revisions made to the 4th edition of the WHO classification of CNS tumours and review the main changes, while highlighting some of the more common diagnostic testing strategies.

Published

2018

22. 49 The biology of paediatric central nervous system tumours at post-mortem

Author

SA Yasin, Ashirwad Merve, Darren Hargrave, Jane Chalker, Jessica C Pickles, Izabella Smolicz, Thomas S. Jacques, Lisa Wilkhu, Thomas J Stone, Jamie Gonzalez Zapata, Brian Harding, Neil J. Sebire, and Amy Fairchild

Subjects

Oncology, medicine.medical_specialty, Palliative care, business.industry, Childhood cancer, Central nervous system, Histology, Autopsy, Time of death, medicine.anatomical_structure, Internal medicine, Cohort, Advanced disease, Medicine, business

Abstract

Background Central nervous system (CNS) tumours are the leading cause of childhood cancer deaths. There is little understanding of why tumours become untreatable but it is likely their biology changes over time and across space as they spread. One way to understand such advanced disease is to study the tumour biology at autopsy. We assembled a cohort of cases who had undergone autopsy for a childhood tumour. We assessed factors that could affect tumour biology in advanced disease and the feasibility of using archival post-mortem tissue with modern genomic technologies. Methods Cases were identified through BRAIN UK and local databases. Clinico-pathological data was analysed for local cases. Twenty-seven cases underwent DNA methylation array profiling and data was processed in R using the DKFZ CNS tumour classifier and Conumee package. Results We identified over 200 post-mortem paediatric CNS tumours across the UK. Among local cases (n=89), the median age was 3.8 years (range 0-31) and the median time between presentation and death was 4.5 months (range 0-144). At time of death, 46% of patients had not received cancer treatment compared to 54% who were receiving or had received treatment; 24% of patients were receiving palliative care. The cohort included a wide range of tumour types and origins. We had anticipated widespread dissemination in most cases but only in 68% of cases did the tumour infiltrate an area outside its origin. We could derive a confident diagnosis in 38% of cases using methylation data and in these, the molecular diagnosis matched the histology. Copy number changes could be interpreted in 81% of cases. Conclusions We established a diverse post-mortem paediatric CNS tumour cohort and demonstrated that both previously known and novel genomic aberrations could be identified within this tissue. Future work will investigate how advanced tumour biology changes in time and space.

Published

2019

23. A mechanistic evaluation of the Syrian hamster embryo cell transformation assay (pH 6.7) and molecular events leading to senescence bypass in SHE cells

Author

Jessica C Pickles, Andrew D. Scott, Lisa A. Mcginty, Hemad Yasaei, Terry Roberts, Robert F. Newbold, and Kamala Pant

Subjects

0301 basic medicine, Senescence, Syrian hamster, Health, Toxicology and Mutagenesis, CTA, cell transformation assay, Senescence bypass, Hamster, Biology, medicine.disease_cause, Article, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Cell transformation assay, CDKN2A, Cricetinae, medicine, Genetics, Animals, Mode of action, Cyclin-Dependent Kinase Inhibitor p16, Carcinogen, Mesocricetus, p16/CDKN2A, DNA Methylation, Phenotype, Molecular biology, Morphological transformation, Transformation (genetics), Cell Transformation, Neoplastic, 030104 developmental biology, SHE, syrian hamster embryo, SH, syrian hamster, 030220 oncology & carcinogenesis, Carcinogens, Carcinogenesis

Abstract

Highlights • Mechanistic evaluation of SHE CTA, specific to B(a)P. • Applicability of the Syrian hamster as a relevant model of carcinogenesis. • Molecular analysis of immortal lines derived from benzo(a)pyrene-induced MT clones. • Morphological transformation (MT) does not guarantee senescence bypass. • Secondary events to MT are necessary for cellular immortalisation., The implementation of the Syrian hamster embryo cell transformation assay (SHE CTA) into test batteries and its relevance in predicting carcinogenicity has been long debated. Despite prevalidation studies to ensure reproducibility and minimise the subjective nature of the assay’s endpoint, an underlying mechanistic and molecular basis supporting morphological transformation (MT) as an indicator of carcinogenesis is still missing. We found that only 20% of benzo(a)pyrene-induced MT clones immortalised suggesting that, alone, the MT phenotype is insufficient for senescence bypass. From a total of 12 B(a)P- immortalised MT lines, inactivating p53 mutations were identified in 30% of clones, and the majority of these were consistent with the potent carcinogen’s mode of action. Expression of p16 was commonly silenced or markedly reduced with extensive promoter methylation observed in 45% of MT clones, while Bmi1 was strongly upregulated in 25% of clones. In instances where secondary events to MT appeared necessary for senescence bypass, as evidenced by a transient cellular crisis, clonal growth correlated with monoallelic deletion of the CDKN2A/B locus. The findings further implicate the importance of p16 and p53 pathways in regulating senescence while providing a molecular evaluation of SHE CTA −derived variant MT clones induced by benzo(a)pyrene.

