Literature DB >> 1527006

Association of blood proteins with large unilamellar liposomes in vivo. Relation to circulation lifetimes.

A Chonn1, S C Semple, P R Cullis.   

Abstract

The proteins associated with liposomes in the circulation of mice were analyzed in order to determine whether bound proteins significantly influence the fate of liposomes in vivo. Liposomes were administered intravenously via the dorsal tail vein of CD1 mice and were isolated from blood after 2 min in the absence of coagulation inhibitors using a rapid "spin column" procedure. Various negatively charged liposomes exhibiting markedly different clearance properties were studied; notably, these included liposomes containing 10 mol % ganglioside GM1 which has been previously shown to effectively limit liposomal uptake by the fixed macrophages of the reticuloendothelial system. The protein binding ability (PB; g of protein/mol of lipid) of the liposomes was quantitated and related to the circulation half-life (tau 1/2) of the liposomes. Liposomes having similar membrane surface charge imparted by different anionic phospholipids were found to exhibit markedly different protein binding potentials. Furthermore, PB values determined from the in vivo experiments were found to be inversely related to circulation half-lives. PB values in excess of 50 g of protein/mol of lipid were observed for rapidly cleared liposomes such as those containing cardiolipin or phosphatidic acid (tau 1/2 less than 2 min). PB values for ganglioside GM1-containing liposomes (tau 1/2 greater than 2 h) were significantly less (PB less than 15 g of total protein/mol of total lipid). PB values were also determined for liposomes recovered from in vitro incubations with isolated human serum; relative PB values obtained from these in vitro experiments were in agreement with relative PB values measured from in vivo experiments. PB values, therefore, could be a useful parameter for predicting the clearance behavior of liposomes in the circulation. Liposomes exhibiting increased PB values in vivo were shown by immunoblot analysis to bind more immune opsonins, leading to a higher probability of phagocytic uptake. Finally, based on results obtained using the in vitro system, it is suggested that the mechanism by which ganglioside GM1 prolongs the murine circulation half-life of liposomes is by reducing the total amount of blood protein bound to the liposomes in a relatively nonspecific manner.

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Year:  1992        PMID: 1527006

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  68 in total

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Journal:  Pharm Res       Date:  2001-01       Impact factor: 4.200

3.  Nano-advantage in enhanced drug delivery with biodegradable nanoparticles: contribution of reduced clearance.

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4.  Administration of liposomal agents and blood clearance capacity of the mononuclear phagocyte system.

Authors:  E W van Etten; M T ten Kate; S V Snijders; I A Bakker-Woudenberg
Journal:  Antimicrob Agents Chemother       Date:  1998-07       Impact factor: 5.191

Review 5.  Lipid Nanoparticle Systems for Enabling Gene Therapies.

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6.  Biodistribution and Toxicity of X-Ray Iodinated Contrast Agent in Nano-emulsions in Function of Their Size.

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7.  Monosialoganglioside GM1 shortens the blood circulation time of liposomes in rats.

Authors:  D Liu; F Liu; Y K Song
Journal:  Pharm Res       Date:  1995-04       Impact factor: 4.200

Review 8.  Clearance properties of nano-sized particles and molecules as imaging agents: considerations and caveats.

Authors:  Michelle Longmire; Peter L Choyke; Hisataka Kobayashi
Journal:  Nanomedicine (Lond)       Date:  2008-10       Impact factor: 5.307

Review 9.  A new look at lipid-membrane structure in relation to drug research.

Authors:  O G Mouritsen; K Jørgensen
Journal:  Pharm Res       Date:  1998-10       Impact factor: 4.200

10.  Effects of chitosan coating on physical properties and pharmacokinetic behavior of mitoxantrone liposomes.

Authors:  Jie Zhuang; Qineng Ping; Yunmei Song; Jianping Qi; Zheng Cui
Journal:  Int J Nanomedicine       Date:  2010-08-09
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