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使用脑切片的2-脱氧葡萄糖代谢动力学模型。

Kinetic model of 2-deoxyglucose metabolism using brain slices.

作者信息

Newman G C, Hospod F E, Patlak C S

机构信息

Department of Neurology, SUNY, Stony Brook 11794.

出版信息

J Cereb Blood Flow Metab. 1990 Jul;10(4):510-26. doi: 10.1038/jcbfm.1990.93.

Abstract

A six-compartment, nine-parameter kinetic model of 2-deoxyglucose (2DG) metabolism, which includes bidirectional tissue transport, phosphorylation, two-step dephosphorylation, phosphoisomerization, and conjugation to UDP and macromolecules, has been derived. Data for analysis were obtained from 540- and 1,000-microns-thick hippocampal and hypothalamic brain slices, which were incubated in buffer containing [14C]2DG, frozen, extracted with perchlorate, and separated on anion-exchange columns. Solutions of the equations of the model were fit to the data by means of nonlinear least-squares analysis. These studies suggest that dephosphorylation is adequately described by a single reaction so that the model reduces to eight parameters. The in vitro rate constants for transport, phosphorylation, and dephosphorylation are very similar to prior in vivo results. The phosphoisomerization rate constant is similar to dephosphorylation, so glycosylated macromolecules slowly accumulate and gradually assume larger relative importance as other compounds disappear more rapidly. Rate constants for 540-microns slices from hypothalamus and hippocampus are similar, while 1,000-microns slices have smaller tissue transport constants and larger phosphorylation constants. The rate equation for glucose utilization of this model is relatively insensitive to uncertainties regarding the rate constants. Including later metabolic components in kinetic models improves the calculations of glucose utilization with long isotope exposures.

摘要

已推导得出一个用于2-脱氧葡萄糖(2DG)代谢的六室、九参数动力学模型,该模型包括双向组织转运、磷酸化、两步去磷酸化、磷酸异构化以及与UDP和大分子的结合。分析数据取自厚度为540微米和1000微米的海马体和下丘脑脑片,这些脑片在含有[14C]2DG的缓冲液中孵育,冷冻后用高氯酸盐提取,并在阴离子交换柱上分离。通过非线性最小二乘法分析,将模型方程的解与数据进行拟合。这些研究表明,去磷酸化可用单一反应充分描述,因此该模型简化为八个参数。转运、磷酸化和去磷酸化的体外速率常数与先前的体内结果非常相似。磷酸异构化速率常数与去磷酸化相似,因此随着其他化合物更快消失,糖基化大分子会缓慢积累并逐渐占据更大的相对重要性。下丘脑和海马体540微米脑片的速率常数相似,而1000微米脑片的组织转运常数较小,磷酸化常数较大。该模型的葡萄糖利用速率方程对速率常数的不确定性相对不敏感。在动力学模型中纳入后期代谢成分可改善长时间同位素暴露下葡萄糖利用的计算。

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