首页> 美国卫生研究院文献>Antimicrobial Agents and Chemotherapy >Comparative pharmacokinetics distributions in tissue and interactions with blood proteins of conventional and sterically stabilized liposomes containing 23-dideoxyinosine.
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Comparative pharmacokinetics distributions in tissue and interactions with blood proteins of conventional and sterically stabilized liposomes containing 23-dideoxyinosine.

机译:比较药代动力学组织中的分布以及与含有23-双脱氧肌苷的常规和空间稳定脂质体的血蛋白相互作用。

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摘要

The pharmacokinetics and distribution in tissue of 2',3'-dideoxyinosine (ddI) encapsulated in sterically stabilized liposomes have been evaluated in rats. Most of the sterically stabilized liposomes concentrated in the spleen with a peak level at 24 h after their intravenous injection. An extended half-life in plasma was observed for sterically stabilized liposomes (14.5 h) compared with that of conventional liposomes (3.9 h). The systemic clearance of ddI incorporated in sterically stabilized liposomes was 180 times lower than that of the free drug. The levels of in vitro and in vivo protein binding on both conventional and sterically stabilized liposomes were also evaluated. Results suggest that the amount of proteins associated with liposomes might not be the only factor involved in the in vivo clearance of liposomes, as this process may also be influenced by the nature of the bound blood proteins.
机译:已经在大鼠中评估了封装在空间稳定脂质体中的2',3'-双脱氧肌苷(ddI)的药代动力学和在组织中的分布。大部分空间稳定的脂质体在静脉注射后24 h集中在脾脏中,并达到峰值。与传统脂质体(3.9小时)相比,空间稳定脂质体(14.5小时)的血浆半衰期延长。掺入到空间稳定脂质体中的ddI的全身清除率比游离药物低180倍。还评估了常规和空间稳定脂质体上体外和体内蛋白质结合的水平。结果表明,与脂质体相关的蛋白质数量可能不是参与脂质体体内清除的唯一因素,因为该过程也可能受结合的血液蛋白质性质的影响。

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