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作为潜在抗疟化合物的合成与天然植物毒性化合物及植物抗毒素调查。

A survey of synthetic and natural phytotoxic compounds and phytoalexins as potential antimalarial compounds.

作者信息

Bajsa Joanna, Singh Kshipra, Nanayakkara Dhammika, Duke Stephen Oscar, Rimando Agnes Mamaril, Evidente Antonio, Tekwani Babu Lal

机构信息

National Center for Natural Products Research, School of Pharmacy, University of Mississippi, MS 38677, U.S.A.

出版信息

Biol Pharm Bull. 2007 Sep;30(9):1740-4. doi: 10.1248/bpb.30.1740.

DOI:10.1248/bpb.30.1740
PMID:17827731
Abstract

The apicomplexan parasites pathogens such as Plasmodium spp. possess an apicoplast, a plastid organelle similar to those of plants. The apicoplast has some essential plant-like metabolic pathways and processes, making these parasites susceptible to inhibitors of these functions. The main objective of this paper is to determine if phytotoxins with plastid target sites are more likely to be good antiplasmodial compounds than are those with other modes of action. The antiplasmodial activities of some compounds with established phytotoxic action were determined in vitro on a chloroquine (CQ) sensitive (D6, Sierra Leone) strain of Plasmodium falciparum. In this study, we provide in vitro activities of almost 50 such compounds, as well as a few phytoalexins against P. falciparum. Endothall, anisomycin, and cerulenin had sufficient antiplasmodial action to be considered as new lead antimalarial structures. Some derivatives of fusicoccin possessed markedly improved antiplasmodial action than the parent compound. Our results suggest that phytotoxins with plastid targets may not necessarily be better antiplasmodials than those that act at other molecular sites. The herbicides, phytotoxins and the phytoalexins reported here with significant antiplasmodial activity may be useful probes for identification of new antimalarial drug targets and may also be used as new lead structures for new antiplasmodial drug discovery.

摘要

顶复门寄生虫病原体,如疟原虫属,拥有一个顶质体,这是一种类似于植物的质体细胞器。顶质体具有一些基本的类似植物的代谢途径和过程,使得这些寄生虫易受针对这些功能的抑制剂的影响。本文的主要目的是确定与具有其他作用模式的毒素相比,作用于质体靶点的植物毒素是否更有可能成为良好的抗疟化合物。在体外对氯喹(CQ)敏感的恶性疟原虫(塞拉利昂D6株)测定了一些具有既定植物毒性作用的化合物的抗疟活性。在本研究中,我们提供了近50种此类化合物以及几种植物抗毒素对恶性疟原虫的体外活性。烯草酮、茴香霉素和浅蓝菌素具有足够的抗疟作用,可被视为新的抗疟先导结构。藤霉素的一些衍生物比母体化合物具有明显改善的抗疟作用。我们的结果表明,作用于质体靶点的植物毒素不一定比作用于其他分子位点的毒素更具抗疟活性。本文报道的具有显著抗疟活性的除草剂、植物毒素和植物抗毒素可能是鉴定新的抗疟药物靶点的有用探针,也可作为发现新的抗疟药物的新先导结构。

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