1p36染色体WNT4区域与子宫内膜异位症相关变异的精细定位

International journal of molecular epidemiology and genetics Pub Date : 2013-11-28 eCollection Date: 2013-01-01
Hien Tt Luong, Jodie N Painter, Konstantin Shakhbazov, Brett Chapman, Anjali K Henders, Joseph E Powell, Dale R Nyholt, Grant W Montgomery
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引用次数: 0

摘要

全基因组关联研究显示,1p36染色体上跨越潜在候选基因WNT4、CDC42和LINC00339的标记与子宫内膜异位症有很强的关联。WNT4参与子宫的发育,CDC42和LINC00339的表达在子宫内膜异位症中发生改变。我们进行了精细的定位,以检查编码变体在WNT4和CDC42中的作用,并确定了在该区域具有最强关联证据的关键snp。我们发现WNT4和CDC42的罕见编码变异只存在于子宫内膜异位症病例中。频率很低,不能解释与子宫内膜异位症风险增加相关的常见信号。与已发表的基因组扫描中报道的rs7521902相比,染色体1p36区域5个常见snp的基因型显示出更强的关联信号。其中,三个snp rs12404660、rs3820282和rs55938609位于具有潜在功能作用的DNA序列中,包括与FOXA1、FOXA2、ESR1和ESR2的转录因子结合位点重叠。需要进行功能研究以确定与子宫内膜异位症风险有关的基因或基因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Fine mapping of variants associated with endometriosis in the WNT4 region on chromosome 1p36.

Fine mapping of variants associated with endometriosis in the WNT4 region on chromosome 1p36.

Fine mapping of variants associated with endometriosis in the WNT4 region on chromosome 1p36.

Fine mapping of variants associated with endometriosis in the WNT4 region on chromosome 1p36.

Genome-wide association studies show strong evidence of association with endometriosis for markers on chromosome 1p36 spanning the potential candidate genes WNT4, CDC42 and LINC00339. WNT4 is involved in development of the uterus, and the expression of CDC42 and LINC00339 are altered in women with endometriosis. We conducted fine mapping to examine the role of coding variants in WNT4 and CDC42 and determine the key SNPs with strongest evidence of association in this region. We identified rare coding variants in WNT4 and CDC42 present only in endometriosis cases. The frequencies were low and cannot account for the common signal associated with increased risk of endometriosis. Genotypes for five common SNPs in the region of chromosome 1p36 show stronger association signals when compared with rs7521902 reported in published genome scans. Of these, three SNPs rs12404660, rs3820282, and rs55938609 were located in DNA sequences with potential functional roles including overlap with transcription factor binding sites for FOXA1, FOXA2, ESR1, and ESR2. Functional studies will be required to identify the gene or genes implicated in endometriosis risk.

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