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健康犬体内13C-氨基比林去甲基化的动力学分析

Kinetic analysis of demethylation of 13C-aminopyrine in healthy dogs.

作者信息

Moeller E Michael, Steiner Jörg M, Williams David A, Tetrick Mark, Burr John

机构信息

Gastrointestinal Laboratory, College of Veterinary Medicine, Texas A&M University, College Station, TX 77843, USA.

出版信息

Am J Vet Res. 2004 Feb;65(2):159-62. doi: 10.2460/ajvr.2004.65.159.

Abstract

OBJECTIVE

To describe the kinetics of demethylation of 13C-aminopyrine in healthy dogs for use in determining the most appropriate time for collection of blood samples for a 13C-aminopyrine demethylation blood test for evaluation of hepatic function.

ANIMALS

9 healthy dogs.

PROCEDURES

A 2-mL baseline blood sample was collected into an evacuated heparinized tube, and 13C-aminopyrine was administered to each dog (2 mg/kg, IV). Additional 2-mL blood samples were collected 15, 30, 45, 60, 75, 90, 105, 120, 135, 150, 180, 240, 300, and 360 minutes after 13C-aminopyrine administration. The CO2 was extracted from blood samples by addition of a strong acid, and the percentage dose of 13CO2 (PCD) in the extracted gas was determined by fractional mass spectrometry.

RESULTS

No dogs had gross evidence of adverse effects, and all had an increase in PCD after IV administration of 13C-aminopyrine. The PCD had the least variability among 5 variables used to evaluate hepatic demethylating capacity. Peak PCD was detected at 30 minutes in 1 dog, 45 minutes in 5 dogs, 60 minutes in 2 dogs, and 75 minutes in 1 dog. The mean PCD for the 9 dogs peaked at 45 minutes after 13C-aminopyrine administration.

CONCLUSIONS AND CLINICAL RELEVANCE

PCD appears to be the preferable variable for evaluation of hepatic demethylating capacity. Intravenous administration of 13C-aminopyrine leads to a consistent increase in PCD. Mean PCD peaked 45 minutes after administration, suggesting that blood sample collection 45 minutes after 13C-aminopyrine administration may be appropriate for use in estimating hepatic demethylating capacity.

摘要

目的

描述健康犬体内13C-氨基比林的去甲基化动力学,以确定用于评估肝功能的13C-氨基比林去甲基化血液检测中采集血样的最合适时间。

动物

9只健康犬。

步骤

采集2 mL基线血样至真空肝素化管中,每只犬静脉注射13C-氨基比林(2 mg/kg)。在注射13C-氨基比林后15、30、45、60、75、90、105、120、135、150、180、240、300和360分钟采集额外的2 mL血样。通过添加强酸从血样中提取二氧化碳,并用分馏质谱法测定提取气体中13CO2的剂量百分比(PCD)。

结果

没有犬出现明显的不良反应迹象,所有犬在静脉注射13C-氨基比林后PCD均升高。在用于评估肝脏去甲基化能力的5个变量中,PCD的变异性最小。1只犬在30分钟时检测到PCD峰值,5只犬在45分钟时检测到,2只犬在60分钟时检测到,1只犬在75分钟时检测到。9只犬的平均PCD在注射13C-氨基比林后45分钟达到峰值。

结论及临床意义

PCD似乎是评估肝脏去甲基化能力的更优变量。静脉注射13C-氨基比林会导致PCD持续升高。平均PCD在注射后45分钟达到峰值,这表明在注射13C-氨基比林后45分钟采集血样可能适合用于估计肝脏去甲基化能力。

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