Germline variation in inflammation-related pathways and risk of Barrett's oesophagus and oesophageal adenocarcinoma

Matthew F. Buas; Qianchuan He; Lisa G. Johnson; Lynn Onstad; David M. Levine; Aaron P. Thrift; Puya Gharahkhani; Claire Palles; Jesper Lagergren; Rebecca C. Fitzgerald; Weimin Ye; Carlos Caldas; Nigel C. Bird; Nicholas J. Shaheen; Leslie Bernstein; Marilie D. Gammon; Anna H. Wu; Laura J. Hardie; Paul D. Pharoah; Geoffrey Liu; Prassad Iyer; Douglas A. Corley; Harvey A. Risch; Wong Ho Chow; Hans Prenen; Laura Chegwidden; Sharon Love; Stephen Attwood; Paul Moayyedi; David MacDonald; Rebecca Harrison; Peter Watson; Hugh Barr; John Decaestecker; Ian Tomlinson; Janusz Jankowski; David C. Whiteman; Stuart MacGregor; Thomas L. Vaughan; Margaret M. Madeleine

doi:10.1136/gutjnl-2016-311622

Germline variation in inflammation-related pathways and risk of Barrett's oesophagus and oesophageal adenocarcinoma

Matthew F. Buas, Qianchuan He, Lisa G. Johnson, Lynn Onstad, David M. Levine, Aaron P. Thrift, Puya Gharahkhani, Claire Palles, Jesper Lagergren, Rebecca C. Fitzgerald, Weimin Ye, Carlos Caldas, Nigel C. Bird, Nicholas J. Shaheen, Leslie Bernstein, Marilie D. Gammon, Anna H. Wu, Laura J. Hardie, Paul D. Pharoah, Geoffrey LiuPrassad Iyer, Douglas A. Corley, Harvey A. Risch, Wong Ho Chow, Hans Prenen, Laura Chegwidden, Sharon Love, Stephen Attwood, Paul Moayyedi, David MacDonald, Rebecca Harrison, Peter Watson, Hugh Barr, John Decaestecker, Ian Tomlinson, Janusz Jankowski, David C. Whiteman, Stuart MacGregor, Thomas L. Vaughan, Margaret M. Madeleine

Gastroenterology and Hepatology

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

Objective Oesophageal adenocarcinoma (OA) incidence has risen sharply in Western countries over recent decades. Local and systemic inflammation is considered an important contributor to OA pathogenesis. Established risk factors for OA and its precursor, Barrett's oesophagus (BE), include symptomatic reflux, obesity and smoking. The role of inherited genetic susceptibility remains an area of active investigation. Here, we explore whether germline variation related to inflammatory processes influences susceptibility to BE/OA. Design We used data from a genomewide association study of 2515 OA cases, 3295 BE cases and 3207 controls. Our analysis included 7863 single-nucleotide polymorphisms (SNPs) in 449 genes assigned to five pathways: Cyclooxygenase (COX), cytokine signalling, oxidative stress, human leucocyte antigen and nuclear factor-Î° B. A principal components-based analytic framework was employed to evaluate pathway-level and gene-level associations with disease risk. Results We identified a significant signal for the COX pathway in relation to BE risk (p=0.0059, false discovery rate q=0.03), and in gene-level analyses found an association with microsomal glutathione-S-transferase 1 (MGST1); (p=0.0005, q=0.005). Assessment of 36 MGST1 SNPs identified 14 variants associated with elevated BE risk (q<0.05). Four of these were subsequently confirmed (p<5.5×10^-5) in a meta-analysis encompassing an independent set of 1851 BE cases and 3496 controls, and are known strong expression quantitative trait loci for MGST1. Three such variants were associated with similar elevations in OA risk. Conclusions This study provides the most comprehensive evaluation of inflammation-related germline variation in relation to risk of BE/OA and suggests that variants in MGST1 influence disease susceptibility.

Original language	English (US)
Pages (from-to)	1739-1747
Number of pages	9
Journal	Gut
Volume	66
Issue number	10
DOIs	https://doi.org/10.1136/gutjnl-2016-311622
State	Published - Oct 1 2017

Keywords

BARRETT'S OESOPHAGUS
GENETIC POLYMORPHISMS
INFLAMMATION
OESOPHAGEAL CANCER

ASJC Scopus subject areas

Gastroenterology

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10.1136/gutjnl-2016-311622

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Buas, M. F., He, Q., Johnson, L. G., Onstad, L., Levine, D. M., Thrift, A. P., Gharahkhani, P., Palles, C., Lagergren, J., Fitzgerald, R. C., Ye, W., Caldas, C., Bird, N. C., Shaheen, N. J., Bernstein, L., Gammon, M. D., Wu, A. H., Hardie, L. J., Pharoah, P. D., ... Madeleine, M. M. (2017). Germline variation in inflammation-related pathways and risk of Barrett's oesophagus and oesophageal adenocarcinoma. Gut, 66(10), 1739-1747. https://doi.org/10.1136/gutjnl-2016-311622

