The University of Southampton
×
Filter your search:
University of Southampton Institutional Repository

Genome-wide association study meta-analysis of chronic widespread pain: evidence for involvement of the 5p15.2 region

Genome-wide association study meta-analysis of chronic widespread pain: evidence for involvement of the 5p15.2 region
Genome-wide association study meta-analysis of chronic widespread pain: evidence for involvement of the 5p15.2 region
Background and objectives: chronic widespread pain (CWP) is a common disorder affecting ∼10% of the general population and has an estimated heritability of 48–52%. In the first large-scale genome-wide association study (GWAS) meta-analysis, we aimed to identify common genetic variants associated with CWP.

Methods: we conducted a GWAS meta-analysis in 1308 female CWP cases and 5791 controls of European descent, and replicated the effects of the genetic variants with suggestive evidence for association in 1480 CWP cases and 7989 controls. Subsequently, we studied gene expression levels of the nearest genes in two chronic inflammatory pain mouse models, and examined 92 genetic variants previously described associated with pain.

Results: the minor C-allele of rs13361160 on chromosome 5p15.2, located upstream of chaperonin-containing-TCP1-complex-5 gene (CCT5) and downstream of FAM173B, was found to be associated with a 30% higher risk of CWP (minor allele frequency=43%; OR=1.30, 95% CI 1.19 to 1.42, p=1.2×10−8). Combined with the replication, we observed a slightly attenuated OR of 1.17 (95% CI 1.10 to 1.24, p=4.7×10−7) with moderate heterogeneity (I2=28.4%). However, in a sensitivity analysis that only allowed studies with joint-specific pain, the combined association was genome-wide significant (OR=1.23, 95% CI 1.14 to 1.32, p=3.4×10−8, I2=0%). Expression levels of Cct5 and Fam173b in mice with inflammatory pain were higher in the lumbar spinal cord, not in the lumbar dorsal root ganglions, compared to mice without pain. None of the 92 genetic variants previously described were significantly associated with pain (p>7.7×10−4).

