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Coding Variants in HOOK2 and GTPBP3 May Contribute to Risk of Primary Angle Closure Glaucoma

机译:Hook2和GTPBP3中的编码变体可能有助于主要角度闭合青光眼的风险

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Primary angle closure glaucoma (PACG) is a major cause of blindness worldwide. This study proposed to screen candidate PACG-associated variants in Chinese Han people. Whole exome sequencing was applied to five confirmed PACG patients and two primary angle closure suspect individuals within a PACG-enriched Chinese Han family. A series of bioinformatics analyses were implemented to obtain high-risk single nucleotide variant (SNV) loci for PACG, which were subsequently used for linkage analysis for identifying linkage genome regions. In addition, MassARRAY SNV genotyping was applied to high-risk PACG loci as well as those within linkage regions in another independent cohort including 251 PACG and 251 normal samples to further screen high-confidence SNVs. A total of 27 loci in 19 genes remained after linkage analysis. The 19 genes were significantly enriched in biological processes tightly related to PACG, including retinol metabolism and salmonella infection. Two nonsynonymous SNV loci, rs897804 in exon15 of HOOK2 and rs3745193 in exon7 of GTPBP3, were recognized with higher variant frequency in PACG samples than that in control samples after association analysis of MassARRAY SNV genotyping data. This study sheds new light on the understanding of PACG incidence among Chinese Han people.
机译:主要角度闭合青光眼(PACG)是全球失明的主要原因。本研究提出在中国汉族人中筛选候选PACG相关变种。将整个exome测序适用于五个确认的PACG患者,并在PACG-RICHED的中国汉族家庭内犯罪嫌疑人。实施了一系列生物信息学分析以获得PACG的高风险单核苷酸变体(SNV)基因座,随后用于识别链接基因组区域的连杆分析。此外,Massarray SNV基因分型应用于高风险的PACG基因座以及另一种独立队列中的联动区内的那些,包括251帕格和251个正常样品,以进一步筛选高击中SNV。连杆分析后,总共27个基因内的基因座。与PACG紧密相关的生物过程中,19个基因显着富集,包括视黄醇代谢和沙门氏菌感染。在GTPBP3的Exon7的Hook2和RS3745193中的两个非同义的SNV基因座,RS897804在PACG样品中的频率较高的频率较高,比对照样品在MassArray SNV基因分型数据的关联分析中的较高。这项研究揭示了对中国汉族人民PACG发病率的了解。

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