Buas, MF, He, Q, Johnson, LG, Onstad, L, Levine, DM, Thrift, AP, Gharahkhani, P, Palles, C, Lagergren, J, Fitzgerald, RC, Ye, W, Caldas, C, Bird, NC, Shaheen, NJ, Bernstein, L, Gammon, MD, Wu, AH, Hardie, LJ, Pharoah, PD, Liu, G, Iyer, P, Corley, DA, Risch, HA, Chow, WH, Prenen, H, Chegwidden, L, Love, S, Attwood, S, Moayyedi, P, MacDonald, D, Harrison, R, Watson, P, Barr, H, Decaestecker, J, Tomlinson, I, Jankowski, J, Whiteman, DC, MacGregor, S, Vaughan, TL & Madeleine, MM 2017, 'Germline variation in inflammation-related pathways and risk of Barrett's oesophagus and oesophageal adenocarcinoma', Gut, vol. 66, no. 10, pp. 1739-1747. https://doi.org/10.1136/gutjnl-2016-311622

@article{86ff838e00244f1ab0dcca79529ed342,

title = "Germline variation in inflammation-related pathways and risk of Barrett's oesophagus and oesophageal adenocarcinoma",

abstract = "Objective Oesophageal adenocarcinoma (OA) incidence has risen sharply in Western countries over recent decades. Local and systemic inflammation is considered an important contributor to OA pathogenesis. Established risk factors for OA and its precursor, Barrett's oesophagus (BE), include symptomatic reflux, obesity and smoking. The role of inherited genetic susceptibility remains an area of active investigation. Here, we explore whether germline variation related to inflammatory processes influences susceptibility to BE/OA. Design We used data from a genomewide association study of 2515 OA cases, 3295 BE cases and 3207 controls. Our analysis included 7863 single-nucleotide polymorphisms (SNPs) in 449 genes assigned to five pathways: Cyclooxygenase (COX), cytokine signalling, oxidative stress, human leucocyte antigen and nuclear factor-{\^I}° B. A principal components-based analytic framework was employed to evaluate pathway-level and gene-level associations with disease risk. Results We identified a significant signal for the COX pathway in relation to BE risk (p=0.0059, false discovery rate q=0.03), and in gene-level analyses found an association with microsomal glutathione-S-transferase 1 (MGST1); (p=0.0005, q=0.005). Assessment of 36 MGST1 SNPs identified 14 variants associated with elevated BE risk (q<0.05). Four of these were subsequently confirmed (p<5.5×10-5) in a meta-analysis encompassing an independent set of 1851 BE cases and 3496 controls, and are known strong expression quantitative trait loci for MGST1. Three such variants were associated with similar elevations in OA risk. Conclusions This study provides the most comprehensive evaluation of inflammation-related germline variation in relation to risk of BE/OA and suggests that variants in MGST1 influence disease susceptibility.",

keywords = "BARRETT'S OESOPHAGUS, GENETIC POLYMORPHISMS, INFLAMMATION, OESOPHAGEAL CANCER",

author = "Buas, {Matthew F.} and Qianchuan He and Johnson, {Lisa G.} and Lynn Onstad and Levine, {David M.} and Thrift, {Aaron P.} and Puya Gharahkhani and Claire Palles and Jesper Lagergren and Fitzgerald, {Rebecca C.} and Weimin Ye and Carlos Caldas and Bird, {Nigel C.} and Shaheen, {Nicholas J.} and Leslie Bernstein and Gammon, {Marilie D.} and Wu, {Anna H.} and Hardie, {Laura J.} and Pharoah, {Paul D.} and Geoffrey Liu and Prassad Iyer and Corley, {Douglas A.} and Risch, {Harvey A.} and Chow, {Wong Ho} and Hans Prenen and Laura Chegwidden and Sharon Love and Stephen Attwood and Paul Moayyedi and David MacDonald and Rebecca Harrison and Peter Watson and Hugh Barr and John Decaestecker and Ian Tomlinson and Janusz Jankowski and Whiteman, {David C.} and Stuart MacGregor and Vaughan, {Thomas L.} and Madeleine, {Margaret M.}",

note = "Publisher Copyright: {\textcopyright} Published by the BMJ Publishing Group Limited.",

year = "2017",

month = oct,

day = "1",

doi = "10.1136/gutjnl-2016-311622",

language = "English (US)",

volume = "66",

pages = "1739--1747",

journal = "Gut",

issn = "0017-5749",

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number = "10",

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TY - JOUR

T1 - Germline variation in inflammation-related pathways and risk of Barrett's oesophagus and oesophageal adenocarcinoma

AU - Buas, Matthew F.

AU - He, Qianchuan

AU - Johnson, Lisa G.

AU - Onstad, Lynn

AU - Levine, David M.

AU - Thrift, Aaron P.

AU - Gharahkhani, Puya

AU - Palles, Claire

AU - Lagergren, Jesper

AU - Fitzgerald, Rebecca C.

AU - Ye, Weimin

AU - Caldas, Carlos

AU - Bird, Nigel C.

