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Trypanosoma cruzi: inhibition of alpha-hydroxyacid dehydrogenase isozyme II by N-allyl and N-propyl oxamates and their effects on intact epimastigotes

机译:克氏锥虫:N-烯丙基和N-丙基草酸酯对α-羟酸脱氢酶同工酶II的抑制及其对完整后鞭毛体的影响

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N-allyl (NAOx) and N-propyl (NPOx) oxamates were designed as inhibitors of alpha-hydroxyacid dehydrogenase (HADH) isozyme II from Trypanosoma cruzi. The kinetic studies showed that NAOx and NPOx were competitive inhibitors of HADH-isozyme II (Ki = 72 μM, IC50 = 0.33 mM and 70 μM, IC50 = 0.32 mM, respectively). The attachment of the allylic and propylic chains to nitrogen of the competitive inhibitor oxamate (Ki = 0.91 mM, IC50 = 4.25 mM), increased 12.6 and 13-folds respectively, the affinity for T. cruzi HADH-isozyme II. NAOx and NPOx were selective inhibitors of HADH-isozyme II, because other T. cruzi dehydrogenases were not inhibited by these substances. Since HADH-isozyme II participates in the energy metabolism of T. cruzi, a trypanocidal effect can be expected with these inhibitors. However, we were not able to detect any trypanocidal activity with these oxamates. When the corresponding ethyl esters of N-allyl (Et-NAOx) and N-propyl (Et-NPOx) oxamates were tested as a possible trypanocidal prodrugs, in comparison with nifurtimox and benznidazole, the expected trypanocidal effects were obtained.
机译:N-烯丙基(NAOx)和N-丙基(NPOx)草酸酯被设计为克鲁斯锥虫的α-羟酸脱氢酶(HADH)同工酶II的抑制剂。动力学研究表明,NAOx和NPOx是HADH同工酶II的竞争性抑制剂(Ki = 72μM,IC50 = 0.33 mM和70μM,IC50 = 0.32 mM)。烯丙基和丙基链与竞争性抑制剂草酸盐的氮的连接(Ki = 0.91 mM,IC50 = 4.25 mM)分别增加了12.6和13倍,这与克鲁氏杆菌HADH同工酶II的亲和力有关。 NAOx和NPOx是HADH同工酶II的选择性抑制剂,因为其他克鲁维酵母T. cruzi脱氢酶不受这些物质的抑制。由于HADH-同工酶II参与了克鲁维酵母的能量代谢,因此使用这些抑制剂可以达到锥虫杀灭作用。但是,我们无法使用这些草酸盐检测到任何锥虫杀灭活性。当测试相应的N-烯丙基(Et-NAOx)和N-丙基(Et-NPOx)的草酸酯作为可能的锥虫杀虫剂前药时,与尼呋替莫司和苯并硝唑相比,可获得预期的锥虫杀虫作用。

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