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首页> 外文期刊>The biochemical journal >The regulatory principles of glycolysis in erythrocytes in vivo and in vitro. A minimal comprehensive model describing steady states, quasi-steady states and time-dependent processes
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The regulatory principles of glycolysis in erythrocytes in vivo and in vitro. A minimal comprehensive model describing steady states, quasi-steady states and time-dependent processes

机译:体内和体外红细胞糖酵解的调节原理。描述稳定状态,准稳态和时间依赖过程的最小综合模型

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pA simple mathematical model for glycolysis in erythrocytes is presented which takes into account ATP synthesis and consumption. The system is described by four ordinary differential equations. Conditions in vivo are described by a stable steady state. The model predicts correctly the metabolite concentrations found in vivo. The parameters involved are in agreement with data on the separate steps. The metabolite changes found in pyruvate kinase-deficient erythrocytes and the species variations among erythrocytes from different animals are described satisfactorily. The roles of the enzymes in the control of metabolites and glycolytic flux are expressed in the form of a control matrix and control strengths [R. Heinrich & T.A. Rapoport (1974) Eur. J. Biochem. 42, 89-95] respectively. Erythrocytes from various species are shown to be adapted to a maximal ATP-consumption rate. The calculated eigenvalues reveal the pronounced time-hierarchy of the glycolytic reactions. Owing to the slowness of the 2,3-bisphospho-glycerate phosphatase reaction, quasi-steady states occur during the time-interval of about 0.5-2h incubation, which are defined by perturbed 2,3-bisphosphoglycerate concentrations. The theoretical predictions agree with experimental data. In the quasi-steady state the flux control is exerted almost entirely by the hexokinase-phosphofructokinase system. The model describes satisfactorily the time-dependent changes after addition of glucose to starved erythrocytes. The theoretical consequences are discussed of the conditions in vitro with lactate accumulation and the existence of a time-independent conservation quantity for the oxidized metabolites. Even in this closed system quasi-steady states occur which are characterized by approximately constant concentrations of all glycolytic metabolites except for the accumulation of lactate, fructose 1,6-bisphosphate and triose phosphate./p
机译:提出了一种简单的糖醇分解的数学模型,其考虑了ATP合成和消费。该系统由四个常微分方程描述。体内的条件是通过稳定的稳态描述的。该模型预测了体内发现的代谢物浓度正确。所涉及的参数与单独步骤的数据一致。在丙酮酸激酶缺陷的红细胞中发现的代谢物变化以及来自不同动物的红细胞的物种变异。令人满意地描述了来自不同动物的红细胞。酶在代谢物和糖酵解通量控制中的作用以对照基质和控制强度的形式表示[R. Heinrich& T.A. Rapoport(1974)欧元。 J. Biochem。 42,89-95]分别。各种物种的红细胞显示出适应最大的ATP消耗率。计算的特征值揭示了糖酵解反应的明显时间等级。由于2,3-双磷磷酸酶反应的缓慢,在约0.5-2小时的时间间隔期间发生准稳态,其由扰动的2,3-双磷基甘露浓度定义。理论预测与实验数据一致。在准稳态中,通过六酮酶 - 磷蛋白酶体系,磁通量控制几乎完全施加。该模型描述了葡萄糖向饥饿的红细胞后的时间依赖性变化令人满意。讨论了乳酸乳酸积累的体外条件的理论后果,并存在于氧化代谢物的时间不依赖性节省量。即使在这种闭合的系统中,也发生了准稳态,其特征在于除了乳酸乳液的积累之外,近似恒定浓度的所有糖酵解代谢物,果糖1,6-双磷酸盐和三糖磷酸盐。

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