Your search keyword '"Rachel, de la Rue"' showing total 8 results

1. Randomized Controlled Trial of the Gastrin/CCK

Author

Julian A, Abrams, Armando, Del Portillo, Caitlin, Hills, Griselda, Compres, Richard A, Friedman, Bin, Cheng, John, Poneros, Charles J, Lightdale, Rachel, De La Rue, Massimiliano, di Pietro, Rebecca C, Fitzgerald, Antonia, Sepulveda, and Timothy C, Wang

Subjects

Male, Benzodiazepinones, Esophageal Mucosa, Esophageal Neoplasms, Phenylurea Compounds, Adenocarcinoma, Middle Aged, Receptor, Cholecystokinin B, Article, Barrett Esophagus, Double-Blind Method, Gastrins, Biomarkers, Tumor, Humans, Female, Esophagoscopy, Aged, Cell Proliferation

Abstract

Hypergastrinemia has been associated with high grade dysplasia and adenocarcinoma in patients with Barrett’s esophagus (BE), and experimental studies suggest pro-inflammatory and pro-neoplastic effects of gastrin on BE. This is of potential concern, as BE patients are treated with medications that suppress gastric acid production, resulting in increased physiologic levels of gastrin. We aimed to determine whether treatment with the novel gastrin/CCK(2) receptor antagonist netazepide reduces expression of markers associated with inflammation and neoplasia in BE. This was a randomized, double-blind, placebo-controlled trial of netazepide in patients with BE without dysplasia. Subjects were treated for 12 weeks, with endoscopic assessment at baseline and at end of treatment. The primary outcome was within-individual change in cellular proliferation as assessed by Ki67. Secondary analyses included changes in gene expression, assessed by RNA-sequencing, and safety and tolerability. A total of 20 subjects completed the study and were included in the analyses. There was no difference between arms in mean change in cellular proliferation (netazepide: +35.6 Ki67+ cells/ mm(2), SD 620.7; placebo: +307.8 Ki67+ cells/ mm(2), SD 640.3; p=0.35). Netazepide treatment resulted in increased expression of genes related to gastric phenotype (TFF2, MUC5B) and certain cancer-associated markers (REG3A, PAX9, MUC1), and decreased expression of intestinal markers MUC2, FABP1, FABP2, and CDX1. No serious adverse events related to study drug occurred. The gastrin/CCK(2) receptor antagonist netazepide did not reduce cellular proliferation in patients with non-dysplastic BE. Further research should focus on the biological effects of gastrin in Barrett’s esophagus.

Published

2021

2. Genomic copy number predicts esophageal cancer years before transformation

Author

Eleanor Gregson, Sarah Killcoyne, Rebecca C. Fitzgerald, Dan J. Woodcock, Sujath Abbas, Rachel de la Rue, Moritz Gerstung, Adrienn Blasko, Aikaterini Varanou Jenkins, David C. Wedge, Cassandra Kosmidou, Matthew D. Eldridge, Ahmad Miremadi, Wladyslaw Januszewicz, Fitzgerald, Rebecca [0000-0002-3434-3568], Eldridge, Matthew [0000-0002-5799-8911], Abbas, Sujath [0000-0002-2541-4969], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Oncology, Male, medicine.medical_specialty, DNA Copy Number Variations, Esophageal Neoplasms, Biopsy, Aneuploidy, Gene mutation, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Barrett Esophagus, 0302 clinical medicine, Internal medicine, Cancer screening, Medicine, Humans, Esophagus, Aged, medicine.diagnostic_test, Manchester Cancer Research Centre, Whole Genome Sequencing, business.industry, Genome, Human, ResearchInstitutes_Networks_Beacons/mcrc, General Medicine, Genomics, Esophageal cancer, Middle Aged, medicine.disease, Human genetics, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Histopathology, Female, business, Precancerous Conditions

Abstract

Recent studies show that aneuploidy and driver gene mutations precede cancer diagnosis by many years1–4. We assess whether these genomic signals can be used for early detection and pre-emptive cancer treatment using the neoplastic precursor lesion Barrett’s esophagus as an exemplar5. Shallow whole-genome sequencing of 777 biopsies, sampled from 88 patients in Barrett’s esophagus surveillance over a period of up to 15 years, shows that genomic signals can distinguish progressive from stable disease even 10 years before histopathological transformation. These findings are validated on two independent cohorts of 76 and 248 patients. These methods are low-cost and applicable to standard clinical biopsy samples. Compared with current management guidelines based on histopathology and clinical presentation, genomic classification enables earlier treatment for high-risk patients as well as reduction of unnecessary treatment and monitoring for patients who are unlikely to develop cancer. Longitudinal molecular profiling of copy number alterations in patients with Barrett’s esophagus can identify patients at higher risk of developing esophageal cancer.

