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Improvement of prognostic performance in severely injured patients by integrated clinico-transcriptomics: a translational approach

机译:整合临床转录组学技术改善重伤患者的预后能力:一种翻译方法

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IntroductionSevere trauma triggers a systemic inflammatory response that contributes to secondary complications, such as nosocomial infections, sepsis or multi-organ failure. The present study was aimed to identify markers predicting complications and an adverse outcome of severely injured patients by an integrated clinico-transcriptomic approach.MethodsIn a prospective study, RNA samples from circulating leukocytes from severely injured patients (injury severity score?≥?17 points; n?=?104) admitted to a Level I Trauma Center were analyzed for dynamic changes in gene expression over a period of 21?days by quantitative RT-PCR. Transcriptomic candidates were selected based on whole genome screening of a representative discovery set (n?=?10 patients) or known mechanisms of the immune response, including mediators of inflammation (IL-8, IL-10, TNF-α, MIF, C5, CD59, SPHK1), danger signaling (HMGB1, TLR2, CD14, IL-33, IL-1RL1), and components of the heme degradation pathway (HP, CD163, HMOX1, BLVRA, BLVRB). Clinical markers comprised standard physiological and laboratory parameters and scoring systems routinely determined in trauma patients.ResultsLeukocytes, thrombocytes and the expression of sphingosine kinase-1 (SPHK1), complement C5, and haptoglobin (HP) have been identified as markers with the best performance. Leukocytes showed a biphasic course with peaks on day 0 and day 11 after trauma, and patients with sepsis exhibited significantly higher leukocyte levels. Thrombocyte numbers showed a typical profile with initial thrombopenia and robust thrombocytosis in week 3 after trauma, ranging 2- to 3-fold above the upper normal value. ‘Relative thrombocytopenia’ was associated with multi-organ dysfunction, the development of sepsis, and mortality, the latter of which could be predicted within 3?days prior to the time point of death. SPHK1 expression at the day of admission indicated mortality with excellent performance. C5-expression on day 1 after trauma correlated with an increased risk for the development of nosocomial infections during the later course, while HP was found to be a marker for the development of sepsis.ConclusionsThe combination of clinical and transcriptomic markers improves the prognostic performance and may represent a useful tool for individual risk stratification in trauma patients.Electronic supplementary materialThe online version of this article (doi:10.1186/s13054-015-1127-y) contains supplementary material, which is available to authorized users.
机译:简介严重的外伤会引起全身性炎症反应,从而导致继发性并发症,例如医院感染,败血症或多器官衰竭。本研究旨在通过综合的临床转录组学方法识别预测重症患者的并发症和不良后果的标志物。方法在一项前瞻性研究中,从重症患者的循环白细胞中提取RNA样本(损伤严重度得分≥17分;通过定量RT-PCR分析了进入I级创伤中心的n≥104)在21天的时间内基因表达的动态变化。基于代表性发现集(n = 10例患者)的全基因组筛选或免疫应答的已知机制,包括炎症介质(IL-8,IL-10,TNF-α,MIF,C5)选择转录组候选物,CD59,SPHK1),危险信号(HMGB1,TLR2,CD14,IL-33,IL-1RL1)和血红素降解途径的成分(HP,CD163,HMOX1,BLVRA,BLVRB)。临床标记包括常规在创伤患者中确定的标准生理和实验室参数以及评分系统。白细胞显示出双相过程,在创伤后第0天和第11天达到峰值,败血症患者的白细胞水平明显升高。创伤后第3周,血小板数目显示出典型的特征,即最初的血小板减少症和强烈的血小板增多,比正常值高2至3倍。 “相对血小板减少症”与多器官功能障碍,败血症的发生和死亡率有关,后者的死亡可以在死亡时间之前的3天之内进行预测。入院当天SPHK1的表达表明死亡率高,表现出色。创伤后第1天C5的表达与后期感染医院感染的风险增加有关,而HP被发现是败血症发生的标志物。结论临床和转录组标志物的组合可改善预后和电子补充材料本文的在线版本(doi:10.1186 / s13054-015-1127-y)包含补充材料,授权用户可以使用。

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