| Literature DB >> 30019117 |
Jiaqi Liu1,2,3, Yangzhong Zhou2,4, Sen Liu1,2,5, Xiaofei Song6, Xin-Zhuang Yang7, Yanhui Fan8, Weisheng Chen1,2,5, Zeynep Coban Akdemir6, Zihui Yan1,2,5, Yuzhi Zuo1,2,5, Renqian Du6, Zhenlei Liu2,9, Bo Yuan6, Sen Zhao1,2,5, Gang Liu1,2,5, Yixin Chen1,2,5, Yanxue Zhao1,2,5, Mao Lin1,2,5, Qiankun Zhu1,2,5, Yuchen Niu2,5,7, Pengfei Liu6, Shiro Ikegawa10, You-Qiang Song8, Jennifer E Posey6, Guixing Qiu1,2,5, Feng Zhang11,12, Zhihong Wu2,5,7, James R Lupski6,13,14, Nan Wu15,16,17.
Abstract
With the recent advance in genome-wide association studies (GWAS), disease-associated single nucleotide polymorphisms (SNPs) and copy number variants (CNVs) have been extensively reported. Accordingly, the issue of incorrect identification of recombination events that can induce the distortion of multi-allelic or hemizygous variants has received more attention. However, the potential distorted calculation bias or significance of a detected association in a GWAS due to the coexistence of CNVs and SNPs in the same genomic region may remain under-recognized. Here we performed the association study within a congenital scoliosis (CS) cohort whose genetic etiology was recently elucidated as a compound inheritance model, including mostly one rare variant deletion CNV null allele and one common variant non-coding hypomorphic haplotype of the TBX6 gene. We demonstrated that the existence of a deletion in TBX6 led to an overestimation of the contribution of the SNPs on the hypomorphic allele. Furthermore, we generalized a model to explain the calculation bias, or distorted significance calculation for an association study, that can be 'induced' by CNVs at a locus. Meanwhile, overlapping between the disease-associated SNPs from published GWAS and common CNVs (overlap 10%) and pathogenic/likely pathogenic CNVs (overlap 99.69%) was significantly higher than the random distribution (p < 1 × 10-6 and p = 0.034, respectively), indicating that such co-existence of CNV and SNV alleles might generally influence data interpretation and potential outcomes of a GWAS. We also verified and assessed the influence of colocalizing CNVs to the detection sensitivity of disease-associated SNP variant alleles in another adolescent idiopathic scoliosis (AIS) genome-wide association study. We proposed that detecting co-existent CNVs when evaluating the association signals between SNPs and disease traits could improve genetic model analyses and better integrate GWAS with robust Mendelian principles.Entities:
Mesh:
Year: 2018 PMID: 30019117 PMCID: PMC6200315 DOI: 10.1007/s00439-018-1910-3
Source DB: PubMed Journal: Hum Genet ISSN: 0340-6717 Impact factor: 4.132