Association analysis between forkhead box E1 gene and non-syndromic cleft lip with or without cleft palate in Han Chinese population.

Hua xi kou qiang yi xue za zhi = Huaxi kouqiang yixue zazhi = West China journal of stomatology Pub Date : 2025-02-01 DOI:10.7518/hxkq.2024.2024110

Sixuan Jia, Sidi Zhang, Yue You, Jialin Sun, Shijun Duan, Bing Shi, Zhonglin Jia

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Abstract

Objectives: This study aims to explore the association between single nucleotide polymorphisms (SNPs) loci near the haplotype region hg19 chr9:100560865-100660865 of the forkhead box E1 (FOXE1) gene and the occurrence of non-syndromic cleft lip with or without cleft palate (NSCL/P) in western Han Chinese population.

Methods: In the first stage, our study recruited 159 NSCL/P patients and performed targeted region sequencing to screen SNPs loci near the haplotype region of the FOXE1 gene associated with NSCL/P. In the second stage, we selected 21 common SNPs and re-enrolled 1 000 non-syndromic cleft lip only (NSCLO) patients, 1 000 non-syndromic cleft palate only (NSCPO) patients, and 1 000 normal controls to verify the association. PLINK software was used to perform Hardy-Weinberg equilibrium (HWE) test. Association analysis for common variants, gene burden analysis for rare mutations, and function prediction of SNPs with non-synonymous mutations were performed using Mutation Taster and other software programs.

Results: In the first stage, 126 variants, including 76 single nucleotide variants and 50 insertion-deletions were identified. All the included SNPs confirmed to HWE, and the results of gene burden analysis and prediction of functional harmfulness for rare variants were not statistically significant. Association analysis showed that rs13292899 of the FOXE1 gene was significantly associated with NSCL/P (P=1.85E-27) and was also correlated with NSCLO (P=6.41E-23) and non-syndromic cleft lip with cleft palate (NSCLP) (P=2.36E-15) subtypes. In the validation phase, rs79268293 (P=0.013, P=0.022), rs10983951 (P=0.009 2, P=0.007 6), rs117227387 (P=0.009 2, P=0.007 6), rs3758250 (P=0.009 2, P=0.007 6), and rs116899397 (P=0.009 2, P=0.007 6) were significantly associated with NSCLO and NSCPO; rs13292899 (P=0.008 5), rs74606599 (P=0.008 3), rs143226042 (P=0.008 3), and rs117236550 (P=0.01) were associated with the occurrence of NSCLO; and rs12343182 (P=0.008 7), rs10119760 (P=0.012), rs10113907 (P=0.012), and rs13299924 (P=0.012) were associated with the occurrence of NSCPO.

Conclusions: This study found a new susceptible SNP rs13292899 of the FOXE1 gene that is closely associated with NSCL/P and NSCLO subtype and 13 other SNPs associated with NSCLO or NSCPO.

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汉族人群叉头盒E1基因与非综合征性唇裂伴或不伴腭裂的相关性分析。

目的：探讨西部汉族人群叉头盒E1 （FOXE1）基因单倍型区域hg19 chr9:100560865-100660865附近的单核苷酸多态性（snp）位点与非综合征性唇裂伴或不伴腭裂（NSCL/P）发生的关系。方法：在第一阶段，我们招募了159例nsl /P患者，并进行了靶向区域测序，以筛选与nsl /P相关的FOXE1基因单倍型区域附近的snp位点。在第二阶段，我们选择了21个常见snp，并重新招募了1000名非综合征性单唇裂（NSCLO）患者、1000名非综合征性单唇裂（NSCPO）患者和1000名正常对照者来验证其相关性。采用PLINK软件进行Hardy-Weinberg平衡（HWE）检验。使用Mutation Taster和其他软件程序进行常见变异的关联分析、罕见突变的基因负担分析和非同义突变snp的功能预测。结果：第一阶段共鉴定出126个变异，包括76个单核苷酸变异和50个插入缺失。所有纳入的SNPs均证实了HWE，基因负担分析和罕见变异功能危害预测结果均无统计学意义。关联分析显示，FOXE1基因rs13292899与NSCL/P显著相关（P=1.85E-27），与NSCLO （P=6.41E-23）和非综合征型唇裂伴腭裂（NSCLP）亚型（P=2.36E-15）也存在相关性。验证期，rs79268293 （P=0.013， P=0.022）、rs10983951 （P=0.009 2， P=0.007 6）、rs117227387 （P=0.009 2， P=0.007 6）、rs3758250 （P=0.009 2， P=0.007 6）、rs116899397 （P=0.009 2， P=0.007 6）与NSCLO和NSCPO显著相关；rs13292899 （P= 0.0085）、rs74606599 （P= 0.0083）、rs143226042 （P= 0.0083）、rs117236550 （P=0.01）与NSCLO发生相关；rs12343182 （P=0.008 7）、rs10119760 （P=0.012）、rs10113907 （P=0.012）、rs13299924 （P=0.012）与NSCPO发生相关。结论：本研究发现与nsscl /P和NSCLO亚型密切相关的FOXE1基因新易感SNP rs13292899和与NSCLO或nsscpo相关的其他13个SNP。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Hua xi kou qiang yi xue za zhi = Huaxi kouqiang yixue zazhi = West China journal of stomatology

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