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在人类创伤中,当损伤严重程度较高时,保护性/修复性细胞因子会受到抑制。

Protective/reparative cytokines are suppressed at high injury severity in human trauma.

作者信息

Cai Jinman, McKinley Todd, Billiar Isabel, Zenati Mazen S, Gaski Greg, Vodovotz Yoram, Gruen Danielle S, Billiar Timothy R, Namas Rami A

机构信息

Department of Surgery, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA.

Department of Orthopedic Surgery, Indiana University School of Medicine, Indianapolis, Indiana, USA.

出版信息

Trauma Surg Acute Care Open. 2021 Mar 2;6(1):e000619. doi: 10.1136/tsaco-2020-000619. eCollection 2021.

Abstract

BACKGROUND

Trauma elicits a complex inflammatory response that, among multiple presenting factors, is greatly impacted by the magnitude of injury severity. Herein, we compared the changes in circulating levels of mediators with known proinflammatory roles to those with known protective/reparative actions as a function of injury severity in injured humans.

METHODS

Clinical and biobank data were obtained from 472 (trauma database-1 (TD-1), University of Pittsburgh) and 89 (trauma database-2 (TD-2), Indiana University) trauma patients admitted to the intensive care unit (ICU) and who survived to discharge. Injury severity was estimated based on the Injury Severity Score (ISS), and this was used as both a continuous variable and for the purpose of grouping patients into severity-based cohorts. Samples within the first 24 hours were obtained from all patients and then daily up to day 7 postinjury in TD-1. Sixteen cytokines were assayed using Luminex and were analyzed using two-way analysis of variance (p<0.05).

RESULTS

Patients with higher ISSs had longer ICU and hospital stays, days on mechanical ventilation and higher rates of nosocomial infection when compared with the mild and moderate groups. Time course analysis and correlations with ISS showed that 11 inflammatory mediators correlated positively with injury severity, consistent with previous reports. However, five mediators (interleukin (IL)-9, IL-21, IL-22, IL-23 and IL-17E/25) were suppressed in patients with high ISS and inversely correlated with ISS.

DISCUSSION

These findings suggest that severe injury is associated with a suppression of a subset of cytokines known to be involved in tissue protection and regeneration (IL-9, IL-22 and IL-17E/25) and lymphocyte differentiation (IL-21 and IL-23), which in turn correlates with adverse clinical outcomes. Thus, patterns of proinflammatory versus protective/reparative mediators diverge with increasing ISS.

摘要

背景

创伤引发复杂的炎症反应,在多种呈现因素中,损伤严重程度对其影响极大。在此,我们比较了已知具有促炎作用的介质与已知具有保护/修复作用的介质在受伤人类体内的循环水平变化与损伤严重程度的关系。

方法

从匹兹堡大学的472例(创伤数据库-1(TD-1))和印第安纳大学的89例(创伤数据库-2(TD-2))入住重症监护病房(ICU)并存活至出院的创伤患者中获取临床和生物样本库数据。根据损伤严重程度评分(ISS)评估损伤严重程度,并将其用作连续变量以及将患者分组为基于严重程度的队列。在TD-1中,所有患者在伤后24小时内采集样本,然后每天采集直至伤后第7天。使用Luminex检测16种细胞因子,并采用双向方差分析进行分析(p<0.05)。

结果

与轻度和中度组相比,ISS较高的患者在ICU和医院的住院时间更长、机械通气天数更多且医院感染率更高。时间进程分析以及与ISS的相关性表明,11种炎症介质与损伤严重程度呈正相关,这与先前的报道一致。然而,5种介质(白细胞介素(IL)-9、IL-21、IL-22、IL-23和IL-17E/25)在ISS高的患者中受到抑制,且与ISS呈负相关。

讨论

这些发现表明,严重损伤与已知参与组织保护和再生(IL-9、IL-22和IL-17E/25)以及淋巴细胞分化(IL-21和IL-23)的细胞因子亚群的抑制有关,这反过来又与不良临床结局相关。因此,促炎介质与保护/修复介质的模式随着ISS的增加而不同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d6b8/7929818/cd47648f4956/tsaco-2020-000619f01.jpg

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