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Association between polymorphisms in the progesterone receptor gene and endometriosis

Treloar, S. A., Zhao, Z. Z., Armitage, T., Duffy, D. L., Wicks, J., O'Connor, D. T., Martin, N. G. and Montgomery, G. W. (2005) Association between polymorphisms in the progesterone receptor gene and endometriosis. Molecular Human Reproduction, 11 9: 641-647.


Author(s) Treloar, S. A.
Zhao, Z. Z.
Armitage, T.
Duffy, D. L.
Wicks, J.
O'Connor, D. T.
Martin, N. G.
Montgomery, G. W.
Title Association between polymorphisms in the progesterone receptor gene and endometriosis
Journal name Molecular Human Reproduction
Publication date 2005
Volume number 11
Issue number 9
ISSN 1360-9947
Start page 641
End page 647
Total pages 7
Editor(s) R. Ivell
Place of publication Oxford, UK
Publisher Oxford University Press
Collection year 2005
Language eng
Subject C1
321011 Medical Genetics
730107 Inherited diseases (incl. gene therapy)
Abstract The progesterone receptor (PR) is a candidate gene for the development of endometriosis, a complex disease with strong hormonal features, common in women of reproductive age. We typed the 306 base pair Alu insertion (AluIns) polymorphism in intron G of PR in 101 individuals, estimated linkage disequilibrium (LD) between five single-nucleotide polymorphisms (SNPs) across the PR locus in 980 Australian triads (endometriosis case and two parents) and used transmission disequilibrium testing (TDT) for association with endometriosis. The five SNPs showed strong pairwise LD, and the AluIns was highly correlated with proximal SNPs rs1042839 ({Delta}2 = 0.877, D9 = 1.00, P < 0.0001) and rs500760 ({Delta}2 = 0.438, D9 = 0.942, P < 0.0001). TDT showed weak evidence of allelic association between endometriosis and rs500760 (P = 0.027) but not in the expected direction. We identified a common susceptibility haplotype GGGCA across the five SNPs (P = 0.0167) in the whole sample, but likelihood ratio testing of haplotype transmission and non-transmission of the AluIns and flanking SNPs showed no significant pattern. Further, analysis of our results pooled with those from two previous studies suggested that neither the T2 allele of the AluIns nor the T1/T2 genotype was associated with endometriosis.
Keyword(s) endometriosis
linkage disequilibrium
polymorphism
progesterone receptor
transmission disequilibrium test
 
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