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酵母聚糖刺激的大鼠体内静脉注射的空间稳定微球的肝脏清除率增强。

Enhanced hepatic clearance of intravenously administered sterically stabilized microspheres in zymosan-stimulated rats.

作者信息

Moghimi S M, Hedeman H, Christy N M, Illum L, Davis S S

机构信息

Department of Pharmaceutical Sciences, University of Nottingham, England.

出版信息

J Leukoc Biol. 1993 Dec;54(6):513-7. doi: 10.1002/jlb.54.6.513.

Abstract

The blood clearance and organ deposition of sterically stabilized (poloxamine-908 coated) polystyrene microspheres of two different sizes (60 and 220 nm in diameter) were compared in control and zymosan-stimulated rats 3 h after intravenous administration. Poloxamine coating dramatically decreased the uptake of 60-nm microspheres by organs of the reticuloendothelial system and, concomitantly, kept microspheres in the blood. Large poloxamine-coated microspheres (220 nm) initially remained in the blood, but eventually a large fraction of these microspheres was filtered by the spleen. Daily administration of zymosan produced a marked increase in the intravascular clearance of the large, but not the small, poloxamine-coated microspheres. The enhanced intravascular clearance of large poloxamine-coated microspheres in zymosan-treated rats was the result of hepatic sequestration. On the other hand, the splenic filtration of these microspheres was depressed by 225% below the control values, despite the dramatic increase in spleen size of zymosan-treated rats. Preincubation of large poloxamine-coated microspheres in serum derived from both the control and zymosan-treated animals suggested that the enhanced hepatic uptake of large sterically stabilized microspheres following zymosan stimulation was not the result of "specific opsonization" processes. Instead, the changes in the proliferative as well as the phagocytic response of Kupffer cells appeared to be responsible for these observations. The preferred hepatic uptake of large poloxamine-coated microspheres, as opposed to smaller particles, is suggested to be due to differences in surface characteristics and the properties of microspheres. These may include differences in polymer density and the surface conformation of the polyoxyethylene segments of the polymer in the biological environment and the way they interact with both plasma components and the macrophage surface. These observations could be of importance in the use of sterically stabilized drug carriers for delivery of therapeutic agents to sites other than the reticuloendothelial system in clinical conditions associated with globally or regionally enhanced reticuloendothelial activity.

摘要

静脉注射后3小时,在对照大鼠和经酵母聚糖刺激的大鼠中,比较了两种不同大小(直径分别为60和220纳米)的空间稳定化(聚氧丙烯胺-908包被)聚苯乙烯微球的血液清除率和器官沉积情况。聚氧丙烯胺包被显著降低了网状内皮系统器官对60纳米微球的摄取,并同时使微球保留在血液中。大的聚氧丙烯胺包被微球(220纳米)最初保留在血液中,但最终这些微球的很大一部分被脾脏滤过。每日给予酵母聚糖使大的聚氧丙烯胺包被微球(而非小的)的血管内清除率显著增加。酵母聚糖处理的大鼠中,大的聚氧丙烯胺包被微球血管内清除率增强是肝脏滞留的结果。另一方面,尽管酵母聚糖处理的大鼠脾脏大小显著增加,但这些微球的脾脏滤过率比对照值降低了225%。将大的聚氧丙烯胺包被微球在对照动物和酵母聚糖处理动物的血清中预孵育表明,酵母聚糖刺激后大的空间稳定化微球肝脏摄取增强并非“特异性调理作用”过程的结果。相反,枯否细胞增殖和吞噬反应的变化似乎是这些观察结果的原因。与较小颗粒相比,大的聚氧丙烯胺包被微球优先被肝脏摄取,这可能是由于表面特性和微球性质的差异。这些差异可能包括聚合物密度、聚合物在生物环境中的聚氧乙烯链段的表面构象以及它们与血浆成分和巨噬细胞表面相互作用方式的不同。这些观察结果对于在网状内皮系统整体或局部活性增强的临床情况下,使用空间稳定化药物载体将治疗剂递送至网状内皮系统以外的部位可能具有重要意义。

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