Published

2016

24. EMBR-15. DIAGNOSTIC RE-EVALUATION AND POOLED CLINICAL DATA ANALYSIS OF PATIENTS WITH PREVIOUS DIAGNOSIS OF CNS-PNET

Author

Nicolas U. Gerber, Peter C. Burger, Stefan M. Pfister, Stefan Rutkowski, Martin Mynarek, Irene Slavc, Theresa de Rojas, Dannis G. van Vuurden, David Capper, Dominique Figarella, Maria Joao Gil da Costa, David Sumerauer, Richard Grundy, Cynthia Hawkins, Dominik Sturm, Charles G. Eberhart, Katja von Hoff, Jaeho Cho, Jessica C Pickles, Eugene Hwang, Barry Pizer, Pieter Wesseling, Andrey Korshunov, Brent A. Orr, Christine Haberler, Peter Hauser, Amar Gajjar, Sandra Jacobs, Felice Giangaspero, Marcel Kool, Giles W. Robinson, Marco Gessi, Torsten Pietsch, Christelle Dufour, Maria Lastowska, Martha Perek, Thomas S. Jacques, and Matija Snuderl

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Cns pnet, business.industry, medicine.medical_treatment, Treatment outcome, medicine.disease, Radiation therapy, 03 medical and health sciences, Abstracts, 030104 developmental biology, 0302 clinical medicine, Text mining, Neuroblastoma, Internal medicine, Glioma, DNA methylation, Medicine, Neurology (clinical), Mn1 gene, business, 030217 neurology & neurosurgery

Abstract

CNS-PNET is no longer regarded a single disease but encompassed many distinct molecular entities. After removal of the term from the 2016 WHO classification of CNS tumours, diagnostic and therapeutic uncertainty remains. Through a world-wide collaboration, tumour samples from patients with the “historic” diagnosis of CNS-PNET were re-evaluated by DNA methylation profiling (n=405) and blinded neuropathological panel review (n=256). Clinical data on treatment and outcome were pooled with data on previously published patients. The given numbers represent preliminary data of the ongoing project. The re-evaluation by DNA methylation identified many distinct entities as expected, including high grade glioma (HGG, n=70), embryonal tumors with multilayered rosettes (ETMR, n=57) and CNS-neuroblastoma with FOXR2 alteration (CNS-NB-FOXR2, n=42) as the most frequent molecular diagnostic categories. Poor clinical outcome was confirmed for patients with HGG (5y-PFS 12%/5y-OS 12%, n=24), and ETMR (5y-PFS 12%/5y-OS 18%, n=62), while most patients with CNS-NB-FOXR2 survived (5y-PFS 52%/5y-OS 96%, n=31). Seven of 12 relapses/progressions of CNS-NB-FOXR2 occurred in radiotherapy-naïve patients. Classification into other newly described and less common entities included HGNET-MN1 (n=19), HGNET-BCOR (n=11), and EFT-CIC (n=13). Independent neuropathological review demonstrated that samples of these entities presented as non-embryonal tumours. Furthermore, marked clinical differences exist (HGNET-MN1: 5y-PFS 25%/5y-OS 95%, n=22; HGNET-BCOR: 5y-PFS 0%/5y-OS 44%, n=16; CNS-EFT-CIC: 5y-PFS 40%/5y-OS 60%, n=10). Our results show that implementation of DNA methylation profiling together with histopathological analysis will improve prospective diagnostic accuracy and facilitates the retrospective outcome analysis of treatment protocols used for this variety of biologically distinct entities.

Published

2018

25. ATRT-23. SMARCB1-DEPENDENCIES IN ATYPICAL TERATOID/RHABDOID TUMOURS: A STRATEGY FOR PRE-CLINICAL THERAPEUTIC TARGET IDENTIFICATION IN THE ABSENCE OF ACTIONABLE MUTATIONS

Author

Jessica C Pickles, Barry Pizer, Darren Hargrave, Steven C. Clifford, Thomas S. Jacques, Aimee Avery, James M Barker, Amanda Smith, Matthew Bashton, James A Wood, Daniel Williamson, Simon Bailey, Matthew Selby, Stephen Lowis, Alicia del Carpio Pons, Bernadette Brennan, Patricia O’Hare, Sarah Batting, Martina Finetti, Stephen Crosier, and Amy R Fairchild

Subjects

Cancer Research, Cyclin-dependent kinase 4, SMARCB1 Protein, Biology, Abstracts, Histone, Oncology, DNA methylation, Cancer research, biology.protein, CRISPR, Identification (biology), Neurology (clinical), SMARCB1, Gene

