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立体动态研究青蒿琥酯中不稳定的手性中心。

Stereodynamic investigation of labile stereogenic centres in dihydroartemisinin.

机构信息

Dipartimento di Chimica e Tecnologie del Farmaco, Sapienza Università di Roma, P. le Aldo Moro 5, 00185 Roma, Italy.

出版信息

Molecules. 2010 Mar 5;15(3):1309-23. doi: 10.3390/molecules15031309.

Abstract

Since its identification in the early 1970s, artemisinin, as well as semi-synthetic derivatives and synthetic trioxanes, have been used in malaria therapy. Reduction of artemisinin by NaBH4 produced dihydroartemisinin (DHA), and yielded a new stereochemically labile centre at C-10, which, in turn, provided two interconverting lactol hemiacetal epimers (namely alpha and beta), whose rate of interconversion depends on buffer, pH, and solvent polarity. Since interconversion of the two epimers occurred on a chromatographic time-scale, this prompted a thorough investigation of the phenomenon as a crucial requisite of any analytical method aimed at quantitating this family of drugs. In this critical review we discuss the current importance of the on-column epimerization of DHA in the development of analytical methods aimed at quantifying the drug, with the purpose of identifying the optimal conditions to minimize on-column epimerization while achieving the best selectivity and efficiency of the overall separation.

摘要

自 20 世纪 70 年代初发现青蒿素以来,青蒿素及其半合成衍生物和合成三氧杂环己烷已被用于疟疾治疗。NaBH4 将青蒿素还原生成二氢青蒿素(DHA),并在 C-10 处产生了一个新的立体化学不稳定中心,进而提供了两个可互变的内酯半缩醛差向异构体(即α和β),它们的互变异构平衡速率取决于缓冲液、pH 值和溶剂极性。由于两个差向异构体在色谱时间尺度上发生互变,因此,这促使人们对这一现象进行了深入研究,认为这是任何旨在定量分析这类药物的分析方法的关键要求。在这篇评论中,我们讨论了 DHA 在柱上差向异构化在开发旨在定量分析药物的分析方法中的当前重要性,目的是确定最佳条件以最小化柱上差向异构化,同时实现整体分离的最佳选择性和效率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7f5b/6257325/97f020794f4c/molecules-15-01309-g001.jpg

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