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首页> 外文期刊>European journal of mass spectrometry >Ion mobility-mass spectrometry analysis of diarylquinoline diastereomers: Drugs used for tuberculosis treatment
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Ion mobility-mass spectrometry analysis of diarylquinoline diastereomers: Drugs used for tuberculosis treatment

机译:二芳基喹啉非对映异构体的离子迁移率 - 质谱分析:用于结核治疗的药物

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摘要

Mycobacterium tuberculosis infection results in more than two million deaths per year and is the leading cause of mortality in people infected with HIV. A new structural class of antimycobacterials, the diarylquinolines, has been synthesized and is being highly effective against both M. tuberculosis and multidrug-resistant tuberculosis. As diarylquinolines are biologically active only under their (R,S) stereoisomeric form, it is essential to differentiate the stereoisomers (R,S) and (R,R). To achieve this, tandem mass spectrometry and ion mobility spectrometry-mass spectrometry have been performed with 10 diarylquinoline diastereomers couples. In this study, we investigated cationization with alkali metal cations and several ion mobility drift gases in order to obtain diastereomer differentiations. We have shown that diastereomers of the diarylquinolines family can be differentiated separately by tandem mass spectrometry and in mixture by ion mobility spectrometry-mass spectrometry. However, although the structure of each diastereomer is close, several behaviors could be observed concerning the cationization and the ion mobility spectrometry separation. The ion mobility spectrometry isomer separation efficiency is not easily predictable; it was however observed for all diastereomeric couples with a significant improvement of separation using alkali adducts compared to protonated molecules. With the use of drift gas with higher polarizability only an improvement of separation was obtained in a few cases. Finally, a good correlation of the experimental collision cross section (relative to three-dimensional structure of ions) and the theoretical collision cross section has been shown.
机译:分枝杆菌结核病感染导致每年超过200万人死亡,是感染艾滋病毒的人民死亡的主要原因。已经合成了一种新的抗细菌,二芳基喹啉的抗细菌性,并且对肺部结核和多药抗性结核的高度有效。作为二芳基喹啉仅在其(R,S)立体异构形式下方是生物活性的,因此必须区分立体异构体(R,S)和(R,R)。为了实现这一点,已经用10个二芳基喹啉代氨酸耦合进行了串联质谱和离子迁移谱图质谱法。在这项研究中,我们研究了碱金属阳离子和几种离子迁移率漂移气体的阳离子化,以获得非对映异构体的分化。我们已经表明,二芳基喹啉家族的非对映异构体可以通过串联质谱和通过离子迁移光谱 - 质谱法以混合物分别分别进行分别分别分开。然而,尽管每个非对映异构体的结构接近,但是关于阳离子化和离子迁移光谱分离可以观察到若干行为。离子迁移光谱法异构体分离效率不易预测;然而,与质子化分子相比,使用碱性加合物具有显着改善的所有非对映异构型伴侣观察到。通过使用较高极化性的漂移气体,在少数情况下仅获得分离的改善。最后,已经示出了实验碰撞横截面(相对于离子的三维结构)和理论碰撞横截面的良好相关性。

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