Genetic analysis of Wnt/PCP genes in neural tube defects

Zhongzhong Chen; Yunping Lei; Xuanye Cao; Yufang Zheng; Fang Wang; Yihua Bao; Rui Peng; Richard H. Finnell; Ting Zhang; Hongyan Wang

doi:10.1186/s12920-018-0355-9

BMC Medical Genomics (Apr 2018)

Affiliations

Zhongzhong Chen: Obstetrics and Gynecology Hospital, State Key Laboratory of Genetic Engineering at School of Life Sciences, Institute of Reproduction and Development, Fudan University
Yunping Lei: Departments of Molecular and Cellular Biology and Medicine, Baylor College of Medicine
Xuanye Cao: Departments of Molecular and Cellular Biology and Medicine, Baylor College of Medicine
Yufang Zheng: Obstetrics and Gynecology Hospital, State Key Laboratory of Genetic Engineering at School of Life Sciences, Institute of Reproduction and Development, Fudan University
Fang Wang: Beijing Municipal Key Laboratory of Child Development and Nutriomics, Capital Institute of Pediatrics
Yihua Bao: Beijing Municipal Key Laboratory of Child Development and Nutriomics, Capital Institute of Pediatrics
Rui Peng: Obstetrics and Gynecology Hospital, State Key Laboratory of Genetic Engineering at School of Life Sciences, Institute of Reproduction and Development, Fudan University
Richard H. Finnell: Obstetrics and Gynecology Hospital, State Key Laboratory of Genetic Engineering at School of Life Sciences, Institute of Reproduction and Development, Fudan University
Ting Zhang: Beijing Municipal Key Laboratory of Child Development and Nutriomics, Capital Institute of Pediatrics
Hongyan Wang: Obstetrics and Gynecology Hospital, State Key Laboratory of Genetic Engineering at School of Life Sciences, Institute of Reproduction and Development, Fudan University

DOI: https://doi.org/10.1186/s12920-018-0355-9
Journal volume & issue: Vol. 11, no. 1
pp. 1 – 9

Abstract

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Abstract Background Mouse homozygous mutants in Wnt/planar cell polarity (PCP) pathway genes have been shown to cause neural tube defects (NTDs) through the disruption of normal morphogenetic processes critical to neural tube closure (NTC). Knockout mice that are heterozygotes of single PCP genes likely fail to produce NTD phenotypes, yet damaging variants detected in human NTDs are almost always heterozygous, suggesting that other deleterious interacting variants are likely to be present. Nonetheless, the Wnt/PCP pathway remains a genetic hotspot. Addressing these issues is essential for understanding the genetic etiology of human NTDs. Methods We performed targeted next-generation sequencing (NGS) on 30 NTD-predisposing Wnt/PCP pathway genes in 184 Chinese NTD cases. We subsequently replicated our findings for the CELSR1 gene in an independent cohort of 292 Caucasian NTD samples from the USA. Functional validations were confirmed using in vitro assays. Results CELSR1, CELSR2 and CELSR3 genes were significantly clustered with rare driver coding mutations (q-value< 0.05) demonstrated by OncodriveCLUST. During the validation stage, the number of rare loss of function (LoF) variants in CELSR1 was significantly enriched in NTDs compared with the LoF counts in the ExAC database (p < 0.001). Functional studies indicated compound heterozygote variants of CELSR2 p.Thr2026Met and DVL3 p.Asp403Asn result in down regulation of PCP signals. Conclusions These data indicate rare damaging variants of the CELSR genes, identified in ~ 14% of NTD cases, are expected to be driver genes in the Wnt/PCP pathway. Compound damaging variants of CELSR genes and other Wnt/PCP genes, which were observed in 3.3% of the studied NTD cohort, are also expected to amplify these effects at the pathway level.

Published in BMC Medical Genomics

ISSN: 1755-8794 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine; Science: Biology (General): Genetics
Website: https://bmcmedgenomics.biomedcentral.com

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