Abstract

ATRTs have low mutation rates and few classically-actionable variants to direct molecularly targeted therapies; loss of SMARCB1 is the sole recurrent mutational event in >90% of ATRTs. We have designed and implemented a genome-scale strategy for target identification and prioritization in tumors devoid of significant actionable mutations. Re-expression of SMARCB1 causes ATRT cells to cease proliferation and differentiate; we therefore hypothesized that identifying and counteracting critical downstream SMARCB1-dependent events represents a primary route to therapeutic intervention. We identify such events using an integrated genome-wide approach encompassing genome-scale CRISPR/Cas9 functional screens (GeCKO screening; 122,411 sgRNAs) alongside expression/DNA methylation profiling of primary ATRTs and ATRT cells following SMARCB1 re-expression and/or treatment with demethylating agents. Cross-referencing these analyses, we use a rational selection algorithm, to identify critical tumorigenic genes/pathways and proceed to validate their ability to be targeted as therapeutic targets. Our strategy identifies, ranks and prioritizes multiple SMARCB1-dependent pathways/genes functionally essential to ATRT, and characteristic of the primary tumour; including those previously described (Rb/CDK4/6, SHH, MYC), those less well evidenced (mTOR, TGF-β, HGF, Stat3/Jak) and novel SMARCB1-dependent synthetic lethalities (NuA4 complex, PIM1). We also describe the repressive genome-wide effect of SMARCB1 mutation on the transcriptome, through altered SWI/SNF binding, associated histone marks and localized hypermethylation and the therapeutic possibilities implied therein. Data and web-based interactive analysis and visualization tools will be made publically available to help guide and benchmark future pre-clinical testing in ATRT. This study pinpoints SMARCB1-dependent therapeutic susceptibilities in MRTs with the capacity to inform future treatment strategies.

Published

2018

26. Intra- and extra-cranial Malignant Rhabdoid Tumours share common location-independent clinical and molecular disease characteristics

Author

Aimee Avery, Amanda Smith, Amy R Fairchild, Darren Hargrave, Matthew Selby, Patricia O’Hare, Stephen Lowis, Jessica C Pickles, Steve Clifford, Bernadette Brennan, Barry Pizer, Edward C. Schwalbe, Daniel Williamson, Thomas S. Jacques, Simon Bailey, John Anderson, Yura Grabovska, Martina Finetti, and Stephen Crosier

Subjects

Pathology, medicine.medical_specialty, business.industry, Medicine, Molecular Disease, business

Published

2018

27. Early Wound Site Seeding in a Patient with Central Nervous System High-Grade Neuroepithelial Tumor with BCOR Alteration

Author

Aimee Avery, Kristian Aquilina, Matthew A. Kirkman, Thomas S. Jacques, Jessica C Pickles, Torsten Pietsch, and Amy R Fairchild

Subjects

Wound site, Male, medicine.medical_specialty, Central nervous system, Nerve Tissue Proteins, Resection, Central Nervous System Neoplasms, 03 medical and health sciences, 0302 clinical medicine, Proto-Oncogene Proteins, medicine, Humans, business.industry, Surgical wound, Magnetic Resonance Imaging, Neoplasms, Neuroepithelial, Neuroepithelial cell, Repressor Proteins, medicine.anatomical_structure, Ki-67 Antigen, Male patient, 030220 oncology & carcinogenesis, Child, Preschool, Disease Progression, Surgery, Neurology (clinical), Radiology, Surveillance imaging, business, Surgical incision, 030217 neurology & neurosurgery, Hydrocephalus

Abstract

Background Advances in molecular profiling have facilitated the emergence of newly defined entities of central nervous system (CNS) tumor, including CNS high-grade neuroepithelial tumor with BCOR alteration (CNS HGNET-BCOR). Relatively little is known about the clinical behavior of these newly characterized tumors. Case Description We describe a pediatric male patient with CNS HGNET-BCOR, who developed seeding of the tumor into the site of the surgical wound within months of surgery and who underwent resection of a residual posterior fossa tumor. Conclusions This case emphasizes 3 important points. First, CNS HGNET-BCOR can be aggressive tumors that necessitate close clinical and radiologic surveillance. Second, surveillance imaging in such cases should incorporate the surgical incision site into the field of view, and this should be closely scrutinized to ensure the timely detection of wound site seeding. Third, wound site seeding may still occur despite the use of meticulous surgical techniques.

