Metallocene antimalarials: the continuing quest.

Margaret A L Blackie, Kelly Chibale
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引用次数: 18

Abstract

Over the last decade, a significant body of research has been developed around the inclusion of a metallocene moiety into known antimalarial compounds. Ferroquine is the most successful of these compounds. Herein, we describe our contribution to metallocene antimalarials. Our approach has sought to introduce diversity sites in the side chain of ferroquine in order to develop a series of ferroquine derivatives. The replacement of the ferrocenyl moiety with ruthenocene has given rise to ruthenoquine and a modest series of analogues. The reaction of ferroquine and selected analogues with Au(PPh3)NO3, Au(C6F5)(tht), and [Rh(COD)Cl2] has resulted in a series of heterobimetallic derivatives. In all cases, compounds have been evaluated for in vitro antiplasmodial activity in both chloroquine-sensitive and chloroquine-resistant strains of Plasmodium falciparum. Preliminary structure-activity relationships have been delineated.

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茂金属抗疟药:持续探索。
在过去十年中,围绕在已知抗疟疾化合物中包含茂金属部分展开了大量研究。亚铁喹是这些化合物中最成功的。在此,我们描述了我们对茂金属抗疟药的贡献。我们的方法是试图在亚铁喹的侧链中引入多样性位点,以开发一系列亚铁喹衍生物。二茂铁部分被钌烯二世取代,产生了钌烯醌和一系列适度的类似物。铁喹及其选定的类似物与Au(PPh3)NO3、Au(C6F5)(tht)和[Rh(COD)Cl2]反应生成了一系列的杂双金属衍生物。在所有情况下,化合物都被评估了对氯喹敏感和耐氯喹的恶性疟原虫菌株的体外抗疟原虫活性。初步描述了构效关系。
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