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奥马珠单抗治疗哮喘患者中应答者和无应答者全血转录变化的比较。

Whole blood transcriptional variations between responders and non-responders in asthma patients receiving omalizumab.

机构信息

Baylor University, Institute for Biomedical Studies, Waco, TX, USA.

Department of Immunology, Mayo Clinic, Scottsdale, AZ, USA.

出版信息

Clin Exp Allergy. 2020 Sep;50(9):1017-1034. doi: 10.1111/cea.13671. Epub 2020 Jul 15.

Abstract

BACKGROUND

Anti-IgE (omalizumab) has been used for the treatment of moderate-to-severe asthma that is not controlled by inhaled steroids. Despite its success, it does not always provide patients with significant clinical benefits.

OBJECTIVE

To investigate the transcriptional variations between omalizumab responders and non-responders and to study the mechanisms of action of omalizumab.

METHODS

The whole blood transcriptomes of moderate-to-severe adult asthma patients (N = 45:34 responders and 11 non-responders) were analysed over the course of omalizumab treatment. Non-asthmatic healthy controls (N = 17) were used as controls.

RESULTS

Transcriptome variations between responders and non-responders were identified using the genes significant (FDR < 0.05) in at least one comparison of each patient response status and time point compared with control subjects. Using gene ontology and network analysis, eight clusters of genes were identified. Longitudinal analyses of individual clusters revealed that responders could maintain changes induced with omalizumab treatment and become more similar to the control subjects, while non-responders tend to remain more similar to their pre-treatment baseline. Further analysis of an inflammatory gene cluster revealed that genes associated with neutrophil/eosinophil activities were up-regulated in non-responders and, more importantly, omalizumab did not significantly alter their expression levels. The application of modular analysis supported our findings and further revealed variations between responders and non-responders.

CONCLUSION AND CLINICAL RELEVANCE

This study provides not only transcriptional variations between omalizumab responders and non-responders, but also molecular insights for controlling asthma by omalizumab.

摘要

背景

抗 IgE(奥马珠单抗)已被用于治疗吸入性类固醇无法控制的中重度哮喘。尽管它取得了成功,但并不总能为患者带来显著的临床获益。

目的

研究奥马珠单抗应答者和无应答者之间的转录变化,并研究奥马珠单抗的作用机制。

方法

对 45 名中重度成年哮喘患者(34 名应答者和 11 名无应答者)的全血转录组进行分析,这些患者在奥马珠单抗治疗过程中进行了研究。非哮喘健康对照者(N=17)被用作对照。

结果

使用每个患者的应答状态和时间点与对照相比至少有一个比较的基因具有显著差异(FDR<0.05),鉴定出应答者和无应答者之间的转录组变化。使用基因本体论和网络分析,确定了 8 个基因簇。对个体簇的纵向分析表明,应答者可以维持奥马珠单抗治疗诱导的变化,并变得更类似于对照,而无应答者则倾向于保持更类似于其治疗前的基线。对一个炎症基因簇的进一步分析表明,与中性粒细胞/嗜酸性粒细胞活性相关的基因在无应答者中上调,更重要的是,奥马珠单抗并没有显著改变它们的表达水平。模块化分析的应用支持了我们的发现,并进一步揭示了应答者和无应答者之间的差异。

结论和临床相关性

这项研究不仅提供了奥马珠单抗应答者和无应答者之间的转录变化,还为奥马珠单抗控制哮喘提供了分子见解。

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