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Role of periostin, FENO, IL-13, lebrikzumab, other IL-13 antagonist and dual IL-4/IL-13 antagonist in asthma

机译:骨膜素,FENO,IL-13,lebrikzumab,其他IL-13拮抗剂和IL-4 / IL-13双重拮抗剂在哮喘中的作用

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Introduction: Asthma markedly diminishes quality of life due to limited activity, absences from work or school and hospitalizations. Patients with severe asthma which are not controlled despite taking effective therapy are most in need of new treatment approaches. IL-13 was demonstrated as 'central mediator of allergic asthma'. Areas covered: IL-13 has been implicated in the pathogenesis of asthma, idiopathic pulmonary fibrosis and COPD. IL-13 levels in the sputum and bronchial biopsy samples remain elevated in severe asthma despite the use of inhaled and systemic corticosteroids. Thus, IL-13 is a mediator involved in corticosteroid resistance. Periostin enhances profibrotic TGF-β signaling in subepithelial fibrosis associated with asthma. IL-13 induces bronchial epithelial cells to secrete periostin. Periostin may be a biomarker for Th2 induced airway inflammation. Lebrikizumab is a monoclonal antibody against IL-13. Lebrikizumab improved lung function in asthmatics who were symptomatic despite treatment with long acting beta agonist and inhaled corticosteroids and provided benefit in the treatment of severe uncontrolled asthma. Expert opinion: Lebrikizumab block IL-13 signaling through the IL-13Rα1/IL-4Rα receptor. There was a larger reduction in FENO in the high periostin subgroup than in the low periostin subgroup (34.4 vs 4.3%). Serum CCL17, CCL13 and total IgE levels decreased in the lebrikizumab group.
机译:简介:由于活动受限,缺勤,缺课和住院,哮喘明显降低了生活质量。尽管接受了有效的治疗但仍无法控制的严重哮喘患者最需要新的治疗方法。 IL-13被证明是“过敏性哮喘的中央介质”。涵盖的领域:IL-13与哮喘,特发性肺纤维化和COPD的发病机制有关。尽管使用吸入性和全身性皮质类固醇,重度哮喘患者痰液和支气管活检样本中的IL-13水平仍然升高。因此,IL-13是参与皮质类固醇抗性的介质。骨膜素增强与哮喘相关的上皮下纤维化中的纤维化TGF-β信号传导。 IL-13诱导支气管上皮细胞分泌骨膜素。骨膜素可能是Th2诱导的气道炎症的生物标志物。 Lebrikizumab是抗IL-13的单克隆抗体。 Lebrikizumab改善了有症状的哮喘患者的肺功能,尽管使用了长效β受体激动剂和吸入皮质类固醇进行治疗,但仍可治疗严重的不受控制的哮喘。专家意见:Lebrikizumab通过IL-13Rα1/IL-4Rα受体阻断IL-13信号传导。高骨膜素亚组的FENO降低量要比低骨膜素亚组的FENO降低幅度更大(34.4对4.3%)。 lebrikizumab组的血清CCL17,CCL13和总IgE水平降低。

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