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首页> 外文期刊>Journal of Medicinal Chemistry >Second generation analogues of the cancer drug clinical candidate tipifarnib for anti-chagas disease drug discovery
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Second generation analogues of the cancer drug clinical candidate tipifarnib for anti-chagas disease drug discovery

机译:用于抗chagas病药物发现的癌症药物临床候选药物替比法尼的第二代类似物

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摘要

We previously reported that the cancer drug clinical candidate tipifarnib kills the causative agent of Chagas disease, Trypanosoma cruzi, by blocking ergosterol biosynthesis at the level of inhibition of lanosterol 14α-demethylase. Tipifarnib is an inhibitor of human protein farnesyltransferase. We synthesized tipifarnib analogues that no longer bind to protein farnesyltransferase and display increased potency for killing parasites. This was achieved in a structure-guided fashion by changing the substituents attached to the phenyl group at the 4-position of the quinoline ring of tipifarnib and by replacing the amino group by OMe. Several compounds that kill Trypanosoma cruzi at subnanomolar concentrations and are devoid of protein farnesyltransferase inhibition were discovered. The compounds are shown to be advantageous over other lanosterol 14α-demethylase inhibitors in that they show only modest potency for inhibition of human cytochrome P450 (3A4). Since tipifarnib displays high oral bioavailability and acceptable pharmacokinetic properties, the newly discovered tipifarnib analogues are ideal leads for the development of drugs to treat Chagas disease.
机译:我们之前曾报道过,该癌症药物临床候选者Tipifarnib通过在抑制羊毛甾醇14α-脱甲基酶的水平上阻断麦角固醇的生物合成,从而杀死了南美锥虫病,即克鲁斯锥虫。 Tipifarnib是人蛋白法尼基转移酶的抑制剂。我们合成了不再与蛋白质法呢基转移酶结合并显示出增加的杀灭寄生虫效力的替非法尼类似物。这是通过改变在蒂法法尼的喹啉环的4-位上与苯基相连的取代基并通过用OMe取代氨基而以结构指导的方式实现的。发现了几种可杀死亚纳摩尔浓度的克氏锥虫且无蛋白法尼基转移酶抑制作用的化合物。该化合物显示出优于其他羊毛甾醇14α-脱甲基酶抑制剂的优势,因为它们仅显示出适度的抑制人细胞色素P450(3A4)的能力。由于替非法尼具有很高的口服生物利用度和可接受的药代动力学特性,因此新发现的替非法尼类似物是开发治疗南美锥虫病药物的理想线索。

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