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Acetic acid-guided biopsies in Barrett’s surveillance for neoplasia detection versus non-targeted biopsies (Seattle protocol): A feasibility study for a randomized tandem endoscopy trial. The ABBA study

BACKGROUND AND STUDY AIMS : Barrett’s esophagus is a potentially pre-cancerous condition, affecting 375,000 people in the UK. Patients receive a 2-yearly endoscopy to detect cancerous changes, as early detection and treatment results in better outcomes. Current treatment requires random mapping biop...

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Autores principales: Chedgy, Fergus, Fogg, Carole, Kandiah, Kesavan, Barr, Hugh, Higgins, Bernard, McCord, Mimi, Dewey, Ann, De Caestecker, John, Gadeke, Lisa, Stokes, Clive, Poller, David, Longcroft-Wheaton, Gaius, Bhandari, Pradeep
Formato: Online Artículo Texto
Lenguaje:English
Publicado: © Georg Thieme Verlag KG 2018
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5766339/
https://www.ncbi.nlm.nih.gov/pubmed/29340297
http://dx.doi.org/10.1055/s-0043-120829
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author Chedgy, Fergus
Fogg, Carole
Kandiah, Kesavan
Barr, Hugh
Higgins, Bernard
McCord, Mimi
Dewey, Ann
De Caestecker, John
Gadeke, Lisa
Stokes, Clive
Poller, David
Longcroft-Wheaton, Gaius
Bhandari, Pradeep
author_facet Chedgy, Fergus
Fogg, Carole
Kandiah, Kesavan
Barr, Hugh
Higgins, Bernard
McCord, Mimi
Dewey, Ann
De Caestecker, John
Gadeke, Lisa
Stokes, Clive
Poller, David
Longcroft-Wheaton, Gaius
Bhandari, Pradeep
author_sort Chedgy, Fergus
collection PubMed
description BACKGROUND AND STUDY AIMS : Barrett’s esophagus is a potentially pre-cancerous condition, affecting 375,000 people in the UK. Patients receive a 2-yearly endoscopy to detect cancerous changes, as early detection and treatment results in better outcomes. Current treatment requires random mapping biopsies along the length of Barrett’s, in addition to biopsy of visible abnormalities. As only 13 % of pre-cancerous changes appear as visible nodules or abnormalities, areas of dysplasia are often missed. Acetic acid chromoendoscopy (AAC) has been shown to improve detection of pre-cancerous and cancerous tissue in observational studies, but no randomized controlled trials (RCTs) have been performed to date. PATIENTS AND METHODS : A “tandem” endoscopy cross-over design. Participants will be randomized to endoscopy using mapping biopsies or AAC, in which dilute acetic acid is sprayed onto the surface of the esophagus, highlighting tissue through an whitening reaction and enhancing visibility of areas with cellular changes for biopsy. After 4 to 10 weeks, participants will undergo a repeat endoscopy, using the second method. Rates of recruitment and retention will be assessed, in addition to the estimated dysplasia detection rate, effectiveness of the endoscopist training program, and rates of adverse events (AEs). Qualitative interviews will explore participant and endoscopist acceptability of study design and delivery, and the acceptability of switching endoscopic techniques for Barrett's surveillance. RESULTS : Endoscopists’ ability to diagnose dysplasia in Barrett’s esophagus can be improved. AAC may offer a simple, universally applicable, easily-acquired technique to improve detection, affording patients earlier diagnosis and treatment, reducing endoscopy time and pathology costs. The ABBA study will determine whether a crossover “tandem” endoscopy design is feasible and acceptable to patients and clinicians and gather outcome data to power a definitive trial.
