Your search keyword '"M. O’Donovan"' showing total 25 results

1. The combination of autofluorescence endoscopy and molecular biomarkers is a novel diagnostic tool for dysplasia in Barrett's oesophagus

Author

Leanne Mills, Xinxue Liu, David F. Boerwinkel, Jacques J. Bergman, Mike Visser, Pierre Lao-Sirieix, Lorenz Wernisch, Krish Ragunath, M O'Donovan, Mohammed Shariff, Emmanouil Telakis, Susan Slininger, Tara Nuckcheddy-Grant, Philip Kaye, Massimiliano di Pietro, Rebecca C. Fitzgerald, Sybren L. Meijer, Elaine C. Walker, George Couch, Other departments, Pathology, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, CCA -Cancer Center Amsterdam, Gastroenterology and Hepatology, Di Pietro, Massimiliano [0000-0003-4866-7026], Fitzgerald, Rebecca [0000-0002-3434-3568], and Apollo - University of Cambridge Repository

Subjects

Adult, Image-Guided Biopsy, Male, Dysplasia, medicine.medical_specialty, Pathology, Aneuploidy, Barrett Esophagus, Biopsy, 1114 Paediatrics And Reproductive Medicine, Humans, Medicine, Barrett's Oesophagus, Prospective Studies, Prospective cohort study, Aged, Aged, 80 and over, Surveillance, Gastroenterology & Hepatology, medicine.diagnostic_test, Receiver operating characteristic, business.industry, Optical Imaging, Gastroenterology, 1103 Clinical Sciences, Endoscopy, Middle Aged, medicine.disease, Autofluorescence, Cross-Sectional Studies, Oesophageal Cancer, Female, Esophagoscopy, Radiology, business, Biomarkers

Abstract

OBJECTIVE: Endoscopic surveillance for Barrett's oesophagus (BO) is limited by sampling error and the subjectivity of diagnosing dysplasia. We aimed to compare a biomarker panel on minimal biopsies directed by autofluorescence imaging (AFI) with the standard surveillance protocol to derive an objective tool for dysplasia assessment. DESIGN: We performed a cross-sectional prospective study in three tertiary referral centres. Patients with BO underwent high-resolution endoscopy followed by AFI-targeted biopsies. 157 patients completed the biopsy protocol. Aneuploidy/tetraploidy; 9p and 17p loss of heterozygosity; RUNX3, HPP1 and p16 methylation; p53 and cyclin A immunohistochemistry were assessed. Bootstrap resampling was used to select the best diagnostic biomarker panel for high-grade dysplasia (HGD) and early cancer (EC). This panel was validated in an independent cohort of 46 patients. RESULTS: Aneuploidy, p53 immunohistochemistry and cyclin A had the strongest association with dysplasia in the per-biopsy analysis and, as a panel, had an area under the receiver operating characteristic curve of 0.97 (95% CI 0.95 to 0.99) for diagnosing HGD/EC. The diagnostic accuracy for HGD/EC of the three-biomarker panel from AFI+ areas was superior to AFI- areas (p

Published

2014

2. PTU-145 Prophylactic total gastrectomy for hereditory gastric cancer syndrome

Author

Susan Richardson, M O'Donovan, Richard H. Hardwick, Rebecca C. Fitzgerald, Marc Tischkowitz, B Tan, C Suo, M Di Pietro, and F Rashid

Subjects

medicine.medical_specialty, business.industry, medicine.medical_treatment, Gastroenterology, Cancer, Histology, Anastomosis, medicine.disease, Resection, Surgery, Cancer syndrome, medicine.anatomical_structure, medicine, Lymphadenectomy, Gastrectomy, business, Lymph node

Abstract

Introduction 1–3% of gastric cancers arise from hereditary predisposition syndromes. E-cadherin gene (CDH1) mutations are the best characterised of these and confer a life-time risk of approximately 80% for patients developing diffuse gastric cancer. Currently, the only definitive treatment available is prophylactic total gastrectomy (PTG). We present our experience of open PTG, focusing on the early outcomes. Method Twenty four consecutive patients with CDH 1 mutation underwent PTG from 2005 to 2014 (median age 33, range 22–51). All patients had at least one gastroscopy with biopsies taken according to the Cambridge Protocol and were assessed by a multi-disciplinary team within a high-volume Cancer Centre. All patients had an open posterior vagal sparing total gastrectomy with stapled oesophagojejunal anastomosis and Roux-en-Y reconstruction by a single surgeon. Twenty three patients had a D0.5 -1 lymphadenectomy; one patient with suspected invasive tumour had a D2 resection. Nasogastric tubes and abdominal drains were not used. Patients were mobilised on the first postoperative day with epidural analgesia. Oral fluids were restarted on postop day 3 and diet on day 5. Results There were two postoperative complications (8%) but no deaths; One patient had a jejuno-jejuno anastomotic leak 10 days after surgery requiring revisional surgery but made a full recovery. Another patient had bleeding which was managed conservatively with transfusion. Two patients developed anastomotic strictures and were successfully treated with endoscopic balloon dilatation. Median follow-up to date is 5 years (range: 3 months to 9 years). Histology showed scattered microscopic foci of intramucosal signet ring carcinoma (pT1a) in 23/24 patients (96%); the median number of foci was 7 (range: 1–182). No invasive tumours were found, all nodes were negative for tumour and all longitudinal margins were clear. The median lymph node yield was 5.5 (range: 1–26) and median hospital stay was 8 days (range: 6–10). Conclusion Open PTG can be performed with acceptable mortality and morbidity. Our challenge for the future is to offer minimally invasive PTG without increasing the risks. Disclosure of interest None Declared.

