CIDCA   05380
CENTRO DE INVESTIGACION Y DESARROLLO EN CRIOTECNOLOGIA DE ALIMENTOS
Unidad Ejecutora - UE
información general
recursos humanos
líneas de investigación
servicios tecnológicos
proyectos financiados por CONICET
proyectos financiados por otras instituciones
artículos
libros
capítulos de libros
congresos y reuniones científicas
informe técnico
artículos
Título:
Endocytosis and intracellular traffic of cholesterol-PDMAEMA liposome complexes in human epithelial-like cells
Autor/es:
SZYMANOWSKI, F.; HUGO, A. A.; ALVES, P.; 3; SIMÕES, P. N.; GÓMEZ-ZAVAGLIA, A. AND PÉREZ, P. F.; SZYMANOWSKI, F.; HUGO, A. A.; ALVES, P.; 3; SIMÕES, P. N.; GÓMEZ-ZAVAGLIA, A. AND PÉREZ, P. F.
Revista:
COLLOIDS AND SURFACES B-BIOINTERFACES
Editorial:
ELSEVIER SCIENCE BV
Referencias:
Lugar: Amsterdam; Año: 2017 vol. 156 p. 38 - 43
ISSN:
0927-7765
Resumen:
Liposomes are generally used as delivery systems, as they are capable of encapsulating a wide variety of molecules (i.e. plasmids, recombinant proteins, therapeutic drugs). However, liposomal drug delivery have to fulfill different requirements, such as the effective internalization by the target cells and avoidance of the degradative activity of the intracellular compartments. The use of polymer lipid complexes (PLCs), by including different polymers in the liposome formulation, could improve internalization and intracellularrelease of drugs. The aim of the present work is to study the mechanisms of cellular uptaking and the intracellular trafficking of PLCs formed with cholesterol-poly(2-(dimethylamino)ethyl methacrylate) CHO-PDMAEMA and lecithin (LC CHO-PD). Calcein-loaded liposomes were used to determine cellular uptake and intracellular localization by flow cytometry and confocal microscopy. Incorporation of CHOPDMAEMA to lecithin liposomes enhanced the internalization capacity of PLCs. Internalization of PLCs by human epithelial-like cells (HEK-293) diminished at 4 ◦C, suggesting uptake by endocytosis. PLCs showed no co-localization with acidic compartments after internalization. Experiments with endocytosis inhibitors and co-localization of liposomes and albumin, suggested the caveolae endocytic pathway as the most probable route for intracellular trafficking of PLCs.In this work, we demonstrated an efficient uptake of LC CHO-PDs by human epithelial-like cells (HEK- 293) through the non-degradative caveolae endocytic pathway. The mode of internalization and the intracellular fate of liposomes under study, suggest a promising use of LC CHO-PDs as drug deliverysystems.