细胞内环磷酸腺苷调节增强人呼吸道上皮细胞长效 β-激动剂和糖皮质激素的反应。
Potentiation of long-acting β-agonist and glucocorticoid responses in human airway epithelial cells by modulation of intracellular cAMP.
机构信息
Firestone Institute for Respiratory Health-Division of Respirology, Department of Medicine, McMaster University, Hamilton, ON, L8N 4A6, Canada.
Division of Respiratory Medicine, Department of Medicine, University of British Columbia, Vancouver, BC, V6H 3Z, Canada.
出版信息
Respir Res. 2021 Oct 19;22(1):266. doi: 10.1186/s12931-021-01862-1.
INTRODUCTION
Over 300 million people in the world live with asthma, resulting in 500,000 annual global deaths with future increases expected. It is estimated that around 50-80% of asthma exacerbations are due to viral infections. Currently, a combination of long-acting beta agonists (LABA) for bronchodilation and glucocorticoids (GCS) to control lung inflammation represent the dominant strategy for the management of asthma, however, it is still sub-optimal in 35-50% of moderate-severe asthmatics resulting in persistent lung inflammation, impairment of lung function, and risk of mortality. Mechanistically, LABA/GCS combination therapy results in synergistic efficacy mediated by intracellular cyclic adenosine monophosphate (cAMP).
HYPOTHESIS
Increasing intracellular cAMP during LABA/GCS combination therapy via inhibiting phosphodiesterase 4 (PDE4) and/or blocking the export of cAMP by ATP Binding Cassette Transporter C4 (ABCC4), will potentiate anti-inflammatory responses of mainstay LABA/GCS therapy.
METHODS
Expression and localization experiments were performed using in situ hybridization and immunohistochemistry in human lung tissue from healthy subjects, while confirmatory transcript and protein expression analyses were performed in primary human airway epithelial cells and cell lines. Intervention experiments were performed on the human airway epithelial cell line, HBEC-6KT, by pre-treatment with combinations of LABA/GCS with PDE4 and/or ABCC4 inhibitors followed by Poly I:C or imiquimod challenge as a model for viral stimuli. Cytokine readouts for IL-6, IL-8, CXCL10/IP-10, and CCL5/RANTES were quantified by ELISA.
RESULTS
Using archived human lung and human airway epithelial cells, ABCC4 gene and protein expression were confirmed in vitro and in situ. LABA/GCS attenuation of Poly I:C or imiquimod-induced IL-6 and IL-8 were potentiated with ABCC4 and PDE4 inhibition, which was greater when ABCC4 and PDE4 inhibition was combined. Modulation of cAMP levels had no impact on LABA/GCS modulation of Poly I:C-induced CXCL10/IP-10 or CCL5/RANTES.
CONCLUSION
Modulation of intracellular cAMP levels by PDE4 or ABCC4 inhibition potentiates LABA/GCS efficacy in human airway epithelial cells challenged with viral stimuli. The data suggest further exploration of the value of adding cAMP modulators to mainstay LABA/GCS therapy in asthma for potentiated anti-inflammatory efficacy.
简介
全球有超过 3 亿人患有哮喘,每年导致全球 50 万人死亡,预计未来还会增加。据估计,约 50-80%的哮喘加重是由病毒感染引起的。目前,长效β激动剂(LABA)用于支气管扩张和糖皮质激素(GCS)来控制肺部炎症,这代表了管理哮喘的主要策略,但在 35-50%的中重度哮喘患者中仍然效果不佳,导致持续的肺部炎症、肺功能受损和死亡风险。从机制上讲,LABA/GCS 联合治疗通过细胞内环磷酸腺苷(cAMP)产生协同疗效。
假设
通过抑制磷酸二酯酶 4(PDE4)和/或阻断 ATP 结合盒转运蛋白 C4(ABCC4)将细胞内的 cAMP 在 LABA/GCS 联合治疗期间增加,将增强主要 LABA/GCS 治疗的抗炎反应。
方法
使用原位杂交和免疫组织化学技术在健康受试者的人肺组织中进行表达和定位实验,同时在原代人气道上皮细胞和细胞系中进行确认的转录和蛋白表达分析。通过用 LABA/GCS 与 PDE4 和/或 ABCC4 抑制剂联合预处理人气道上皮细胞系 HBEC-6KT,然后用 Poly I:C 或咪喹莫特作为病毒刺激的模型进行干预实验。通过 ELISA 定量测定细胞因子 IL-6、IL-8、CXCL10/IP-10 和 CCL5/RANTES 的读数。
结果
使用存档的人肺和人气道上皮细胞,在体外和体内证实了 ABCC4 基因和蛋白的表达。ABCC4 和 PDE4 抑制增强了 LABA/GCS 对 Poly I:C 或咪喹莫特诱导的 IL-6 和 IL-8 的抑制作用,当 ABCC4 和 PDE4 抑制联合使用时效果更大。cAMP 水平的调节对 LABA/GCS 调节 Poly I:C 诱导的 CXCL10/IP-10 或 CCL5/RANTES 没有影响。
结论
通过 PDE4 或 ABCC4 抑制调节细胞内 cAMP 水平增强了人气道上皮细胞在病毒刺激下的 LABA/GCS 疗效。数据表明,进一步探索在哮喘中添加 cAMP 调节剂以增强主要 LABA/GCS 治疗的抗炎疗效具有价值。
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