Published

2015

3. DNA methylation as a biomarker of progression in barrett's carcinogenesis

Author

Nicholas B. Shannon, M O'Donovan, M A Alvi, Lorenz Wernisch, Rebecca C. Fitzgerald, and R Newton

Subjects

Genetics, Gastroenterology, Methylation, Biology, medicine.disease_cause, medicine.disease, CpG site, Dysplasia, DNA methylation, medicine, Cancer research, Pyrosequencing, Biomarker (medicine), Carcinogenesis, Gene

Abstract

Introduction Barrett9s oesophagus (BO) increases the risk of developing oesophageal adenocarcinoma (OAC) by around 40-fold. OAC incidence rates have increased sixfold since the 1970s but the bleak prognosis for this disease is improved by early detection. The intermediate dysplastic stage between BO and OAC is the most reliable marker of progression. However the histological presence of dysplasia is subjective due to known sampling bias along with a high inter and intraobserver variability. Aberrant DNA methylation is shown to be characteristic of certain tumours and is known to occur early during transformation. We therefore hypothesise that DNA methylation changes take place early during carcinogenesis in BO patients which could be utilised as progression biomarkers. The study aims were therefore to identify genes showing a variation in methylation through progression and to then validate them on an independent dataset. Methods DNA methylation levels were assessed across 27 578 CpG loci covering 14 000 genes in 24 of each BO and OAC test samples using arrays. Both supervised clustering (GSEA software) and unsupervised clustering (R software) were used to identify genes with a statistically significant difference in methylation in BO versus OAC. Genes present in both the lists were selected for validation. Internal validation and external validation on an independent set of 48 BO, 31 BO with dysplasia and 68 OAC samples was carried out using pyrosequencing assays. Results Supervised clustering came up with 2822 hypermethylated and 645 hypomethylated genes (p≤0.001) and unsupervised with 1563 hypermethylated and 610 hypomethylated genes (p≤0.01). Genes successfully validated include RGN (senescence marker protein-30), SLC22A18 (tumour suppressing subtransferable candidate 5), PIGR (polymeric immunoglobulin receptor), GJA12 (gap junction protein, γ2) and TCEAL7 (transcription elongation factor A – like 7). After internal validation (spearman9s correlation p RGN (ANOVA p SLC22A18 (ANOVA p PIGR (ANOVA p GJA12 (ANOVA p TCEAL7 (ANOVA p=0.008, JT p=0.001). Conclusion High throughput DNA methylation screening using arrays and robust external validation has allowed us to identify novel genes having biomarker potential previously unknown to play a role in Barrett9s carcinogenesis. Further validation in an EDRN phase III study is underway.

Published

2011

4. Trimodal imaging to identify microscopic foci of signet ring cells in hereditary diffuse gastric cancer

Author

Yean Cheant Lim, Carlos Caldas, Krish Ragunath, M Di Pietro, Susan Richardson, M O'Donovan, Sarah Dwerryhouse, Irene Debiram, and Rebecca C. Fitzgerald

Subjects

Pathology, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Signet ring cell, medicine.medical_treatment, Stomach, Gastroenterology, Fundus (eye), medicine.disease, Endoscopy, Autofluorescence, medicine.anatomical_structure, Medicine, Gastrectomy, Hereditary diffuse gastric cancer, business, Antrum

Abstract

Introduction Patients fulfilling the criteria for Hereditary Diffuse Gastric Cancer (HDGC) may undergo endoscopic surveillance to help detect microscopic foci of signet ring cells and guide decisions about prophylactic gastrectomy. Current guidelines suggest a minimum of 30 random gastric biopsies sampled annually in patients fulfilling HDGC criteria. However, the wide distribution and small size of malignant foci makes them difficult to identify. The authors report the first prospective study to examine whether tri-modal imaging can aid detection of microscopic foci. Methods Patients fulfilling the criteria for HDGC attended for trimodal imaging endoscopy. A strict protocol was used with N-acetyl cysteine as a mucolytic, the stomach was inspected with white light followed by autofluorescence (AFI) to highlight areas of concern which were then visualised using narrow band imaging (NBI). A single endoscopist performed all procedures and a second endoscopist confirmed all findings at the time. In addition to any targeted biopsies, 24 random biopsies (prepylorus × 4, antrum × 4, t-zone × 6, body × 4, fundus × 4 and cardia × 2) were taken in each case and all specimens were examined by an expert histopathologist. Results Between October 2007 to March 2009, a total of 19 patients (7 with confirmed genetic CDH1 mutation) underwent 27 endoscopic surveillance procedures. The most common abnormality seen was pale areas in the antrum (8/27). These could be appreciated with white light endoscopy and were further highlighted with AFI with 2 showing abnormal pit patterns on NBI. Additional targeted biopsies were taken in 16 procedures. A total of 9 cases were positive for signet cells (4 fundus, 3 transitional zone, 1 body and 1 unspecified) 7 of the 9 positive cases were picked up solely on random biopsies. The two positive targeted biopsies were from a pale area at the transitional zone in the same patient who did not wish to undergo gastrectomy. Conclusion Careful inspection with standard white light and multiple random biopsies will detect microscopic foci in these high risk patients. Trimodal imaging helps delineate pale areas of concern but did not pick up additional foci.

Published

2011

5. OC-066 The Cancer Research UK (Cruk) Funded ICGC Oesophageal Adenocarcinoma Project: MRC Research Centre and Cruk Cambridge Research Institute

Author

Arusha Oloumi, Nicholas B. Shannon, Tim Forshew, Muhammed Murtaza, Richard H. Hardwick, Laura Smith, J. H. Davies, Andrew May, Paw Edwards, Mark J Dunning, Rebecca C. Fitzgerald, C-A Ong, M O'Donovan, J M J Weaver, Carlos Caldas, Mariagnese Barbera, Nicola Grehan, Simon Tavaré, Mike Smith, Samuel Aparicio, Matthew D. Eldridge, Pierre Lao-Sirieix, Nitzan Rosenfeld, Beatriz Carvalho, Caryn S. Ross-Innes, Timothy J. Underwood, and Andy G. Lynch

Subjects

Whole genome sequencing, ARID1A, business.industry, Gastroenterology, Cancer, Disease, Amplicon, medicine.disease, medicine.disease_cause, Causes of cancer, CDKN2A, Cancer research, medicine, business, Carcinogenesis

