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Mitochondrially Targeted Nanoparticles Based on α‐TOS for the Selective Cancer Treatment
Authors:María Rosa Aguilar  Carolina Sánchez‐Rodríguez  Francisco Parra  Mar Fernández  Juan Parra  Juan Riestra‐Ayora  Ricardo Sanz‐Fernández  Julio San Román
Affiliation:1. Group of Biomaterials, Department of Polymeric Nanomaterials and Biomaterials, Institute of Polymer Science and Technology, Madrid, Spain;2. Networking Biomedical Research Centre in Bioengineering, Biomaterials, and Nanomedicine, CIBER‐BBN, Spain;3. Foundation for Biomedical Research, University Hospital of Getafe, Getafe, Madrid, Spain;4. European University of Madrid, C/Tajo s/n. 28670, Villaviciosa de Odón, Madrid, Spain;5. Clinical Research and Experimental Biopathology Unit, Healthcare Complex of ávila, SACYL. C/Jesús del Gran Poder 42, ávila, Spain
Abstract:The aim of this work is the preparation of an active nanovehicle for the effective administration of α‐tocopheryl succinate (α‐TOS). α‐TOS is loaded in the core of nanoparticles (NPs) based on amphiphilic pseudo‐block copolymers of N‐vinyl pyrrolidone and a methacrylic derivative of α‐TOS. These well‐defined spherical NPs have sizes below 165 nm and high encapsulation efficiencies. In vitro activity of NPs is tested in hypopharynx squamous carcinoma (FaDu) cells and nonmalignant epithelial cells, demonstrating that the presence of additional α‐TOS significantly enhances its antiproliferative activity; however, a range of selective concentrations is observed. These NPs induce apoptosis of FaDu cells by activating the mitochondria death pathway (via caspase‐9). Both loaded and unloaded NPs act via complex II and produce high levels of reactive oxygen species that trigger apoptosis. Additionally, these NPs effectively suppress the vascular endothelial growth factor (VEGF) expression of human umbilical vein endothelial cells (HUVECs). These results open the possibility to use this promising nanoformulation as an α‐TOS delivery system for the effective cancer treatment, effectively resolving the current limitations of free α‐TOS administration.
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Keywords:α  ‐tocopheryl succinate  anticancer  apoptosis  nanovehicle  polymer drug
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