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高维分析揭示了模型动物感染胸膜肺炎放线杆菌性肺炎肺组织中的免疫图谱和新型中性粒细胞簇。

High-dimensional analysis reveals an immune atlas and novel neutrophil clusters in the lungs of model animals with Actinobacillus pleuropneumoniae-induced pneumonia.

机构信息

State Key Laboratory for Zoonotic Diseases, Key Laboratory of Zoonosis Research, Ministry of Education, College of Veterinary Medicine, Jilin University, Changchun, China.

Leiden Computational Biology Center, Leiden University Medical Center, Leiden, The Netherlands.

出版信息

Vet Res. 2023 Sep 13;54(1):76. doi: 10.1186/s13567-023-01207-4.

Abstract

Due to the increase in bacterial resistance, improving the anti-infectious immunity of the host is rapidly becoming a new strategy for the prevention and treatment of bacterial pneumonia. However, the specific lung immune responses and key immune cell subsets involved in bacterial infection are obscure. Actinobacillus pleuropneumoniae (APP) can cause porcine pleuropneumonia, a highly contagious respiratory disease that has caused severe economic losses in the swine industry. Here, using high-dimensional mass cytometry, the major immune cell repertoire in the lungs of mice with APP infection was profiled. Various phenotypically distinct neutrophil subsets and Ly-6C inflammatory monocytes/macrophages accumulated post-infection. Moreover, a linear differentiation trajectory from inactivated to activated to apoptotic neutrophils corresponded with the stages of uninfected, onset, and recovery of APP infection. CD14 neutrophils, which mainly increased in number during the recovery stage of infection, were revealed to have a stronger ability to produce cytokines, especially IL-10 and IL-21, than their CD14 counterparts. Importantly, MHC-II neutrophils with antigen-presenting cell features were identified, and their numbers increased in the lung after APP infection. Similar results were further confirmed in the lungs of piglets infected with APP and Klebsiella pneumoniae infection by using a single-cell RNA-seq technique. Additionally, a correlation analysis between cluster composition and the infection process yielded a dynamic and temporally associated immune landscape where key immune clusters, including previously unrecognized ones, marked various stages of infection. Thus, these results reveal the characteristics of key neutrophil clusters and provide a detailed understanding of the immune response to bacterial pneumonia.

摘要

由于细菌耐药性的增加,提高宿主抗感染免疫能力迅速成为预防和治疗细菌性肺炎的新策略。然而,细菌感染中具体的肺部免疫反应和关键免疫细胞亚群尚不清楚。胸膜肺炎放线杆菌(APP)可引起猪传染性胸膜肺炎,这是一种高度传染性的呼吸道疾病,给养猪业造成了严重的经济损失。在这里,我们使用高维液质联用技术对 APP 感染小鼠肺部的主要免疫细胞库进行了分析。感染后,各种表型不同的中性粒细胞亚群和 Ly-6C 炎症性单核细胞/巨噬细胞大量积累。此外,从失活到活化再到凋亡的中性粒细胞线性分化轨迹与未感染、发病和 APP 感染恢复阶段相对应。在感染恢复阶段主要数量增加的 CD14 中性粒细胞被揭示出比其 CD14 对应物具有更强的产生细胞因子的能力,尤其是 IL-10 和 IL-21。重要的是,鉴定出具有抗原呈递细胞特征的 MHC-II 中性粒细胞,并且它们在 APP 感染后肺部的数量增加。使用单细胞 RNA-seq 技术进一步在感染 APP 和肺炎克雷伯菌的仔猪肺部证实了类似的结果。此外,对聚类组成与感染过程之间的相关性分析产生了一个动态的、与时间相关的免疫景观,其中关键免疫聚类,包括以前未被识别的聚类,标记了感染的各个阶段。因此,这些结果揭示了关键中性粒细胞聚类的特征,并提供了对细菌性肺炎免疫反应的详细了解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/56ee/10500746/9d1c45b44852/13567_2023_1207_Fig1_HTML.jpg

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