Conclusions: we identified a common genetic variant on chromosome 5p15.2 associated with joint-specific CWP in humans. This work suggests that CCT5 and FAM173B are promising targets in the regulation of pain.
0003-4967
Peters, Marjolein J.
a1db2568-cc2a-4672-8765-6340ee2d4972
Broer, Linda
842d7191-08ad-4533-8c49-f4d7c0d463b0
Willemen, Hanneke L.D.M.
05365dd3-7e6d-4400-a4c1-d8a337a4c7c5
Eiriksdottir, G.
96b3f034-ed58-4731-95a1-aed7e62a054d
Hocking, L.J.
6c37348f-8f1d-4c34-a6e5-6de2a238d5ed
Holliday, K.L.
58c01428-143a-4fc8-bd97-eb513573a697
Horan, M.A.
38e35ccc-0531-443e-81ca-01c9c41e1302
Meulenbelt, I.
f02e5902-5916-40f5-bdff-b02355cd348d
Neogi, T.
4864516c-ef09-42f9-aaa7-321f24a19081
Popham, M.
e8923e2d-3536-4fd9-9917-bb18de0ff4f7
Schmidt, C.O.
6c55f161-8207-4a00-b819-e7dca2778621
Soni, A.
7a4196ff-0f6b-429e-af54-d1036e9c433b
Valdes, A.M.
4e4c3f14-3895-4129-94ca-f4176dd83e94
Amin, N.
0ed94dbd-2fb8-4d44-be2f-a60adaaacb1a
Dennison, Elaine M.
ee647287-edb4-4392-8361-e59fd505b1d1
Eijkelkamp, N.
df461dc9-9f86-4d08-b6bc-8c5cedce96a7
Harris, T.B.
caddeefd-558a-4b63-9a62-76db71886d20
Hart, D.J.
c5f8047d-0e34-430b-9a03-854212f72f2a
Hofman, A.
ece9dbea-8c2b-4f2f-81eb-7aa28075cf7a
Huygen, F.J.P.M.
712e8df3-5d61-4aa8-b0e2-266c71086f44
Jameson, Karen A.
d5fb142d-06af-456e-9016-17497f94e9f2
Jones, G.T.
ce3cf060-87fe-49db-9258-9bd48c14d84c
Launer, L.J.
ec96a484-c5d4-4c5e-8375-429d243a61cd
Kerkhof, H.J.M.
1e6a9470-6023-4897-ad2d-fd697a772f62
De Kruijf, M.
6ce20726-3c0d-4bb7-b9c2-79fd04282298
McBeth, John
98012716-66ba-480b-9e43-ac53b51dce61
Kloppenburg, M.
eb293575-62ec-463c-a6c1-4ef41eb2ea82
Ollier, W.E.
78b94975-c863-4253-a309-91bb3092aad8
Oostra, B.
2ae09c37-7adc-499f-80a7-5ee3ef3e78ce
Payton, A.
ed18d1fc-c89f-40b6-b89b-55e202bcae15
Rivadeneira, F.
642dbd8d-88a9-469d-826c-b75280f5620d
Smith, B.H.
fe4fefa6-33de-4dfc-b9e2-361b3d36729b
Smith, A.V.
ab42094a-cdb4-4b9f-963e-53b24e2e8656
Stolk, L.
162c1cbf-0e75-4770-9946-b793e31a5129
Teumer, A.
318741af-604f-45db-ae0f-4394e7bc9f30
Thomson, W.
1e15e3f0-5128-496d-a2bd-da122d42ddfa
Uitterlinden, A.G.
a1cba0b3-0fea-487b-8d8c-dcafc1655f67
Wang, K.
35ab64db-e4d5-4b4b-9225-54c9bcc6d143
Van Wingerden, S.H.
1aeb2b4b-f96e-4638-b4b1-bdba08ad5d09
Arden, Nigel K.
23af958d-835c-4d79-be54-4bbe4c68077f
Cooper, Cyrus
e05f5612-b493-4273-9b71-9e0ce32bdad6
Felson, D.
87990fc1-6730-4739-9b18-1a027bc7484b
Gudnason, V.
174d32af-83c9-4b84-a29b-7855843e2a21
Macfarlane, G.J.
e17bbdb7-9d82-42ac-8a0a-09bf10885e3c
Pendleton, N.
33b5acf5-6ff9-4607-bf0c-4858d603b6f0
Slagboom, P.E.
25165476-1811-4817-bf5d-e9d2eba15683
Spector, T.D.
29debf10-949d-4094-8f5f-9a8614511ccb
Völzke, H.
7a82b5da-95dd-4f33-9e7f-693e50ff19cb
