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CpG-寡脱氧核苷酸治疗对创伤和继发性肺部感染的有益作用。

Beneficial Effects of CpG-Oligodeoxynucleotide Treatment on Trauma and Secondary Lung Infection.

作者信息

Wanke-Jellinek Lorenz, Keegan Joshua W, Dolan James W, Guo Fei, Chen Jianfei, Lederer James A

机构信息

Department of Surgery, Brigham and Women's Hospital and Harvard Medical School, Boston, MA 02115; Department of Trauma Surgery, Technical University of Munich, 81675 Munich, Germany;

Department of Surgery, Brigham and Women's Hospital and Harvard Medical School, Boston, MA 02115;

出版信息

J Immunol. 2016 Jan 15;196(2):767-77. doi: 10.4049/jimmunol.1500597. Epub 2015 Dec 16.

Abstract

Although Streptococcus pneumoniae is usually found as a commensal in healthy individuals, it can act as a pathogen in trauma patients, causing such complications as early-onset pneumonia and sepsis. We discovered that treating mice with an A-class CpG-oligodeoxynucleotide (ODN) at 2 h after traumatic injury significantly improved mouse survival following early-onset secondary lung infection with S. pneumoniae. This study used mass cytometry (cytometry by time-of-flight) and Luminex technologies to characterize the cellular immune response to secondary S. pneumoniae lung infection at 1 and 3 d postinfection. We found increased expression of CD14, CD64, and PD-L1 on F4-80(+) and F4-80(+)CD11c(+) macrophages, CD11c(+) dendritic cells, and CD14(+)CD172a(+) cells after burn-injury and infection, supporting previous reports of innate immune cell activation in sepsis. CpG-ODN treatment at 2 h after burn-injury reversed these effects; improved pathogen clearance; and led to an increased expression of CD25, CD27, MHCII, and IL-17 on or in TCRγδ cells at 1 d postinfection. At 3 d postinfection, CpG-ODN treatment increased the expression of PD-L1 on innate cell subsets. Furthermore, we analyzed cytokine levels in lung-washout samples of TCRγδ cell-depleted (TCRγδ(-)) mice to demonstrate that the effects of CpG-ODN on cytokine expression after burn-injury and S. pneumoniae infection rely on functional TCRγδ cells. In summary, we demonstrate that cytometry by time-of-flight provides an effective strategy to systematically identify specific cellular phenotypic responses to trauma and bacterial pneumonia and to discover changes in immune system phenotypes associated with beneficial immunotherapy.

摘要

虽然肺炎链球菌通常在健康个体中作为共生菌存在,但它可在创伤患者中作为病原体,引发早发性肺炎和败血症等并发症。我们发现,在创伤性损伤后2小时用A级CpG寡脱氧核苷酸(ODN)治疗小鼠,可显著提高小鼠在早发性继发性肺炎链球菌肺部感染后的存活率。本研究使用质谱流式细胞术(飞行时间流式细胞术)和Luminex技术来表征感染后1天和3天对继发性肺炎链球菌肺部感染的细胞免疫反应。我们发现,烧伤和感染后,F4-80(+)和F4-80(+)CD11c(+)巨噬细胞、CD11c(+)树突状细胞以及CD14(+)CD172a(+)细胞上CD14、CD64和PD-L1的表达增加,这支持了先前关于败血症中固有免疫细胞激活的报道。烧伤后2小时进行CpG-ODN治疗可逆转这些效应;改善病原体清除;并导致感染后1天TCRγδ细胞上或其内部CD25、CD27、MHCII和IL-17的表达增加。感染后3天,CpG-ODN治疗增加了固有细胞亚群上PD-L1的表达。此外,我们分析了TCRγδ细胞耗竭(TCRγδ(-))小鼠肺冲洗样本中的细胞因子水平,以证明CpG-ODN对烧伤和肺炎链球菌感染后细胞因子表达的影响依赖于功能性TCRγδ细胞。总之,我们证明飞行时间流式细胞术提供了一种有效的策略,可系统地识别对创伤和细菌性肺炎的特定细胞表型反应,并发现与有益免疫治疗相关的免疫系统表型变化。

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