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首页> 外文期刊>Biotechnology Journal: Healthcare,Nutrition,Technology >Querying quantitative logic models (Q2LM) to study intracellular signaling networks and cell-cytokine interactions
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Querying quantitative logic models (Q2LM) to study intracellular signaling networks and cell-cytokine interactions

机译:查询定量逻辑模型(Q2LM)以研究细胞内信号传递网络和细胞因子相互作用

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Mathematical models have substantially improved our ability to predict the response of a complex biological system to perturbation, but their use is typically limited by difficulties in specifying model topology and parameter values. Additionally, incorporating entities across different biological scales ranging from molecular to organismal in the same model is not trivial. Here, we present a framework called "querying quantitative logic models" (Q2LM) for building and asking questions of constrained fuzzy logic (cFL) models. cFL is a recently developed modeling formalism that uses logic gates to describe influences among entities, with transfer functions to describe quantitative dependencies. Q2LM does not rely on dedicated data to train the parameters of the transfer functions, and it permits straight-forward incorporation of entities at multiple biological scales. The Q2LM framework can be employed to ask questions such as: which therapeutic perturbations accomplish a designated goal, and under what environmental conditions will these perturbations be effective? We demonstrate the utility of this framework for generating testable hypotheses in two examples: (i) a intracellular signaling network model; and (ii) a model for pharmacokinetics and pharmacodynamics of cell-cytokine interactions; in the latter, we validate hypotheses concerning molecular design of granulocyte colony stimulating factor.
机译:数学模型已经大大提高了我们预测复杂生物系统对扰动的响应的能力,但是数学模型的使用通常受到指定模型拓扑和参数值的困难的限制。另外,在同一模型中并入从分子到有机体的不同生物学规模的实体并非易事。在这里,我们提出了一个称为“查询定量逻辑模型”(Q2LM)的框架,用于建立和询问约束模糊逻辑(cFL)模型的问题。 cFL是最近开发的建模形式主义,它使用逻辑门来描述实体之间的影响,并使用传递函数来描述数量依赖性。 Q2LM不依赖于专用数据来训练传递函数的参数,它允许直接整合多个生物学规模的实体。可以使用Q2LM框架来提出以下问题:哪些治疗性扰动实现了指定的目标,以及这些扰动在什么环境条件下有效?我们在两个例子中证明了该框架用于产生可检验假设的效用:(i)细胞内信号网络模型; (ii)细胞-细胞因子相互作用的药代动力学和药效学模型;在后者中,我们验证了有关粒细胞集落刺激因子分子设计的假设。

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