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人中性粒细胞从溶液和脂质体中对液相标记物的细胞摄取。

Cellular uptake of a fluid-phase marker by human neutrophils from solutions and liposomes.

作者信息

Scieszka J F, Cho M J

机构信息

Drug Delivery Systems Research, Upjohn Company, Kalamazoo, Michigan 49001.

出版信息

Pharm Res. 1988 Jun;5(6):352-8. doi: 10.1023/a:1015903510262.

Abstract

In assessing the feasibility of utilizing the phagocytic activity of polymorphonuclear leukocytes (PMNs) for a more efficient drug delivery to the cell, the uptake of the fluid-phase marker lucifer yellow CH (LY) at 37 degrees C by human PMNs from LY-containing liposomes was compared with that from solutions. In the presence of 10% autologous serum, the LY uptake at 37 degrees C via phagocytosis of a given PMN source when the concentrations of PMN, LY, and total lipid were in the range of 10(7) cells/ml, 0.5 mg/ml, and 50 mumol/ml, respectively. As expected, the LY uptake via phagocytosis was critically dependent upon the LY entrapment efficiency in the liposome preparation. Interestingly, little LY uptake was found when the serum was heat inactivated (56 degrees C x 30 min). The serum effect was upon liposome vesicles rather than upon the cells. The present study demonstrates that the use of particular drug carriers for targeted drug delivery to PMNs and possible to an extravascular site mediated by the cell infiltration is a viable approach.

摘要

在评估利用多形核白细胞(PMN)的吞噬活性以更有效地将药物递送至细胞的可行性时,比较了人PMN在37℃下从含荧光素黄CH(LY)的脂质体和溶液中摄取液相标记物荧光素黄CH(LY)的情况。在10%自体血清存在下,当PMN、LY和总脂质的浓度分别在10⁷个细胞/ml、0.5mg/ml和50μmol/ml范围内时,给定PMN来源在37℃下通过吞噬作用摄取LY。正如预期的那样,通过吞噬作用摄取LY严重依赖于脂质体制剂中LY的包封效率。有趣的是,当血清热灭活(56℃×30分钟)时,几乎没有发现LY摄取。血清作用于脂质体囊泡而非细胞。本研究表明,使用特定的药物载体将药物靶向递送至PMN,并可能通过细胞浸润介导至血管外部位是一种可行的方法。

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