Abstract

Introduction Esophageal adenocarcinoma (EAC) has one of the fastest rising incidences of any cancer in the western world. With a 5-year survival below 10% it is one of the most common causes of cancer death in US and UK. Currently little is understood about the genetic alterations that drive the development of OAC. Better understanding of these alterations may allow the development of novel therepeutic approaches Methods We have performed whole genome sequencing on 22 cases. Targeted amplicon resequencing of 27 recurrently mutated genes was performed on a validation cohort of 100 further oesophageal adenocarcinomas. Results In the discover set of 22 OACs we identified recurrent mutations (>3 tumours) in 31 genes including several implicated in tumorigenesis; TP53, CDKN2A, ARID1A. Strikingly in the validation cohort we observed that > 30% of EAC samples harbour mutation of one or both of the SWI/SNF complex members ARID1A and SMARCA4. In addition we identified highly recurrent mutations in several additional genes including TRIM58, SSTR4 and MYO18B. Conclusion Whole genome sequencing provides an unbiased screen of mutational architecture of OAC. This has allowed the identification of several recurrently mutated genes not previously implicated in this disease providing a unique insight to it’s pathogenesis Disclosure of Interest None Declared

Published

2013

6. PTU-172 C-Myc as a Biomarker in Barrett’S Oesophagus: Abstract PTU-172 Table 1

Author

M O'Donovan, Caryn S. Ross-Innes, Pierre Lao-Sirieix, S Varghese, and Rebecca C. Fitzgerald

Subjects

medicine.medical_specialty, Tissue microarray, medicine.diagnostic_test, business.industry, education, Gastroenterology, Cancer, medicine.disease, digestive system diseases, Dysplasia, Internal medicine, Barrett's oesophagus, Biopsy, medicine, Biomarker (medicine), Immunohistochemistry, Stage (cooking), business

Abstract

Introduction Identifying Barrett’s oesophagus (BE) patients at risk of progressing to oesophageal adenocarcinoma (EA) remains a challenge. Diagnosis of low grade dysplasia is limited by considerable intra and inter-observer variability and inflammation in biopsy samples can lead to a diagnosis of indefinite for dysplasia. Immunostaining using molecular biomarkers would therefore be useful as a diagnostic adjunct in the assessment of dysplasia. The Aim of this study was to identify and validate a molecular biomarker that can objectively determine dysplasia status and thereby determine cancer risk in BE. Methods Biomarkers of interest were identified through mining of a microarray gene expression dataset from 59 oesophageal samples with strict consensus diagnosis by expert pathologists [21 BE with no dysplasia (NDBE), 10 BE with low grade dysplasia (LGD), 13 BE with high grade dysplasia (HGD) and 8 EA]. Subsequent validation was performed on a BE tissue microarray (TMA) (60 NDBE, 19 LGD and 29 HGD), and EA TMA (n = 278). Results Seventy eight genes were differentially expressed between NDBE and HGD. c-MYC was selected as a top target as the expression levels progressively increased with dysplasia stage and cancer with a fold change of 2.46 between NDBE and HGD. mRNA expression levels were significantly higher in HGD and EA compared to NDBE (p Table 1. Immunohistochemistry for c-MYC in oesophageal samples. NDBE: Non-dysplastic Barrett’s oesophagus, LGD: Low-grade dysplasia, HGD: High grade dysplasia. Conclusion Immunohistochemistry for c-MYC is a promising molecular biomarker in Barrett’s oesophagus. It could also enable better risk stratification in patients with samples in the LGD and indefinite for dysplasia categories. Disclosure of Interest None Declared.

Published

2013

7. OC-027 Defining Cancer Risk in Barrett’S Oesophagus using a 90-Gene Signature

Author

S Varghese, R Newton, C S Ross-Innes, K K Krishnadath, P Lao-Sirieix, M O’Donovan, L Wernisch, J J Bergman, and R C Fitzgerald

Subjects

Gastroenterology

Published

2013

8. PTU-173 Gord Symptoms and Demographic Factors as a Pre-Screening tool for Barrett’S Oesophagus

Author

X Liu, A Wong, S R Kadri, M O’Donovan, P Lao-Sirieix, R Burnham, and R Fitzgerald

Subjects

Gastroenterology

Published

2013

9. OC-017 TRIM44: from prognosis to therapy in oesophageal adenocarcinoma and breast cancer

Author

C A J Ong, N B Shannon, P Lao-Sirieix, C Ross-Innes, M O'Donovan, O M Rueda, C E Walker, A Noorani, R Hardwick, C Caldas, and R C Fitzgerald

Subjects

Gastroenterology

Published

2012

10. PTU-192 Time: prospective study combining endoscopic trimodal imaging and molecular endpoints to risk stratify Barrett's oesophagus

Author

Mike Visser, Emmanouil Telakis, P Lao Sirieix, D Boerwinkle, M O'Donovan, Rebecca C. Fitzgerald, Leanne Mills, Kareem M. Shariff, Susan Slininger, Elaine C. Walker, Jjghm Bergman, Krish Ragunath, Xinxue Liu, Philip Kaye, and M Di Pietro

Subjects

medicine.medical_specialty, Pathology, medicine.diagnostic_test, Gastroenterology, Aneuploidy, Biology, medicine.disease, Dysplasia, Internal medicine, Barrett's oesophagus, Biopsy, medicine, Biomarker (medicine), Immunohistochemistry, False positive rate, Prospective cohort study

Abstract

Introduction Biomarkers have been proposed to improve risk stratification in Barrett9s oesophagus (BO), however molecular heterogeneity of BO can hamper detection of molecular changes in random biopsies. Use of Autofluorescence Imaging (AFI) within endoscopic Trimodal Imaging (ETMI) can improve dysplasia detection, but has high false positive rate. Aims of study were (a) validate biomarkers previously published in separate patient cohorts in single study (b) assess whether AFI can increase detection of biomarkers (c) combine ETMI and biomarkers to improve risk stratification of patients with BO. Methods Prospective European multicentre study. Each patient underwent ETMI with targeted biopsies on AFI positive (AFI+) areas and one AFI negative (AFI−) area, as well as random quadrantic biopsies. DNA content abnormalities (aneuploidy/tetraploidy); loss of heterozygosity (LOH) at 9p and 17p loci; RUNX3, HPP1 and p16 methylation; immunohistochemistry (IHC) for p53 and Cyclin A were tested on targeted biopsies. Each biomarker was correlated with the dysplasia and AFI status. Results 111 patients with 210 biopsy areas were included in the analysis (AFI+, n=120; AFI-, n=90). Univariate per-biopsy analysis showed that all biomarkers correlated with dysplasia (p Conclusion AFI increases detection rate for molecular biomarkers. A panel of 3 molecular biomarkers on a small number of AFI targeted biopsies can efficiently predict the dysplasia status and potentially inform therapeutic management of patients with BE. Competing interests None declared.

