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首页> 外文期刊>Bioorganic and Medicinal Chemistry Letters >Kinesin spindle protein (KSP) inhibitors. Part V: discovery of 2-propylamino-2,4-diaryl-2,5-dihydropyrroles as potent, water-soluble KSP inhibitors, and modulation of their basicity by beta-fluorination to overcome cellular efflux by P-glycoprotein.
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Kinesin spindle protein (KSP) inhibitors. Part V: discovery of 2-propylamino-2,4-diaryl-2,5-dihydropyrroles as potent, water-soluble KSP inhibitors, and modulation of their basicity by beta-fluorination to overcome cellular efflux by P-glycoprotein.

机译:驱动蛋白纺锤体蛋白(KSP)抑制剂。第五部分:发现2-丙基氨基-2,4-二芳基-2,5-二氢吡咯为有效的水溶性KSP抑制剂,并通过β氟化作用调节其碱性以克服P-糖蛋白的细胞外排作用。

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摘要

Installation of a C2-aminopropyl side chain to the 2,4-diaryl-2,5-dihydropyrrole series of kinesin spindle protein (KSP) inhibitors results in potent, water soluble compounds, but the aminopropyl group induces susceptibility to cellular efflux by P-glycoprotein (Pgp). We show that by carefully modulating the basicity of the amino group by beta-fluorination, this series of inhibitors maintains potency against KSP and has greatly improved efficacy in a Pgp-overexpressing cell line. The discovery that cellular efflux by Pgp can be overcome by carefully modulating the basicity of an amine may be of general use to medicinal chemists attempting to transform leading compounds into cancer cell- or CNS-penetrant drugs.
机译:在驱动蛋白纺锤体蛋白(KSP)抑制剂的2,4-二芳基-2,5-二氢吡咯系列上安装C2-氨基丙基侧链可产生强效的水溶性化合物,但氨基丙基可诱导P-对细胞外排的敏感性糖蛋白(Pgp)。我们显示通过通过β-氟化仔细调节氨基的碱性,该系列抑制剂可维持针对KSP的效力,并大大提高了Pgp过表达细胞系的功效。通过小心地调节胺的碱性可以克服Pgp引起的细胞外排的发现,对于试图将主要化合物转化为癌细胞或CNS穿透性药物的药物化学家来说,可能是普遍使用的。

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