The Maternal ITPK1 Gene Polymorphism is Associated with Neural Tube Defects in a High-risk Chinese Population

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2014 Jan 28

PMID 24465924

Citations 12

Authors

Zhen Guan

Jianhua Wang

Jin Guo

Fang Wang

Xiuwei Wang

Guannan Li

Qiu Xie

Xu Han

Bo Niu

Ting Zhang

Affiliations

Soon will be listed here.

Abstract

Background: Epidemiological surveys and animal studies have revealed that inositol metabolism is associated with NTDs, but the mechanisms are not clear. Inositol 1,3,4-trisphosphate 5/6-kinase (ITPK1) is a pivotal regulatory enzyme in inositol metabolic pathway. The objective was to assess the potential impact of the maternal ITPK1 genotypes on the inositol parameter and on the NTD risk in a NTD high-risk area in China.

Methodology/results: A case-control study of pregnant women affected with NTDs (n = 200) and controls (n = 320) was carried out. 13 tag SNPs of ITPK1 were selected and genotyped by the Sequenom MassArray system. We found that 4 tag SNPs were statistically significant in spina bifida group (P<0.05). MACH was used to impute the un-genotyped SNPs in ITPK1 locus and showed that 3 meaningful SNPs in the non-coding regions were significant. We also predicted the binding capacity of transcription factors in the positive SNPs using the bioinformatics method and found that only rs3783903 was located in the conserved sequence of activator protein-1 (AP-1). To further study the association between biochemical values and genotypes, maternal plasma inositol hexakisphosphate (IP6) levels were also assessed using LC-MS. The maternal plasma IP6 concentrations in the spina bifida subgroup were 7.1% lower than control (136.67 vs. 147.05 ng mL(-1), P<0.05), and significantly lower in rs3783903 GG genotype than others (P<0.05). EMSA showed a different allelic binding capacity of AP-1 in rs3783903, which was affected by an A→G exchange. The RT-PCR suggested the ITPK1 expression was decreased significantly in mutant-type of rs3783903 compared with wild-type in the 60 healthy pregnancies (P<0.05).

Conclusions/significance: These results suggested that the maternal rs3783903 of ITPK1 might be associated with spina bifida, and the allele G of rs3783903 might affect the binding of AP-1 and the decrease of maternal plasma IP6 concentration in this Chinese population.

Citing Articles

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Tian H, Guan Z, Li S, Wang J Front Neurol. 2024; 15:1411184.

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Investigating Genetic Determinants of Plasma Inositol Status in Adult Humans.

Weston E, Pangilinan F, Eaton S, Orford M, Leung K, Copp A J Nutr. 2023; 152(11):2333-2342.

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Yang A, Li S, Zhang Y, Wang X, Guan Z, Zhu Z Int J Mol Sci. 2022; 23(23).

PMID: 36499158 PMC: 9735442. DOI: 10.3390/ijms232314831.

Genetic Effects of ITPK1 Polymorphisms on the Risk of Neural Tube Defects: a Population-Based Study.

Guan Z, Liang Y, Zhu Z, Yang A, Li S, Wang X Reprod Sci. 2022; 30(5):1585-1593.

PMID: 36323916 DOI: 10.1007/s43032-022-01116-5.

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Adams J, Kirby J, Sorensen J, Pollard E, Audhya T Matern Health Neonatol Perinatol. 2022; 8(1):4.

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