Published

2012

11. PTU-218 Pilot randomised cross-over study comparing the efficacy of transnasal Endosheath® to standard endoscopy to detect Barrett's oesophagus

Author

Kareem M. Shariff, M O'Donovan, Jane M Blazeby, Rebecca C. Fitzgerald, Z Abdullahi, and S Verghese

Subjects

education.field_of_study, medicine.medical_specialty, medicine.diagnostic_test, Visual analogue scale, business.industry, Population, Gastroenterology, Intestinal metaplasia, Gold standard (test), medicine.disease, Crossover study, Surgery, Endoscopy, Biopsy, Barrett's oesophagus, medicine, education, business

Abstract

Introduction A less expensive and safer alternative to standard sedated endoscopy (SE) needs to be considered as a screening method to detect Barrett9s oesophagus (BE) in the population, with the aim of reducing the mortality associated with oesophageal adenocarcinoma. The Endosheath® transnasal oesophagoscope (TNE) can potentially offer a new alternative to conventional standard endoscopy in diagnosing Barrett9s oesophagus. The Endosheath® technology uses a sterile, disposable sheath which covers the ultra thin flexible oesophagoscope and isolates it from the patient. The oesophagoscope is placed in a new sheath prior to each procedure which obviates the need for machine washing and permits a quick turnaround. Aim: A pilot study to evaluate the efficacy of TNE in diagnosing BE compared with SE and to assess patient acceptability of TNE. Methods Patients referred for surveillance endoscopy for BE or a clinically indicated routine endoscopy were recruited to both TNE and SE in a randomised cross-over design. The interval between the procedures was at least 6 weeks. TNE findings of endoscopic BE, and presence of intestinal metaplasia (IM) on the biopsy samples were compared against SE, which was used as gold standard. A 10-point visual analogue scale (0 represented the worst experience and 10 the best experience) to assess the post-endoscopy experience and a single question addressing preference for endoscopy type were used to measure patient acceptability of the procedures. Results 15 patients completed the study, 10 males and 5 females with a mean age of 62.85 years (range 50–76 years). Nine of which were BE surveillance patients and six were referred for a clinically indicated routine endoscopy. Eight patients were randomised to the SE as the first procedure. All the 11 patients with an endoscopic diagnosis of BE on SE were accurately identified with the TNE (sensitivity 100%; specificity 100%). Biopsies were taken in all the 11 Barrett9s segments except in one Conclusion Endosheath® transnasal oesophagoscope is accurate in diagnosing endoscopic BE and can detect IM. It is better tolerated and preferred by patients, making it a useful screening tool for BE with potential for use in primary care. Competing interests None declared.

Published

2012

12. Molecular imaging via novel application of fluorescent lectins permits rapid endoscopic identification of dysplasia in barrett's oesophagus

Author

E. L. Bird-Lieberman, A. A. Neves, P. Lao-Sirieix, M. O'Donovan, L. B. Lovat, L. K. Mahal, K. M. Brindle, and R. C. Fitzgerald

Subjects

Gastroenterology

Published

2011

13. A systematic approach to therapeutic target selection in gastro-esophageal adenocarcinoma

Author

A. L. Paterson, N. B. Shannon, P. Lao-Sirieix, C. J. Peters, M. O'Donovan, and R. C. Fitzgerald

Subjects

Gastroenterology

Published

2011

14. PTU-019 Nasal or standard endoscopy (nose) for diagnosis of Barrett's oesophagus – efficacy and patient tolerance: Abstract PTU-019

Author

S L Vowler, M O'Donovan, K M Shariff, Z Abdullahi, Jane M Blazeby, Elizabeth L. Bird-Lieberman, and Rebecca C. Fitzgerald

Subjects

medicine.medical_specialty, education.field_of_study, medicine.diagnostic_test, business.industry, Visual analogue scale, Population, Gastroenterology, Intestinal metaplasia, Gold standard (test), medicine.disease, Endoscopy, Surgery, medicine.anatomical_structure, Dysplasia, Biopsy, Medicine, business, education, Nose

Abstract

Introduction In order to detect all cases of Barrett9s oesophagus (BE) in the population, with the aim of reducing adenocarcinoma associated mortality, screening needs to be considered. Unsedated transnasal endoscopy (TNE) can potentially offer a safer and less expensive alternative to conventional sedated endoscopy (CE) for detecting BE. Aims (1) To evaluate the sensitivity and specificity of TNE in diagnosing BE compared with CE. (2) To assess patient acceptability of TNE for a future multicentre screening trial. Methods Patients with known BE under surveillance and those referred for routine endoscopy for other reasons underwent both TNE and CE in a randomised cross-over design. TNE findings of endoscopic BE, biopsy size and presence of intestinal metaplasia (IM) were compared against CE, which was used as gold standard. Pre and post endoscopy short-form spielberger state-trait questionnaires (SF6), a visual analogue scale and a single question addressing preference for endoscopy type were used to measure patient acceptability of the procedures. Results Of 57 patients randomised, 50 completed the study. All 22 BE cases with columnar lined epithelium (CLE) on CE were correctly diagnosed by TNE. Although the biopsy size of TNE was significantly smaller compared to CE (mean size 2.59 vs 4.74 p Conclusion TNE is accurate in diagnosing BE and detecting IM. Despite the smaller biopsy size, it detected an equal number of IM cases and showed potential to detect dysplasia. It was well tolerated and preferred by patients and may be an efficient screening method for BE.

Published

2010

15. OC-060 A clinically applicable three gene signature is independently highly prognostic in oesophageal and junctional adenocarcinoma

Author

C J Peters, J R E Rees, J S Hardwick, S L Vowler, C J Ong, C Zhang, V Save, M O'Donovan, D Rassl, C Caldas, D Alderson, R H Hardwick, and R C Fitzgerald

Subjects

Gastroenterology

Published

2010

16. Understanding the malignant potential of gastric metaplasia of the oesophagus and its relevance to Barrett's oesophagus surveillance: individual-level data analysis.

