肿瘤坏死因子α(TNFα)基因启动子多态性和单倍型与热性惊厥(FS)和TNFα血清水平有关。

IF 0.8 Q4 CLINICAL NEUROLOGY
Iranian Journal of Child Neurology Pub Date : 2023-01-01 Epub Date: 2023-10-26 DOI:10.22037/ijcn.v18i1.36719
Bahar Ghanbarzadeh, Elnaz Dadashzadeh, Mojtaba Zare Ebrahimabad Zare Ebrahimabad, Mina Rahmati, Nasser Behnampour, Parniansadat Hosseini, Saeed Mohammadi, Seyed Ahmad Hosseini
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引用次数: 0

摘要

目的:热性惊厥(FS)是一种神经炎症性疾病,由发热诱发,影响生命早期阶段的儿童。据报道,TNFα是一种促炎细胞因子,在FS中会升高。TNFα的特定启动子变异可能与细胞因子表达升高和FS易感性有关。本研究分析了特定 TNFα 变体(包括 TNFα -238 G/A (rs361525)、TNFα -308 G/A (rs1800629) 和 TNFα -376 G/A (rs1800750))启动子多态性与 FS 易感性以及伊朗人群中 TNFα 血清水平的关系:共纳入 68 名 FS 患者和 136 名对照者。采用 SSP-PCR 方法分析 TNFα 启动子基因型。本研究还通过对 10 例患者和正常对照组样本进行测序,确认了基因分型结果:结果:-238 SNP的GG基因型与FS风险增加有关[OR = 12.65,95% CI (2.83-56.60),P值 = 0.0012]。308区域的AA基因型在FS患者中增加,并与疾病相关[OR = 4.62,95% CI (1.46-14.56),P值 = 0.028]。对照组中-376 SNP杂合AG的发生率增加与FS风险降低有关[OR = 0.22,95% CI (0.11-0.43),P值 = 0.0001]。本研究发现,在对照组中频率最高的AGA(-238/ -308/-376)单倍型与FS风险降低有关,而GAA(-238/ -308/-376)携带者更易患FS:本研究表明,TNFα基因启动子变异rs361525、rs1800629和rs1800750可能与FS易感性和血清TNFα水平的改变有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Tumor Necrosis Factor Alpha (TNFα) Gene Promoter Polymorphisms and Haplotypes are Associated with the Febrile Seizure (FS) and TNFα Serum Levels.

Objectives: Febrile seizure (FS) is a neuroinflammatory disease involving fever-induced seizures affecting children in the early stages of life. TNFα is a pro-inflammatory cytokine reported to be elevated in FS. Specific promoter variants of TNFα could be associated with its elevated cytokine expression and susceptibility to FS. The present study analyzed the association of specific TNFα variants, including TNFα -238 G/A (rs361525), TNFα -308 G/A (rs1800629), and TNFα -376 G/A (rs1800750) promoter polymorphisms, with FS susceptibility, and TNFα serum levels in an Iranian population.

Materials & methods: Sixty-eight FS patients and 136 controls were enrolled. The SSP-PCR method was utilized to analyze TNFα promoter genotypes. This research also confirmed the genotyping results by sequencing samples of ten patients and normal controls.

Results: The GG genotype of -238 SNP was associated with the increased risk of FS [OR = 12.65, 95% CI (2.83-56.60), P-value = 0.0012]. The AA genotype in the-308 region was increased in patients with FS and associated with the disease [OR = 4.62, 95% CI (1.46-14.56), P-value = 0.028]. The increased occurrence of heterozygous AG in the -376 SNP among control groups has been linked to a decreased risk of FS [OR = 0.22, 95% CI (0.11-0.43), P-value = 0.0001]. This study revealed that AGA (-238/ -308/ -376) haplotype with the highest frequency in controls was associated with a decreased risk of FS, while GAA (-238/ -308/ -376) carriers were more susceptible to FS.

Conclusion: The current study suggested that TNFα gene promoter variants at rs361525, rs1800629, and rs1800750 could be associated with the susceptibility to FS and altered serum levels of TNFα.

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