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A System Dynamics Model to Predict the Human Monocyte Response to Endotoxins

机译:预测人类单核细胞对内毒素反应的系统动力学模型

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摘要

System dynamics is a powerful tool that allows modeling of complex and highly networked systems such as those found in the human immune system. We have developed a model that reproduces how the exposure of human monocytes to lipopolysaccharides (LPSs) induces an inflammatory state characterized by high production of tumor necrosis factor alpha (TNFα), which is rapidly modulated to enter into a tolerant state, known as endotoxin tolerance (ET). The model contains two subsystems with a total of six states, seven flows, two auxiliary variables, and 14 parameters that interact through six differential and nine algebraic equations. The parameters were estimated and optimized to obtain a model that fits the experimental data obtained from human monocytes treated with various LPS doses. In contrast to publications on other animal models, stimulation of human monocytes with super-low-dose LPSs did not alter the response to a second LPSs challenge, neither inducing ET, nor enhancing the inflammatory response. Moreover, the model confirms the low production of TNFα and increased levels of C–C motif ligand 2 when monocytes exhibit a tolerant state similar to that of patients with sepsis. At present, the model can help us better understand the ET response and might offer new insights on sepsis diagnostics and prognosis by examining the monocyte response to endotoxins in patients with sepsis.
机译:系统动力学是功能强大的工具,可用于对复杂且高度网络化的系统进行建模,例如人类免疫系统中发现的系统。我们已经开发了一个模型,该模型可以重现人类单核细胞暴露于脂多糖(LPS)的炎症状态,该炎症状态的特点是大量产生肿瘤坏死因子α(TNFα),并迅速调节其进入耐受状态,称为内毒素耐受性(ET)。该模型包含两个子系统,这些子系统共有六个状态,七个流,两个辅助变量以及通过六个微分方程和九个代数方程式进行交互的14个参数。估计并优化参数以获得适合于从用各种LPS剂量治疗的人单核细胞获得的实验数据的模型。与其他动物模型上的出版物相反,用超低剂量LPS​​刺激人单核细胞不会改变对第二个LPS激发的反应,既不会诱导ET,也不会增强炎症反应。此外,该模型证实了当单核细胞表现出与败血症患者相似的耐受状态时,TNFα的产量低且C–​​C基序配体2水平升高。目前,该模型可以帮助我们更好地了解ET反应,并可能通过检查脓毒症患者对内毒素的单核细胞反应,为脓毒症的诊断和预后提供新的见解。

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