四环素类抗生素色谱信号分离实验数据的数学建模处理

A. Mukharlyamova, Biological Safety, A. M. Saifutdinov, E. Rakhmetova, A. G. Mukhammetshina, A. Z. Gaynullin, A. Likhacheva, I. Fitsev
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引用次数: 0

摘要

磺胺类抗生素、霉素类抗生素和四环素类抗生素,如四环素、土霉素和金四素,用于控制蜜蜂的传染病。此外,四环素类抗生素可以在植物开花期间直接添加到植物中。高浓度的抗生素污染了花,就有可能把抗生素残留转移到蜂蜜中。因此,这些抗生素作为污染物持续存在于蜂蜜中,蜂蜜样品中这些药物的测定具有重要意义。四环素对革兰氏阳性和革兰氏阴性细菌具有广谱活性。四环素的基本结构是由含有四个环的氢化萘骨架组成的。由于其可能的毒性或过敏反应以及病原体可能对这些药物产生耐药性,四环素类药物最近受到了广泛关注。对于食品中抗生素残留量的检测,越来越需要可靠的分析方法。目前测定四环素类抗生素的主要方法是高效液相色谱法,但由于其残留浓度极小,色谱条件不理想,可能出现峰重叠,制样条件不完善,可能出现基质成分重叠,使得该方法在定量计算时存在困难。本文介绍了一种利用数学模型计算强度和峰宽初始值的方法。通过对实际色谱数据的分析,证明了该方法在四环素类抗生素定量分析中的适用性。
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Processing of experimental data for the separation of chromatographic signals of tetracycline group antibiotics by mathematical modeling
Antibiotics belonging to the classes of sulfonamides, amphenicols and tetracyclines, such as tetracycline, oxytetracycline and chlortetracycline, are used to control infectious diseases of honeybees. In addition, tetracycline group antibiotics can be added directly to plants during flowering. Contamination of the flower with high concentrations of antibiotics entails the risk of transferring antibiotic residues to honey. Consequently, these antibiotics persist as contaminants in honey, and the determination of these drugs in honey samples is of great importance. Tetracyclines have a broad spectrum of activity against gram-positive and gram-negative bacteria. The basic structure of tetracyclines consists of a hydro-naphthacene framework containing four rings. Due to their possible toxic or allergic reactions and the possibility that pathogens may become resistant to these drugs, much attention has recently been paid to tetracyclines. For the detection of residual quantities of antibiotics in food products increasingly requires reliable analytical methods. The main method for determining tetracycline group antibiotics is the method of high-performance liquid chromatography, but the micro-quantities of their residual concentration and unsatisfactory chromatographic conditions, under which peaks may overlap, as well as insufficient sample preparation conditions, under which matrix components may overlap, make quantitative calculations difficult when using this method. This article describes a method for calculating the initial value of intesiveness and peak width using mathematical modeling. Based on the analysis of real chromatographic data, the applicability of this method for the quantitative determination of tetracycline group antibiotics is shown.
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