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A genome-wide association study identifies novel susceptibility genetic variation for thyrotoxic hypokalemic periodic paralysis

机译:全基因组关联研究确定了甲状腺毒性低钾性周期性麻痹的新型易感性遗传变异

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摘要

Several lines of evidence have pointed out that genetic components have roles in thyrotoxic hypokalemic periodic paralysis (TTPP). In this study, for the first time we performed genome-wide association study (GWAS) in male hyperthyroid subjects in order to identify genetic loci conferring susceptibility to TTPP. We genotyped 78 Thai male TTPP cases and 74 Thai male hyperthyroid patients without hypokalemia as controls with Illumina Human-Hap610 Genotyping BeadChip. Among the SNPs analyzed in the GWAS, rs312729 at chromosome 17q revealed the lowest P-value for association (P=2.09 × 10 -7). After fine mapping for linkage disequilibrium blocks surrounding the landmark SNP, we found a significant association of rs623011; located at 75 kb downstream of KCNJ2 on chromosome 17q, reached the GWAS significance after Bonferroni's adjustment (P=3.23 × 10 -8, odds ratio (OR)=6.72; 95% confidence interval (CI)=3.11-14.5). The result was confirmed in an independent cohort of samples consisting of 28 TTPP patients and 48 controls using the same clinical criteria diagnosis (replication analysis P=3.44 × 10 -5, OR=5.13; 95% CI=1.87-14.1; combined-analysis P=3.71 × 10 -12, OR=5.47; 95% CI=3.04-9.83).
机译:有几条证据指出,遗传成分在甲状腺毒性低钾性周期性麻痹(TTPP)中起作用。在这项研究中,我们首次在男性甲状腺功能亢进受试者中进行了全基因组关联研究(GWAS),以鉴定赋予TTPP敏感性的遗传基因座。我们使用Illumina Human-Hap610基因分型BeadChip对78例泰国男性TTPP患者和74例无低钾血症的泰国男性甲状腺功能亢进患者进行了基因分型。在GWAS中分析的SNP中,染色体17q的rs312729揭示了最低的关联P值(P = 2.09×10 -7)。在对具有标志性的SNP周围的连锁不平衡区进行精细映射后,我们发现rs623011的显着关联。位于第17q染色体KCNJ2下游75 kb处的基因,经Bonferroni调整后达到GWAS显着性(P = 3.23×10 -8,优势比(OR)= 6.72; 95%置信区间(CI)= 3.11-14.5)。在相同的临床标准诊断下,在由28名TTPP患者和48名对照组成的独立样本中证实了该结果(重复分析P = 3.44×10 -5,OR = 5.13; 95%CI = 1.87-14.1;联合分析P = 3.71×10 -12,OR = 5.47; 95%CI = 3.04-9.83)。

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