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神经调节失调的白细胞介素-17A 在战斗伤员全身和局部炎症的动态网络中起核心作用。

Central role for neurally dysregulated IL-17A in dynamic networks of systemic and local inflammation in combat casualties.

机构信息

Department of Surgery, University of Pittsburgh, W944 Starzl Biomedical Sciences Tower, 200 Lothrop St., Pittsburgh, PA, 15213, USA.

Center for Inflammation and Regeneration Modeling, McGowan Institute for Regenerative Medicine, Pittsburgh, PA, 15219, USA.

出版信息

Sci Rep. 2023 Apr 24;13(1):6618. doi: 10.1038/s41598-023-33623-z.

Abstract

Dynamic Network Analysis (DyNA) and Dynamic Hypergraphs (DyHyp) were used to define protein-level inflammatory networks at the local (wound effluent) and systemic circulation (serum) levels from 140 active-duty, injured service members (59 with TBI and 81 non-TBI). Interleukin (IL)-17A was the only biomarker elevated significantly in both serum and effluent in TBI vs. non-TBI casualties, and the mediator with the most DyNA connections in TBI wounds. DyNA combining serum and effluent data to define cross-compartment correlations suggested that IL-17A bridges local and systemic circulation at late time points. DyHyp suggested that systemic IL-17A upregulation in TBI patients was associated with tumor necrosis factor-α, while IL-17A downregulation in non-TBI patients was associated with interferon-γ. Correlation analysis suggested differential upregulation of pathogenic Th17 cells, non-pathogenic Th17 cells, and memory/effector T cells. This was associated with reduced procalcitonin in both effluent and serum of TBI patients, in support of an antibacterial effect of Th17 cells in TBI patients. Dysregulation of Th17 responses following TBI may drive cross-compartment inflammation following combat injury, counteracting wound infection at the cost of elevated systemic inflammation.

摘要

采用动态网络分析(DyNA)和动态超图(DyHyp),从 140 名现役、受伤的军人(59 名患有 TBI 和 81 名非 TBI)的局部(伤口渗出液)和全身循环(血清)水平定义蛋白质水平的炎症网络。白细胞介素(IL)-17A 是 TBI 与非 TBI 伤员的血清和渗出液中唯一显著升高的生物标志物,也是 TBI 伤口中 DyNA 连接最多的介质。DyNA 将血清和渗出液数据结合起来定义跨腔室相关性表明,IL-17A 在晚期将局部和全身循环联系起来。DyHyp 表明,TBI 患者的系统性 IL-17A 上调与肿瘤坏死因子-α有关,而非 TBI 患者的 IL-17A 下调与干扰素-γ有关。相关性分析表明,致病性 Th17 细胞、非致病性 Th17 细胞和记忆/效应 T 细胞的表达存在差异上调。这与 TBI 患者的渗出液和血清中降钙素原的降低有关,支持 TBI 患者 Th17 细胞具有抗细菌作用。TBI 后 Th17 反应的失调可能会在战斗伤害后引发跨腔室炎症,从而在全身炎症升高的情况下抵消伤口感染。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0779/10126120/5049748d017d/41598_2023_33623_Fig1_HTML.jpg

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