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阿莫地喹及其主要代谢产物去乙基阿莫地喹与青蒿素、奎宁和阿托伐醌在体外恶性疟原虫中的药效学相互作用。

Pharmacodynamic interactions of amodiaquine and its major metabolite desethylamodiaquine with artemisinin, quinine and atovaquone in Plasmodium falciparum in vitro.

作者信息

Mariga S T, Gil J P, Wernsdorfer W H, Björkman A

机构信息

Department of Infectious Diseases, Malaria Research Laboratory, M9, Karolinska Hospital, Stockholm 17176, Sweden.

出版信息

Acta Trop. 2005 Mar;93(3):221-31. doi: 10.1016/j.actatropica.2005.01.007.

Abstract

The antimalarial in vitro activities of amodiaquine and desethylamodiaquine in combination with atovaquone, quinine and artemisinin against Plasmodium falciparum were investigated in strains F-32, FCR-3 and K-1. These parasitic strains have different sensitivity profiles to the standard antimalarial chloroquine, but all can be considered sensitive to the test drugs, representing the recommended situation for introduction of two partner drugs in combination therapy. Amodiaquine showed marked synergism when combined with each of the three partner compounds at concentration ratios between 90 and 9x10(-7), including the therapeutically relevant range. The interaction profiles of desethylamodiaquine with quinine and artemisinin also showed predominantly synergism over a wide range of concentration ratios between 70 and 9x10(-7). The responses to all combinations exhibited signs of strain-specificity, but such phenomena were usually observed outside the therapeutic range of the concentration ratios. Synergism was generally more marked with increasing EC values, i.e. at concentrations expected to be therapeutically effective and thus clinically relevant. Even trace quantities of amodiaquine were able to potentiate the activity of structurally unrelated antimalarial drugs.

摘要

在F-32、FCR-3和K-1菌株中,研究了阿莫地喹和去乙基阿莫地喹分别与阿托伐醌、奎宁和青蒿素联合对恶性疟原虫的体外抗疟活性。这些寄生虫菌株对标准抗疟药氯喹有不同的敏感性,但对测试药物均敏感,代表了联合治疗中引入两种联合用药的推荐情况。当阿莫地喹与三种联合化合物中的每一种以90至9×10⁻⁷的浓度比联合时,包括治疗相关范围,均表现出显著的协同作用。去乙基阿莫地喹与奎宁和青蒿素的相互作用曲线在70至9×10⁻⁷ 的广泛浓度比范围内也主要表现为协同作用。对所有联合用药的反应均表现出菌株特异性迹象,但此类现象通常在浓度比的治疗范围之外观察到。一般来说,随着EC值增加,即预期具有治疗效果且因此具有临床相关性的浓度下,协同作用更为显著。即使是痕量的阿莫地喹也能够增强结构不相关的抗疟药物的活性。

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