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首页> 外文期刊>The Journal of toxicological sciences >Association of pharmacokinetic profiles of lenalidomide in human plasma simulated using pharmacokinetic data in humanized-liver mice with liver toxicity detected by human serum albumin RNA
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Association of pharmacokinetic profiles of lenalidomide in human plasma simulated using pharmacokinetic data in humanized-liver mice with liver toxicity detected by human serum albumin RNA

机译:使用人源化肝小鼠药代动力学数据模拟来那度胺在人血浆中的药代动力学谱与人血清白蛋白RNA检测到的肝毒性的关联

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Lenalidomide has been shown to be potentially teratogenic in thalidomide-sensitive animal species. Screening for thalidomide analogs devoid of teratogenicity/toxicity—attributable to drug metabolism and disposition, but having immunomodulatory properties—is a strategic pathway towards development of new anticancer drugs. Plasma concentrations of lenalidomide were investigated in immunodeficient control and humanized-liver mice following oral administration of lenalidomide (50 mg/kg). Plasma concentrations of lenalidomide (1-2 hr after administration) were slightly but significantly higher in humanized-liver mice than in control mice ( p
机译:在对沙利度胺敏感的动物物种中,来那度胺被证明具有潜在的致畸性。筛选没有致畸/毒性(可归因于药物代谢和处置,但具有免疫调节特性)的沙利度胺类似物是开发新的抗癌药物的战略途径。口服来那度胺(50 mg / kg)后,在免疫缺陷对照和人源化肝小鼠中研究了来那度胺的血浆浓度。人源化肝小鼠中来那度胺的血浆浓度(给药后1-2小时)比对照小鼠略高,但明显更高(p

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