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ALOX5 promoter genotype and response to montelukast in moderate persistent asthma

机译:中度持续性哮喘中ALOX5启动子的基因型和对孟鲁司特的反应

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摘要

[Background]: It was hypothesized that asthmatic patients with mutant alleles in the leukotriene pathway should not respond to leukotriene receptor antagonists and the concept of a tailored treatment is increasingly supported. [Methods]: Sixty-one patients (mean age 24.9 years, range 14-52) with moderate persistent asthma were clinical and immunological assess prior and after a 6-month treatment with montelukast. Tandem repeat polymorphisms were genotyped in the promoter (-147 to -176) of 5-lipoxygenase gene (ALOX5). [Results]: Thirty-two patients (52.5%) were homozygous for the five repeats allele; 17 (27.9%) were heterozygous (4/5 repeats) and 12 (19.7%) were homozygous for 4/4 repeats. After the montelukast treatment decrease number of asthma exacerbations, improvement of FEV1 and decreased use of β2 agonists was observed in patients with 5/5 or 4/5 repeats. Conversely, the patients with 4/4 repeats genotype did not modify these data after treatment. [Conclusions]: It was confirmed that ALOX5 promoter polymorphisms have a clear influence in montelukast response in atopic moderate persistent asthma patients. The genetic study could identify those patients most likely to respond to montelukast. © 2008 Elsevier Ltd. All rights reserved.
机译:[背景]:假设白三烯途径中突变等位基因的哮喘患者不应对白三烯受体拮抗剂产生反应,并且越来越多地支持量身定制的治疗概念。 [方法]:对6例孟鲁司特治疗前后的中度持续性哮喘患者(平均年龄24.9岁,范围14-52)进行了临床和免疫学评估。在5-脂氧合酶基因(ALOX5)的启动子(-147至-176)中对串联重复序列多态性进行基因分型。结果:52例患者中5个重复等位基因为纯合子; 52.5%为纯合子。 17个(27.9%)是杂合的(4/5重复)和12(19.7%)是纯合的4/4重复。孟鲁司特治疗减少哮喘发作次数后,在重复次数为5/5或4/5的患者中观察到FEV1的改善和β2激动剂的使用减少。相反,具有4/4重复基因型的患者在治疗后没有改变这些数据。 [结论]:证实ALOX5启动子多态性对特应性中度持续性哮喘患者的孟鲁司特反应有明显影响。遗传研究可以确定最可能对孟鲁司特有反应的患者。 ©2008 Elsevier Ltd.保留所有权利。

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