文章基本信息
- 标题:Acetylcholine Regulates Pulmonary Pathology During Viral Infection and Recovery
- 本地全文:下载
- 作者:Alexander P Horkowitz ; Ashley V Schwartz ; Carlos A Alvarez 等
- 期刊名称:ImmunoTargets and Therapy
- 电子版ISSN:2253-1556
- 出版年度:2020
- 卷号:Volume 9
- 页码:333-350
- DOI:10.2147/ITT.S279228
- 出版社:Dove Medical Press Ltd
- 摘要:Introduction :This study was designed to explore the role of acetylcholine (ACh) in pulmonary viral infection and recovery. Inflammatory control is critical to recovery from respiratory viral infection. ACh secreted from non-neuronal sources, including lymphocytes, plays an important, albeit underappreciated, role in regulating immune-mediated inflammation. Methods :ACh and lymphocyte cholinergic status in the lungs were measured over the course of influenza infection and recovery. The role of ACh was examined by inhibiting ACh synthesis in vivo. Pulmonary inflammation was monitored by Iba1 immunofluorescence, using a novel automated algorithm. Tissue repair was monitored histologically. Results :Pulmonary ACh remained constant through the early stage of infection and increased during the peak of the acquired immune response. As the concentration of ACh increased, cholinergic lymphocytes appeared in the BAL and lungs. Cholinergic capacity was found primarily in CD4 T cells, but also in B cells and CD8 T cells. The cholinergic CD4 T cells bound to influenza-specific tetramers and were retained in the resident memory regions of the lung up to 2 months after infection. Histologically, cholinergic lymphocytes were found in direct physical contact with activated macrophages throughout the lung. Inflammation was monitored by ionized calcium-binding adapter molecule 1 (Iba1) immunofluorescence, using a novel automated algorithm. When ACh production was inhibited, mice exhibited increased tissue inflammation and delayed recovery. Histologic examination revealed abnormal tissue repair when ACh was limited. Conclusion :These findings point to a previously unrecognized role for ACh in the transition from active immunity to recovery and pulmonary repair following respiratory viral infection. © 2020 Horkowitz et al.
- 关键词:Aif-1;CD4 resident memory;ChAT;Iba1;MATLAB;acetylcholine;acetylcholinesterase;automated algorithm;cholinergic anti-inflammatory pathway;cholinergic lymphocytes;inflammaging;inflammation;influenza;pulmonary repair