Published

2020

3. Identification of subtypes of Barrett's esophagus and esophageal adenocarcinoma based on DNA methylation profiles and integration of transcriptome and genome data

Author

Timothy J. Underwood, Sujath Abbas, Rachel de la Rue, Jason Crawte, Juliane Perner, Richard C. Turkington, Paul A.W. Edwards, Sriganesh Jammula, Fergus Noble, Hugh Barr, Andy G. Lynch, Sari Suortamo, Catherine Harden, Vijayendran Sujendran, Maria Secrier, Sonia Puig, Sarah Oakes, Francesca D. Ciccarelli, Daniele Biasci, Monika Tripathi, Peter Safranek, Krishna Moorthy, Jim Davies, Constanza Linossi, Ula Mahadeva, Jan Bornschein, Richard Berrisford, Ted R. Hupp, Shaun R. Preston, Ayesha Noorani, Xiaodun Li, Michael Scott, Barbara Nutzinger, Annalise Katz-Summercorn, Neil A. Shepherd, Elwira Fidziukiewicz, Charles Crichton, Philippe Taniere, Adrienn Blasko, Amber Grantham, John H. Saunders, Michael P. Lewis, Caitriona Hughes, Ahmad Miremadi, Grant Sanders, Andrew D Beggs, Sharmila Sothi, Shona MacRae, Simon Tavaré, Ginny Devonshire, Sarah Killcoyne, Lawrence Bower, Christopher J. Peters, James A. Gossage, Shalini Malhotra, Laszlo Igali, Suzy Lishman, Philip Kaye, Simon L. Parsons, Alex Northrop, J. Robert O’Neill, Gianmarco Contino, Nicola Grehan, Maria O'Donovan, Olga Tucker, Elizabeth C Smyth, Yeng Ang, Irshad Soomro, Vinod V. Subash, Andrew Hindmarsh, Jesper Lagergren, Anna M. Grabowska, Izhar Bagwan, Andrew Davies, Rehan Haidry, Fuju Chang, Bhaskar Kumar, Jack Owsley, Rebecca C. Fitzgerald, Laurence Lovat, George B. Hanna, Matthew D. Eldridge, Stephen J. Hayes, J Zylstra, Vicky Goh, Richard J E Skipworth, Nick Carroll, Matthew Eldridge, Vicki Save, Ed Cheong, Filip Wronowski, Oliver Old, Biasci, Daniele [0000-0003-3148-8152], Abbas, Sujath [0000-0002-2541-4969], Eldridge, Matthew [0000-0002-5799-8911], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Epigenomics, Male, Esophageal Mucosa, Esophageal Neoplasms, gene repression, RNA-Seq, Antineoplastic Agents, Biology, Adenocarcinoma, Article, Epigenesis, Genetic, Transcriptome, 03 medical and health sciences, Barrett Esophagus, 0302 clinical medicine, Gene duplication, Cyclin E, Temozolomide, Humans, Epigenetics, prognostic factor, Promoter Regions, Genetic, Gene, Aged, Retrospective Studies, Oncogene Proteins, Hepatology, Whole Genome Sequencing, Gastroenterology, Gene Amplification, Methylation, DNA Methylation, Middle Aged, antitumor immune response, Gene Expression Regulation, Neoplastic, 030104 developmental biology, CpG site, DNA methylation, Cancer research, Disease Progression, response to treatment, 030211 gastroenterology & hepatology, Female

