北京大学学报(医学版) ›› 2024, Vol. 56 ›› Issue (5): 775-780. doi: 10.19723/j.issn.1671-167X.2024.05.004

• 论著 • 上一篇    下一篇

中国人群非综合征型唇裂伴或不伴腭裂的单核苷酸多态性遗传度

薛恩慈1, 陈曦1, 王雪珩1, 王斯悦1, 王梦莹1, 李劲1, 秦雪英1, 武轶群1, 李楠2, 李静3, 周治波2, 朱洪平2, 吴涛1,*(), 陈大方1, 胡永华1   

  1. 1. 北京大学公共卫生学院流行病与卫生统计学系,北京 100191
    2. 北京大学口腔医学院口腔颌面外科,北京 100081
    3. 北京大学口腔医学院儿童口腔科,北京 100081
  • 收稿日期:2021-03-18 出版日期:2024-10-18 发布日期:2024-10-16
  • 通讯作者: 吴涛 E-mail:twu@bjmu.edu.cn
  • 基金资助:
    国家自然科学基金(81102178)

Single nucleotide polymorphism heritability of non-syndromic cleft lip with or without cleft palate in Chinese population

Enci XUE1, Xi CHEN1, Xueheng WANG1, Siyue WANG1, Mengying WANG1, Jin LI1, Xueying QIN1, Yiqun WU1, Nan LI2, Jing LI3, Zhibo ZHOU2, Hongping ZHU2, Tao WU1,*(), Dafang CHEN1, Yonghua HU1   

  1. 1. Department of Epidemiology and Biostatistics, Peking University School of Public Health, Beijing 100191, China
    2. Department of Oral and Maxillofacial Surgery, Peking University School of Stomatology, Beijing 100081, China
    3. Department of Pediatric Dentistry, Peking University School of Stomatology, Beijing 100081, China
  • Received:2021-03-18 Online:2024-10-18 Published:2024-10-16
  • Contact: Tao WU E-mail:twu@bjmu.edu.cn
  • Supported by:
    the National Natural Science Foundation of China(81102178)

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摘要:

目的: 探索非综合征型唇裂伴或不伴腭裂(non-syndromic cleft lip with or without cleft palate, NSCL/P)全基因组常见遗传变异对NSCL/P风险的影响。方法: 利用全基因组关联研究(genome-wide association study, GWAS)数据,以全基因组单核苷酸多态性(single nucleotide polymorphism, SNP)遗传度和基因组不同分区SNP遗传度评估基因组上常见变异的效应。对GWAS汇总数据进行质量控制,标准包括数据中无缺失值、弱势等位基因频率≥1%、P值在0~1、SNP正负链明确等。利用连锁不平衡得分回归计算NSCL/P的SNP遗传度,采用分层的连锁不平衡得分回归计算基因组编码区、启动子区、内含子区、增强子区和超级增强子区的分区SNP遗传度,并评估不同分区内的富集度,分析工具为LDSC (v1.0.1)软件。结果: 纳入中国人群806个NSCL/P核心家系(2 418人)的GWAS数据,490 593个SNP通过质量控制,被纳入到SNP遗传度的计算中。观测样本中NSCL/P的SNP遗传度为0.55(95%CI: 0.28~0.82), 由于观测样本患病率较高,按中国人群患病率转换为一般人群后SNP遗传度为0.37(95%CI: 0.19~0.55)。SNP遗传度在增强子区的富集度为15.70(P=0.04),在超级增强子区的富集度为3.18(P=0.03)。结论: 基因组常见变异有助于解释一部分中国人群NSCL/P目前未被解释的遗传度,同时中国人群NSCL/P的SNP遗传度在增强子分区和超级增强子分区中显著富集,提示该区域中可能存在未被发现的遗传致病因素。

关键词: 非综合征型唇裂伴或不伴腭裂, 单核苷酸多态性遗传度, 核心家系

Abstract:

Objective: To delve into the intricate relationship between common genetic variations across the entire genome and the risk of non-syndromic cleft lip with or without cleft palate (NSCL/P). Methods: Utilizing summary statistics data from genome-wide association studies (GWAS), a thorough investigation to evaluate the impact of common variations on the genome were undertook. This involved assessing single nucleotide polymorphism (SNP) heritability across the entire genome, as well as within specific genomic regions. To ensure the robustness of our analysis, stringent quality control measures were applied to the GWAS summary statistics data. Criteria for inclusion encompassed the absence of missing values, a minor allele frequency ≥1%, P-values falling within the range of 0 to 1, and clear SNP strand orientation. SNP meeting these stringent criteria were then meticulously included in our analysis. The SNP heritability of NSCL/P was calculated using linkage disequilibrium score regression. Additionally, hierarchical linkage disequilibrium score regression to partition SNP heritability within coding regions, promoters, introns, enhancers, and super enhancers were employed, and the enrichment levels within different genomic regions using LDSC (v1.0.1) software were further elucidated. Results: Our study drew upon GWAS summary statistics data obtained from 806 NSCL/P trios, comprising a total of 2 418 individuals from the Chinese population. Following rigorous quality control procedures, 490 593 out of 492 993 SNP were deemed suitable for inclusion in SNP heritability calculations. The observed SNP heritability of NSCL/P was 0.55 (95%CI: 0.28-0.82). Adjusting for the elevated disease pre-valence within our sample, the SNP heritability scaled down to 0.37 (95%CI: 0.19-0.55) based on the prevalence observed in the general Chinese population. Notably, our enrichment analysis unveiled significant enrichment of SNP heritability within enhancer regions (15.70, P=0.04) and super enhancer regions (3.18, P=0.03). Conclusion: Our study sheds light on the intricate interplay between common genetic variations and the risk of NSCL/P in the Chinese population. By elucidating the SNP heritability landscape across different genomic regions, we contribute valuable insights into the genetic basis of NSCL/P. The significant enrichment of SNP heritability within enhancer and super enhancer regions underscores the potential role of these regulatory elements in shaping the genetic susceptibility to NSCL/P. This paves the way for further research aimed at uncovering novel genetic pathogenic factors underlying NSCL/P pathogenesis.

Key words: Non-syndromic cleft lip with or without cleft palate, Single nucleotide polymorphism heritability, Case-parent trios

中图分类号: 

  • R394.1

表1

806个中国NSCL/P核心家系的地区和性别分布"

Site Male Female Total
China Taiwan, n 139 94 233
Shandong, n 193 81 274
Hubei, n 132 55 187
Sichuan, n 75 37 112
Total, n 539 267 806

表2

NSCL/P的分区SNP遗传度分析"

Annotation Proportion of SNP Proportion of SNP heritability Enrichment P for enrichment
Coding 0.014 0.035 2.44 0.91
Promoter 0.046 0.144 3.12 0.70
Intron 0.388 0.289 0.74 0.63
Enhancer 0.042 0.654 15.70 0.04
Super-enhancer 0.167 0.532 3.18 0.03
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