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肝脏白蛋白和尿素合成:[14C]碳酸盐衍生的胍基标记精氨酸在离体灌注大鼠肝脏中的动力学数学建模。

Hepatic albumin and urea synthesis: The mathematical modelling of the dynamics of [14C]carbonate-derived guanidine-labelled arginine in the isolated perfused rat liver.

作者信息

Tavill A S, Nadkarni D, Metcalfe J, Black E, Hoffenberg R, Carson E R

出版信息

Biochem J. 1975 Sep;150(3):495-509. doi: 10.1042/bj1500495.

Abstract

A mathematical model was constructed to define the dynamics of incorporation of radioactivity into urea carbon and the guanidine carbon of arginine in plasma albumin after the rapid intraportal-venous administration of Na214CO3 in the isolated perfused rat liver. 2. The model was formulated in terms of compartmental analysis and additional experiments were designed to provide further information on subsystem dynamics and to discriminate between alternative model structures. 3. Evidence for the rapid-time-constant of labelling of intracellular arginine was provided by precursor-product analysis of precursor [14C]carboante and product [14C]urea in the perfusate. 4. Compartmental analysis of the dynamics of newly synthesized urea was based on the fate of exogenous [13C]urea, endogenous [14C]urea and the accumulation of [12C]urea in perfusate water, confirming the early completion of urea carbon labelling, the absence of continuing synthesis of labelled urea, and the presence of a small intrahepatic urea-delay pool. 5. Analysis of the perfusate dynamics of endogenously synthesized and exogenously administered [6-14C]arginine indicated that although the capacity for extrahepatic formation of [14C]-urea exists, little or no arginine formed within the intrahepatic urea cycle was transported out of the liver. However, the presence of a rapidly turning-over intrahepatic arginine pool was confirmed. 6. On the basis of these subsystem analyses it was possible to offer feasible estimations for the parameters of the mathematical model. However, it was not possible to stimulate the form and magnitude of the dynamics of newly synthesized labelled urea and albumin which were simultaneously observed after administration of [14C]carbonate on the basis of a preliminary model which postulated that both products were derived from a single hepatic pool of [16-14C]arginine. On the other hand these observed dynamics could be satisfied to a two-compartment arginine model, which also provided an explanation for discrepancies observed between albumin synthesis measured radioisotopically and immunologically. This was based on a relative overestimation of [14C]urea specific radioactivity resulting from the rapid dynamics of [14C]carbonate and the [14C]urea subsystem relative to the labelled albumin subsystem. The effects of arginine compartmentalization could be minimized in the model by minor slowing of the rate of [14C]carbonate turnover or by constant infusion of [14C]carbonate, both of which permitted valid determination of albumin-synthesis rates.

摘要
  1. 构建了一个数学模型,以确定在离体灌注大鼠肝脏中快速门静脉内注射Na214CO3后,放射性物质掺入血浆白蛋白中尿素碳和精氨酸胍基碳的动力学。2. 该模型根据房室分析制定,并设计了额外的实验,以提供有关子系统动力学的更多信息,并区分替代模型结构。3. 通过对灌注液中前体[14C]碳酸盐和产物[14C]尿素进行前体-产物分析,提供了细胞内精氨酸标记快速时间常数的证据。4. 对新合成尿素动力学的房室分析基于外源性[13C]尿素、内源性[14C]尿素的命运以及灌注液水中[12C]尿素的积累,证实了尿素碳标记的早期完成、标记尿素持续合成的不存在以及肝内小尿素延迟池的存在。5. 对内源性合成和外源性给予的[6-14C]精氨酸的灌注液动力学分析表明,虽然存在肝外形成[14C]尿素的能力,但肝内尿素循环中形成的精氨酸很少或没有转运出肝脏。然而,证实了存在快速周转的肝内精氨酸池。6. 根据这些子系统分析,可以对数学模型的参数进行可行的估计。然而,基于假设两种产物均来自单一肝[16-14C]精氨酸池的初步模型,无法模拟给予[14C]碳酸盐后同时观察到的新合成标记尿素和白蛋白动力学的形式和大小。另一方面,这些观察到的动力学可以由两房室精氨酸模型满足,该模型也为放射性同位素法和免疫学法测量白蛋白合成之间观察到的差异提供了解释。这是基于相对于标记白蛋白子系统,[14C]碳酸盐和[14C]尿素子系统的快速动力学导致[14C]尿素比放射性的相对高估。在模型中,通过稍微减慢[14C]碳酸盐周转速率或通过持续输注[14C]碳酸盐,可以将精氨酸区室化的影响最小化,这两种方法都允许有效测定白蛋白合成速率。

相似文献

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Metabolism of arginine by the isolated perfused rat kidney.离体灌注大鼠肾脏对精氨酸的代谢
Am J Physiol. 1978 Oct;235(4):F376-80. doi: 10.1152/ajprenal.1978.235.4.F376.

本文引用的文献

1
AMINO ACID METABOLISM IN THE PERFUSED RAT LIVER.灌注大鼠肝脏中的氨基酸代谢
J Physiol. 1964 Nov;174(2):273-94. doi: 10.1113/jphysiol.1964.sp007487.
5
The formulation and testing of models.模型的构建与测试。
Ann N Y Acad Sci. 1963 May 10;108:182-94. doi: 10.1111/j.1749-6632.1963.tb13373.x.
8
An automatic method for colorimetric analysis.一种比色分析的自动方法。
Am J Clin Pathol. 1957 Sep;28(3):311-22. doi: 10.1093/ajcp/28.3_ts.311.

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