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丝聚合蛋白基因P478S多态性与特应性皮炎之间的关联。

Association between P478S polymorphism of the filaggrin gene & atopic dermatitis.

作者信息

Kim Seon-Young, Yang Sung Wan, Kim Hye-Lin, Kim Sung-Hoon, Kim Seong Joon, Park Sun-Min, Son Musong, Ryu Sahyun, Pyo Young-Seok, Lee Jae-Seok, Kim Kyu Seok, Kim Yoon Bum, Hong Seung-Heon, Um Jae-Young

机构信息

College of Korean Medicine, Institute of Korean Medicine, Kyung Hee University, Seoul, Korea.

出版信息

Indian J Med Res. 2013 Dec;138(6):922-7.

Abstract

BACKGROUND & OBJECTIVES: Atopic diseases, including atopic dermatitis (AD), allergy and asthma, are complex diseases resulting from the effect of multiple genetic and interacting environmental factors on their pathophysiology. The genetic basis is incompletely understood; however, recent studies have shown an association between loss-of-function variants of the filaggrin gene (FLG) and atopic dermatitis. The aim of this study was to determine whether FLG variants can serve as a predictor for atopic diseases in Korean individuals.

METHODS

A total of 648 subjects were genotyped for the FLG P478S (rs11584340, C/T base change) polymorphism (322 patients and 326 controls). Serum levels of free fatty acids (FFA) and IgE were later stratified to determine the effects of the FLG polymorphism on AD.

RESULTS

A significant difference in genotype frequency was found between AD patients and controls in the FLG P478S polymorphism. The FLG P478S T allele carrier (TT+TC) was associated with AD risk (odds ratio = 1.877, 95% confidence interval 1.089 to 3.234). In addition, the P478S T allele was related to high levels of FFA in AD patients (471.79 ± 298.96 vs. 333.54 ± 175.82 μg eq/l, P <0.05).

INTERPRETATION & CONCLUSIONS: The results of the present study suggest that the FLG P478S polymorphism alone and combined with other factors influences FFA levels and increases the susceptibility to AD.

摘要

背景与目的

特应性疾病,包括特应性皮炎(AD)、过敏和哮喘,是由多种遗传因素与相互作用的环境因素对其病理生理学产生影响而导致的复杂疾病。其遗传基础尚未完全明确;然而,最近的研究表明,丝聚合蛋白基因(FLG)功能缺失变异与特应性皮炎之间存在关联。本研究的目的是确定FLG变异是否可作为韩国人特应性疾病的预测指标。

方法

对648名受试者进行FLG P478S(rs11584340,C/T碱基变化)多态性基因分型(322例患者和326例对照)。随后对游离脂肪酸(FFA)和IgE的血清水平进行分层,以确定FLG多态性对AD的影响。

结果

在FLG P478S多态性方面,AD患者与对照之间的基因型频率存在显著差异。FLG P478S T等位基因携带者(TT + TC)与AD风险相关(优势比 = 1.877,95%置信区间1.089至3.234)。此外,P478S T等位基因与AD患者中高水平的FFA相关(471.79 ± 298.96 vs. 333.54 ± 175.82 μg eq/l,P <0.05)。

解读与结论

本研究结果表明,单独的FLG P478S多态性以及与其他因素相结合会影响FFA水平,并增加患AD的易感性。

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