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Ordering of mutations in preinvasive disease stages of esophageal carcinogenesis

Ordering of mutations in preinvasive disease stages of esophageal carcinogenesis
Ordering of mutations in preinvasive disease stages of esophageal carcinogenesis
Cancer genome sequencing studies have identified numerous driver genes, but the relative timing of mutations in carcinogenesis remains unclear. The gradual progression from premalignant Barrett's esophagus to esophageal adenocarcinoma (EAC) provides an ideal model to study the ordering of somatic mutations. We identified recurrently mutated genes and assessed clonal structure using whole-genome sequencing and amplicon resequencing of 112 EACs. We next screened a cohort of 109 biopsies from 2 key transition points in the development of malignancy: benign metaplastic never-dysplastic Barrett's esophagus (NDBE; n = 66) and high-grade dysplasia (HGD; n = 43). Unexpectedly, the majority of recurrently mutated genes in EAC were also mutated in NDBE. Only TP53 and SMAD4 mutations occurred in a stage-specific manner, confined to HGD and EAC, respectively. Finally, we applied this knowledge to identify high-risk Barrett's esophagus in a new non-endoscopic test. In conclusion, mutations in EAC driver genes generally occur exceptionally early in disease development with profound implications for diagnostic and therapeutic strategies.
1061-4036
837-843
Weaver, Jamie M.J.
26c54649-c975-4712-bf8b-0121e9d8f792
Ross-Innes, Caryn S.
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Shannon, Nicholas
331c269d-8136-40ba-b857-0c4a8adb8b17
Lynch, Andy G.
f2c4a9f4-3d65-46c0-ac71-69502c041539
Forshew, Tim
dd2cce6a-4850-4bd5-8114-84260c79d60f
Barbera, Mariagnese
883b0e38-e07f-49fa-9ca1-d0cb18b57f1c
Murtaza, Muhammed
cd05e5fa-638f-4d00-8c20-1488c5b07746
Ong, Chin-Ann J.
fe359d88-70ad-4b03-a8b7-210a30255355
Lao-Sirieix, Pierre
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Dunning, Mark J.
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Smith, Laura
cce2d99b-dfce-4b13-87cf-adca2c457c7c
Smith, Mike L.
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Anderson, Charlotte L.
e58272d0-bf45-4ffe-b41d-8c716afac3de
Carvalho, Benilton
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O'Donovan, Maria
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Underwood, Timothy J.
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May, Andrew P.
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Grehan, Nicola
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Hardwick, Richard
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Davies, Jim
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Oloumi, Arusha
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Aparicio, Sam
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Caldas, Carlos
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Eldridge, Matthew D.
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Edwards, Paul A.W.
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Rosenfeld, Nitzan
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Tavaré, Simon
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Fitzgerald, Rebecca C.
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OCCAMS Consortium
Weaver, Jamie M.J.
26c54649-c975-4712-bf8b-0121e9d8f792
Ross-Innes, Caryn S.
5b4717cb-9cf9-4559-ad1f-c5be87705ac6
Shannon, Nicholas
331c269d-8136-40ba-b857-0c4a8adb8b17
Lynch, Andy G.
f2c4a9f4-3d65-46c0-ac71-69502c041539
Forshew, Tim
dd2cce6a-4850-4bd5-8114-84260c79d60f
Barbera, Mariagnese
883b0e38-e07f-49fa-9ca1-d0cb18b57f1c
Murtaza, Muhammed
cd05e5fa-638f-4d00-8c20-1488c5b07746
Ong, Chin-Ann J.
fe359d88-70ad-4b03-a8b7-210a30255355
Lao-Sirieix, Pierre
88a35f4e-49b4-4cfb-ba83-522c48b0de81
Dunning, Mark J.
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Smith, Laura
cce2d99b-dfce-4b13-87cf-adca2c457c7c
Smith, Mike L.
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Anderson, Charlotte L.
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Carvalho, Benilton
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O'Donovan, Maria
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Underwood, Timothy J.
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May, Andrew P.
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Grehan, Nicola
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Hardwick, Richard
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Davies, Jim
22357eff-a45a-468f-a706-649cccf1872f
Oloumi, Arusha
809dbb92-51f8-4c01-b470-dcde2852655c
Aparicio, Sam
aa70944d-1f51-4b5f-b40d-d86d9557667f
Caldas, Carlos
96032f49-a8e5-45e0-a5f0-128b15f91944
Eldridge, Matthew D.
de7cb99a-f065-4ff8-bb10-bd0b4f99d30d
Edwards, Paul A.W.
04a46a01-d4aa-41f5-bbe8-869a424efe92
Rosenfeld, Nitzan
88325461-2fa9-4ae3-87da-7eab829d6098
Tavaré, Simon
a18ea48e-9f97-49a8-92fc-8daec649e655
Fitzgerald, Rebecca C.
b69743f5-b2c8-4e24-b729-f42cb0fc9c97

