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一种代表灌注大鼠心脏细胞外O-甲基化系统的数学模型。

A mathematical model representing the extraneuronal O-methylating system of the perfused rat heart.

作者信息

Kurahashi K, Rawlow A, Trendelenburg U

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 1980 Feb;311(1):17-32. doi: 10.1007/BF00500298.

Abstract
  1. A mathematical model was developed to mimic the function of the extraneuronal O-methylating system of the rat heart. Its essential features are: a saturable uptake process (uptake 2), a saturable, intracompartmental enzyme (COMT), the ability of the catecholamine to penetrate the membrane of the model compartment by a diffusional flux obeying first-order kinetics, and the ability of the metabolite to leave the compartment by an efflux obeying first-order kinetics. 2. Of the six kinetic constants of the model compartment five are known from experiments with hearts perfused with 3H-isoprenaline (Kmuptake, Vmaxuptake, Vmaxenzyme, k for amine, k for metabolite); only one constant is unknown (Kmenzyme) for the intact heart cells. 3. Results calculated with the help of the mathematical model were compared with results obtained from rat hearts perfused with 3H-isoprenaline. Although full congruency of results cannot be expected, there was satisfactory agreement between the two sets of results. Apparently, the mathematical model is able to simulate the function of the O-methylating system of the rat heart. 4. Comparison of the two sets of results leads to a definition of the function of the O-methylating system of the perfused rat heart. if all cells of the rat heart participate in the O-methylating system, the Km of the COMT of intact heart cells must be very low (i.e., somewhere between 2 and 5 microM isoprenaline). However, if the O-methylating system comprises only a small fraction of all cells, the COMT of the intact heart cells may well have a correspondingly higher Km.
摘要
  1. 建立了一个数学模型来模拟大鼠心脏细胞外O-甲基化系统的功能。其基本特征包括:一个可饱和的摄取过程(摄取2)、一个可饱和的细胞内酶(儿茶酚-O-甲基转移酶)、儿茶酚胺通过遵循一级动力学的扩散通量穿透模型隔室膜的能力,以及代谢产物通过遵循一级动力学的流出离开隔室的能力。2. 模型隔室的六个动力学常数中,有五个是通过用3H-异丙肾上腺素灌注心脏的实验得知的(摄取的Km、最大摄取速率、最大酶活性、胺的k、代谢产物的k);完整心脏细胞中只有一个常数未知(酶的Km)。3. 将借助数学模型计算的结果与用3H-异丙肾上腺素灌注大鼠心脏得到的结果进行了比较。虽然不能期望结果完全一致,但两组结果之间有令人满意的一致性。显然,该数学模型能够模拟大鼠心脏O-甲基化系统的功能。4. 两组结果的比较得出了灌注大鼠心脏O-甲基化系统功能的定义。如果大鼠心脏的所有细胞都参与O-甲基化系统,完整心脏细胞的儿茶酚-O-甲基转移酶的Km必须非常低(即,在2至5微摩尔异丙肾上腺素之间的某个值)。然而,如果O-甲基化系统仅包含所有细胞中的一小部分,完整心脏细胞的儿茶酚-O-甲基转移酶的Km很可能相应更高。

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