Author

Black EL, Ococks E, Devonshire G, Ng AWT, O'Donovan M, Malhotra S, Tripathi M, Miremadi A, Freeman A, Coles H, and Fitzgerald RC

Subjects

Humans, Metaplasia, Endoscopy, Gastrointestinal, Barrett Esophagus diagnosis, Barrett Esophagus genetics, Barrett Esophagus complications, Esophageal Neoplasms diagnosis, Esophageal Neoplasms genetics, Adenocarcinoma

Abstract

Objective: Whether gastric metaplasia (GM) of the oesophagus should be considered as Barrett's oesophagus (BO) is controversial. Given concern intestinal metaplasia (IM) may be missed due to sampling, the UK guidelines include GM as a type of BO. Here, we investigated whether the risk of misdiagnosis and the malignant potential of GM warrant its place in the UK surveillance., Design: We performed a thorough pathology and endoscopy review to follow clinical outcomes in a novel UK cohort of 244 patients, covering 1854 person years of follow-up. We complemented this with a comparative genomic analysis of 160 GM and IM specimens, focused on early molecular hallmarks of BO and oesophageal adenocarcinoma (OAC)., Results: We found that 58 of 77 short-segment ( < 3 cm) GM (SS-GM) cases (75%) continued to be observed as GM-only across a median of 4.4 years of follow-up. We observed that disease progression in GM-only cases and GM+IM cases (cases with reported GM on some occasions, IM on others) was significantly lower than in the IM-only cases (Kaplan-Meier, p=0.03). Genomic analysis revealed that the mutation burden in GM is significantly lower than in IM (p<0.01). Moreover, GM does not bear the mutational hallmarks of OAC, with an absence of associated signatures and driver gene mutations. Finally, we established that GM found adjacent to OAC is evolutionarily distant from cancer., Conclusion: SS-GM is a distinct entity from SS-IM and the malignant potential of GM is lower than IM. It is questionable whether SS-GM warrants inclusion in BO surveillance., Competing Interests: Competing interests: RCF and MOD are named on patents for Cytosponge and associated technology, licensed to Covidien GI solutions (now Medtronic). RCF and MOD are shareholders of Cyted Ltd., a company working on early detection technology. The other authors declare no competing interests., (© Author(s) (or their employer(s)) 2024. Re-use permitted under CC BY. Published by BMJ.)

Published

2024

17. Kyoto international consensus report on anatomy, pathophysiology and clinical significance of the gastro-oesophageal junction.

Author

Sugano K, Spechler SJ, El-Omar EM, McColl KEL, Takubo K, Gotoda T, Fujishiro M, Iijima K, Inoue H, Kawai T, Kinoshita Y, Miwa H, Mukaisho KI, Murakami K, Seto Y, Tajiri H, Bhatia S, Choi MG, Fitzgerald RC, Fock KM, Goh KL, Ho KY, Mahachai V, O'Donovan M, Odze R, Peek R, Rugge M, Sharma P, Sollano JD, Vieth M, Wu J, Wu MS, Zou D, Kaminishi M, and Malfertheiner P

Subjects

Consensus, Esophagogastric Junction, Humans, Inflammation, Metaplasia, Barrett Esophagus diagnosis, Barrett Esophagus epidemiology, Barrett Esophagus etiology, Gastroesophageal Reflux

Abstract

Objective: An international meeting was organised to develop consensus on (1) the landmarks to define the gastro-oesophageal junction (GOJ), (2) the occurrence and pathophysiological significance of the cardiac gland, (3) the definition of the gastro-oesophageal junctional zone (GOJZ) and (4) the causes of inflammation, metaplasia and neoplasia occurring in the GOJZ., Design: Clinical questions relevant to the afore-mentioned major issues were drafted for which expert panels formulated relevant statements and textural explanations.A Delphi method using an anonymous system was employed to develop the consensus, the level of which was predefined as ≥80% of agreement. Two rounds of voting and amendments were completed before the meeting at which clinical questions and consensus were finalised., Results: Twenty eight clinical questions and statements were finalised after extensive amendments. Critical consensus was achieved: (1) definition for the GOJ, (2) definition of the GOJZ spanning 1 cm proximal and distal to the GOJ as defined by the end of palisade vessels was accepted based on the anatomical distribution of cardiac type gland, (3) chemical and bacterial ( Helicobacter pylori ) factors as the primary causes of inflammation, metaplasia and neoplasia occurring in the GOJZ, (4) a new definition of Barrett's oesophagus (BO)., Conclusions: This international consensus on the new definitions of BO, GOJ and the GOJZ will be instrumental in future studies aiming to resolve many issues on this important anatomic area and hopefully will lead to better classification and management of the diseases surrounding the GOJ., Competing Interests: Competing interests: KS serves as an advisor for Fujifilm Medical Co. and received a lecture fee from Fujifilm Medical Co. MF received lecture fee from Olympus Medical Systems Co. and Fujifilm Medical Co. He also received research grant from Olympus Medical Systems Co, Fujifilm Medical Co. and HOYA Pentax Co. HI serves as an advisor for Olympus Medical Systems Co. HM received a lecture fee from Fujifilm Medical Co. GT and HT received lecture fees from Olympus Medical Co. and Fujifilm Medical Co. Other authors have declared no competing interests regarding this manuscript, (© Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2022

18. Methylation panel is a diagnostic biomarker for Barrett's oesophagus in endoscopic biopsies and non-endoscopic cytology specimens.

Author

Chettouh H, Mowforth O, Galeano-Dalmau N, Bezawada N, Ross-Innes C, MacRae S, Debiram-Beecham I, O'Donovan M, and Fitzgerald RC

Subjects

Adult, Aged, Barrett Esophagus metabolism, Barrett Esophagus pathology, Biopsy, Cytological Techniques methods, Esophagoscopy methods, Esophagus metabolism, Female, Humans, Immunohistochemistry methods, Male, Middle Aged, Polymerase Chain Reaction, Sensitivity and Specificity, Barrett Esophagus diagnosis, Biomarkers metabolism, DNA Methylation genetics, Esophagus pathology