Abstract

BACKGROUND & AIMS: Esophageal adenocarcinomas (EACs) are heterogeneous and often preceded by Barrett's esophagus (BE). Many genomic changes have been associated with development of BE and EAC, but little is known about epigenetic alterations. We performed epigenetic analyses of BE and EAC tissues and combined these data with transcriptome and genomic data to identify mechanisms that control gene expression and genome integrity.METHODS: In a retrospective cohort study, we collected tissue samples and clinical data from 150 BE and 285 EAC cases from the Oesophageal Cancer Classification and Molecular Stratification consortium in the United Kingdom. We analyzed methylation profiles of all BE and EAC tissues and assigned them to subgroups using non-negative matrix factorization with k-means clustering. Data from whole-genome sequencing and transcriptome studies were then incorporated; we performed integrative methylation and RNA-sequencing analyses to identify genes that were suppressed with increased methylation in promoter regions. Levels of different immune cell types were computed using single-sample gene set enrichment methods. We derived 8 organoids from 8 EAC tissues and tested their sensitivity to different drugs.RESULTS: BE and EAC samples shared genome-wide methylation features, compared with normal tissues (esophageal, gastric, and duodenum; controls) from the same patients and grouped into 4 subtypes. Subtype 1 was characterized by DNA hypermethylation with a high mutation burden and multiple mutations in genes in cell cycle and receptor tyrosine signaling pathways. Subtype 2 was characterized by a gene expression pattern associated with metabolic processes (ATP synthesis and fatty acid oxidation) and lack methylation at specific binding sites for transcription factors; 83% of samples of this subtype were BE and 17% were EAC. The third subtype did not have changes in methylation pattern, compared with control tissue, but had a gene expression pattern that indicated immune cell infiltration; this tumor type was associated with the shortest time of patient survival. The fourth subtype was characterized by DNA hypomethylation associated with structure rearrangements, copy number alterations, with preferential amplification of CCNE1 (cells with this gene amplification have been reported to be sensitive to CDK2 inhibitors). Organoids with reduced levels of MGMT and CHFR expression were sensitive to temozolomide and taxane drugs.CONCLUSIONS: In a comprehensive integrated analysis of methylation, transcriptome, and genome profiles of more than 400 BE and EAC tissues, along with clinical data, we identified 4 subtypes that were associated with patient outcomes and potential responses to therapy.

Published

2020

4. Genomic copy number predicts esophageal cancer years before transformation

Author

Sarah, Killcoyne, Eleanor, Gregson, David C, Wedge, Dan J, Woodcock, Matthew D, Eldridge, Rachel, de la Rue, Ahmad, Miremadi, Sujath, Abbas, Adrienn, Blasko, Cassandra, Kosmidou, Wladyslaw, Januszewicz, Aikaterini Varanou, Jenkins, Moritz, Gerstung, and Rebecca C, Fitzgerald

Subjects

Male, DNA Copy Number Variations, Esophageal Neoplasms, Whole Genome Sequencing, Genome, Human, Biopsy, Genomics, Middle Aged, Aneuploidy, Barrett Esophagus, Humans, Female, Precancerous Conditions, Aged

Abstract

Recent studies show that aneuploidy and driver gene mutations precede cancer diagnosis by many years

Published

2020

5. Genomic copy number predicts oesophageal cancer years before transformation

Author

Dan J. Woodcock, Rachel de la Rue, Wladyslaw Januszewicz, Eleanor Gregson, David C. Wedge, Matthew D. Eldridge, Moritz Gerstung, Sujath Abbas, Adrienn Blasko, Ahmad Miremadi, Sarah Killcoyne, Rebecca C. Fitzgerald, and Aikaterini Varanou Jenkins

Subjects

Whole genome sequencing, Oncology, medicine.medical_specialty, Manchester Cancer Research Centre, business.industry, ResearchInstitutes_Networks_Beacons/mcrc, Cancer, Early detection, Gene mutation, medicine.disease, Somatic evolution in cancer, Stable Disease, Internal medicine, medicine, DISEASE TRANSFORMATION, Risk classification, business

Abstract

SummaryCancer arises through a process of somatic evolution and recent studies have shown that aneuploidies and driver gene mutations precede cancer diagnosis by several years to decades1–4 Here, we address the question whether such genomic signals can be used for early detection and pre-emptive cancer treatment. To this end we study Barrett’s oesophagus, a genomic copy number driven neoplastic precursor lesion to oesophageal adenocarcinoma5. We use shallow whole genome sequencing of 777 biopsies sampled from 88 patients in surveillance for Barrett’s oesophagus over a period of up to 15 years. These data show that genomic signals exist that distinguish progressive from stable disease with an AUC of 0.87 and a sensitivity of 50% even ten years prior to histopathological disease transformation. These finding are validated on two independent cohorts of 75 and 248 patients. Compared against current patient management guidelines genomic risk classification enables earlier treatment for high risk patients as well as reduction of unnecessary treatment and monitoring for patients who are unlikely to develop cancer.

