Allelic association and functional studies of promoter polymorphism in the leukotriene C4 synthase gene (LTC4S) in asthma
Allelic association and functional studies of promoter polymorphism in the leukotriene C4 synthase gene (LTC4S) in asthma
Background:
LTC4 synthase is essential for the production of cysteinyl leukotrienes (Cys-LT), critical mediators in asthma. We have identified a novel promoter polymorphism at position –1072 (G/A) and a –444 (A/C) polymorphism has previously been reported. The role of these polymorphisms in the genetic susceptibility to asthma was examined.
Methods:
To test for genetic association with asthma phenotypes, 341 white families (two asthmatic siblings) and 184 non-asthmatic control subjects were genotyped. Genetic association was assessed using case control and transmission disequilibrium test (TDT) analyses. LTC4S promoter luciferase constructs
and transiently transfected human HeLa and KU812F cells were generated to determine the functional role of these polymorphisms on basal transcription.
Results:
No associations were observed in case control analyses (–1072 A, q=0.09; –444 C, q=0.29); the TDT identified a borderline association between the –444 C allele and bronchial responsiveness to methacholine (p=0.065). Asthmatic children with the –444 C allele had a lower mean basal forced expiratory volume in 1 second (97.4 v 92.7% predicted, p=0.005). LTC4S promoter luciferase analyses provided no evidence for a functional role of either polymorphism in determining basal transcription.
Conclusion:
This study does not support a role for these polymorphisms in genetic susceptibility to asthma but provides evidence to suggest a role in determining lung function parameters.
leukotriene C4 synthase gene (LTC4S), asthma, polymorphism
417-424
Sayers, I.
230e01df-0685-438a-9173-df1aead72390
Barton, S.
4f674382-ca0b-44ad-9670-e71a0b134ef0
Rorke, S.
ca4b3d19-8862-40e7-8f33-b20da825b08d
Beghe, B.
d4335e8e-fd57-41e3-9d71-69c0886bf145
Hayward, B.
bf2e18a3-70a4-472e-9a10-1b55ca288e05
Van Eerdewegh, P.
28d6e7cb-08ce-41d9-b560-021caba9ae30
Keith, T.
763038f9-17c3-4e83-b7a1-3fd562b87a66
Clough, J.B.
54c3712a-f495-4ba6-b190-73fa0ba2b30f
Ye, S.
73027825-861c-4bca-8ce6-67a325fa2d2c
Holloway, J.W.
4bbd77e6-c095-445d-a36b-a50a72f6fe1a
Sampson, A.P.
4ca76f6f-ff35-425d-a7e7-c2bd2ea2df60
Holgate, S.T.
2e7c17a9-6796-436e-8772-1fe6d2ac5edc
2003
Sayers, I.
230e01df-0685-438a-9173-df1aead72390
Barton, S.
4f674382-ca0b-44ad-9670-e71a0b134ef0
Rorke, S.
ca4b3d19-8862-40e7-8f33-b20da825b08d
Beghe, B.
d4335e8e-fd57-41e3-9d71-69c0886bf145
Hayward, B.
bf2e18a3-70a4-472e-9a10-1b55ca288e05
Van Eerdewegh, P.
28d6e7cb-08ce-41d9-b560-021caba9ae30
Keith, T.
763038f9-17c3-4e83-b7a1-3fd562b87a66
Clough, J.B.
54c3712a-f495-4ba6-b190-73fa0ba2b30f
Ye, S.
73027825-861c-4bca-8ce6-67a325fa2d2c
Holloway, J.W.
4bbd77e6-c095-445d-a36b-a50a72f6fe1a
Sampson, A.P.
4ca76f6f-ff35-425d-a7e7-c2bd2ea2df60
Holgate, S.T.
2e7c17a9-6796-436e-8772-1fe6d2ac5edc
Sayers, I., Barton, S., Rorke, S., Beghe, B., Hayward, B., Van Eerdewegh, P., Keith, T., Clough, J.B., Ye, S., Holloway, J.W., Sampson, A.P. and Holgate, S.T.
(2003)
Allelic association and functional studies of promoter polymorphism in the leukotriene C4 synthase gene (LTC4S) in asthma.
Thorax, 58 (5), .
(doi:10.1136/thorax.58.5.417).
Abstract
Background:
LTC4 synthase is essential for the production of cysteinyl leukotrienes (Cys-LT), critical mediators in asthma. We have identified a novel promoter polymorphism at position –1072 (G/A) and a –444 (A/C) polymorphism has previously been reported. The role of these polymorphisms in the genetic susceptibility to asthma was examined.
Methods:
To test for genetic association with asthma phenotypes, 341 white families (two asthmatic siblings) and 184 non-asthmatic control subjects were genotyped. Genetic association was assessed using case control and transmission disequilibrium test (TDT) analyses. LTC4S promoter luciferase constructs
and transiently transfected human HeLa and KU812F cells were generated to determine the functional role of these polymorphisms on basal transcription.
Results:
No associations were observed in case control analyses (–1072 A, q=0.09; –444 C, q=0.29); the TDT identified a borderline association between the –444 C allele and bronchial responsiveness to methacholine (p=0.065). Asthmatic children with the –444 C allele had a lower mean basal forced expiratory volume in 1 second (97.4 v 92.7% predicted, p=0.005). LTC4S promoter luciferase analyses provided no evidence for a functional role of either polymorphism in determining basal transcription.
Conclusion:
This study does not support a role for these polymorphisms in genetic susceptibility to asthma but provides evidence to suggest a role in determining lung function parameters.
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More information
Published date: 2003
Keywords:
leukotriene C4 synthase gene (LTC4S), asthma, polymorphism
Identifiers
Local EPrints ID: 24936
URI: http://eprints.soton.ac.uk/id/eprint/24936
ISSN: 0040-6376
PURE UUID: 63192231-56bf-4146-9ccf-c89f2ecd040b
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Date deposited: 05 Apr 2006
Last modified: 16 Mar 2024 03:22
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Contributors
Author:
I. Sayers
Author:
S. Rorke
Author:
B. Beghe
Author:
B. Hayward
Author:
P. Van Eerdewegh
Author:
T. Keith
Author:
J.B. Clough
Author:
S. Ye
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