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体外脂质体与细胞相互作用的定量分析:悬浮和贴壁J774细胞及人单核细胞的结合和内吞速率常数

Quantitative analysis of liposome-cell interactions in vitro: rate constants of binding and endocytosis with suspension and adherent J774 cells and human monocytes.

作者信息

Lee K D, Nir S, Papahadjopoulos D

机构信息

Cancer Research Institute, University of California, San Francisco 94143-0128.

出版信息

Biochemistry. 1993 Jan 26;32(3):889-99. doi: 10.1021/bi00054a021.

Abstract

We have characterized the parameters describing the total association (uptake) of liposomes with murine macrophage-like cell line J774 cells and human peripheral blood monocytes at 4 degrees C and at 37 degrees C with or without inhibitors of endocytosis. The uptake of neutral liposomes composed of phosphatidylcholine (PC)/cholesterol (Chol) (2:1 mole ratio) is about 10-fold lower than that of negatively charged liposomes composed of phosphatidylserine (PS)/PC/Chol (1:1:1). However, the rate of uptake of PC/Chol liposomes at 37 degrees C is still 10-fold higher than that by fluid-phase pinocytosis. The uptake of liposomes, which is mediated by high-affinity binding to the cell surface binding sites and subsequent endocytosis, could be simulated and predicted by model calculations employing mass action kinetics. The number of binding sites, affinity constants of binding at 37 degrees C and 4 degrees C, on- and off-rate constants of binding, and endocytic rate constants for both types of liposomes were determined. The number of binding sites and the binding constants for PS/PC/Chol liposomes binding to J774 cells is severalfold to an order of magnitude higher than that for PC/Chol liposomes, but the rate constants at which they are endocytosed following binding to the cells are similar for both liposome types. The binding of liposomes, especially PS/PC/Chol, to J774 cells and monocytes is greatly enhanced by adherence of cells to plastic substratum and is also increased by maturation/differentiation in the case of monocytes. Our quantitative analysis indicates that the binding and endocytosis of liposomes, especially PS-containing liposomes, is mediated by binding sites that have strong affinity, comparable to or about an order of magnitude smaller than other known particle-cell interactions with specific receptors such as virus and lipoproteins binding to cells.

摘要

我们已经对描述脂质体与小鼠巨噬细胞样细胞系J774细胞以及人外周血单核细胞在4℃和37℃条件下,有无内吞作用抑制剂时的总结合(摄取)情况的参数进行了表征。由磷脂酰胆碱(PC)/胆固醇(Chol)(摩尔比2:1)组成的中性脂质体的摄取量比由磷脂酰丝氨酸(PS)/PC/Chol(1:1:1)组成的带负电荷脂质体的摄取量低约10倍。然而,PC/Chol脂质体在37℃时的摄取速率仍比液相胞饮作用高10倍。脂质体的摄取是由与细胞表面结合位点的高亲和力结合以及随后的内吞作用介导的,可通过采用质量作用动力学的模型计算进行模拟和预测。测定了两种脂质体的结合位点数、37℃和4℃时的结合亲和常数、结合和解离速率常数以及内吞速率常数。PS/PC/Chol脂质体与J774细胞结合的结合位点数和结合常数比PC/Chol脂质体高几倍到一个数量级,但两种脂质体与细胞结合后被内吞的速率常数相似。脂质体,尤其是PS/PC/Chol,与J774细胞和单核细胞的结合会因细胞黏附于塑料基质而大大增强,在单核细胞的情况下,也会因成熟/分化而增加。我们的定量分析表明,脂质体,尤其是含PS脂质体的结合和内吞作用是由具有强亲和力的结合位点介导的,该亲和力与其他已知的颗粒-细胞与特定受体的相互作用(如病毒和脂蛋白与细胞的结合)相当或小一个数量级左右。

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