首页> 外文期刊>Mass Spectrometry Letters >Characterization of Preclinical in Vitro and in Vivo Pharmacokinetic Properties of KPLA-012, a Benzopyranyl 1,2,3-Triazole Compound, with Anti-Angiogenetic and Anti-Tumor Progressive Effects
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Characterization of Preclinical in Vitro and in Vivo Pharmacokinetic Properties of KPLA-012, a Benzopyranyl 1,2,3-Triazole Compound, with Anti-Angiogenetic and Anti-Tumor Progressive Effects

机译:临床前和体内药代动力学特性KPLA-012,一种苯并吡喃基1,2,3-三唑化合物具有抗血管生成和抗肿瘤进展的作用

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KPLA-012, a benzopyranyl 1,2,3-triazole compound, is considered a potent inhibitor based on the chemical library screening, and is known to exhibit anti-angiogenetic and anti-tumor progressive effects. The aim of this study was to investigate the pharmacokinetic properties of KPLA-012 in ICR mice and to investigate in vitro characteristics including the intestinal absorption, distribution, metabolism, and excretion of KPLA-012. The oral bioavailability of KPLA-012 was 33.3% in mice. The pharmacokinetics of KPLA-012 changed in a metabolism-dependent manner, which was evident by the low recovery of parent KPLA-012 from urine and feces and metabolic instability in the liver microsomes. However, KPLA-012 exhibited moderate permeability in Caco-2 cells ( ) and the metabolic stability increased in humans compared to that in mice (% remaining after 1 h; 47.4% in humans vs 14.8% in mice). Overall, the results suggest that KPLA-012 might have more effective pharmacokinetic properties in humans than in mice although further studies on its metabolism are necessary.
机译:基于化学文库筛选,苯并吡喃基1,2,3-三唑化合物KPLA-012被认为是有效的抑制剂,并且已知具有抗血管生成和抗肿瘤的进行性作用。这项研究的目的是研究KPLA-012在ICR小鼠中的药代动力学特性,并研究KPLA-012在体外的特性,包括肠道吸收,分布,代谢和排泄。 KPLA-012在小鼠中的口服生物利用度为33.3%。 KPLA-012的药代动力学以代谢依赖的方式发生变化,这可以通过尿液和粪便中母体KPLA-012的回收率低以及肝微粒体的代谢不稳定来证明。然而,与小鼠相比,KPLA-012在Caco-2细胞中表现出适度的通透性,并且人体内的代谢稳定性有所提高(1小时后保留的百分比;人47.4%,小鼠14.8%)。总体而言,结果表明,KPLA-012在人体内可能比在小鼠中具有更有效的药代动力学特性,尽管有必要对其代谢进行进一步研究。

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