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Combined NMR Experimental and Computer-Simulation Study of 2,3-Bisphosphoglycerate Metabolism in Human Erythrocytes

机译:联合NMR实验性和计算机仿真研究对人红细胞2,3-双次磷酸酯代谢的研究

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We have developed a new model of the metabolism of the human erythrocyte that is sufficiently comprehensive to explain the responses under many reproducible experimental conditions. The task has been addressed extensively in previous publications (Rapoport et al., 1976; Heinrich et al., 1977; Schuster et al., 1988; Johi & Palsson, 1989; Schuster & Holzhutter, 1995) but all earlier models fall short of providing a satisfactory comparison between their predictions and experimental data on carbon and phosphate flux into and out of the Rapoport-Luebering shunt, glycolysis and the phosphate flux into and out of the Rapoport-Luebering shunt, glycolysis and the pentose phosphate pathway, theat can be obtained by using ~1H, ~(13)C and ~(31)P NMR spectroscopy (Oxley et al., 1984; Thorburn & Kuchel, 1985; McIntyre et al., 1989; berthon et al., 1993). On the other hand, the previous models did serve to identify the many features of the regulation and control of glycolysis and were instrumental in the development of metabolic control theory (Heinrich et al., 1977).
机译:我们开发了一种新的人红细胞新陈代谢模型,该模型是足够综合的,以解释在许多可重复的实验条件下的反应。在以前的出版物(Rapoport等人,1976年,1976年,1977年,1977年,1977年,1988年,1988年,1989年; Schuster&Palzhutter,1995年),1995年,1995年,所有早期模型尚不缩短在Rapoport-Luebering分流,糖酵解和磷酸盐通量进出Rapoport-Luebering分流,糖酵解和磷酸磷酸盐途径中,提供了对碳和磷酸盐通量的预测和实验数据之间的令人满意的比较和磷酸盐的呼吸源,糖醇分子和磷酸磷酸盐途径。通过使用〜1H,〜(13)C和〜(31)P NMR光谱(1984年,1984; Thorburn&Kuchel,1985; Mcintyre等,1989; Berthon等,1993)。另一方面,以前的模型确实用于确定糖酵解的调节和控制的许多特征,并且在代谢控制理论的发展中是有乐器(Heinrich等,1977)。

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