Kavelaars, A.
e26bbe8f-5e49-4a0f-897e-4e1441657010
Van Duijn, C.M.
9b3e1061-a24b-4768-94c5-61247744b448
et al.
Peters, Marjolein J.
a1db2568-cc2a-4672-8765-6340ee2d4972
Broer, Linda
842d7191-08ad-4533-8c49-f4d7c0d463b0
Willemen, Hanneke L.D.M.
05365dd3-7e6d-4400-a4c1-d8a337a4c7c5
Eiriksdottir, G.
96b3f034-ed58-4731-95a1-aed7e62a054d
Hocking, L.J.
6c37348f-8f1d-4c34-a6e5-6de2a238d5ed
Holliday, K.L.
58c01428-143a-4fc8-bd97-eb513573a697
Horan, M.A.
38e35ccc-0531-443e-81ca-01c9c41e1302
Meulenbelt, I.
f02e5902-5916-40f5-bdff-b02355cd348d
Neogi, T.
4864516c-ef09-42f9-aaa7-321f24a19081
Popham, M.
e8923e2d-3536-4fd9-9917-bb18de0ff4f7
Schmidt, C.O.
6c55f161-8207-4a00-b819-e7dca2778621
Soni, A.
7a4196ff-0f6b-429e-af54-d1036e9c433b
Valdes, A.M.
4e4c3f14-3895-4129-94ca-f4176dd83e94
Amin, N.
0ed94dbd-2fb8-4d44-be2f-a60adaaacb1a
Dennison, Elaine M.
ee647287-edb4-4392-8361-e59fd505b1d1
Eijkelkamp, N.
df461dc9-9f86-4d08-b6bc-8c5cedce96a7
Harris, T.B.
caddeefd-558a-4b63-9a62-76db71886d20
Hart, D.J.
c5f8047d-0e34-430b-9a03-854212f72f2a
Hofman, A.
ece9dbea-8c2b-4f2f-81eb-7aa28075cf7a
Huygen, F.J.P.M.
712e8df3-5d61-4aa8-b0e2-266c71086f44
Jameson, Karen A.
d5fb142d-06af-456e-9016-17497f94e9f2
Jones, G.T.
ce3cf060-87fe-49db-9258-9bd48c14d84c
Launer, L.J.
ec96a484-c5d4-4c5e-8375-429d243a61cd
Kerkhof, H.J.M.
1e6a9470-6023-4897-ad2d-fd697a772f62
De Kruijf, M.
6ce20726-3c0d-4bb7-b9c2-79fd04282298
McBeth, John
98012716-66ba-480b-9e43-ac53b51dce61
Kloppenburg, M.
eb293575-62ec-463c-a6c1-4ef41eb2ea82
Ollier, W.E.
78b94975-c863-4253-a309-91bb3092aad8
Oostra, B.
2ae09c37-7adc-499f-80a7-5ee3ef3e78ce
Payton, A.
ed18d1fc-c89f-40b6-b89b-55e202bcae15
Rivadeneira, F.
642dbd8d-88a9-469d-826c-b75280f5620d
Smith, B.H.
fe4fefa6-33de-4dfc-b9e2-361b3d36729b
Smith, A.V.
ab42094a-cdb4-4b9f-963e-53b24e2e8656
Stolk, L.
162c1cbf-0e75-4770-9946-b793e31a5129
Teumer, A.
318741af-604f-45db-ae0f-4394e7bc9f30
Thomson, W.
1e15e3f0-5128-496d-a2bd-da122d42ddfa
Uitterlinden, A.G.
a1cba0b3-0fea-487b-8d8c-dcafc1655f67
Wang, K.
35ab64db-e4d5-4b4b-9225-54c9bcc6d143
Van Wingerden, S.H.
1aeb2b4b-f96e-4638-b4b1-bdba08ad5d09
Arden, Nigel K.
23af958d-835c-4d79-be54-4bbe4c68077f
Cooper, Cyrus
e05f5612-b493-4273-9b71-9e0ce32bdad6
Felson, D.
87990fc1-6730-4739-9b18-1a027bc7484b
Gudnason, V.
174d32af-83c9-4b84-a29b-7855843e2a21
Macfarlane, G.J.
e17bbdb7-9d82-42ac-8a0a-09bf10885e3c
Pendleton, N.
33b5acf5-6ff9-4607-bf0c-4858d603b6f0
Slagboom, P.E.
25165476-1811-4817-bf5d-e9d2eba15683
Spector, T.D.
29debf10-949d-4094-8f5f-9a8614511ccb
Völzke, H.
7a82b5da-95dd-4f33-9e7f-693e50ff19cb
Kavelaars, A.
e26bbe8f-5e49-4a0f-897e-4e1441657010
Van Duijn, C.M.
9b3e1061-a24b-4768-94c5-61247744b448

