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Development of a genomic metric that can be rapidly used to predict clinical outcome in severely injured trauma patients

机译:开发可快速用于预测重伤患者的临床结果的基因组学指标

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OBJECTIVE: Many patients have complicated recoveries following severe trauma due to the development of organ injury. Physiological and anatomical prognosticators have had limited success in predicting clinical trajectories. We report on the development and retrospective validation of a simple genomic composite score that can be rapidly used to predict clinical outcomes. DESIGN: Retrospective cohort study. SETTING: Multi-institutional level 1 trauma centers. PATIENTS: Data were collected from 167 severely traumatized (injury severity score >15) adult (18-55 yr) patients. METHODS: Microarray-derived genomic data obtained from 167 severely traumatized patients over 28 days were assessed for differences in messenger RNA abundance among individuals with different clinical trajectories. Once a set of genes was identified based on differences in expression over the entire study period, messenger RNA abundance from these subjects obtained in the first 24 hours was analyzed in a blinded fashion using a rapid multiplex platform, and genomic data reduced to a single metric. RESULTS: From the existing genomic dataset, we identified 63 genes whose leukocyte expression differed between an uncomplicated and complicated clinical outcome over 28 days. Using a multiplex approach that can quantitate messenger RNA abundance in less than 12 hours, we reassessed total messenger RNA abundance from the first 24 hours after trauma and reduced the genomic data to a single composite score using the difference from reference. This composite score showed good discriminatory capacity to distinguish patients with a complicated outcome (area under a receiver-operator curve, 0.811; p <0.001). This was significantly better than the predictive power of either Acute Physiology and Chronic Health Evaluation II or new injury severity score scoring systems. CONCLUSIONS: A rapid genomic composite score obtained in the first 24 hours after trauma can retrospectively identify trauma patients who are likely to develop complicated clinical trajectories. A novel platform is described in which this genomic score can be obtained within 12 hours of blood collection, making it available for clinical decision making.
机译:目的:由于器官损伤的发展,许多患者在严重的创伤后恢复复杂。生理和解剖学预测者在预测临床轨迹方面的成功有限。我们报告了一个简单的基因组综合评分的发展和回顾性验证,该评分可快速用于预测临床结果。设计:回顾性队列研究。地点:多机构一级创伤中心。患者:数据收集自167名严重外伤(严重程度评分> 15)成年(18-55岁)患者。方法:从28天的167名严重创伤患者中获得的微阵列基因组数据,评估了具有不同临床轨迹的个体在信使RNA丰度方面的差异。根据整个研究期间的表达差异确定了一组基因后,便使用快速多重平台以盲法分析了前24小时从这些受试者获得的信使RNA的丰度,并将基因组数据简化为一个指标。结果:从现有的基因组数据集中,我们鉴定出63个基因,其白细胞表达在28天的简单和复杂临床结果之间有所不同。使用可以在不到12小时内量化信使RNA丰度的多重方法,我们从创伤后的最初24小时重新评估了总信使RNA丰度,并使用与参考文献的差异将基因组数据减少到单个综合评分。该综合评分显示出很好的区分能力,可以区分具有复杂结局的患者(接受者-操作者曲线下的面积为0.811; p <0.001)。这明显好于急性生理学和慢性健康评估II或新的损伤严重程度评分系统的预测能力。结论:创伤后24小时内获得的快速基因组综合评分可以回顾性地鉴定出可能发展为复杂临床轨迹的创伤患者。描述了一种新颖的平台,其中该基因组分数可在采血后12小时内获得,使其可用于临床决策。

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