Abstract

Objective: Barrett's oesophagus is a premalignant condition that occurs in the context of gastro-oesophageal reflux. However, most Barrett's cases are undiagnosed because of reliance on endoscopy. We have developed a non-endoscopic tool: the Cytosponge, which when combined with trefoil factor 3 immunohistochemistry, can diagnose Barrett's oesophagus. We investigated whether a quantitative methylation test that is not reliant on histopathological analysis could be used to diagnose Barrett's oesophagus., Design: Differentially methylated genes between Barrett's and normal squamous oesophageal biopsies were identified from whole methylome data and confirmed using MethyLight PCR in biopsy samples of squamous oesophagus, gastric cardia and Barrett's oesophagus. Selected genes were then tested on Cytosponge BEST2 trial samples comprising a pilot cohort (n=20 cases, n=10 controls) and a validation cohort (n=149 cases, n=129 controls)., Results: Eighteen genes were differentially methylated in patients with Barrett'soesophagus compared with squamous controls. Hypermethylation of TFPI2, TWIST1, ZNF345 and ZNF569 was confirmed in Barrett's biopsies compared with biopsies from squamous oesophagus and gastric cardia (p<0.05). When tested in Cytosponge samples, these four genes were hypermethylated in patients with Barrett's oesophagus compared with patients with reflux symptoms (p<0.001). The optimum biomarker to diagnose Barrett's oesophagus was TFPI2 with a sensitivity and specificity of 82.2% and 95.7%, respectively., Conclusion: TFPI2, TWIST1, ZNF345 and ZNF569 methylation have promise as diagnostic biomarkers for Barrett's oesophagus when used in combination with a simple and cost effective non-endoscopic cell collection device., Competing Interests: Competing interests: Since this study was conducted, the Cytosponge™-TFF3 technology has been licensed to Covidien GI solutions (now owned by Medtronic) by the Medical Research Council. Rebecca Fitzgerald and Maria O’Donovan are named inventors on patents pertaining to the Cytosponge™. Covidien Solutions and Medtronic have not been privy to this manuscript or the data therein. All other authors declare no conflicts of interest., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2018. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2018

19. The combination of autofluorescence endoscopy and molecular biomarkers is a novel diagnostic tool for dysplasia in Barrett's oesophagus.

Author

di Pietro M, Boerwinkel DF, Shariff MK, Liu X, Telakis E, Lao-Sirieix P, Walker E, Couch G, Mills L, Nuckcheddy-Grant T, Slininger S, O'Donovan M, Visser M, Meijer SL, Kaye PV, Wernisch L, Ragunath K, Bergman JJ, and Fitzgerald RC

Subjects

Adult, Aged, Aged, 80 and over, Cross-Sectional Studies, Female, Humans, Image-Guided Biopsy methods, Male, Middle Aged, Optical Imaging, Prospective Studies, Barrett Esophagus pathology, Biomarkers analysis, Esophagoscopy

Abstract

Objective: Endoscopic surveillance for Barrett's oesophagus (BO) is limited by sampling error and the subjectivity of diagnosing dysplasia. We aimed to compare a biomarker panel on minimal biopsies directed by autofluorescence imaging (AFI) with the standard surveillance protocol to derive an objective tool for dysplasia assessment., Design: We performed a cross-sectional prospective study in three tertiary referral centres. Patients with BO underwent high-resolution endoscopy followed by AFI-targeted biopsies. 157 patients completed the biopsy protocol. Aneuploidy/tetraploidy; 9p and 17p loss of heterozygosity; RUNX3, HPP1 and p16 methylation; p53 and cyclin A immunohistochemistry were assessed. Bootstrap resampling was used to select the best diagnostic biomarker panel for high-grade dysplasia (HGD) and early cancer (EC). This panel was validated in an independent cohort of 46 patients., Results: Aneuploidy, p53 immunohistochemistry and cyclin A had the strongest association with dysplasia in the per-biopsy analysis and, as a panel, had an area under the receiver operating characteristic curve of 0.97 (95% CI 0.95 to 0.99) for diagnosing HGD/EC. The diagnostic accuracy for HGD/EC of the three-biomarker panel from AFI+ areas was superior to AFI- areas (p<0.001). Compared with the standard protocol, this panel had equal sensitivity for HGD/EC, with a 4.5-fold reduction in the number of biopsies. In an independent cohort of patients, the panel had a sensitivity and specificity for HGD/EC of 100% and 85%, respectively., Conclusions: A three-biomarker panel on a small number of AFI-targeted biopsies provides an accurate and objective diagnosis of dysplasia in BO. The clinical implications have to be studied further., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://group.bmj.com/group/rights-licensing/permissions.)

Published

2015

20. British Society of Gastroenterology guidelines on the diagnosis and management of Barrett's oesophagus.

Author

Fitzgerald RC, di Pietro M, Ragunath K, Ang Y, Kang JY, Watson P, Trudgill N, Patel P, Kaye PV, Sanders S, O'Donovan M, Bird-Lieberman E, Bhandari P, Jankowski JA, Attwood S, Parsons SL, Loft D, Lagergren J, Moayyedi P, Lyratzopoulos G, and de Caestecker J

Subjects

Ablation Techniques, Adenocarcinoma diagnosis, Adenocarcinoma economics, Adenocarcinoma etiology, Adenocarcinoma therapy, Biopsy, Cost-Benefit Analysis, Decision Support Techniques, Early Detection of Cancer economics, Early Detection of Cancer methods, Esophageal Neoplasms diagnosis, Esophageal Neoplasms economics, Esophageal Neoplasms etiology, Esophageal Neoplasms therapy, Esophagectomy, Esophagoscopy economics, Esophagoscopy methods, Esophagus pathology, Esophagus surgery, Humans, Risk Assessment methods, Risk Factors, United Kingdom, United States, Barrett Esophagus complications, Barrett Esophagus diagnosis, Barrett Esophagus economics, Barrett Esophagus therapy

Abstract

These guidelines provide a practical and evidence-based resource for the management of patients with Barrett's oesophagus and related early neoplasia. The Appraisal of Guidelines for Research and Evaluation (AGREE II) instrument was followed to provide a methodological strategy for the guideline development. A systematic review of the literature was performed for English language articles published up until December 2012 in order to address controversial issues in Barrett's oesophagus including definition, screening and diagnosis, surveillance, pathological grading for dysplasia, management of dysplasia, and early cancer including training requirements. The rigour and quality of the studies was evaluated using the SIGN checklist system. Recommendations on each topic were scored by each author using a five-tier system (A+, strong agreement, to D+, strongly disagree). Statements that failed to reach substantial agreement among authors, defined as >80% agreement (A or A+), were revisited and modified until substantial agreement (>80%) was reached. In formulating these guidelines, we took into consideration benefits and risks for the population and national health system, as well as patient perspectives. For the first time, we have suggested stratification of patients according to their estimated cancer risk based on clinical and histopathological criteria. In order to improve communication between clinicians, we recommend the use of minimum datasets for reporting endoscopic and pathological findings. We advocate endoscopic therapy for high-grade dysplasia and early cancer, which should be performed in high-volume centres. We hope that these guidelines will standardise and improve management for patients with Barrett's oesophagus and related neoplasia.

