Genome-wide analysis of parent-of-origin effects in non-syndromic orofacial clefts

被引:0
作者
Paras Garg
Kerstin U Ludwig
Anne C Böhmer
Michele Rubini
Regine Steegers-Theunissen
Peter A Mossey
Elisabeth Mangold
Andrew J Sharp
机构
[1] Icahn School of Medicine at Mount Sinai,Department of Genetics and Genomic Sciences
[2] Hess Center for Science and Medicine,Department of Genomics
[3] Life and Brain Center,Department of Experimental and Diagnostic Medicine
[4] University of Bonn,Department of Obstetrics and Gynaecology
[5] Institute of Human Genetics,Department of Epidemiology
[6] University of Bonn,undefined
[7] Medical Genetics Unit,undefined
[8] University of Ferrara,undefined
[9] and Clinical Genetics,undefined
[10] Erasmus Medical Center,undefined
[11] University Medical Center,undefined
[12] Radboud University Nijmegen,undefined
[13] Orthodontic Unit,undefined
[14] Dental Hospital and School,undefined
[15] University of Dundee,undefined
来源
European Journal of Human Genetics | 2014年 / 22卷
关键词
maternal effect; folic acid; imprinting; cleft lip; cleft palate;
D O I
暂无
中图分类号
学科分类号
摘要
Parent-of-origin (PofO) effects, such as imprinting are a phenomenon where the effect of variants depends on parental origin. Conventional association studies assume that phenotypic effects are independent of parental origin, and are thus severely underpowered to detect such non-Mendelian effects. Risk of orofacial clefts is influenced by genetic and environmental effects, the latter including maternal-specific factors such as perinatal smoking and folate intake. To identify variants showing PofO effects in orofacial clefts we have used a modification of the family-based transmission disequilibrium test to screen for biased transmission from mothers and fathers to affected offspring, biased ratios of maternal versus paternal transmission, and biased frequencies of reciprocal classes of heterozygotes among offspring. We applied these methods to analyze published genome-wide single-nucleotide polymorphism (SNP) data from ∼2500 trios mainly of European and Asian ethnicity with non-syndromic orofacial clefts, followed by analysis of 64 candidate SNPs in a replication cohort of ∼1200 trios of European origin. In our combined analysis, we did not identify any SNPs achieving conventional genome-wide significance (P<5 × 10−8). However, we observed an overall excess of loci showing maternal versus paternal transmission bias (P=0.013), and identified two loci that showed nominally significant effects in the same direction in both the discovery and replication cohorts, raising the potential for PofO effects. These include a possible maternal-specific transmission bias associated with rs12543318 at 8q21.3, a locus identified in a recent meta-analysis of non-syndromic cleft (maternal-specific P=1.5 × 10−7, paternal-specific P=0.17). Overall, we conclude from this analysis that there are subtle hints of PofO effects in orofacial clefting.
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页码:822 / 830
页数:8
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