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形成胶束的聚合物-药物缀合物的生物分布

Biodistribution of micelle-forming polymer-drug conjugates.

作者信息

Kwon G S, Yokoyama M, Okano T, Sakurai Y, Kataoka K

机构信息

International Center for Biomaterials Science, Science University of Tokyo, Chiba, Japan.

出版信息

Pharm Res. 1993 Jul;10(7):970-4. doi: 10.1023/a:1018998203127.

Abstract

Polymeric micelles have potential utility as drug carriers. To this end, polymeric micelles based on AB block copolymers of polyethylene oxide (PEO) and poly(aspartic acid) [p(Asp)] with covalently bound Adriamycin (ADR) were prepared. The micelle forming polymer-drug conjugates [PEO-p(Asp(ADR)] were radiolabeled and their biodistribution was investigated after intravenous injection in mice. Long circulation times in blood for some compositions of PEO-p[Asp(ADR)] conjugates were evident, which are usually atypical of colloidal drug carriers. This was attributed to the low interaction of the PEO corona region of the micelles with biocomponents (e.g., proteins, cells). Low uptake of the PEO-p(Asp(ADR)] conjugates in the liver and spleen was determined. The biodistribution of the PEO-p[Asp(ADR)] conjugates was apparently dependent on micelle stability; stable micelles could maintain circulation in blood, while unstable micelles readily formed free polymer chains which rapidly underwent renal excretion. Long circulation times in blood of PEO-p(Asp(ADR)] conjugates are thought to be prerequisite for enhanced uptake at target sites (e.g., tumors).

摘要

聚合物胶束作为药物载体具有潜在应用价值。为此,制备了基于聚环氧乙烷(PEO)和聚天冬氨酸[p(Asp)]的AB嵌段共聚物且共价连接阿霉素(ADR)的聚合物胶束。将形成胶束的聚合物-药物缀合物[PEO-p(Asp(ADR)]进行放射性标记,并在小鼠静脉注射后研究其生物分布。某些组成的PEO-p[Asp(ADR)]缀合物在血液中的循环时间较长,这在胶体药物载体中通常并不典型。这归因于胶束的PEO冠层区域与生物成分(如蛋白质、细胞)的相互作用较低。已测定PEO-p(Asp(ADR)]缀合物在肝脏和脾脏中的摄取量较低。PEO-p[Asp(ADR)]缀合物的生物分布显然取决于胶束稳定性;稳定的胶束可在血液中维持循环,而不稳定的胶束容易形成游离聚合物链,这些链会迅速经肾脏排泄。PEO-p(Asp(ADR)]缀合物在血液中的长循环时间被认为是在靶部位(如肿瘤)增强摄取的先决条件。

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