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人类和家畜3-甲基组氨酸代谢的房室模型的开发与应用。

Development and application of a compartmental model of 3-methylhistidine metabolism in humans and domestic animals.

作者信息

Rathmacher J A, Nissen S L

机构信息

Department of Animal Science, Iowa State University, Ames 50011, USA.

出版信息

Adv Exp Med Biol. 1998;445:303-24. doi: 10.1007/978-1-4899-1959-5_20.

Abstract

Measurement of urinary 3-methylhistidine (3MH) excretion is the primary in vivo method to measure skeletal muscle (myofibrillar) protein breakdown. This method requires quantitative collection of urine and is based on the assumption that no metabolism of 3MH occurs once it is released from actin and myosin. This is true in most species, but in sheep and swine a proportion is retained in muscle as a dipeptide, balenine. In neither of these species does urine 3MH yield any data on the metabolism of 3MH. We have conducted studies that propose that 3MH metabolism in humans, cattle, dogs, swine, and sheep can be defined from a single bolus infusion of a stable isotope 3-[methyl-2H3]-methylhistidine. Following the bolus dose of the stable isotope tracer, serial blood samples and/or urine was collected over three to five days. A minimum of three exponentials were required to describe the plasma decay curve adequately. The kinetic linear-time-invariant models of 3MH metabolism in the whole animal were constructed by using the SAAM/CONSAM modeling program. Three different configurations of a three-compartment model are described: (A) A simple three-compartment model for humans, cattle, and dogs, in which plasma kinetics (3-[methyl-2H3]-MH/3MH) are described by compartment 1 and with one urinary exit from compartment 1. (B) A plasma-urinary kinetic three-compartment model with two exits was used for sheep with a urinary exit out of compartment 1 and a balenine exit out of a tissue compartment 3. (C) A plasma three-compartment model was used in swine with an exit out of a tissue compartment 3. The kinetic parameters reflect the differences in known physiology of humans, cattle, and dogs as compared to sheep and swine that do not quantitatively excrete 3MH into the urine. Steady-state model calculations define masses and fluxes of 3MH between three compartments and, importantly, the de novo production of 3MH. The de novo production of 3MH for humans, cattle, dogs, sheep, and swine are 3.1, 6.0, 12.1, 10.3, and 7.2 mumol x kg-1 x d-1, respectively. The de novo production of 3MH as calculated by the compartmental model was not different when compared to 3MH production as calculated via traditional urinary collection. Additionally, data suggest that steady-state compartment masses and mass transfer rates may be related to fat free mass and muscle mass in humans and swine, respectively. In conclusion, models of 3MH metabolism have been developed in numerous species, and these models can be used for the assessment of muscle proteolysis and 3MH kinetics without the collection of urine. This methodology is less evasive and will be useful in testing further experimental designs that alter myofibrillar protein breakdown.

摘要

测量尿中3 - 甲基组氨酸(3MH)排泄量是测定骨骼肌(肌原纤维)蛋白质分解代谢的主要体内方法。该方法需要定量收集尿液,并且基于这样的假设:3MH一旦从肌动蛋白和肌球蛋白释放出来就不会发生代谢。在大多数物种中确实如此,但在绵羊和猪中,一部分3MH会以二肽——肌肽的形式保留在肌肉中。在这两种物种中,尿中3MH都无法提供有关3MH代谢的任何数据。我们进行的研究表明,人类、牛、狗、猪和绵羊体内的3MH代谢可以通过单次推注稳定同位素3 - [甲基 - 2H3] - 甲基组氨酸来定义。在推注稳定同位素示踪剂后,在三到五天内采集系列血样和/或尿液。至少需要三个指数来充分描述血浆衰变曲线。使用SAAM/CONSAM建模程序构建了全动物体内3MH代谢的动力学线性时不变模型。描述了三室模型的三种不同构型:(A)适用于人类、牛和狗的简单三室模型,其中血浆动力学(3 - [甲基 - 2H3] - MH/3MH)由第1室描述,且有一个从第1室通向尿液的出口。(B)具有两个出口的血浆 - 尿液动力学三室模型用于绵羊,一个尿液出口来自第1室,一个肌肽出口来自组织第3室。(C)血浆三室模型用于猪,有一个出口来自组织第3室。动力学参数反映了人类、牛和狗与绵羊和猪已知生理学的差异,绵羊和猪不会将3MH定量排泄到尿液中。稳态模型计算定义了三个室之间3MH的质量和通量,重要的是,定义了3MH的从头生成量。人类、牛、狗、绵羊和猪的3MH从头生成量分别为3.1、6.0、12.1、10.3和7.2 μmol·kg⁻¹·d⁻¹。通过三室模型计算的3MH从头生成量与通过传统尿液收集计算的3MH生成量相比没有差异。此外,数据表明,稳态室质量和质量转移率可能分别与人类和猪的去脂体重和肌肉质量有关。总之,已经在多种物种中建立了3MH代谢模型,这些模型可用于评估肌肉蛋白水解和3MH动力学,而无需收集尿液。这种方法侵入性较小,将有助于测试改变肌原纤维蛋白分解代谢的进一步实验设计。

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