Published

2020

6. Machine learning to predict early recurrence after oesophageal cancer surgery

Author

S A Rahman, R C Walker, M A Lloyd, B L Grace, G I van Boxel, B F Kingma, J P Ruurda, R van Hillegersberg, S Harris, S Parsons, S Mercer, E A Griffiths, J R O'Neill, R Turkington, R C Fitzgerald, T J Underwood, Ayesha Noorani, Rachael Fels Elliott, Paul A W Edwards, Nicola Grehan, Barbara Nutzinger, Jason Crawte, Hamza Chettouh, Gianmarco Contino, Xiaodun Li, Eleanor Gregson, Sebastian Zeki, Rachel de la Rue, Shalini Malhotra, Simon Tavaré, Andy G Lynch, Mike L Smith, Jim Davies, Charles Crichton, Nick Carroll, Peter Safranek, Andrew Hindmarsh, Vijayendran Sujendran, Stephen J Hayes, Yeng Ang, Shaun R Preston, Sarah Oakes, Izhar Bagwan, Vicki Save, Richard J E Skipworth, Ted R Hupp, J Robert O'Neill, Olga Tucker, Andrew Beggs, Philippe Taniere, Sonia Puig, Timothy J Underwood, Fergus Noble, James P Byrne, Jamie J Kelly, Jack Owsley, Hugh Barr, Neil Shepherd, Oliver Old, Jesper Lagergren, James Gossage, Andrew Davies Fuju Chang, Janine Zylstra, Vicky Goh, Francesca D Ciccarelli, Grant Sanders, Richard Berrisford, Catherine Harden, David Bunting, Mike Lewis, Ed Cheong, Bhaskar Kumar, Simon L Parsons, Irshad Soomro, Philip Kaye, John Saunders, Laurence Lovat, Rehan Haidry, Victor Eneh, Laszlo Igali, Michael Scott, Shamila Sothi, Sari Suortamo, Suzy Lishman, George B Hanna, Christopher J Peters, and Anna Grabowska

Subjects

Male, Esophageal Neoplasms, Lymphovascular invasion, medicine.medical_treatment, 030230 surgery, computer.software_genre, Machine Learning, 0302 clinical medicine, Upper GI, Neoadjuvant therapy, Aged, 80 and over, Incidence (epidemiology), General Medicine, Middle Aged, Esophageal cancer, Regression, Random forest, Oncology, Esophagectomy, Area Under Curve, 030220 oncology & carcinogenesis, Cohort, Adenocarcinoma, Female, Original Article, Elastic net regularization, Adult, medicine.medical_specialty, Early Recurrence, Machine learning, Risk Assessment, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Clinical Decision Rules, medicine, Humans, Aged, Ensemble forecasting, Receiver operating characteristic, business.industry, General surgery, Original Articles, medicine.disease, ROC Curve, Surgery, Artificial intelligence, Neoplasm Recurrence, Local, business, computer, Cancer surgery

Abstract

Background Early cancer recurrence after oesophagectomy is a common problem, with an incidence of 20–30 per cent despite the widespread use of neoadjuvant treatment. Quantification of this risk is difficult and existing models perform poorly. This study aimed to develop a predictive model for early recurrence after surgery for oesophageal adenocarcinoma using a large multinational cohort and machine learning approaches. Methods Consecutive patients who underwent oesophagectomy for adenocarcinoma and had neoadjuvant treatment in one Dutch and six UK oesophagogastric units were analysed. Using clinical characteristics and postoperative histopathology, models were generated using elastic net regression (ELR) and the machine learning methods random forest (RF) and extreme gradient boosting (XGB). Finally, a combined (ensemble) model of these was generated. The relative importance of factors to outcome was calculated as a percentage contribution to the model. Results A total of 812 patients were included. The recurrence rate at less than 1 year was 29·1 per cent. All of the models demonstrated good discrimination. Internally validated areas under the receiver operating characteristic (ROC) curve (AUCs) were similar, with the ensemble model performing best (AUC 0·791 for ELR, 0·801 for RF, 0·804 for XGB, 0·805 for ensemble). Performance was similar when internal–external validation was used (validation across sites, AUC 0·804 for ensemble). In the final model, the most important variables were number of positive lymph nodes (25·7 per cent) and lymphovascular invasion (16·9 per cent). Conclusion The model derived using machine learning approaches and an international data set provided excellent performance in quantifying the risk of early recurrence after surgery, and will be useful in prognostication for clinicians and patients., Early recurrence after surgery for adenocarcinoma of the oesophagus is common. A risk prediction model was derived using modern machine learning methods that accurately predicts risk of early recurrence using postoperative pathology. Machine learning may help