Published

2014

21. A systematic approach to therapeutic target selection in oesophago-gastric cancer.

Author

Paterson AL, Shannon NB, Lao-Sirieix P, Ong CA, Peters CJ, O'Donovan M, and Fitzgerald RC

Subjects

Adult, Aged, Aged, 80 and over, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacology, Barrett Esophagus drug therapy, Barrett Esophagus genetics, Barrett Esophagus metabolism, Barrett Esophagus pathology, Biomarkers, Tumor metabolism, Cell Death drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Discovery methods, Enzyme Activation drug effects, Esophageal Neoplasms genetics, Esophageal Neoplasms metabolism, Esophageal Neoplasms pathology, Feasibility Studies, Female, Gene Expression Profiling methods, Humans, MAP Kinase Signaling System physiology, Male, Middle Aged, Neoplasm Staging, Phosphorylation drug effects, Precancerous Conditions drug therapy, Precancerous Conditions genetics, Precancerous Conditions metabolism, Precancerous Conditions pathology, Precision Medicine methods, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors pharmacology, Protein-Tyrosine Kinases antagonists & inhibitors, Receptor Protein-Tyrosine Kinases antagonists & inhibitors, Receptor Protein-Tyrosine Kinases genetics, Receptor Protein-Tyrosine Kinases metabolism, Stomach Neoplasms genetics, Stomach Neoplasms metabolism, Stomach Neoplasms pathology, Esophageal Neoplasms drug therapy, Stomach Neoplasms drug therapy

Abstract

Objective: The success of personalised therapy depends on identification and inhibition of the oncogene(s) on which that tumour is dependent. We aimed to determine whether a receptor tyrosine kinase (RTK) array could be used to select the most effective therapeutic strategies in molecularly heterogeneous oesophago-gastric adenocarcinomas., Design: Gene expression profiling from oesophago-gastric tumours (n=75) and preinvasive stages (n=57) identified the active signalling pathways, which was confirmed using immunohistochemistry (n=434). RTK arrays on a cell line panel (n=14) determined therapeutic targets for in vitro cytotoxic testing. Feasibility of this personalised approach was tested in tumour samples (n=46)., Results: MAPK was the most frequently activated pathway (32/75 samples (42.7%)) with progressive enrichment in preinvasive disease stages (p<0.05) and ERK phosphorylation in 148/434 (34.3%) independent samples. Cell lines displayed a range of RTK activation profiles. When no RTKs were activated, tyrosine kinase inhibitors (TKIs) and a Mek inhibitor were not useful (MKN1). In lines with a dominant phosphorylated RTK (OE19, MKN45 and KATOIII), selection of this TKI or Mek in nM concentrations induced cytotoxicity and inhibited Erk and Akt phosphorylation. In cells lines with complex activation profiles (HSC39 and OE33), a combination of TKIs or Mek inhibition (in nM concentrations) was necessary for cytotoxicity and inhibition of Erk and Akt phosphorylation. Human tumours demonstrated diverse activation profiles and 65% of cases had two or more active RTKs., Conclusions: The MAPK pathway is commonly activated in oesophago-gastric cancer following activation of a variety of RTKs. Molecular phenotyping can inform a rational choice of targeted therapy.

Published

2013

22. Integrative analysis of array-comparative genomic hybridisation and matched gene expression profiling data reveals novel genes with prognostic significance in oesophageal adenocarcinoma.

Author

Goh XY, Rees JR, Paterson AL, Chin SF, Marioni JC, Save V, O'Donovan M, Eijk PP, Alderson D, Ylstra B, Caldas C, and Fitzgerald RC

Subjects

Adenocarcinoma mortality, Adenocarcinoma pathology, Aged, Aged, 80 and over, Biomarkers, Tumor biosynthesis, Biomarkers, Tumor genetics, ErbB Receptors biosynthesis, Esophageal Neoplasms mortality, Esophageal Neoplasms pathology, Female, Follow-Up Studies, Humans, Immunohistochemistry, Kaplan-Meier Estimate, Male, Microarray Analysis, Middle Aged, Polymerase Chain Reaction, Prognosis, Retrospective Studies, Survival Rate, Time Factors, United Kingdom epidemiology, Adenocarcinoma genetics, Comparative Genomic Hybridization methods, DNA, Neoplasm genetics, ErbB Receptors genetics, Esophageal Neoplasms genetics, Gene Expression Profiling methods, Gene Expression Regulation, Neoplastic

Abstract

Background and Aims: The incidence of oesophageal adenocarcinoma (OAC) has been increasing rapidly with a dismal survival rate of less than 20%. Understanding the genomic aberrations and biology of this cancer may enhance disease interventions. This study aimed to use genome-wide genomic and expression data to enhance the understanding of OAC pathogenesis and identify groups with differential outcomes., Methods: Array-comparative genomic hybridisation (aCGH) analysis was carried out on 56 fresh frozen OAC resection samples with long-term clinical follow-up data. Samples with aberrations were further analysed with whole-genome single-nucleotide polymorphism arrays to confirm aCGH findings. Matched gene expression microarray data were used to identify genes with high copy number-expression correlations. Nested-multiplex PCR on DNA from microdissected specimens and fluorescence in situ hybridisation assays were used for target validation. Immunohistochemistry on the same cohort and independent samples (n=371) was used for subsequent validation. Kaplan-Meier survival analyses were performed based on aCGH data after unsupervised K-means clustering (K=5, 50 iterations) and immunohistochemistry data., Results: aCGH identified 17 common regions (>5% samples) of gains and 11 common regions of losses, including novel regions in OAC (loci 11p13 and 21q21.2). Integration of aCGH data with matched gene expression microarray data highlighted genes with high copy number-expression correlations: two deletions (p16/CDKN2A, MBNL1) and four gains (EGFR, WT1, NEIL2, MTMR9). Immunohistochemistry demonstrated protein over-expression of targets with gains: EGFR (10%), WT1 (20%), NEIL2 (14%) and MTMR9 (25%). These targets individually (p<0.060) and in combination had prognostic significance (p=0.008). On the genomic level, K-means clustering identified a cluster (32% of cohort) with differential log(2) ratios of 16 CGH probes (p<4×10(-7)) and a worse prognosis (median survival=1.37 years; p=0.015)., Conclusions: Integration of aCGH and gene expression data identified copy number aberrations and novel genes with prognostic potential in OAC.