AU - Shaheen, Nicholas J.

AU - Bernstein, Leslie

AU - Gammon, Marilie D.

AU - Wu, Anna H.

AU - Hardie, Laura J.

AU - Pharoah, Paul D.

AU - Liu, Geoffrey

AU - Iyer, Prassad

AU - Corley, Douglas A.

AU - Risch, Harvey A.

AU - Chow, Wong Ho

AU - Prenen, Hans

AU - Chegwidden, Laura

AU - Love, Sharon

AU - Attwood, Stephen

AU - Moayyedi, Paul

AU - MacDonald, David

AU - Harrison, Rebecca

AU - Watson, Peter

AU - Barr, Hugh

AU - Decaestecker, John

AU - Tomlinson, Ian

AU - Jankowski, Janusz

AU - Whiteman, David C.

AU - MacGregor, Stuart

AU - Vaughan, Thomas L.

AU - Madeleine, Margaret M.

PY - 2017/10/1

Y1 - 2017/10/1

N2 - Objective Oesophageal adenocarcinoma (OA) incidence has risen sharply in Western countries over recent decades. Local and systemic inflammation is considered an important contributor to OA pathogenesis. Established risk factors for OA and its precursor, Barrett's oesophagus (BE), include symptomatic reflux, obesity and smoking. The role of inherited genetic susceptibility remains an area of active investigation. Here, we explore whether germline variation related to inflammatory processes influences susceptibility to BE/OA. Design We used data from a genomewide association study of 2515 OA cases, 3295 BE cases and 3207 controls. Our analysis included 7863 single-nucleotide polymorphisms (SNPs) in 449 genes assigned to five pathways: Cyclooxygenase (COX), cytokine signalling, oxidative stress, human leucocyte antigen and nuclear factor-Î° B. A principal components-based analytic framework was employed to evaluate pathway-level and gene-level associations with disease risk. Results We identified a significant signal for the COX pathway in relation to BE risk (p=0.0059, false discovery rate q=0.03), and in gene-level analyses found an association with microsomal glutathione-S-transferase 1 (MGST1); (p=0.0005, q=0.005). Assessment of 36 MGST1 SNPs identified 14 variants associated with elevated BE risk (q<0.05). Four of these were subsequently confirmed (p<5.5×10-5) in a meta-analysis encompassing an independent set of 1851 BE cases and 3496 controls, and are known strong expression quantitative trait loci for MGST1. Three such variants were associated with similar elevations in OA risk. Conclusions This study provides the most comprehensive evaluation of inflammation-related germline variation in relation to risk of BE/OA and suggests that variants in MGST1 influence disease susceptibility.

AB - Objective Oesophageal adenocarcinoma (OA) incidence has risen sharply in Western countries over recent decades. Local and systemic inflammation is considered an important contributor to OA pathogenesis. Established risk factors for OA and its precursor, Barrett's oesophagus (BE), include symptomatic reflux, obesity and smoking. The role of inherited genetic susceptibility remains an area of active investigation. Here, we explore whether germline variation related to inflammatory processes influences susceptibility to BE/OA. Design We used data from a genomewide association study of 2515 OA cases, 3295 BE cases and 3207 controls. Our analysis included 7863 single-nucleotide polymorphisms (SNPs) in 449 genes assigned to five pathways: Cyclooxygenase (COX), cytokine signalling, oxidative stress, human leucocyte antigen and nuclear factor-Î° B. A principal components-based analytic framework was employed to evaluate pathway-level and gene-level associations with disease risk. Results We identified a significant signal for the COX pathway in relation to BE risk (p=0.0059, false discovery rate q=0.03), and in gene-level analyses found an association with microsomal glutathione-S-transferase 1 (MGST1); (p=0.0005, q=0.005). Assessment of 36 MGST1 SNPs identified 14 variants associated with elevated BE risk (q<0.05). Four of these were subsequently confirmed (p<5.5×10-5) in a meta-analysis encompassing an independent set of 1851 BE cases and 3496 controls, and are known strong expression quantitative trait loci for MGST1. Three such variants were associated with similar elevations in OA risk. Conclusions This study provides the most comprehensive evaluation of inflammation-related germline variation in relation to risk of BE/OA and suggests that variants in MGST1 influence disease susceptibility.

KW - BARRETT'S OESOPHAGUS

KW - GENETIC POLYMORPHISMS

KW - INFLAMMATION

KW - OESOPHAGEAL CANCER

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UR - http://www.scopus.com/inward/citedby.url?scp=84982867194&partnerID=8YFLogxK

U2 - 10.1136/gutjnl-2016-311622

DO - 10.1136/gutjnl-2016-311622

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AN - SCOPUS:84982867194

SN - 0017-5749

VL - 66

SP - 1739

EP - 1747

JO - Gut

JF - Gut

IS - 10

ER -

Germline variation in inflammation-related pathways and risk of Barrett's oesophagus and oesophageal adenocarcinoma

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ASJC Scopus subject areas

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