Peters, Marjolein J., Broer, Linda and Willemen, Hanneke L.D.M. , et al. (2012) Genome-wide association study meta-analysis of chronic widespread pain: evidence for involvement of the 5p15.2 region. Annals of the Rheumatic Diseases, 72 (3). (doi:10.1136/annrheumdis-2012-201742).

Record type: Article

Abstract

Background and objectives: chronic widespread pain (CWP) is a common disorder affecting ∼10% of the general population and has an estimated heritability of 48–52%. In the first large-scale genome-wide association study (GWAS) meta-analysis, we aimed to identify common genetic variants associated with CWP.

Methods: we conducted a GWAS meta-analysis in 1308 female CWP cases and 5791 controls of European descent, and replicated the effects of the genetic variants with suggestive evidence for association in 1480 CWP cases and 7989 controls. Subsequently, we studied gene expression levels of the nearest genes in two chronic inflammatory pain mouse models, and examined 92 genetic variants previously described associated with pain.

Results: the minor C-allele of rs13361160 on chromosome 5p15.2, located upstream of chaperonin-containing-TCP1-complex-5 gene (CCT5) and downstream of FAM173B, was found to be associated with a 30% higher risk of CWP (minor allele frequency=43%; OR=1.30, 95% CI 1.19 to 1.42, p=1.2×10−8). Combined with the replication, we observed a slightly attenuated OR of 1.17 (95% CI 1.10 to 1.24, p=4.7×10−7) with moderate heterogeneity (I2=28.4%). However, in a sensitivity analysis that only allowed studies with joint-specific pain, the combined association was genome-wide significant (OR=1.23, 95% CI 1.14 to 1.32, p=3.4×10−8, I2=0%). Expression levels of Cct5 and Fam173b in mice with inflammatory pain were higher in the lumbar spinal cord, not in the lumbar dorsal root ganglions, compared to mice without pain. None of the 92 genetic variants previously described were significantly associated with pain (p>7.7×10−4).

Conclusions: we identified a common genetic variant on chromosome 5p15.2 associated with joint-specific CWP in humans. This work suggests that CCT5 and FAM173B are promising targets in the regulation of pain.

Text
427.full - Version of Record
Available under License Creative Commons Attribution.
Download (512kB)

More information

Accepted/In Press date: 19 July 2012
e-pub ahead of print date: 6 September 2012

Identifiers

Local EPrints ID: 491724
URI: http://eprints.soton.ac.uk/id/eprint/491724
DOI: doi:10.1136/annrheumdis-2012-201742
ISSN: 0003-4967
PURE UUID: 8eecd5ae-e085-455b-8e07-b52439a15552
ORCID for Elaine M. Dennison: ORCID iD orcid.org/0000-0002-3048-4961
ORCID for John McBeth: ORCID iD orcid.org/0000-0001-7047-2183
ORCID for Cyrus Cooper: ORCID iD orcid.org/0000-0003-3510-0709

Catalogue record

Date deposited: 03 Jul 2024 16:45
Last modified: 12 Jul 2024 02:17

Export record

Altmetrics

Contributors

Author: Marjolein J. Peters
Author: Linda Broer
Author: Hanneke L.D.M. Willemen
Author: G. Eiriksdottir
Author: L.J. Hocking
Author: K.L. Holliday
Author: M.A. Horan
Author: I. Meulenbelt
Author: T. Neogi
Author: M. Popham
Author: C.O. Schmidt
Author: A. Soni
Author: A.M. Valdes
Author: N. Amin
Author: Elaine M. Dennison ORCID iD
Author: N. Eijkelkamp
Author: T.B. Harris
Author: D.J. Hart
Author: A. Hofman
Author: F.J.P.M. Huygen
Author: Karen A. Jameson
Author: G.T. Jones
Author: L.J. Launer
Author: H.J.M. Kerkhof
Author: M. De Kruijf
Author: John McBeth ORCID iD
Author: M. Kloppenburg
Author: W.E. Ollier
Author: B. Oostra
Author: A. Payton
Author: F. Rivadeneira
Author: B.H. Smith
Author: A.V. Smith
Author: L. Stolk
Author: A. Teumer
Author: W. Thomson
Author: A.G. Uitterlinden
Author: K. Wang
Author: S.H. Van Wingerden
Author: Nigel K. Arden
Author: Cyrus Cooper ORCID iD
Author: D. Felson
Author: V. Gudnason
Author: G.J. Macfarlane
Author: N. Pendleton
Author: P.E. Slagboom
Author: T.D. Spector
Author: H. Völzke
Author: A. Kavelaars
Author: C.M. Van Duijn
Corporate Author: et al.

Download statistics

Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.

View more statistics

Library staff additional information
Atom RSS 1.0 RSS 2.0

Contact ePrints Soton: eprints@soton.ac.uk

ePrints Soton supports OAI 2.0 with a base URL of http://eprints.soton.ac.uk/cgi/oai2

This repository has been built using EPrints software, developed at the University of Southampton, but available to everyone to use.

We use cookies to ensure that we give you the best experience on our website. If you continue without changing your settings, we will assume that you are happy to receive cookies on the University of Southampton website.

×