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Activity of purine analogs against Leishmania tropica within human macrophages in vitro.

机译:嘌呤类似物在人类巨噬细胞中对热带利什曼原虫的活性。

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摘要

The activity of purine analogs against Leishmania tropica in human monocyte-derived macrophages in vitro was determined. Formycin B, formycin A, formycin B and A monophosphate, and formycin A triphosphate all had 50% effective doses of 0.02 to 0.04 microM and eliminated 90% of organisms at less than or equal to 0.5 microM. Allopurinol ribonucleoside was much less active: the 50% effective dose was 76 to 190 microM, and 90% of organisms were not eliminated at the highest dose tested (190 microM). 7-Deazainosine had a low 50% effective dose (0.2 microM), but only 80% of organisms were eliminated at 4 microM. Thio derivatives were as active as or less active than the parent compounds. These data suggest that certain inosine analogs are much more active than others against macrophage-contained Leishmania spp. such as are found in human lesions. However, because toxicity to the human macrophage hosts generally paralleled antileishmanial activity, the more active compounds might also be more toxic to human cells. The activity of 3-deazaguanosine (50% effective dose, 3.6 microM) in this model suggests that guanosine derivatives may have potential as antileishmanial agents.
机译:测定了嘌呤类似物在人单核细胞衍生的巨噬细胞中对热带利什曼原虫的活性。甲霉素B,甲霉素A,甲霉素B和A的单磷酸酯和甲霉素A三磷酸酯均具有0.02至0.04 microM的50%有效剂量,并消除了小于或等于0.5 microM的90%的生物。别嘌呤醇核糖核苷的活性要低得多:50%的有效剂量为76至190 microM,在最高测试剂量(190 microM)下没有消除90%的生物。 7-脱氮芥子碱的有效剂量低至50%(0.2 microM),但在4 microM时仅消灭了80%的生物。硫代衍生物的活性与母体化合物相同或更低。这些数据表明,某些肌苷类似物对包含巨噬细胞的利什曼原虫(Leishmania spp)具有比其他肌苷类似的活性。如在人类病变中发现的。但是,由于对人类巨噬细胞宿主的毒性通常与抗噬菌体活性平行,因此活性较高的化合物对人类细胞的毒性也可能更大。在该模型中,3-脱氮鸟嘌呤核苷的活性(50%有效剂量,3.6 microM)表明鸟嘌呤衍生物可能具有作为抗疟药的潜力。

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