Interaction of liposomes with Kupffer cells in vitro

“…The negatively charged liposomes used here have been shown to be endocytosed rapidly by Kupffer cells [171, and endothelial cells present in our hepatic cell preparation do not take up liposomes [15]. Since the main mechanism of interaction of liposomes with Kupffer cells in vitro is adsorptive endocytosis [18], we examined the effect of cholesterol and serum on adsorption of liposomes at 4°C. At this temperature liposomes are predominantly adsorbed onto the cell surface and not phagocytosed [18].…”

“…Since the main mechanism of interaction of liposomes with Kupffer cells in vitro is adsorptive endocytosis [18], we examined the effect of cholesterol and serum on adsorption of liposomes at 4°C. At this temperature liposomes are predominantly adsorbed onto the cell surface and not phagocytosed [18]. It was found (see table 1) that the presence of cholesterol in liposomes reduces adsorption and serum further hinders this process for all liposomes in hepatic and splenic cells except the adsorption of cholesterol-rich liposomes on splenic ceils which, in contrast, is enhanced.…”

Tissue specific opsonins for phagocytic cells and their different affinity for cholesterol‐rich liposomes

“…The negatively charged liposomes used here have been shown to be endocytosed rapidly by Kupffer cells [171, and endothelial cells present in our hepatic cell preparation do not take up liposomes [15]. Since the main mechanism of interaction of liposomes with Kupffer cells in vitro is adsorptive endocytosis [18], we examined the effect of cholesterol and serum on adsorption of liposomes at 4°C. At this temperature liposomes are predominantly adsorbed onto the cell surface and not phagocytosed [18].…”

“…Since the main mechanism of interaction of liposomes with Kupffer cells in vitro is adsorptive endocytosis [18], we examined the effect of cholesterol and serum on adsorption of liposomes at 4°C. At this temperature liposomes are predominantly adsorbed onto the cell surface and not phagocytosed [18]. It was found (see table 1) that the presence of cholesterol in liposomes reduces adsorption and serum further hinders this process for all liposomes in hepatic and splenic cells except the adsorption of cholesterol-rich liposomes on splenic ceils which, in contrast, is enhanced.…”

Tissue specific opsonins for phagocytic cells and their different affinity for cholesterol‐rich liposomes

“…Such a system in vitro provides the most direct approach to investigate the mechanism of liposome-Kupffer cell interaction and to answer questions arising from studies in vivo [2,61. From a previous study we concluded that the major mechanism by which liposomes, at 37"C, interact with Kupffer cells is a process of adsorptive endocytosis [4]. After internalization of the vesicles, radioactively labeled lipid and encapsulated protein were both effectively degraded by the cells.…”

“…Fluorescence and electron microscopic observations indicated that the lysosomes are the intracellular degradation sites of the liposomal components and a study of the effects of lysosomotropic amines on uptake and degradation of liposomal constituents confirmed the involvement of the lysosomal system in the breakdown of internalized vesicles [55]. In comparison with the almost complete degradation of entrapped albumin, liposomal phospholipid was degraded to a much lower extent [5].…”

Uptake and processing of liposomal phospholipids by Kupffer cells in vitro

“…In at least one case the affinity of the MHC for reconstiOne of the better known observations in the cell tution into liposomes was so great that a liposome biology of liposomes is that liposomes are taken up reconstitution procedure was actually suggested as a avidly by macrophages both in vitro [40][41][42][43][44][45][46][47], and in method for purifying the MHC [30]. An interesting vivo .…”

Immunologic aspects of liposomes: presentation and processing of liposomal protein and phospholipid antigens