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使用[U-13C]葡萄糖和质量同位素异构体分析进行葡萄糖同位素、碳循环和糖异生作用研究。

Glucose isotope, carbon recycling, and gluconeogenesis using [U-13C]glucose and mass isotopomer analysis.

作者信息

Lee W N, Sorou S, Bergner E A

机构信息

Department of Pediatrics, Harbor-UCLA Medical Center, Torrance 90509.

出版信息

Biochem Med Metab Biol. 1991 Jun;45(3):298-309. doi: 10.1016/0885-4505(91)90034-i.

Abstract

Experimental determinations of glucose carbon recycling using 14C or 13C glucose tracer often underestimate true Cori cycle activity because of dilution and exchange of isotope tracer through the tricarboxylic acid (TCA) cycle. The term glucose isotope recycling therefore is used to distinguish recycling of isotope from recycling of glucose carbon, the actual quantity of circulating glucose recycled. Recently, per-labeled glucose ([U-13C6]glucose) has been used to estimate glucose appearance rate and glucose isotope recycling. Chemical structural information determined by mass isotopomer analysis has been used to correct for dilution of isotope through the TCA cycle. In this report, we present experiments in the study of glucose turnover and recycling using [U-13C6]glucose. Methods of single injection and continuous infusion of [U-13C6]glucose are compared. A formula for the calculation of a dilution factor using TCA cycle parameters is derived. In this study of six rabbits, glucose turnover rate ranged from 3.4 to 8.8 mg/kg/min, and glucose m + 3 mass isotopomer recycling from 7 to 12%. The rate of pyruvate carboxylation (Y) was comparable to that of citrate synthetase, having an average relative flux of 0.89. Applying the correction factor for tracer dilution to the observed mass isotopomer recycling, we determined glucose carbon recycling (or Cori cycle activity) to be 22-35% of hepatic glucose output.

摘要

使用¹⁴C或¹³C葡萄糖示踪剂对葡萄糖碳循环进行的实验测定,常常会低估真正的科里循环活性,这是因为同位素示踪剂会通过三羧酸(TCA)循环发生稀释和交换。因此,术语“葡萄糖同位素循环”用于区分同位素的循环与葡萄糖碳的循环,即循环利用的循环葡萄糖的实际量。最近,全标记葡萄糖([U-¹³C₆]葡萄糖)已被用于估计葡萄糖出现率和葡萄糖同位素循环。通过质量同位素异构体分析确定的化学结构信息已用于校正通过TCA循环的同位素稀释。在本报告中,我们展示了使用[U-¹³C₆]葡萄糖研究葡萄糖周转和循环的实验。比较了单次注射和连续输注[U-¹³C₆]葡萄糖的方法。推导了一个使用TCA循环参数计算稀释因子的公式。在这项对六只兔子的研究中,葡萄糖周转率在3.4至8.8mg/kg/min之间,葡萄糖m + 3质量同位素异构体循环率在7%至12%之间。丙酮酸羧化率(Y)与柠檬酸合酶的羧化率相当,平均相对通量为0.89。将示踪剂稀释的校正因子应用于观察到的质量同位素异构体循环,我们确定葡萄糖碳循环(或科里循环活性)为肝脏葡萄糖输出的22 - 35%。

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