多组学综合分析确定了导致非综合征性唇裂伴或不伴有腭裂的基因变异。

Shu Lou, Jing Yang, Gui Rong Zhu, Dan Dan Li, Lan Ma, Lin Wang, Yong Chu Pan
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引用次数: 0

摘要

目的通过整合多组学数据和探索与 NSCL/P 相关的易感基因,为非综合征唇裂伴或不伴腭裂(NSCL/P)的病因学提供新的见解:对 NSCL/P 进行了两阶段全基因组关联研究(GWAS),共涉及 1,069 例病例和 1,724 例对照。利用人类胚胎干细胞(hESC)启动子捕获Hi-C(pCHi-C)数据集和颅面组织染色质免疫沉淀测序(ChIP-seq),我们筛选出了顺式调控活跃的单核苷酸多态性(SNPs)及其靶基因。此外,我们还利用表达量性状位点(eQTL)分析来确定候选基因:结果:13 个 SNPs 被鉴定为与 NSCL/P 风险相关的顺式调控单元。结果:13 个 SNPs 被鉴定为与 NSCL/P 风险相关的顺式调控单元,其中 5 个 SNPs 被证明在人类早期颅面发育的染色质状态中处于活跃状态(rs7218002:几率比 [OR] 1.50,P = 8.14E-08;rs835367:几率比 [OR] 0.78,P = 3.14E-08):OR 0.78,P = 3.48E-05;rs77022994:OR 0.55,P = 1.05E-04;rs961470:OR0.73,P=1.38E-04;rs17314727:OR0.73,P=1.85E-04)。此外,pCHi-C 和 eQTL 分析优先考虑了三个候选基因(rs7218002:NTN1、rs835367:FGGY、LINC01135)。NTN1 和 FGGY 在小鼠口面部发育过程中表达。NTN1、FGGY 和 LINC01135 的缺失分别与腭裂和唇裂、面部形态异常和悬雍垂双裂以及面部异常有关:我们的研究发现了与 NSCL/P 相关的五个 SNPs(rs7218002、rs835367、rs77022994、rs961470 和 rs17314727)和三个易感基因(NTN1、FGGY 和 LINC01135)。这些发现有助于更好地了解相关遗传因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Integrative Multi-omics Analysis Identifies Genetic Variants Contributing to Non-syndromic Cleft Lip with or without Cleft Palate.

Objective: To provide novel insights into the aetiology of non-syndromic cleft lip with or without cleft palate (NSCL/P) by integrating multi-omics data and exploring susceptibility genes associated with NSCL/P.

Methods: A two-stage genome-wide association study (GWAS) of NSCL/P was performed, involving a total of 1,069 cases and 1,724 controls. Using promoter capture Hi-C (pCHi-C) datasets in human embryonic stem cells (hESC) and chromatin immunoprecipitation sequencing (ChIP-seq) in craniofacial tissues, we filtered out single nucleotide polymorphisms (SNPs) with active cis-regulation and their target genes. Additionally, we employed expression quantitative trait loci (eQTL) analysis to identify candidate genes.

Results: Thirteen SNPs were identified as cis-regulation units associated with the risk of NSCL/P. Five of these were proven to be active in chromatin states in early human craniofacial development (rs7218002: odds ratio [OR] 1.50, P = 8.14E-08; rs835367: OR 0.78, P = 3.48E- 05; rs77022994: OR 0.55, P = 1.05E-04; rs961470: OR 0.73, P = 1.38E-04; rs17314727: OR 0.73, P = 1.85E-04). Additionally, pCHi-C and eQTL analysis prioritised three candidate genes (rs7218002: NTN1, rs835367: FGGY, LINC01135). NTN1 and FGGY were expressed in mouse orofacial development. Deficiencies in NTN1, FGGY and LINC01135 were associated with cleft palate and cleft lip, abnormal facial shape and bifid uvula, and abnormality of the face, respectively.

Conclusion: Our study identified five SNPs (rs7218002, rs835367, rs77022994, rs961470 and rs17314727) and three susceptibility genes (NTN1, FGGY and LINC01135) associated with NSCL/P. These findings contribute to a better understanding of the genetic factors involved.

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