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创伤的计算机模拟:个体特异性的数学模型和虚拟临床人群。

Trauma in silico: Individual-specific mathematical models and virtual clinical populations.

机构信息

Immunetrics Inc., Pittsburgh, PA 15219, USA.

Department of Surgery, University of Pittsburgh School of Medicine, Pittsburgh, PA 15213, USA.

出版信息

Sci Transl Med. 2015 Apr 29;7(285):285ra61. doi: 10.1126/scitranslmed.aaa3636.

Abstract

Trauma-induced critical illness is driven by acute inflammation, and elevated systemic interleukin-6 (IL-6) after trauma is a biomarker of adverse outcomes. We constructed a multicompartment, ordinary differential equation model that represents a virtual trauma patient. Individual-specific variants of this model reproduced both systemic inflammation and outcomes of 33 blunt trauma survivors, from which a cohort of 10,000 virtual trauma patients was generated. Model-predicted length of stay in the intensive care unit, degree of multiple organ dysfunction, and IL-6 area under the curve as a function of injury severity were in concordance with the results from a validation cohort of 147 blunt trauma patients. In a subcohort of 98 trauma patients, those with high-IL-6 single-nucleotide polymorphisms (SNPs) exhibited higher plasma IL-6 levels than those with low IL-6 SNPs, matching model predictions. Although IL-6 could drive mortality in individual virtual patients, simulated outcomes in the overall cohort were independent of the propensity to produce IL-6, a prediction verified in the 98-patient subcohort. In silico randomized clinical trials suggested a small survival benefit of IL-6 inhibition, little benefit of IL-1β inhibition, and worse survival after tumor necrosis factor-α inhibition. This study demonstrates the limitations of extrapolating from reductionist mechanisms to outcomes in individuals and populations and demonstrates the use of mechanistic simulation in complex diseases.

摘要

创伤后导致的危重症是由急性炎症引起的,创伤后系统白细胞介素-6(IL-6)升高是不良结局的生物标志物。我们构建了一个多室、常微分方程模型,代表了一个虚拟的创伤患者。该模型的个体特定变体再现了 33 名钝器伤幸存者的全身炎症和结局,由此产生了 10000 名虚拟创伤患者的队列。模型预测的 ICU 住院时间、多器官功能障碍程度以及作为损伤严重程度函数的 IL-6 曲线下面积与 147 名钝器伤患者的验证队列的结果一致。在 98 名创伤患者的亚组中,高 IL-6 单核苷酸多态性(SNP)的患者比低 IL-6 SNP 的患者具有更高的血浆 IL-6 水平,与模型预测相符。尽管 IL-6 可能导致个别虚拟患者的死亡,但在整个队列中的模拟结果与产生 IL-6 的倾向无关,这一预测在 98 名患者的亚组中得到了验证。模拟随机临床试验表明,IL-6 抑制有较小的生存获益,IL-1β 抑制获益较小,而 TNF-α 抑制后的生存更差。这项研究表明,从简化机制推断个体和人群的结果存在局限性,并展示了在复杂疾病中使用机制模拟的方法。

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