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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Pharmacokinetic analysis of hepatic uptake of galactosylated bovine serum albumin in a perfused rat liver
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Pharmacokinetic analysis of hepatic uptake of galactosylated bovine serum albumin in a perfused rat liver

机译:灌流大鼠肝脏中半乳糖基化牛血清白蛋白摄取肝的药代动力学分析

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Hepatic uptake of In-111-labelled galactosylated bovine serum albumin (GaL-BSA) with different number of galactose residues per BSA were studied in rat liver perfusion experiments. During a single-pass constant infusion mode, [In-111]Gal-BSAs (0.1-2.0 mu g/ml) were continuously extracted by the liver and its extraction ratio at steady-state (E-ss) was lowered as the inflow concentration increased. Hepatic clearances of [In-111]Gal-BSAs increased significantly according to the increase in the number of galactose residues per BSA at an inflow concentration of 0.7 mu g/ml. The outflow patterns of [In-111]Gal-BSAs at various inflow concentrations were simultaneously fitted to a one-organ pharmacokinetic model, by which we can characterize their binding to the cell surface and internalization processes separately. The parameters obtained were varied significantly among [In-111]Gal-BSAs depending on the number of galactose residues and indicate that not only the binding to the receptors but also the internalization after the binding are regulated by the number of galactose residues per BSA during hepatic uptake. (C) 1998 Elsevier Science B.V. [References: 25]
机译:在大鼠肝灌注实验中研究了In-111标记的半乳糖基化牛血清白蛋白(GaL-BSA)在每个BSA中具有不同半乳糖残基的肝摄取量。在单次恒定输注模式下,肝脏连续提取[In-111] Gal-BSA(0.1-2.0μg / ml),并且随着流入量的增加,稳态下的提取率(E-ss)降低浓度增加。 [In-111] Gal-BSA的肝清除率随着流入浓度为0.7μg / ml的每个BSA中半乳糖残基数量的增加而显着增加。将[In-111] Gal-BSA在各种流入浓度下的流出模式同时拟合到一个器官的药代动力学模型,由此我们可以分别表征它们与细胞表面的结合和内在化过程。取决于半乳糖残基的数量,[In-111] Gal-BSA中获得的参数存在显着差异,并且表明在该过程中,不仅与受体的结合,而且结合后的内在化还受到每个BSA中半乳糖残基的数目的调节。肝吸收。 (C)1998 Elsevier Science B.V. [参考:25]

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