Journal ArticleDOI
Pegylated poly(lactide) and poly(lactide-co-glycolide) nanoparticles: preparation, properties and possible applications in drug delivery.
TLDR
The ability of the PLA-Peg and PLGA-PEG nanoparticles to evade rapid phagocytocis has extended the range of sites within the body that the nanoparticles can reach, which has significant implications with regard to their application in controlled drug delivery and targeting.Abstract:
The preparation, properties and potential applications in drug delivery of biocompatible and biodegradable PLA-PEG and PLGA-PEG nanoparticles are discussed. PLA-PEG and PLGA-PEG nanoparticles have been produced by emulsification-solvent evaporation, solvent displacement and salting out methods. The nanoparticles can be stored as freeze-dried powders, but an adequate amount of a suitable lyoprotectant should be added prior lyophilisation to prevent nanoparticle aggregation and retain nanoparticle redispersibility. The nanoparticles have a core-shell structure with a PLA core and a PEG coating. Their basic colloidal properties and degradation depend on copolymer composition. The PLA-PEG and PLGA-PEG nanoparticles exhibit prolonged blood circulation following intravenous administration to animals. The composition of the nanoparticles determine their biodistribution properties, probably through its effects on the effectiveness of the PEG steric barrier and the size of the nanoparticles. The ability of the PLA-PEG and PLGA-PEG nanoparticles to evade rapid phagocytocis has extended the range of sites within the body that the nanoparticles can reach, which has significant implications with regard to their application in controlled drug delivery and targeting. The PLA-PEG and PLGA-PEG nanoparticles can be loaded with a variety of bioactive agents achieving satisfactory loading, especially in the case of hydrophobic drugs. The nanoparticles have been investigated for the treatment of infectious diseases and cancer, the intravenous and mucosal delivery of proteins, and oligonucleotide and gene delivery. The results have been encouraging and PLA-PEG and PLGA-PEG nanoparticle formulations, improving the therapeutic potential of both established and new drugs, may be expected to be available in the near future.read more
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Journal ArticleDOI
PEGylated human serum albumin (HSA) nanoparticles: preparation, characterization and quantification of the PEGylation extent.
TL;DR: A size exclusion chromatography method with refractive index detection was established which enabled the quantification of unreacted PEG in the supernatant and the positive effect of PEGylation on plasma half-life was demonstrated in an in vivo study in mice.
Journal ArticleDOI
Recent developments in multifunctional hybrid nanoparticles: opportunities and challenges in cancer therapy.
Carolina Salvador-Morales,Pedro M. Valencia,Anjali B Thakkar,Edward W. Swanson,Robert Langer +4 more
TL;DR: The most recent synthetic strategies to create these hybrid systems are discussed and four key design aspects are analyzed: stability, encapsulation of therapeutic and imaging agents, controlled release of encapsulated agents, and biocompatibility.
Journal ArticleDOI
Influences of surface coating of PLGA nanoparticles on immune activation of macrophages.
Xinyi Chen,Changyou Gao +1 more
TL;DR: NPs of PLGA with 3 different molecular weights were fabricated using bovine serum albumin (BSA) and polyethyleneimine (PEI) as dispersing agents and induced a significantly higher expression of TNF-α, likely due to the heterogeneous albumin and existence of endotoxin.
Journal ArticleDOI
Lymphatic Biodistribution of Polylactide Nanoparticles
TL;DR: This technique has the potential for providing optical contrast and drug delivery through the lymphatic circulation for the treatment of metastatic cancer.
Journal ArticleDOI
PEGylated and CD47-conjugated nanoellipsoidal artificial antigen-presenting cells minimize phagocytosis and augment anti-tumor T-cell responses.
Shilong Song,Xiaoxiao Jin,Lei Zhang,Chen Zhao,Yan Ding,Qianqian Ang,Odontuya Khaidav,Chuanlai Shen +7 more
TL;DR: The superimposed or synergistic effects of ellipsoidal stretch, PEGylation, and CD47-Fc conjugation minimized cellular uptake of nano-aAPCs and enhanced their functionality to expand antigen-specific T cells and inhibit tumor growth, thus suggesting a more valuable strategy to design “stealth” nanoscale aAPCs suitable for tumor active immunotherapy.