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[vc_row][vc_column][vc_row_inner][vc_column_inner][vc_separator css=”.vc_custom_1624529070653{padding-top: 30px !important;padding-bottom: 30px !important;}”][/vc_column_inner][/vc_row_inner][vc_row_inner layout=”boxed”][vc_column_inner width=”3/4″ css=”.vc_custom_1624695412187{border-right-width: 1px !important;border-right-color: #dddddd !important;border-right-style: solid !important;border-radius: 1px !important;}”][vc_empty_space][megatron_heading title=”Abstract” size=”size-sm” text_align=”text-left”][vc_column_text]© The Royal Society of Chemistry 2015.In this study, novel hybrid nanocarriers composed of carboxymethyl-hexanoyl chitosan (Chitosonic® Acid, CA) and 1,2-distearoyl-sn-glycero-3-phosphoethanolamine (DSPE)-liposomes were developed. CA was immobilized onto the DSPE-liposomes by EDC/NHS reaction using the carboxyl group of CA and the amino group of DSPE. The characteristics of the resultant CA-modified liposomes were evaluated by transmission electron microscopy, dynamic light scattering, zeta potential, FTIR spectroscopy, X-ray photoelectron spectroscopy, and contact angle measurement. The results show that the particle size and surface charge of the CA-modified liposomes varied with the concentration of CA, and exhibited pH-sensitive behavior. In vitro drug release studies demonstrated the sustained release behavior of the doxorubicin in the CA-modified liposomes, related to the rapid release in the free doxorubicin. Interestingly, the doxorubicin release rate from CA-modified liposomes was lower at higher pH values (pH 7.4) than at lower pH values (pH 4), indicating that the drug carrier displayed pH-sensitive released behavior. Furthermore, CA-modified liposomes exhibited no cytotoxicity toward the fibroblast cells (L-929 cells), suggesting an excellent biocompatibility. Fluorescence and confocal microscopy images showed good cellular internalization of the CA-modified liposomes into the cellular compartment. These results confirm that the novel CA-modified liposomes could respond to pH environment, which is promising for drug controlled release applications, especially in the field of cancer cell therapy (lower pH environments).[/vc_column_text][vc_empty_space][vc_separator css=”.vc_custom_1624528584150{padding-top: 25px !important;padding-bottom: 25px !important;}”][vc_empty_space][megatron_heading title=”Author keywords” size=”size-sm” text_align=”text-left”][vc_column_text]Cellular compartments,Cellular internalization,Drug controlled release,Fibroblast cells,Hexanoyl chitosan,Particle size and surfaces,pH environments,Sustained release[/vc_column_text][vc_empty_space][vc_separator css=”.vc_custom_1624528584150{padding-top: 25px !important;padding-bottom: 25px !important;}”][vc_empty_space][megatron_heading title=”Indexed keywords” size=”size-sm” text_align=”text-left”][vc_column_text][/vc_column_text][vc_empty_space][vc_separator css=”.vc_custom_1624528584150{padding-top: 25px !important;padding-bottom: 25px !important;}”][vc_empty_space][megatron_heading title=”Funding details” size=”size-sm” text_align=”text-left”][vc_column_text][/vc_column_text][vc_empty_space][vc_separator css=”.vc_custom_1624528584150{padding-top: 25px !important;padding-bottom: 25px !important;}”][vc_empty_space][megatron_heading title=”DOI” size=”size-sm” text_align=”text-left”][vc_column_text]https://doi.org/10.1039/c4ra14834g[/vc_column_text][/vc_column_inner][vc_column_inner width=”1/4″][vc_column_text]Widget Plumx[/vc_column_text][/vc_column_inner][/vc_row_inner][/vc_column][/vc_row][vc_row][vc_column][vc_separator css=”.vc_custom_1624528584150{padding-top: 25px !important;padding-bottom: 25px !important;}”][/vc_column][/vc_row]