Published

2019

7. Identification of Prognostic Phenotypes of Esophageal Adenocarcinoma in 2 Independent Cohorts

Author

Tarek Sawas, Sarah Killcoyne, Prasad G. Iyer, Kenneth K. Wang, Thomas C. Smyrk, John B. Kisiel, Yi Qin, David A. Ahlquist, Anil K. Rustgi, Rui J. Costa, Moritz Gerstung, Rebecca C. Fitzgerald, David A. Katzka, Ayesha Noorani, Paul A.W. Edwards, Nicola Grehan, Barbara Nutzinger, Caitriona Hughes, Elwira Fidziukiewicz, Jan Bornschein, Shona MacRae, Jason Crawte, Gianmarco Contino, Xiaodun Li, Rachel de la Rue, Maria O’Donovan, Ahmad Miremad, Shalini Malhotra, Monika Tripathi, Simon Tavaré, Andy G. Lynch, Matthew Eldridge, Maria Secrier, Lawrence Bower, Ginny Devonshire, Juliane Perner, Sriganesh Jammula, Jim Davies, Charles Crichton, Nick Carroll, Peter Safranek, Andrew Hindmarsh, Vijayendran Sujendran, Stephen J. Hayes, Yeng Ang, Shaun R. Preston, Sarah Oakes, Izhar Bagwan, Vicki Save, Richard J.E. Skipworth, Ted R. Hupp, J. Robert O’Neill, Olga Tucker, Andrew Beggs, Philippe Taniere, Sonia Puig, Timothy J. Underwood, Fergus Noble, Jack Owsley, Hugh Barr, Neil Shepherd, Oliver Old, Jesper Lagergren, James Gossage, Andrew Davies, Fuju Chang, Janine Zylstra, Ula Mahadeva, Vicky Goh, Francesca D. Ciccarelli, Grant Sanders, Richard Berrisford, Catherine Harden, David Bunting, Mike Lewis, Ed Cheong, Bhaskar Kumar, Simon L. Parsons, Irshad Soomro, Philip Kaye, John Saunders, Laurence Lovat, Rehan Haidry, Victor Eneh, Laszlo Igali, Michael Scott, Sharmila Sothi, Sari Suortamo, Suzy Lishman, George B. Hanna, Christopher J. Peters, Anna Grabowska, and Richard Turkington

Subjects

Oncology, Male, medicine.medical_specialty, Esophageal Neoplasms, Survival, Adenocarcinoma, Article, 03 medical and health sciences, Barrett Esophagus, 0302 clinical medicine, Esophagus, Interquartile range, Internal medicine, medicine, Humans, Stage (cooking), Esophageal Adenocarcinoma, Aged, Neoplasm Staging, Proportional Hazards Models, Metaplasia, Hepatology, business.industry, Hazard ratio, Gastroenterology, Intestinal metaplasia, Middle Aged, medicine.disease, Prognosis, United Kingdom, United States, Intestines, medicine.anatomical_structure, Phenotype, 030220 oncology & carcinogenesis, Barrett's esophagus, Cohort, Etiology, Regression Analysis, 030211 gastroenterology & hepatology, business

Abstract

Background & Aims: Most patients with esophageal adenocarcinoma (EAC) present with de novo tumors. Although this could be due to inadequate screening strategies, the precise reason for this observation is not clear. We compared survival of patients with prevalent EAC with and without synchronous Barrett esophagus (BE) with intestinal metaplasia (IM) at the time of EAC diagnosis. Methods: Clinical data were studied using Cox proportional hazards regression to evaluate the effect of synchronous BE-IM on EAC survival independent of age, sex, TNM stage, and tumor location. We analyzed data from a cohort of patients with EAC from the Mayo Clinic (n=411; 203 with BE and IM) and a multicenter cohort from the United Kingdom (n=1417; 638 with BE and IM). Results: In the Mayo cohort, BE with IM had a reduced risk of death compared to patients without BE and IM (hazard ratio [HR] 0.44; 95% CI, 0.34–0.57; PConclusion: Two types of EAC can be characterized based on the presence or absence of BE. These findings could increase our understanding the etiology of EAC, and be used in management and prognosis of patients.

Published

2018

8. Shallow Whole Genome Sequencing can Detect Copy Number Changes in FFPE Material in the Progression of Barrett's Esophagus

Author

David C. Wedge, Eleanor Gregson, Matthew D. Eldridge, Katerina Jenkins, Lawrence Bower, Ahmad Miremadi, Rachel de la Rue, Sarah Killcoyne, and Rebecca C. Fitzgerald

Subjects

Whole genome sequencing, Genetics, Hepatology, Barrett's esophagus, Gastroenterology, medicine, Biology, medicine.disease

Published

2017