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首页> 外文期刊>Journal of Asthma and Allergy >Anti-IL5 Therapies for Severe Eosinophilic Asthma: Literature Review and Practical Insights
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Anti-IL5 Therapies for Severe Eosinophilic Asthma: Literature Review and Practical Insights

机译:抗IL5严重嗜酸性哮喘疗法:文献综述和实用见解

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Severe refractory asthma (SRA) still has a high economic and social impact, including a reduction in quality of life (QoL), productivity, a greater risk of exacerbations and emergency department (ED) visits. Another major issue is the need of oral corticosteroids (OCS), often due to a poor response to standard therapies or the lack of indication for currently available biological drugs. A thorough understanding of the immunological pathways and eosinophilopoietic processes allows a correct application of the new pharmacological strategies and leads to better clinical responses. For these unmet needs, several monoclonal antibody (mAb) drugs have been introduced over the past few years. These are mainly available for allergic and especially eosinophilic uncontrolled refractory asthma. As the number of therapeutic options increases, the choice of biological drugs can be made only after careful considerations of the particular asthma endotype, patients’ comorbidities and clinical data. The selection of the correct therapeutic option can therefore be guided after a careful evaluation of the particular endotype and phenotype, from the combined evaluation of inflammatory biomarkers, clinical picture and comorbidities. The careful evaluation of all these parameters can therefore help the physician in the optimal management of these complex patients, for whom it is often possible to achieve exceptional results by managing the available options in the best possible way. The aim of this review is to define the positioning of the biological drugs currently available for type 2 asthma, with a special focus on options for eosinophilic asthma in the context of the most recent knowledge of immunological pathways.
机译:严重的难治性哮喘(SRA)仍然具有很高的经济和社会影响,包括降低生活质量(QOL),生产力,更大的恶化风险和急诊部门(ED)访问。另一个主要问题是需要口腔皮质类固醇(OCS),通常由于对标准疗法的良差或目前可用的生物药物缺乏迹象。彻底了解免疫途径和嗜酸性嗜胞细胞过程允许正确地应用新的药理学策略并导致更好的临床反应。对于这些未满足的需求,在过去几年中已经引入了几种单克隆抗体(MAB)药物。这些主要用于过敏性和尤其是嗜酸性不受控制的难治性哮喘。随着治疗性选项的数量增加,可以在仔细考虑特定哮喘内型,患者的合并症和临床数据后才能进行生物药物的选择。因此,在临床生物标志物,临床影像和组织的组合评估中,可以在仔细评估特定的子型和表型后引导正确的治疗选择。因此,对所有这些参数的仔细评估可以帮助医生在这些复杂患者的最佳管理中,因为通过以最佳方式管理可用选项,通常可以实现卓越的结果。本综述的目的是定义目前可用于2型哮喘的生物药物的定位,特别关注在最近的免疫途径知识的背景下的嗜酸性嗜型哮喘的选择。

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