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青蒿琥酯和三氧喹DU1301(两种抗疟三恶烷)对血红素的烷基化作用

Heme alkylation by artesunic acid and trioxaquine DU1301, two antimalarial trioxanes.

作者信息

Laurent Sophie A-L, Loup Christophe, Mourgues Sophie, Robert Anne, Meunier Bernard

机构信息

Laboratoire de Chimie de Coordination du CNRS, 205 route de Narbonne, 31077 Toulouse Cedex 4, France.

出版信息

Chembiochem. 2005 Apr;6(4):653-8. doi: 10.1002/cbic.200400249.

Abstract

The sesquiterpene Artemisinin, an antimalarial drug that is effective against multidrug-resistant Plasmodium falciparum strains, contains a 1,2,4-trioxane, and the endoperoxide function plays a key role in its biological activity. However, its poor solubility means that hemisynthetic derivatives, such as artesunic acid, are preferred for drugs. The reductive activation of the peroxide function of artemisinin by iron(II)-heme produces heme derivatives that are alkylated at meso positions by a C-centered radical derived from artemisinin. We checked if the alkylating ability of trioxane-based drugs toward heme, which might be related to its parasiticidal activity, is a general feature by comparing the chemical reactivity toward heme of the clinically relevant derivative artesunic acid and DU1301, a drug of the trioxaquine family, that is active against P. falciparum. Both artesunic acid and trioxaquine DU1301 efficiently alkylated the heme macrocycle after activation of their peroxide function by the iron(II) of heme itself and thus gave rise to covalently coupled heme-drug products. This heme-drug adduct formation might be related to the high antimalarial activity of DU1301.

摘要

倍半萜青蒿素是一种抗疟药物,对多重耐药恶性疟原虫菌株有效,它含有一个1,2,4 - 三氧杂环己烷,内过氧化物官能团在其生物活性中起关键作用。然而,其溶解度差意味着半合成衍生物,如青蒿琥酯,更适合用作药物。青蒿素的过氧化物官能团被亚铁血红素还原激活后会产生血红素衍生物,这些衍生物会被青蒿素衍生的碳中心自由基在中位烷基化。我们通过比较临床相关衍生物青蒿琥酯和对恶性疟原虫有活性的三氧喹啉家族药物DU1301对血红素的化学反应性,来检验基于三氧杂环己烷的药物对血红素的烷基化能力(这可能与其杀寄生虫活性有关)是否是一个普遍特征。青蒿琥酯和三氧喹啉DU1301在被血红素自身的亚铁离子激活其过氧化物官能团后,都能有效地使血红素大环烷基化,从而产生共价偶联的血红素 - 药物产物。这种血红素 - 药物加合物的形成可能与DU1301的高抗疟活性有关。

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