Published

2018

28. ATRT-20. INTRA- AND EXTRA-CRANIAL MALIGNANT RHABDOID TUMOURS SHARE COMMON LOCATION-INDEPENDENT CLINICAL AND MOLECULAR DISEASE CHARACTERISTICS

Author

Bernadette Brennan, John Anderson, Daniel Williamson, Thomas S. Jacques, Jessica C Pickles, Yura Grabovska, Steven C. Clifford, Aimee Avery, Matthew Selby, Simon Bailey, Darren Hargrave, Amanda Smith, Barry Pizer, Amy R Fairchild, Martina Finetti, Stephen Crosier, Patricia O’Hare, and Edward C. Schwalbe

Subjects

Abstracts, Cancer Research, Pathology, medicine.medical_specialty, Text mining, Oncology, business.industry, Medicine, Molecular Disease, Neurology (clinical), business

Abstract

Atypical Teratoid/Rhabdoid Tumours (ATRT) are the CNS located members of a larger family of Malignant Rhabdoid Tumours (MRT); aggressive early childhood tumours characterised by biallelic inactivation of SMARCB1. ATRT and extra-cranial rhabdoid tumours (ECRT) are often treated as distinct entities therapeutically and in clinical/biological studies. We investigated to what extent this division is justified by the underlying molecular biology. RNA-Seq and methylation profiling of primary MRT was performed on 56 clinico-pathologically annotated tumour profiles from UK cancer centres and combined with published MRT data (n=394) in a meta-analysis. To characterise the common biological features of MRT regardless of location, differential expression, methylation, gene/pathway analyses were compared to other paediatric embryonal tumour expression (n=1073) and methylation (n=520) profiles (i.e. Medulloblastoma, Ewings Sarcoma, Rhabdomyosarcoma, Wilms tumour and Neuroblastoma). Clustering all MRT together recapitulates the subgroups observed in ATRT alone; broadly overlapping with recently published 3 ATRT subgroup models. We further describe a putative expanded subgrouping model encompassing all MRT. While expression, methylation, genetic and clinico-pathological differences by anatomical site are observed these are not innate but rather differences between ATRT and ECRT may be explained by differences in the molecular subgroup membership. We propose that anatomical site does not exclusively predetermine subgroup identity and that the overarching SMARCB1-dependent genetic, epigenetic and transcriptomic commonality is the “main event” in MRT tumorigenesis. Our findings demonstrate a need for common therapeutic approaches and targeting strategies across all MRTs, irrespective of location; these findings have important implications for clinical trial planning and future research studies.

Published

2018

29. Carcinogen-specific mutational and epigenetic alterations in INK4A, INK4B and p53 tumour-suppressor genes drive induced senescence bypass in normal diploid mammalian cells

Author

Hemad Yasaei, E Gilham, Michael R. O’Donovan, Jessica C Pickles, Robert F. Newbold, and Terry Roberts

Subjects

Senescence, Cancer Research, Biology, Cell Line, law.invention, Nickel, law, Cricetinae, Benzo(a)pyrene, Genetics, Animals, Humans, Epigenetics, Molecular Biology, Gene, Cellular Senescence, Cyclin-Dependent Kinase Inhibitor p16, Carcinogen, Cyclin-Dependent Kinase Inhibitor p15, Mesocricetus, Epithelial Cells, Genes, p53, Cell biology, Mutation, Carcinogens, Suppressor, Tumor Suppressor Protein p53, Ploidy, Gene Deletion

Abstract

Immortalization (senescence bypass) is a critical rate-limiting step in the malignant transformation of mammalian somatic cells. Human cells must breach at least two distinct senescence barriers to permit unfettered clonal evolution during cancer development: (1) stress- or oncogene-induced premature senescence (SIPS/OIS), mediated via the p16-Rb and/or ARF-p53-p21 tumour-suppressive pathways, and (2) replicative senescence triggered by telomere shortening. In contrast, because their telomerase is constitutively active, cells from small rodents possess only the SIPS/OIS barrier, and are therefore useful for studying SIPS/OIS bypass in isolation. Dermal fibroblasts from the Syrian hamster (SHD cells) are exceptionally resistant to spontaneous SIPS bypass, but it can be readily induced following exposure to a wide range of chemical and physical carcinogens. Here we show that a spectrum of carcinogen-specific mutational and epigenetic alterations involving the INK4A (p16), p53 and INK4B (p15) genes are associated with induced SIPS bypass. With ionizing radiation, immortalization is invariably accompanied by efficient biallelic deletion of the complete INK4/CDKN2 locus. In comparison, SHD cells immortalized by the powerful polycyclic hydrocarbon carcinogen benzo(a)pyrene display transversion point mutations in the DNA-binding domain of p53 coupled with INK4 alterations such as loss of expression of p15. Epimutational silencing of p16 is the primary event associated with immortalization by nickel, a human non-genotoxic carcinogen. As SIPS/OIS bypass is a prerequisite for the immortalization of normal diploid human epithelial cells, our results with the SHD model will provide a basis for delineating combinations of key molecular changes underpinning this important event in human carcinogenesis.

Published

2012