首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Liposome formulations with prolonged circulation time in blood and enhanced uptake by tumors.
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Liposome formulations with prolonged circulation time in blood and enhanced uptake by tumors.

机译:具有延长的血液循环时间和增加的肿瘤摄取的脂质体制剂。

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摘要

The rapid clearance of circulating liposomes from the bloodstream, coupled with their high uptake by liver and spleen, has thus far been an obstacle to any attempts at targeting to tumors. We have assessed the impact of liposome composition on their clearance from the circulation in normal and tumor-bearing mice and on their uptake by tumors and various normal tissues. By selective changes in lipid composition, while maintaining a mean particle diameter of approximately equal to 100 nm, we have achieved up to a 60-fold increase in the fraction of recovered dose present in blood 24 hr after i.v. injection. Concomitantly, there was a decrease by a factor of 4 of the recovered dose localizing in the liver and spleen, the major organs of the reticuloendothelial system. Parallel experiments in tumor-bearing mice demonstrated a 25-fold increase of the liposome concentration in the tumor when formulations with long and short blood residence time were compared. The most favorable results were obtained with liposomes containing a small molar fraction of a negatively charged glycolipid, such as monosialoganglioside or phosphatidylinositol, and a solid-phase neutral phospholipid as the bulk component. The bio-distribution of such formulations is of considerable therapeutic potential in cancer for increasing the concentration of cytotoxic agents in tumors while minimizing the likelihood of toxicity to the reticuloendothelial system.
机译:迄今为止,循环脂质体从血流中的快速清除,以及肝脏和脾脏对它们的高摄取,一直是任何针对肿瘤的尝试的障碍。我们已经评估了脂质体组合物对它们在正常和荷瘤小鼠中从循环中清除的影响以及对它们被肿瘤和各种​​正常组织摄取的影响。通过选择性改变脂质组成,同时保持平均粒径约等于100 nm,我们在静脉注射后24小时血液中的回收剂量比例增加了多达60倍。注射。同时,在网状内皮系统的主要器官肝脏和脾脏中,所恢复的剂量减少了4倍。在荷瘤小鼠中的平行实验表明,当比较具有长和短血液停留时间的制剂时,肿瘤中脂质体浓度增加了25倍。用含有少量摩尔分数带负电荷的糖脂(如单唾液酸神经节苷脂或磷脂酰肌醇)和固相中性磷脂作为主体组分的脂质体可获得最有利的结果。这种制剂的生物分布在癌症中具有相当大的治疗潜力,用于增加肿瘤中细胞毒性剂的浓度,同时使对网状内皮系统毒性的可能性最小化。

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