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Candidate States of Helicobacter pylori's Genome-Scale Metabolic Network upon Application of “Loop Law” Thermodynamic Constraints

机译:应用“循环定律”热力学约束的幽门螺杆菌基因组规模代谢网络的候选状态

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摘要

Constraint-based modeling has proven to be a useful tool in the analysis of biochemical networks. To date, most studies in this field have focused on the use of linear constraints, resulting from mass balance and capacity constraints, which lead to the definition of convex solution spaces. One additional constraint arising out of thermodynamics is known as the “loop law” for reaction fluxes, which states that the net flux around a closed biochemical loop must be zero because no net thermodynamic driving force exists. The imposition of the loop-law can lead to nonconvex solution spaces making the analysis of the consequences of its imposition challenging. A four-step approach is developed here to apply the loop-law to study metabolic network properties: 1), determine linear equality constraints that are necessary (but not necessarily sufficient) for thermodynamic feasibility; 2), tighten Vmax and Vmin constraints to enclose the remaining nonconvex space; 3), uniformly sample the convex space that encloses the nonconvex space using standard Monte Carlo techniques; and 4), eliminate from the resulting set all solutions that violate the loop-law, leaving a subset of steady-state solutions. This subset of solutions represents a uniform random sample of the space that is defined by the additional imposition of the loop-law. This approach is used to evaluate the effect of imposing the loop-law on predicted candidate states of the genome-scale metabolic network of Helicobacter pylori.
机译:基于约束的建模已被证明是分析生化网络的有用工具。迄今为止,该领域中的大多数研究都集中在由于质量平衡和容量约束而导致的线性约束的使用上,这导致了凸解空间的定义。由热力学引起的另外一个约束条件是反应通量的“回路定律”,该定律指出,由于不存在净热力学驱动力,因此围绕生化回路的净通量必须为零。施加环律可能会导致非凸解空间,这使得对其施加的后果进行分析具有挑战性。这里开发了一种四步方法来应用环路定律来研究代谢网络的特性:1)确定热力学可行性所必需(但不一定足够)的线性等式约束; 2)收紧Vmax和Vmin约束以包围剩余的非凸空间; 3)使用标准的蒙特卡洛技术对包围非凸空间的凸空间进行均匀采样;和4),从结果集中消除所有违反环路定律的解,剩下稳态解的子集。解决方案的此子集表示空间的统一随机样本,该样本由环律的附加强加定义。该方法用于评估对幽门螺杆菌基因组规模代谢网络的预测候选状态施加环律的效果。

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