Genetic variation at the chromosome 16 chemokine gene cluster: Development of a strategy for association studies in complex disease

Sheila A. Fisher; A. Moody; M. M. Mirza; A. P. Cuthbert; J. Hampe; A. Macpherson; J. Sanderson; A. Forbes; J. Mansfield; S. Schreiber; C. M. Lewis; C. G. Mathew

doi:10.1046/j.1469-1809.2003.00040.x

Genetic variation at the chromosome 16 chemokine gene cluster: Development of a strategy for association studies in complex disease

Sheila A. Fisher, A. Moody, M. M. Mirza, A. P. Cuthbert, J. Hampe, A. Macpherson, J. Sanderson, A. Forbes, J. Mansfield, S. Schreiber, C. M. Lewis, C. G. Mathew

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6 Scopus citations

Abstract

The chemokine gene cluster [CCL22, CX3CL1, CCL17] (previously known as [SCYA22, SCYD1, SCYA17]) is a candidate locus for one of the susceptibility genes for inflammatory bowel disease that are located in the pericentromeric region of chromosome 16. Screening for sequence variation at this locus led to the detection of 14 single nucleotide polymorphisms (SNPs). An efficient experimental and computational approach was developed to estimate allele frequencies and pairwise linkage disequilibrium relationships between SNPs at this locus, and to test them for association with inflammatory bowel disease. The 12 common SNPs were assigned to 5 distinct linkage disequilibrium groups. Genotyping of one SNP from each linkage disequilibrium group in a large cohort of families with inflammatory bowel disease did not provide convincing evidence of association with either Crohn's disease or ulcerative colitis. We describe an efficient experimental design from SNP screening to association testing. This strategy can be used to test candidate genes for involvement in susceptibility to complex disease.

Original language	English
Pages (from-to)	377-390
Number of pages	14
Journal	Annals of Human Genetics
Volume	67
Issue number	5
DOIs	https://doi.org/10.1046/j.1469-1809.2003.00040.x
State	Published - Sep 2003
Externally published	Yes

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Fisher, S. A., Moody, A., Mirza, M. M., Cuthbert, A. P., Hampe, J., Macpherson, A., Sanderson, J., Forbes, A., Mansfield, J., Schreiber, S., Lewis, C. M., & Mathew, C. G. (2003). Genetic variation at the chromosome 16 chemokine gene cluster: Development of a strategy for association studies in complex disease. Annals of Human Genetics, 67(5), 377-390. https://doi.org/10.1046/j.1469-1809.2003.00040.x

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title = "Genetic variation at the chromosome 16 chemokine gene cluster: Development of a strategy for association studies in complex disease",

abstract = "The chemokine gene cluster [CCL22, CX3CL1, CCL17] (previously known as [SCYA22, SCYD1, SCYA17]) is a candidate locus for one of the susceptibility genes for inflammatory bowel disease that are located in the pericentromeric region of chromosome 16. Screening for sequence variation at this locus led to the detection of 14 single nucleotide polymorphisms (SNPs). An efficient experimental and computational approach was developed to estimate allele frequencies and pairwise linkage disequilibrium relationships between SNPs at this locus, and to test them for association with inflammatory bowel disease. The 12 common SNPs were assigned to 5 distinct linkage disequilibrium groups. Genotyping of one SNP from each linkage disequilibrium group in a large cohort of families with inflammatory bowel disease did not provide convincing evidence of association with either Crohn's disease or ulcerative colitis. We describe an efficient experimental design from SNP screening to association testing. This strategy can be used to test candidate genes for involvement in susceptibility to complex disease.",

author = "Fisher, {Sheila A.} and A. Moody and Mirza, {M. M.} and Cuthbert, {A. P.} and J. Hampe and A. Macpherson and J. Sanderson and A. Forbes and J. Mansfield and S. Schreiber and Lewis, {C. M.} and Mathew, {C. G.}",

year = "2003",

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Fisher, SA, Moody, A, Mirza, MM, Cuthbert, AP, Hampe, J, Macpherson, A, Sanderson, J, Forbes, A, Mansfield, J, Schreiber, S, Lewis, CM & Mathew, CG 2003, 'Genetic variation at the chromosome 16 chemokine gene cluster: Development of a strategy for association studies in complex disease', Annals of Human Genetics, vol. 67, no. 5, pp. 377-390. https://doi.org/10.1046/j.1469-1809.2003.00040.x

TY - JOUR

T1 - Genetic variation at the chromosome 16 chemokine gene cluster

T2 - Development of a strategy for association studies in complex disease

AU - Fisher, Sheila A.

AU - Moody, A.

AU - Mirza, M. M.

AU - Cuthbert, A. P.

AU - Hampe, J.

AU - Macpherson, A.

AU - Sanderson, J.

AU - Forbes, A.

AU - Mansfield, J.

AU - Schreiber, S.

AU - Lewis, C. M.

AU - Mathew, C. G.

PY - 2003/9

Y1 - 2003/9

N2 - The chemokine gene cluster [CCL22, CX3CL1, CCL17] (previously known as [SCYA22, SCYD1, SCYA17]) is a candidate locus for one of the susceptibility genes for inflammatory bowel disease that are located in the pericentromeric region of chromosome 16. Screening for sequence variation at this locus led to the detection of 14 single nucleotide polymorphisms (SNPs). An efficient experimental and computational approach was developed to estimate allele frequencies and pairwise linkage disequilibrium relationships between SNPs at this locus, and to test them for association with inflammatory bowel disease. The 12 common SNPs were assigned to 5 distinct linkage disequilibrium groups. Genotyping of one SNP from each linkage disequilibrium group in a large cohort of families with inflammatory bowel disease did not provide convincing evidence of association with either Crohn's disease or ulcerative colitis. We describe an efficient experimental design from SNP screening to association testing. This strategy can be used to test candidate genes for involvement in susceptibility to complex disease.

AB - The chemokine gene cluster [CCL22, CX3CL1, CCL17] (previously known as [SCYA22, SCYD1, SCYA17]) is a candidate locus for one of the susceptibility genes for inflammatory bowel disease that are located in the pericentromeric region of chromosome 16. Screening for sequence variation at this locus led to the detection of 14 single nucleotide polymorphisms (SNPs). An efficient experimental and computational approach was developed to estimate allele frequencies and pairwise linkage disequilibrium relationships between SNPs at this locus, and to test them for association with inflammatory bowel disease. The 12 common SNPs were assigned to 5 distinct linkage disequilibrium groups. Genotyping of one SNP from each linkage disequilibrium group in a large cohort of families with inflammatory bowel disease did not provide convincing evidence of association with either Crohn's disease or ulcerative colitis. We describe an efficient experimental design from SNP screening to association testing. This strategy can be used to test candidate genes for involvement in susceptibility to complex disease.

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JF - Annals of Human Genetics

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Genetic variation at the chromosome 16 chemokine gene cluster: Development of a strategy for association studies in complex disease

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