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基于药代动力学研究的基因药物递送系统的开发。

Development of gene drug delivery systems based on pharmacokinetic studies.

作者信息

Takakura Y, Nishikawa M, Yamashita F, Hashida M

机构信息

Department of Drug Metabolism, Graduate School of Pharmaceutical Sciences, Kyoto University, Sakyo-ku, 606-8501, Kyoto, Japan.

出版信息

Eur J Pharm Sci. 2001 Apr;13(1):71-6. doi: 10.1016/s0928-0987(00)00209-8.

Abstract

A series of pharmacokinetic studies following systemic or local administration for the development of delivery systems for gene drugs, such as plasmid DNA and oligonucleotides, are reviewed. The pharmacokinetics of gene drugs after intravenous injection into mice was evaluated based on clearance concepts. Pharmacokinetic analysis revealed that the overall disposition characteristics of the gene drug itself were determined by the physicochemical properties of its polyanionic DNA. Based on these findings, liver cell-specific carrier systems via receptor-mediated endocytosis were successfully developed by optimizing physicochemical characteristics. On the other hand, the pharmacokinetics of gene drugs after intratumoral injection were assessed in a tissue-isolated tumor perfusion system. The relationship between the physicochemical properties of gene drug delivery systems and intratumoral pharmacokinetics was determined and the therapeutic effect was also discussed in relation to pharmacokinetics. Collectively, it was demonstrated that a rational design of gene drug delivery systems that can control their in vivo disposition is possible by means of pharmacokinetic studies at whole body, organ and cellular levels.

摘要

本文综述了一系列用于基因药物(如质粒DNA和寡核苷酸)递送系统开发的全身或局部给药后的药代动力学研究。基于清除率概念评估了基因药物静脉注射到小鼠体内后的药代动力学。药代动力学分析表明,基因药物本身的整体处置特征由其聚阴离子DNA的物理化学性质决定。基于这些发现,通过优化物理化学特性成功开发了通过受体介导的内吞作用的肝细胞特异性载体系统。另一方面,在组织分离的肿瘤灌注系统中评估了瘤内注射后基因药物的药代动力学。确定了基因药物递送系统的物理化学性质与瘤内药代动力学之间的关系,并结合药代动力学讨论了治疗效果。总体而言,通过在全身、器官和细胞水平上进行药代动力学研究,证明了合理设计能够控制其体内处置的基因药物递送系统是可行的。

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