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spelling pubmed-57663392018-01-16 Acetic acid-guided biopsies in Barrett’s surveillance for neoplasia detection versus non-targeted biopsies (Seattle protocol): A feasibility study for a randomized tandem endoscopy trial. The ABBA study Chedgy, Fergus Fogg, Carole Kandiah, Kesavan Barr, Hugh Higgins, Bernard McCord, Mimi Dewey, Ann De Caestecker, John Gadeke, Lisa Stokes, Clive Poller, David Longcroft-Wheaton, Gaius Bhandari, Pradeep Endosc Int Open BACKGROUND AND STUDY AIMS : Barrett’s esophagus is a potentially pre-cancerous condition, affecting 375,000 people in the UK. Patients receive a 2-yearly endoscopy to detect cancerous changes, as early detection and treatment results in better outcomes. Current treatment requires random mapping biopsies along the length of Barrett’s, in addition to biopsy of visible abnormalities. As only 13 % of pre-cancerous changes appear as visible nodules or abnormalities, areas of dysplasia are often missed. Acetic acid chromoendoscopy (AAC) has been shown to improve detection of pre-cancerous and cancerous tissue in observational studies, but no randomized controlled trials (RCTs) have been performed to date. PATIENTS AND METHODS : A “tandem” endoscopy cross-over design. Participants will be randomized to endoscopy using mapping biopsies or AAC, in which dilute acetic acid is sprayed onto the surface of the esophagus, highlighting tissue through an whitening reaction and enhancing visibility of areas with cellular changes for biopsy. After 4 to 10 weeks, participants will undergo a repeat endoscopy, using the second method. Rates of recruitment and retention will be assessed, in addition to the estimated dysplasia detection rate, effectiveness of the endoscopist training program, and rates of adverse events (AEs). Qualitative interviews will explore participant and endoscopist acceptability of study design and delivery, and the acceptability of switching endoscopic techniques for Barrett's surveillance. RESULTS : Endoscopists’ ability to diagnose dysplasia in Barrett’s esophagus can be improved. AAC may offer a simple, universally applicable, easily-acquired technique to improve detection, affording patients earlier diagnosis and treatment, reducing endoscopy time and pathology costs. The ABBA study will determine whether a crossover “tandem” endoscopy design is feasible and acceptable to patients and clinicians and gather outcome data to power a definitive trial. © Georg Thieme Verlag KG 2018-01 2018-01-12 /pmc/articles/PMC5766339/ /pubmed/29340297 http://dx.doi.org/10.1055/s-0043-120829 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives License, which permits unrestricted reproduction and distribution, for non-commercial purposes only; and use and reproduction, but not distribution, of adapted material for non-commercial purposes only, provided the original work is properly cited.
spellingShingle Chedgy, Fergus
Fogg, Carole
Kandiah, Kesavan
Barr, Hugh
Higgins, Bernard
McCord, Mimi
Dewey, Ann
De Caestecker, John
Gadeke, Lisa
Stokes, Clive
Poller, David
Longcroft-Wheaton, Gaius
Bhandari, Pradeep
Acetic acid-guided biopsies in Barrett’s surveillance for neoplasia detection versus non-targeted biopsies (Seattle protocol): A feasibility study for a randomized tandem endoscopy trial. The ABBA study
title Acetic acid-guided biopsies in Barrett’s surveillance for neoplasia detection versus non-targeted biopsies (Seattle protocol): A feasibility study for a randomized tandem endoscopy trial. The ABBA study
title_full Acetic acid-guided biopsies in Barrett’s surveillance for neoplasia detection versus non-targeted biopsies (Seattle protocol): A feasibility study for a randomized tandem endoscopy trial. The ABBA study
title_fullStr Acetic acid-guided biopsies in Barrett’s surveillance for neoplasia detection versus non-targeted biopsies (Seattle protocol): A feasibility study for a randomized tandem endoscopy trial. The ABBA study
title_full_unstemmed Acetic acid-guided biopsies in Barrett’s surveillance for neoplasia detection versus non-targeted biopsies (Seattle protocol): A feasibility study for a randomized tandem endoscopy trial. The ABBA study
title_short Acetic acid-guided biopsies in Barrett’s surveillance for neoplasia detection versus non-targeted biopsies (Seattle protocol): A feasibility study for a randomized tandem endoscopy trial. The ABBA study
title_sort acetic acid-guided biopsies in barrett’s surveillance for neoplasia detection versus non-targeted biopsies (seattle protocol): a feasibility study for a randomized tandem endoscopy trial. the abba study
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5766339/
https://www.ncbi.nlm.nih.gov/pubmed/29340297
http://dx.doi.org/10.1055/s-0043-120829
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