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Association studies of variants in MEIS1, BTBD9, and MAP2K5/SKOR1 with restless legs syndrome in a US population.

机译:在美国人群中,MEIS1,BTBD9和MAP2K5 / SKOR1中的变异与腿不安综合症的关联研究。

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BACKGROUND: A genome-wide association study (GWAS) identified significant association between variants in MEIS1, BTBD9, and MAP2K5/SKOR1 and restless legs syndrome (RLS). However, many independent replication studies are needed to unequivocally establish a valid genotype-phenotype association across various populations. To further validate the GWAS findings, we investigated three variants, rs2300478 in MEIS1, rs9357271 in BTBD9, and rs1026732 in MAP2K5/SKOR1 in 38 RLS families and 189 RLS patients/560 controls from the US for their association with RLS. METHOD: Both family-based and population-based case-control association studies were carried out. RESULTS: The family-based study showed that SNP rs1026732 in MAP2K5/SKOR1 was significantly associated with RLS (P=0.01). Case-control association studies showed significant association between all three variants and RLS (P=0.0001/OR=1.65, P=0.0021/OR=1.59, and P=0.0011/OR=1.55 for rs2300478, rs9357271, and rs1026732, respectively). CONCLUSION: Variants in MEIS1, BTBD9, and MAP2K5/SKOR1 confer a significant risk of RLS in a US population.
机译:背景:全基因组关联研究(GWAS)确定了MEIS1,BTBD9和MAP2K5 / SKOR1变异与不安腿综合征(RLS)之间的显着关联。但是,需要许多独立的复制研究来明确地建立跨各种人群的有效基因型-表型关联。为了进一步验证GWAS的发现,我们研究了38个RLS家庭和189个来自美国的RLS患者/ 560对照的3个变体,分别是MEIS1中的rs2300478,BTBD9中的rs9357271和MAP2K5 / SKOR1中的rs1026732。方法:进行了基于家庭和基于人口的病例对照协会研究。结果:基于家庭的研究表明,MAP2K5 / SKOR1中的SNP rs1026732与RLS显着相关(P = 0.01)。病例对照关联研究显示,这三个变体与RLS之间存在显着关联(对于rs2300478,rs9357271和rs1026732,分别为P = 0.0001 / OR = 1.65,P = 0.0021 / OR = 1.59和P = 0.0011 / OR = 1.55)。结论:MEIS1,BTBD9和MAP2K5 / SKOR1的变异在美国人群中具有显着的RLS风险。

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