Published

2011

23. Non-endoscopic screening biomarkers for Barrett's oesophagus: from microarray analysis to the clinic.

Author

Lao-Sirieix P, Boussioutas A, Kadri SR, O'Donovan M, Debiram I, Das M, Harihar L, and Fitzgerald RC

Subjects

Aged, Barrett Esophagus metabolism, Esophageal Neoplasms metabolism, Female, Gastric Mucosa metabolism, Humans, Immunohistochemistry, Male, Middle Aged, Precancerous Conditions metabolism, Protein Array Analysis, Reference Values, Trefoil Factor-3, Up-Regulation, Barrett Esophagus genetics, Biomarkers, Tumor metabolism, Dopa Decarboxylase metabolism, Esophageal Neoplasms genetics, Peptides metabolism, Precancerous Conditions genetics

Abstract

Background and Aims: Barrett's oesophagus predisposes to oesophageal adenocarcinoma but the majority of patients are undiagnosed. A novel non-endoscopic cytological screening device, called a capsule sponge, makes population-based screening for the disease a feasible option. However, due to the mixed cell population retrieved by the capsule sponge, biomarkers specific for Barrett's oesophagus are required., Methods: Three publically available microarray datasets were used to identify putative biomarkers present in Barrett's oesophagus but absent from normal oesophagus and gastric mucosa. Validation was performed by qPCR (n = 10 each of normal oesophagus, Barrett's oesophagus, gastric mucosa) and immunohistochemistry (normal oesophagus, n = 20; Barrett's oesophagus, n = 21; gastric mucosa, n = 24; duodenum, n = 18). The biomarker was then prospectively evaluated on capsule sponge specimens from 47 patients with Barrett's oesophagus and 99 healthy controls., Results: 2/14 genes identified, dopa decarboxylase (DDC) and Trefoil factor 3 (TFF3), were confirmed by qPCR to be upregulated in Barrett's oesophagus compared to normal oesophagus (p<0.01) and gastric mucosa (p<0.01 and p<0.05, respectively). Immunohistochemistry confirmed that DDC protein expression was restricted to Barrett's oesophagus but was confined to <1% of the cells within the crypt compartment. TFF3 protein was expressed to high levels at the luminal surface of Barrett's oesophagus compared to absent expression in normal oesophagus and gastric mucosa (p<0.001). Using the capsule sponge 36/46 patients with Barrett's oesophagus (one inadequate sample) and 6/96 controls were positive for TFF3 giving a sensitivity of 78% and a specificity of 94%., Conclusions: TFF3 is a promising marker for Barrett's oesophagus screening since it is expressed at the luminal surface of Barrett's oesophagus but not in adjacent tissue types and may be applied to a non-endoscopic screening device.

Published

2009

24. Non-endoscopic immunocytological screening test for Barrett's oesophagus.

Author

Lao-Sirieix P, Rous B, O'Donovan M, Hardwick RH, Debiram I, and Fitzgerald RC

Subjects

Adult, Cytodiagnosis methods, Humans, Mass Screening methods, Middle Aged, Specimen Handling methods, Barrett Esophagus diagnosis, Esophageal Neoplasms diagnosis, Precancerous Conditions diagnosis

Published

2007

25. Elastic scattering spectroscopy accurately detects high grade dysplasia and cancer in Barrett's oesophagus.

Author

Lovat LB, Johnson K, Mackenzie GD, Clark BR, Novelli MR, Davies S, O'Donovan M, Selvasekar C, Thorpe SM, Pickard D, Fitzgerald R, Fearn T, Bigio I, and Bown SG

Subjects

Adenocarcinoma pathology, Algorithms, Barrett Esophagus pathology, Biopsy, Diagnosis, Differential, Elasticity, Esophageal Neoplasms pathology, Esophagitis diagnosis, Esophagitis pathology, Esophagoscopy, Humans, Population Surveillance, Precancerous Conditions pathology, Sensitivity and Specificity, Spectrum Analysis methods, Adenocarcinoma diagnosis, Barrett Esophagus diagnosis, Esophageal Neoplasms diagnosis, Precancerous Conditions diagnosis

Abstract

Background and Aims: Endoscopic surveillance of Barrett's oesophagus currently relies on multiple random biopsies. This approach is time consuming, has a poor diagnostic yield, and significant interobserver variability. Elastic scattering spectroscopy is a real time in vivo optical technique which detects changes in the physical properties of cells. The aim of this study was to assess the potential for elastic scattering to detect high grade dysplasia or cancer within Barrett's oesophagus., Methods: Elastic scattering spectroscopy measurements collected in vivo were matched with histological specimens taken from identical sites within Barrett's oesophagus. All biopsies were reviewed by three gastrointestinal pathologists and defined as either "low risk" (non-dysplastic or low grade dysplasia) or "high risk" (high grade dysplasia or cancer). Two different statistical approaches (leave one out and block validation) were used to validate the model., Results: A total of 181 matched biopsy sites from 81 patients, where histopathological consensus was reached, were analysed. There was good pathologist agreement in differentiating high grade dysplasia and cancer from other pathology (kappa = 0.72). Elastic scattering spectroscopy detected high risk sites with 92% sensitivity and 60% specificity and differentiated high risk sites from inflammation with a sensitivity and specificity of 79%. If used to target biopsies during endoscopy, the number of low risk biopsies taken would decrease by 60% with minimal loss of accuracy. A negative spectroscopy result would exclude high grade dysplasia or cancer with an accuracy of >99.5%., Conclusions: These preliminary results show that elastic scattering spectroscopy has the potential to target conventional biopsies in Barrett's surveillance saving significant endoscopist and pathologist time with consequent financial savings. This technique now requires validation in prospective studies.

Published

2006