■ Mathematical treatment of chemiluminescence data allowing an optimised kinetic analysis of vascular NAD(P)H-dependent superoxide anion production

J. Iliou, N. Villeneuve, M. Fournet-Bourguignon, F. Robin, C. Jacquemin, V. Lestriez, C. Petit, A. Pillon, J. Vilaine
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引用次数: 3

Abstract

Regulation of vascular redox homeostasis plays a central role in the control of vascular tone (e.g.: redox modulation of endothelial NO synthase and soluble guanylate cyclase activities). Superoxide anion is one of the main reactive oxygen species involved in the modulation of the redox status of the vessel. It is crucial to know if pathological situations or drug treatments are able to modify NAD(P)H oxidase-dependent production of O 2 - . As a steady-state approach is the only way for a valid assessment of these parameters, a mathematical treatment allowing visualisation of the linear portion of the initial velocity of O 2 - production was developed. Using two vascular preparations (rat aortic rings and mouse thoracic aortae), the chemiluminescence (CL) in the presence of lucigenin was recorded every second in the 15-30 minute period after successive injections of NADPH and superoxide dismutase (SOD). Because, both O 2 - and photons are labile and evanescent products, visualisation of the steady-state requires calculation of their cumulative production by integral calculus using a first order integral equation. The cumulative production of CL and/or O 2 - was plotted as a function of the NADPH concentrations, were determined from the linear portion of these plots. For a precise molar quantification of O 2 - production, a calibration curve of initial velocities using xanthine oxidase + xanthine as a source of O 2 - was plotted by comparing CL and cytochrome C reduction. The NADPH-dependent CL production exihibited Michaelian behavior and SOD acted as a noncompetitive inhibitor. For example, the values for NADPH oxidase in rat aorta were: Km = 237 ± 2μM; Vmax = 500-600 pmol O 2 - /min/ring.
■化学发光数据的数学处理,可以优化血管NAD(P) h依赖性超氧阴离子产生的动力学分析
血管氧化还原稳态的调节在血管张力的控制中起着核心作用(例如:内皮NO合成酶和可溶性鸟苷酸环化酶活性的氧化还原调节)。超氧阴离子是参与调节血管氧化还原状态的主要活性氧之一。了解病理情况或药物治疗是否能够改变NAD(P)H氧化酶依赖性o2 -的产生是至关重要的。由于稳态方法是有效评估这些参数的唯一方法,因此开发了一种数学处理方法,可以将o2生产初速度的线性部分可视化。采用两种血管制剂(大鼠主动脉环和小鼠胸主动脉),连续注射NADPH和超氧化物歧化酶(SOD)后,在15 ~ 30分钟内每秒钟记录lucigenin存在下的化学发光(CL)。因为o2和光子都是不稳定的、易逝的产物,所以要想可视化稳态,就需要用一阶积分方程通过积分计算它们的累积产量。CL和/或o2 -的累积产量被绘制为NADPH浓度的函数,由这些图的线性部分确定。通过比较CL和细胞色素C还原量,绘制了以黄嘌呤氧化酶+黄嘌呤为o2 -源的初始速度标定曲线。nadph依赖性CL的产生表现出Michaelian行为,SOD作为非竞争性抑制剂。例如,大鼠主动脉内NADPH氧化酶值为:Km = 237±2μM;Vmax = 500-600 pmol o2 - /min/环。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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