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用3H和14C标记的乳酸测定体内乳酸周转率。示踪剂给药部位和取样的意义。

The determination of lactate turnover in vivo with 3H- and 14C-labelled lactate. The significance of sites of tracer administration and sampling.

作者信息

Katz J, Okajima F, Chenoweth M, Dunn A

出版信息

Biochem J. 1981 Feb 15;194(2):513-24. doi: 10.1042/bj1940513.

Abstract

L-[3-3H,U-14C]Lactate was administered to starved rats either as a bolus or by continuous infusion. Tracer administration was performed two ways: injection into the vena cava and sampling from the aorta (V-A mode), or injection into the aorta and sampling from the vena cava (A-VC mode). The specific-radioactivity curves after infusion or injection differed markedly with the two procedures. However, the specific radioactivities of 14C-labelled glucose derived from [U-14C]lactate were similar in the two modes. The apparent turnover rates of lactate calculated from the 3H specific-radioactivity curves in the V-A mode were about half those obtained from the 3H specific-radioactivity curves in the A-VC mode. The apparent contribution of lactate carbon to glucose carbon calculated from specific-radioactivity curves of the A-VC mode was greater than that obtained from the V-A mode. The apparent recycling of lactate carbon calculated from the specific radioactivities for [U-14C]- and [3-3H]-lactate was greater in the A-VC mode than the V-A mode. [U-14C] Glucose was administered in the two modes, but in contrast with lactate the specific radioactivities were only slightly different. An analysis to account for these observations is presented. It is shown that the two modes represent sampling from different pools of lactate. The significance of sites of tracer administration and sampling for the interpretation of tracer kinetics of compounds present in intracellular and extracellular spaces, and with a high turnover rate, is discussed. We propose that for such compounds, including lactate, alanine and glycerol, the widely used V-A mode leads to a marked underestimate of replacement, mass and carbon recycling, and that the A-VC mode is the preferred method for the assessment of these parameters.

摘要

将L-[3-³H,U-¹⁴C]乳酸盐以推注或持续输注的方式给予饥饿的大鼠。示踪剂的给予通过两种方式进行:注入腔静脉并从主动脉取样(V-A模式),或注入主动脉并从腔静脉取样(A-VC模式)。输注或注射后的比放射性曲线在这两种操作中明显不同。然而,由[U-¹⁴C]乳酸盐衍生的¹⁴C标记葡萄糖的比放射性在两种模式中相似。根据V-A模式中³H比放射性曲线计算的乳酸表观周转率约为A-VC模式中从³H比放射性曲线获得的值的一半。根据A-VC模式的比放射性曲线计算的乳酸碳对葡萄糖碳的表观贡献大于从V-A模式获得的贡献。根据[U-¹⁴C]-和[3-³H]-乳酸盐的比放射性计算的乳酸碳的表观再循环在A-VC模式中比V-A模式更大。以两种模式给予[U-¹⁴C]葡萄糖,但与乳酸不同的是,比放射性仅略有差异。本文提出了对这些观察结果的分析。结果表明,这两种模式代表了从不同的乳酸池取样。讨论了示踪剂给药和取样部位对解释细胞内和细胞外空间中存在的、具有高周转率的化合物的示踪动力学的意义。我们提出,对于包括乳酸、丙氨酸和甘油在内的此类化合物,广泛使用的V-A模式会导致对替代、质量和碳再循环的显著低估,而A-VC模式是评估这些参数的首选方法。

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