Extracellular vesicle-bound S100A8/A9 is differentially expressed in septic shock and prompts acute lung injury.

IF 5.8 2区医学 Q1 Medicine Respiratory Research Pub Date : 2025-03-18 DOI:10.1186/s12931-025-03181-1

Jiangmei Wang, Weiliang Wu, Tingting Wen, Guoping Zheng, Guanguan Qiu, Huifeng Qian, Ruoyang Zhang, Jie Xia, Yaoqin Hu, Ruoqiong Huang, Ruoxi Zang, Zhenkai Le, Qiang Shu, Jianguo Xu

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Abstract

Background: Sepsis is a common indirect insult leading to acute respiratory distress syndrome (ARDS). Circulating extracellular vesicles (EVs) have been reported to participate in the pathogenesis of sepsis. However, the alteration of EV-bound S100A8/A9 during septic shock, along with the role of S100A8/A9 in driving acute lung injury, remains unexplored.

Methods: EVs were isolated from the plasma of patients upon admission with sepsis or septic shock, as well as from healthy controls. Levels of EV S100A8/A9 were assayed via ELISA. To examine the effects and underlying mechanisms of septic shock EVs in acute lung injury, these EVs were administered intratracheally into wild-type C57BL/6 mice or mice with a deficiency of advanced glycation end-products (RAGE). In addition, a mouse model of polymicrobial sepsis was introduced using cecal ligation and puncture (CLP).

Results: Levels of EV S100A8/A9 were significantly elevated in patients with sepsis or septic shock compared to healthy controls. Receiver operating characteristic (ROC) analysis demonstrated that EV S100A8/A9 effectively distinguished between septic shock and sepsis and had predictive potential for the development of ARDS. Notably, the levels of S100A8/A9 in EVs and alveolar macrophages from CLP mice were significantly higher than those in sham mice. Intratracheal administration of septic shock EVs directly induced acute lung injury and M1 macrophage polarization in a lipopolysaccharide-independent manner. Septic shock EVs were efficiently taken up by alveolar macrophages in vivo, leading to a significant increase in S100A8/A9 levels, which was inhibited by preincubating the EVs with an S100A8/A9 neutralizing antibody. Additionally, mice with deficiency in RAGE, a receptor for S100A8/A9, were partially protected from acute lung injury induced by septic shock EVs. In vitro, septic shock EVs prompted a proinflammatory response in bone marrow-derived macrophages. This response was blocked by preincubating the EVs with the S100A8/A9 neutralizing antibody.

Conclusions: Our results suggested that EV S100A8/A9 has potential value in distinguishing septic shock from sepsis and predicting the development of ARDS. Septic shock EVs-induced lung injury is at least partially mediated through S100A8/A9-RAGE pathway, involving the activation of alveolar macrophages.

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细胞外囊泡结合的 S100A8/A9 在脓毒性休克和急性肺损伤中表达不同。

背景：脓毒症是导致急性呼吸窘迫综合征（ARDS）的常见间接损害。循环细胞外囊泡（EVs）已被报道参与脓毒症的发病机制。然而，脓毒性休克期间ev结合的S100A8/A9的改变，以及S100A8/A9在急性肺损伤中的作用尚不清楚。方法：从脓毒症或感染性休克入院患者和健康对照者的血浆中分离出ev。ELISA法检测EV S100A8/A9水平。为了研究感染性休克ev在急性肺损伤中的作用和潜在机制，研究人员将这些ev经气管注入野生型C57BL/6小鼠或晚期糖基化终产物（RAGE）缺乏的小鼠。采用盲肠结扎穿刺法（CLP）建立小鼠多微生物脓毒症模型。结果：与健康对照组相比，败血症或感染性休克患者的EV S100A8/A9水平显著升高。受试者工作特征（ROC）分析表明，EV S100A8/A9能有效区分脓毒性休克和败血症，对ARDS的发展具有预测潜力。值得注意的是，CLP小鼠的ev和肺泡巨噬细胞中S100A8/A9的水平显著高于假药小鼠。脓毒性休克EVs气管内直接诱导急性肺损伤和M1巨噬细胞以脂多糖不依赖的方式极化。脓毒性休克EVs在体内被肺泡巨噬细胞有效吞噬，导致S100A8/A9水平显著升高，用S100A8/A9中和抗体预孵育EVs可抑制S100A8/A9水平。此外，缺乏RAGE （S100A8/A9的受体）的小鼠可以部分保护感染性休克ev引起的急性肺损伤。在体外，感染性休克EVs促进骨髓源性巨噬细胞的促炎反应。用S100A8/A9中和抗体对ev进行预孵育可以阻断这种反应。结论：我们的结果提示EV S100A8/A9在区分脓毒症和败血症以及预测ARDS发展方面具有潜在价值。感染性休克ev诱导的肺损伤至少部分通过S100A8/A9-RAGE通路介导，涉及肺泡巨噬细胞的激活。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Respiratory Research RESPIRATORY SYSTEM-

CiteScore

9.70

自引率

1.70%

发文量

314

审稿时长

4-8 weeks

期刊介绍： Respiratory Research publishes high-quality clinical and basic research, review and commentary articles on all aspects of respiratory medicine and related diseases. As the leading fully open access journal in the field, Respiratory Research provides an essential resource for pulmonologists, allergists, immunologists and other physicians, researchers, healthcare workers and medical students with worldwide dissemination of articles resulting in high visibility and generating international discussion. Topics of specific interest include asthma, chronic obstructive pulmonary disease, cystic fibrosis, genetics, infectious diseases, interstitial lung diseases, lung development, lung tumors, occupational and environmental factors, pulmonary circulation, pulmonary pharmacology and therapeutics, respiratory immunology, respiratory physiology, and sleep-related respiratory problems.