特发性肺纤维化患者咳嗽严重程度与muc5b基因型相关。

Cough (London, England) Pub Date : 2014-03-25 eCollection Date: 2014-01-01 DOI:10.1186/1745-9974-10-3
Mary Beth Scholand, Roger Wolff, Peter Fredrick Crossno, Krishna Sundar, Molly Winegar, Spencer Whipple, Patrick Carey, Nicholas Sunchild, Hilary Coon
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引用次数: 32

摘要

背景:黏液蛋白MUC5B启动子区域的多态性(rs35705950)与家族性和散发性特发性肺纤维化有关。我们假设这种常见的MUC5B变异会影响咳嗽的表达,咳嗽是IPF患者常见的致残症状。方法:对136例IPF患者进行基因分型。所有活着的受试者均填写莱斯特咳嗽问卷(Leicester Cough Questionnaire, LCQ)来测量咳嗽的严重程度。我们使用SAS通用线性模型(GLM)评估了MUC5B多态性对IPF患者LCQ评分的等位基因影响。结果:在136例返回LCQ的IPF患者中的68例中,MUC5B次要等位基因频率(T)与先前发表的研究一致(31%)。我们发现T等位基因对LCQ评分有显著的独立影响(IPF受试者的p = 0.002)。这种效果独立于其他常见的咳嗽原因,包括胃食管反流病和上呼吸道咳嗽综合征。结论:咳嗽严重程度是IPF常见的致残表型成分,与MUC5B启动子多态性的次要等位基因的存在显著相关。这项研究强调了肺纤维化表型异质性的可能遗传机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Severity of cough in idiopathic pulmonary fibrosis is associated with MUC5 B genotype.

Background: A polymorphism (rs35705950) in the promoter region of the mucin MUC5B is associated with both familial and sporadic forms of idiopathic pulmonary fibrosis. (IPF) We hypothesize that this common MUC5B variant will impact the expression of cough, a frequent disabling symptom seen in subjects with IPF.

Methods: We genotyped 136 subjects with IPF. All living subjects were provided with a Leicester Cough Questionnaire (LCQ) to measure cough severity. We assessed allele effects of the MUC5B polymorphism on the LCQ scores using SAS General Linear Models (GLM) in the patients with IPF.

Results: In the 68 of the total 136 IPF patients who returned the LCQ, MUC5B minor allele frequency (T) is consistent with prior published studies (31%). We found a significant independent effect of the T allele on the LCQ score (p = 0.002 for subjects with IPF). This effect is independent of other common causes of cough, including gastroesophogeal reflux disease and upper airway cough syndrome.

Conclusions: Cough severity, a common disabling phenotypic component of IPF, is significantly associated with the presence of the minor allele of a MUC5B promoter polymorphism. This study highlights a possible genetic mechanism for phenotypic heterogeneity in pulmonary fibrosis.

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