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Journal ArticleDOI

Polymeric worm micelles as nano-carriers for drug delivery.

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TLDR
W worm micelles as blends of degradable polylactic acid and inert block copolymer amphiphiles were prepared for controlled release and initial study of carrier transport through nano-porous media, suggesting a new class of hydrophobic drug nano-carriers that are capable of tissue permeation as well as controlled release.
Abstract
Nanoscale carriers of active compounds, especially drugs, need not be spherical in shape. Worm micelles as blends of degradable polylactic acid (PLA) and inert block copolymer amphiphiles were prepared for controlled release and initial study of carrier transport through nano-porous media. The loading capacity of a typical hydrophobic drug, Triamterene, and the release of hydrophobic dyes were evaluated together with morphological changes of the micelles. Degradation of PLA by hydrolysis led to the self-shortening of worms and a clear transition towards spherical micelles, correlating with the release of hydrophobic dyes. Perhaps equally important for application is the flexibility of worm micelles, which we show allows them to penetrate nanoporous gels where 100 nm sized vesicles cannot enter. Such gels have served as tissue models, and so the results here collectively suggest a new class of hydrophobic drug nano-carriers that are capable of tissue permeation as well as controlled release.

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Journal ArticleDOI

Endogenous Stimuli‐Sensitive Multistage Polymeric Micelleplex Anticancer Drug Delivery System for Efficient Tumor Penetration and Cellular Internalization

TL;DR: In vivo investigation reveals that the Pt(IV)‐loading micelleplexes significantly suppress tumor growth via intravenous injection due to synergistic effect of long circulation in bloodstream, high tumor accumulation, deep tumor tissue penetration, and efficient cellular internalization.
Journal ArticleDOI

Novel self-assembled nano-tubular mixed micelles of Pluronics P123, Pluronic F127 and phosphatidylcholine for oral delivery of nimodipine: In vitro characterization, ex vivo transport and in vivo pharmacokinetic studies

TL;DR: The in vivo pharmacokinetic study showed greater bioavailability of NM in plasma and brain of rats from NM-loaded PPPMM compared to that of the drug solution due to the efficiency of flexible NTMM to enhance absorption of NM from the intestinal mucosa, which could be promising to improve oral and parenteral delivery of NM.
Book ChapterDOI

Block Copolymer Nanotubes Derived from Self-Assembly

TL;DR: In this paper, the preparation, dilutesolution properties, and chemical reactions of block copolymer nanotubes are discussed, as well as their preparation and dilution properties.
Journal ArticleDOI

Development of a vessel-simulating flow-through cell method for the in vitro evaluation of release and distribution from drug-eluting stents

TL;DR: The necessity to adapt dissolution testing for DES to the unique conditions influencing delivery to the vessel wall to learn more about local distribution and to anticipate the in vivo performance of DES is emphasized.
Journal ArticleDOI

Additive induced core and corona specific dehydration and ensuing growth and interaction of Pluronic F127 micelles.

TL;DR: DLS, SANS, fluorescence and rheological studies on the effects of NaCl and butan-1-ol on the properties of Pluronic F127 micelles in the aqueous medium show that corona specific micellar dehydration by NaCl induces inter micellAR attraction and consequent formation of micellars clusters.
References
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Journal ArticleDOI

Block copolymer micelles for drug delivery: design, characterization and biological significance

TL;DR: The utility of polymeric micelles formed through the multimolecular assembly of block copolymers as novel core-shell typed colloidal carriers for drug and gene targeting and their feasibility as non-viral gene vectors is highlighted.
Journal ArticleDOI

Polymeric micelles - a new generation of colloidal drug carriers.

TL;DR: This review examines the chemical nature of polymeric micelles as well as the methods used to characterize them with regard to drug delivery and potential medical applications, especially in cancer chemotherapy, are described and discussed.
Journal ArticleDOI

On the Origins of Morphological Complexity in Block Copolymer Surfactants

TL;DR: Experiments with poly(1,2-butadiene-b-ethylene oxide) diblock copolymers are described, which form Y-junctions and three-dimensional networks in water at weight fractions of PEO intermediate to those associated with vesicle and wormlike micelle morphologies.
Journal ArticleDOI

Self-porating polymersomes of PEG-PLA and PEG-PCL: hydrolysis-triggered controlled release vesicles.

TL;DR: With all compositions, in both 100 nm and giant vesicles, the average release time reflects a highly quantized process in which any given vesicle is either intact and retains its encapsulant, or is porated and slowly disintegrates.
Journal ArticleDOI

Giant Wormlike Rubber Micelles

TL;DR: A low molecular weight poly(ethyleneoxide)-poly(butadiene) (PEO-PB) diblock copolymer containing 50 weight percent PEO forms gigantic wormlike micelles at low concentrations (<5 percent by weight) in water.
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