C-reactive protein and its role in metabolic syndrome: mendelian randomisation study
C-reactive protein and its role in metabolic syndrome: mendelian randomisation study
Background: Circulating C-reactive protein (CRP) is associated with the metabolic syndrome and might be causally linked to it. Our aim was to generate estimates of the association between plasma CRP and metabolic syndrome phenotypes that were free from confounding and reverse causation, to assess the causal role of this protein.
Methods: We examined associations between serum CRP concentration and metabolic syndrome phenotypes in the British Women's Heart and Health Study. We then compared these estimates with those derived from a mendelian randomised framework with common CRP gene haplotypes to generate unconfounded and unbiased estimates of any causal associations.
Findings: In a sample of British women, body-mass index (BMI), systolic blood pressure, waist-to-hip ratio, serum concentrations of HDL cholesterol and triglycerides, and insulin resistance were all associated with plasma CRP concentration. CRP haplotypes were associated with plasma CRP concentration (p<0·0001). With instrumental variable analyses, there was no association between plasma CRP concentration and any of the metabolic syndrome phenotypes analysed. There was strong evidence that linear regression and mendelian randomisation based estimation gave conflicting results for the CRP–BMI association (p=0·0002), and some evidence of conflicting results for the association of CRP with the score for insulin resistance (p=0·0139), triglycerides (p=0·0313), and HDL cholesterol (p=0·0688).
Interpretation: Disparity between estimates of the association between plasma CRP and phenotypes comprising the metabolic syndrome derived from conventional analyses and those from a mendelian randomisation approach suggests that there is no causal association between CRP and the metabolic syndrome phenotypes.
1954-1959
Timpson, N.J.
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Lawlor, D.A.
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Harbord, R.M.
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Gaunt, T.R.
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Day, I.N.
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Palmer, L.J.
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Hattersley, A.T.
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Ebrahim, S.
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Lowe, G.D.
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Rumley, A.
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Davey Smith, G.
cb29a020-3ad3-4bcd-95dc-a1a43d4fe26f
2005
Timpson, N.J.
757b845f-0901-431a-abc1-786d22646e9e
Lawlor, D.A.
666139b1-03b8-4d92-bee7-98b5913fcb31
Harbord, R.M.
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Gaunt, T.R.
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Day, I.N.
e9cacaf7-f4c8-4ef0-82fa-b459ad683d50
Palmer, L.J.
b91d6236-22d5-405b-a653-bb831ae3002f
Hattersley, A.T.
c555d835-dd08-415c-be14-26940d5c582d
Ebrahim, S.
cc462d6d-f796-479f-8126-7a48fcb965d4
Lowe, G.D.
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Rumley, A.
fbd7303e-ae20-4025-8373-3a11f1cad8a8
Davey Smith, G.
cb29a020-3ad3-4bcd-95dc-a1a43d4fe26f
Timpson, N.J., Lawlor, D.A., Harbord, R.M., Gaunt, T.R., Day, I.N., Palmer, L.J., Hattersley, A.T., Ebrahim, S., Lowe, G.D., Rumley, A. and Davey Smith, G.
(2005)
C-reactive protein and its role in metabolic syndrome: mendelian randomisation study.
The Lancet, 366 (9501), .
(doi:10.1016/S0140-6736(05)67786-0).
Abstract
Background: Circulating C-reactive protein (CRP) is associated with the metabolic syndrome and might be causally linked to it. Our aim was to generate estimates of the association between plasma CRP and metabolic syndrome phenotypes that were free from confounding and reverse causation, to assess the causal role of this protein.
Methods: We examined associations between serum CRP concentration and metabolic syndrome phenotypes in the British Women's Heart and Health Study. We then compared these estimates with those derived from a mendelian randomised framework with common CRP gene haplotypes to generate unconfounded and unbiased estimates of any causal associations.
Findings: In a sample of British women, body-mass index (BMI), systolic blood pressure, waist-to-hip ratio, serum concentrations of HDL cholesterol and triglycerides, and insulin resistance were all associated with plasma CRP concentration. CRP haplotypes were associated with plasma CRP concentration (p<0·0001). With instrumental variable analyses, there was no association between plasma CRP concentration and any of the metabolic syndrome phenotypes analysed. There was strong evidence that linear regression and mendelian randomisation based estimation gave conflicting results for the CRP–BMI association (p=0·0002), and some evidence of conflicting results for the association of CRP with the score for insulin resistance (p=0·0139), triglycerides (p=0·0313), and HDL cholesterol (p=0·0688).
Interpretation: Disparity between estimates of the association between plasma CRP and phenotypes comprising the metabolic syndrome derived from conventional analyses and those from a mendelian randomisation approach suggests that there is no causal association between CRP and the metabolic syndrome phenotypes.
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Published date: 2005
Organisations:
Human Genetics
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Local EPrints ID: 24990
URI: http://eprints.soton.ac.uk/id/eprint/24990
PURE UUID: 6459779e-089d-4f77-b25a-60499baf56b3
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Date deposited: 03 Apr 2006
Last modified: 15 Aug 2024 17:10
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Contributors
Author:
N.J. Timpson
Author:
D.A. Lawlor
Author:
R.M. Harbord
Author:
T.R. Gaunt
Author:
I.N. Day
Author:
L.J. Palmer
Author:
A.T. Hattersley
Author:
S. Ebrahim
Author:
G.D. Lowe
Author:
A. Rumley
Author:
G. Davey Smith
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