在非人类灵长类动物模型中,细菌性败血症期间低密度中性粒细胞中脾脏酪氨酸激酶升高

Heather L Teague, Seth Warner, Andrew P Platt, Sydney Stein, Marcos J Ramos-Benitez, Sabrina Ramelli, Shelly Curran, Izabella Lach, Kiana Allen, Heritage Adetola, Trevor Stantliff, Raquel Santana da Cruz, Mahnaz Minai, Heather Kendall, Kevin M Vannella, Derron A Alves, Richard Herbert, Daniel S Chertow, Jeffrey R Strich
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Dimensional reduction with clustering via FlowSOM and traditional gating strategies were used to compare WBNs to LDNs and delineate spleen tyrosine kinase (SYK) expression across neutrophils subsets. We measured soluble biomarkers of end-organ dysfunction and neutrophil activation and quantified SYK and myeloperoxidase in tissue. Results At T6, we identified populations of active immature WBNs and a population of LDNs not detected at baseline. At T24, neutrophil heterogeneity increased across WBNs and LDNs with differential expression of myeloperoxidase (MPO). Compared to WBNs, LDNs were more activated with increased MPO expression. At T6, SYK expression surged in WBNs and LDNs and SYK+WBNs and LDNs expressed higher levels of MPO and lactoferrin compared to SYK- neutrophils. Circulating levels of SYK+LDNs significantly correlated with serum creatinine levels, indicative of acute kidney injury; prolonged prothrombin time and decreased fibrinogen, indicative of consumptive coagulopathy; and SYK expression in tissues. Conclusions Bacterial sepsis leads to heterogenous populations of circulating neutrophils, including LDNs. 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引用次数: 0

摘要

脓毒症是世界范围内的主要死亡原因。识别新的宿主导向治疗靶点可能改善败血症的预后。方法对6例感染肺炎克雷伯菌的非人灵长类动物进行感染性休克治疗,并给予长达72小时的支持治疗。流式细胞术检测感染后(T0)、T6、T24和t48小时全血中性粒细胞(WBNs)和低密度中性粒细胞(LDNs);以及验尸(即尸检)。通过FlowSOM聚类降维和传统的门控策略来比较wbn和ldn,并描绘脾脏酪氨酸激酶(SYK)在中性粒细胞亚群中的表达。我们测量了终末器官功能障碍和中性粒细胞活化的可溶性生物标志物,并量化了组织中的SYK和髓过氧化物酶。在T6时,我们发现了活跃的未成熟wbn群体和基线时未检测到的ldn群体。在T24时,随着髓过氧化物酶(MPO)的差异表达,wbn和ldn之间的中性粒细胞异质性增加。与wbn相比,ldn随着MPO表达的增加而更加活跃。在T6时,SYK在wbn和ldn中的表达激增,与SYK-中性粒细胞相比,SYK+ wbn和ldn表达更高水平的MPO和乳铁蛋白。循环SYK+ ldn水平与血清肌酐水平显著相关,提示急性肾损伤;凝血酶原时间延长,纤维蛋白原降低,提示消耗性凝血功能障碍;组织中SYK的表达。结论细菌性脓毒症导致循环中性粒细胞的异质性,包括ldn。SYK在wbn和ldn中的表达升高与终末器官功能障碍相关,这表明SYK是细菌性脓毒症的潜在治疗靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Elevated Spleen Tyrosine Kinase in Low-Density Neutrophils During Bacterial Sepsis in a Nonhuman Primate Model
Background Sepsis is a leading cause of death world-wide. Identifying novel host-directed therapeutic targets may improve sepsis outcomes. Methods Six nonhuman primates were infected with Klebsiella pneumoniae to induce septic shock and provided supportive care for up to 72 hours. Flow cytometry was used to characterize whole blood neutrophils (WBNs) and low-density neutrophils (LDNs) at time (T0), T6, T24, and T48-hours post-infection; and postmortem examination (i.e. necropsy). Dimensional reduction with clustering via FlowSOM and traditional gating strategies were used to compare WBNs to LDNs and delineate spleen tyrosine kinase (SYK) expression across neutrophils subsets. We measured soluble biomarkers of end-organ dysfunction and neutrophil activation and quantified SYK and myeloperoxidase in tissue. Results At T6, we identified populations of active immature WBNs and a population of LDNs not detected at baseline. At T24, neutrophil heterogeneity increased across WBNs and LDNs with differential expression of myeloperoxidase (MPO). Compared to WBNs, LDNs were more activated with increased MPO expression. At T6, SYK expression surged in WBNs and LDNs and SYK+WBNs and LDNs expressed higher levels of MPO and lactoferrin compared to SYK- neutrophils. Circulating levels of SYK+LDNs significantly correlated with serum creatinine levels, indicative of acute kidney injury; prolonged prothrombin time and decreased fibrinogen, indicative of consumptive coagulopathy; and SYK expression in tissues. Conclusions Bacterial sepsis leads to heterogenous populations of circulating neutrophils, including LDNs. Elevated SYK expression in WBNs and LDNs correlates with end-organ dysfunction, highlighting SYK as a potential therapeutic target in bacterial sepsis.
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