OCCAMS Consortium (2014) Ordering of mutations in preinvasive disease stages of esophageal carcinogenesis. Nature Genetics, 46 (8), 837-843. (doi:10.1038/ng.3013). (PMID:24952744)

Record type: Article

Abstract

Cancer genome sequencing studies have identified numerous driver genes, but the relative timing of mutations in carcinogenesis remains unclear. The gradual progression from premalignant Barrett's esophagus to esophageal adenocarcinoma (EAC) provides an ideal model to study the ordering of somatic mutations. We identified recurrently mutated genes and assessed clonal structure using whole-genome sequencing and amplicon resequencing of 112 EACs. We next screened a cohort of 109 biopsies from 2 key transition points in the development of malignancy: benign metaplastic never-dysplastic Barrett's esophagus (NDBE; n = 66) and high-grade dysplasia (HGD; n = 43). Unexpectedly, the majority of recurrently mutated genes in EAC were also mutated in NDBE. Only TP53 and SMAD4 mutations occurred in a stage-specific manner, confined to HGD and EAC, respectively. Finally, we applied this knowledge to identify high-risk Barrett's esophagus in a new non-endoscopic test. In conclusion, mutations in EAC driver genes generally occur exceptionally early in disease development with profound implications for diagnostic and therapeutic strategies.

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More information

e-pub ahead of print date: 22 June 2014
Published date: August 2014
Organisations: Cancer Sciences

Identifiers

Local EPrints ID: 366505
URI: http://eprints.soton.ac.uk/id/eprint/366505
ISSN: 1061-4036
PURE UUID: c06a5d45-9b8c-46af-8304-9afcbfb999ee
ORCID for Timothy J. Underwood: ORCID iD orcid.org/0000-0001-9455-2188

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Date deposited: 01 Jul 2014 14:12
Last modified: 15 Mar 2024 03:17

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Contributors

Author: Jamie M.J. Weaver
Author: Caryn S. Ross-Innes
Author: Nicholas Shannon
Author: Andy G. Lynch
Author: Tim Forshew
Author: Mariagnese Barbera
Author: Muhammed Murtaza
Author: Chin-Ann J. Ong
Author: Pierre Lao-Sirieix
Author: Mark J. Dunning
Author: Laura Smith
Author: Mike L. Smith
Author: Charlotte L. Anderson
Author: Benilton Carvalho
Author: Maria O'Donovan
Author: Andrew P. May
Author: Nicola Grehan
Author: Richard Hardwick
Author: Jim Davies
Author: Arusha Oloumi
Author: Sam Aparicio
Author: Carlos Caldas
Author: Matthew D. Eldridge
Author: Paul A.W. Edwards
Author: Nitzan Rosenfeld
Author: Simon Tavaré
Author: Rebecca C. Fitzgerald
Corporate Author: OCCAMS Consortium

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