Literature DB >> 24065591

PLGA/liposome hybrid nanoparticles for short-chain ceramide delivery.

Peng Zou1, Stephan T Stern, Duxin Sun.   

Abstract

PURPOSE: Rapid premature release of lipophilic drugs from liposomal lipid bilayer to plasma proteins and biological membranes is a challenge for targeted drug delivery. The purpose of this study is to reduce premature release of lipophilic short-chain ceramides by encapsulating ceramides into liposomal aqueous interior with the aid of poly (lactic-coglycolicacid) (PLGA).
METHODS: BODIPY FL labeled ceramide (FL-ceramide) and BODIPY-TR labeled ceramide (TR-ceramide) were encapsulated into carboxy-terminated PLGA nanoparticles. The negatively charged PLGA nanoparticles were then encapsulated into cationic liposomes to obtain PLGA/liposome hybrids. As a control, FL-ceramide and/or TR ceramide co-loaded liposomes without PLGA were prepared. The release of ceramides from PLGA/liposome hybrids and liposomes in rat plasma, cultured MDA-MB-231 cells, and rat blood circulation was compared using fluorescence resonance energy transfer (FRET) between FL-ceramide (donor) and TR-ceramide (acceptor).
RESULTS: FRET analysis showed that FL-ceramide and TR-ceramide in liposomal lipid bilayer were rapidly released during incubation with rat plasma. In contrast, the FL-ceramide and TR-ceramide in PLGA/liposome hybrids showed extended release. FRET images of cells revealed that ceramides in liposomal bilayer were rapidly transferred to cell membranes. In contrast, ceramides in PLGA/liposome hybrids were internalized into cells with nanoparticles simultaneously. Upon intravenous administration to rats, ceramides encapsulated in liposomal bilayer were completely released in 2 min. In contrast, ceramides encapsulated in the PLGA core were retained in PLGA/liposome hybrids for 4 h.
CONCLUSIONS: The PLGA/liposome hybrid nanoparticles reduced in vitro and in vivo premature release of ceramides and offer a viable platform for targeted delivery of lipophilic drugs.

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Year:  2013        PMID: 24065591      PMCID: PMC4164208          DOI: 10.1007/s11095-013-1190-5

Source DB:  PubMed          Journal:  Pharm Res        ISSN: 0724-8741            Impact factor:   4.200


  33 in total

1.  Development of an in vitro drug release assay that accurately predicts in vivo drug retention for liposome-based delivery systems.

Authors:  Jennifer A Shabbits; Gigi N C Chiu; Lawrence D Mayer
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Review 2.  Regulation of ceramide production and apoptosis.

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4.  Erythrocyte membrane-cloaked polymeric nanoparticles for controlled drug loading and release.

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Journal:  Nanomedicine (Lond)       Date:  2013-02-14       Impact factor: 5.307

5.  Simultaneous quantitative determination method for sphingolipid metabolites by liquid chromatography/ionspray ionization tandem mass spectrometry.

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6.  Liposomal delivery enhances short-chain ceramide-induced apoptosis of breast cancer cells.

Authors:  Tom Stover; Mark Kester
Journal:  J Pharmacol Exp Ther       Date:  2003-09-15       Impact factor: 4.030

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Authors:  Jennifer A Shabbits; Lawrence D Mayer
Journal:  Anticancer Res       Date:  2003 Sep-Oct       Impact factor: 2.480

8.  Intracellular delivery of ceramide lipids via liposomes enhances apoptosis in vitro.

Authors:  Jennifer A Shabbits; Lawrence D Mayer
Journal:  Biochim Biophys Acta       Date:  2003-05-02

9.  Drug release characteristics of lipid based benzoporphyrin derivative.

Authors:  Rubinah K Chowdhary; Isha Shariff; David Dolphin
Journal:  J Pharm Pharm Sci       Date:  2003 Jan-Apr       Impact factor: 2.327

Review 10.  In vitro tests to predict in vivo performance of liposomal dosage forms.

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Journal:  Chem Phys Lipids       Date:  1993-09       Impact factor: 3.329

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  3 in total

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Journal:  Mol Cancer Ther       Date:  2019-10-23       Impact factor: 6.261

2.  Förster Resonance Energy Transfer-Based Stability Assessment of PLGA Nanoparticles in Vitro and in Vivo.

Authors:  Edyta Swider; Sanish Maharjan; Karlijne Houkes; Nicolaas Koen van Riessen; Carl Figdor; Mangala Srinivas; Oya Tagit
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3.  A Combined Antitumor Strategy Mediated by a New Targeted Nanosystem to Hepatocellular Carcinoma.

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