Cubosomes as Targeted Drug Delivery Systems - A Biopharmaceutical Approach

Lakshmi, Naga M.; Yalavarthi, Prasanna Raju; Vadlamudi, Harini Chowdary; Thanniru, Jyotsna; Yaga, Gowri; K, Haritha

doi:10.2174/1570163811666140505125923

Cited by 33 publications

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“…Cubosomes, nanostructured particles of bicontinuous cubic liquid crystalline phase, are formulated easily by a hydrating mixture of glyceryl-monooleate and poloxamer 407. The cubic phase produces colloidal and thermodynamically stable particulate dispersions [ 15 , 16 ]. Cubosomes have many benefits, such as high drug encapsulating and loading ability of hydrophilic and hydrophobic active pharmaceutical ingredients (APIs), simple preparation techniques, lipids biodegradability, and both sustained and targeted release of drugs [ 15 , 16 , 17 , 18 ].…”

Section: Introductionmentioning

confidence: 99%

Bioavailability and Antidiabetic Activity of Gliclazide-Loaded Cubosomal Nanoparticles

et al. 2021

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In this study, gliclazide-loaded cubosomal particles were prepared for improving the oral bioavailability and antidiabetic activity of gliclazide. Four formulations of gliclazide-loaded cubosomal nanoparticles dispersions were prepared by the emulsification method using four different concentrations of glyceryl monooleate (GMO) and poloxamer 407 (P407) as the stabilizer. The prepared formulations were in vitro and in vivo evaluated. In vitro, the prepared gliclazide-loaded cubosomal dispersions exhibited disaggregated regular poly-angular particles with a nanometer-sized particle range from 220.60 ± 1.39 to 234.00 ± 2.90 nm and entrapped 73.84 ± 3.03 to 88.81 ± 0.94 of gliclazide. In vitro gliclazide release from cubosomal nanoparticles revealed an initially higher drug release during the first 2 h in acidic pH medium; subsequently, a comparatively higher drug release in alkaline medium relative to gliclazide suspension was observed. An in vivo absorption study in rats revealed a two-fold increase in the bioavailability of gliclazide cubosomal formulation relative to plain gliclazide suspension. Moreover, the study of in vivo hypoglycemic activity indicated that a higher percentage reduction in glucose level was observed after the administration of gliclazide cubosomal nanoparticles to rats. In conclusion, gliclazide-loaded cubosomal nanoparticles could be a promising delivery system for improving the oral absorption and antidiabetic activity of gliclazide.

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Section: Introductionmentioning

confidence: 99%

Bioavailability and Antidiabetic Activity of Gliclazide-Loaded Cubosomal Nanoparticles

et al. 2021

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“…Cubosomes are formed from lipid cubic phases and have gained much attention for drug delivery purposes. [17][18][19] For structure, monoolein and phytantriol are commonly employed as lipids in cubosomes. 20 Cubosomes have been reported to enhance the solubility and bioavailability of drugs by various routes of administration including intranasal deliver to target the brain.…”

Section: Introductionmentioning

confidence: 99%

<p>Nanosized Cubosomal Thermogelling Dispersion Loaded with Saquinavir Mesylate to Improve Its Bioavailability: Preparation, Optimization, in vitro and in vivo Evaluation</p>

Hosny¹

2020

IJN

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Background: Low bioavailability and poor permeability of the blood-brain barrier are problematic when delivering therapeutic agents and particularly anti-human immunodeficiency virus therapy to the central nervous system. The intranasal route offers an alternative for central nervous system delivery. Cubosomes have been reported as helpful vehicles for intranasal delivery of therapeutics to enable brain targeting. Objective: In this study, we aimed to develop the intranasal cubosomal thermogelling dispersion of saquinavir mesylate for central nervous system delivery. Methods: The Box-Behnken design was applied to study the effect of monoolein, Poloxamer 407, and polyvinyl alcohol as independent factors and the particle size, entrapment efficiency, gelation temperature, and stability index as responses. The optimized cubosomes were evaluated using transmission electron microscopy, ex vivo permeation, and in vivo pharmacokinetics. Results: The optimized formula consisting of monoolein (8.96%), Poloxamer 407 (17.45%), and polyvinyl alcohol (7.5%) was prepared and evaluated. Higher values for the steady-state flux, permeability coefficient, and enhancement factor were observed for the cubosomal thermogelling dispersion of saquinavir during ex vivo permeation in comparison with an aqueous suspension of saquinavir. From the pharmacokinetic profile, the relative bioavailability for the intranasal optimized formula was approximately 12-fold higher when compared with oral aqueous suspension and 2.5-fold greater when compared to the intranasal aqueous suspension of saquinavir. Conclusion: Overall, the saquinavir-loaded cubosomal thermogelling formulation is promising for central nervous system delivery by intranasal administration.

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“…Like their lamellar counterparts, engineered cubosomes are expected to find use in the pharmaceutical industry as delivery vehicles, their higher membrane surface area making them ideal structures for hydrophobic cargo transport and release. 50,[58][59][60] Some work has gone into cubosomal formulations with encapsulated gene-silencing RNA and other functional peptides, displaying exceptionally well-controlled diffusion rates. [61][62][63] Cubosomes have been shown to provide a certain degree of in vivo protection to biomolecules that would otherwise be sensitive to enzymatic degradation, highly advantageous in the delivery of immunogenic therapeutics.…”

Section: Cubosomesmentioning

confidence: 99%

Microfluidic technologies for the synthesis and manipulation of biomimetic membranous nano-assemblies

Pilkington

Seddon

Elani

2021

Phys. Chem. Chem. Phys.

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Cubosomes as Targeted Drug Delivery Systems - A Biopharmaceutical Approach

Cited by 33 publications

References 0 publications

Bioavailability and Antidiabetic Activity of Gliclazide-Loaded Cubosomal Nanoparticles

Bioavailability and Antidiabetic Activity of Gliclazide-Loaded Cubosomal Nanoparticles

<p>Nanosized Cubosomal Thermogelling Dispersion Loaded with Saquinavir Mesylate to Improve Its Bioavailability: Preparation, Optimization, in vitro and in vivo Evaluation</p>

Microfluidic technologies for the synthesis and manipulation of biomimetic membranous nano-assemblies

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