Solid lipid microparticles: formulation, preparation, characterisation, drug release and applications

Jaspart, Séverine; Piel, Géraldine; Delattre, Luc; Évrard, Brigitte

doi:10.1517/17425247.2.1.75

Cited by 162 publications

(128 citation statements)

References 44 publications

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“…The first strategy is depot formulations, which provide an extended drug payout from the site of administration into the systemic circulation, using polymeric and lipid microparticulate systems, in-situ depotforming systems and implants (refer to reviews [17][18][19]) that allow proteins and peptides ("the active drug") to be continuously released from the subcutaneous tissue for extended periods of time at sufficiently high concentrations to exert pharmacological activity. In general, therapeutic peptides or proteins in this approach require limited or no molecular engineering, as ideally the depot formulation protects against metabolism, and renal clearance is overcome by constantly releasing the peptide or protein into the circulation [17][18][19].…”

Section: Half-life Extension Technologiesmentioning

confidence: 99%

“…In general, therapeutic peptides or proteins in this approach require limited or no molecular engineering, as ideally the depot formulation protects against metabolism, and renal clearance is overcome by constantly releasing the peptide or protein into the circulation [17][18][19]. One example of an extended-release formulation of a small peptide is Exenatide extendedrelease (ER) (Bydureon ® , Astra Zeneca, for type 2 diabetes mellitus) for once weekly subcutaneous administration.…”

Section: Half-life Extension Technologiesmentioning

confidence: 99%

See 1 more Smart Citation

A New Approach to Drug Therapy: Fc-Fusion Technology

Pechtner¹,

Ca²,

Le³

et al. 2017

Primary Health Care

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Section: Half-life Extension Technologiesmentioning

confidence: 99%

Section: Half-life Extension Technologiesmentioning

confidence: 99%

A New Approach to Drug Therapy: Fc-Fusion Technology

Pechtner¹,

Ca²,

Le³

et al. 2017

Primary Health Care

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“…In this case, solid lipid particles are smaller than the initial oil droplets, whereas with a temperature-controlled emulsification, solid lipid microparticles are of the same size as the initial oil droplets. Watersoluble substances can be encapsulated by forming a W/O/W prior to solvent evaporation or cooling (Jaspart et al 2005).…”

Section: Micellization Ppmentioning

confidence: 99%

Encapsulation Techniques

Vladisavljević

2016

Encyclopedia of Membranes

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“…Solid lipid microparticles (SLMs) were developed in early 1990s and have since been considered to be promising drug carrier systems, especially with a view to give the incorporated active substance a sustained release profile (Jaspart et al, 2005;Pilaniya et al, 2011;Obitte et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

Formulation development and evaluation of the anti-malaria properties of sustained release artesunate-loaded solid lipid microparticles based on phytolipids

et al. 2014

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Contexts: Artemisinins and its derivatives are considered the basis in the treatment of Plasmodium falciparum malaria due to their high potency and rapid action. However, they have short half life, low solubility, and poor oral bioavailability, hence the need to formulate sustained release lipid particulate dosage form of these drugs. Objectives: To formulate and evaluate artesunate-loaded solid lipid microparticles (SLMs) based on structured lipid matrices consisting of soybean oil and dika wax. Materials and methods: The lipid matrices were characterized by differential scanning calorimetry (DSC), small-angle X-ray diffraction (SAXD), and wide-angle X-ray diffraction (WAXD). The SLMs were prepared by hot melt-homogenization. Time-dependent particle size analysis, time-dependent pH stability studies, encapsulation efficiency (EE%), and in vitro drug release were carried out on the SLMs. In vivo anti-malarial studies were performed using a modified Peter's 4-day suppressive protocol using Plasmodium berghei infected mice. Results and discussion: Thermograms of the lipid matrices showed modifications in the microstructure of dika wax as a result of inclusion of soybean oil. SAXD and WAXD diffractograms showed that the lipid matrices were found to be non-lamellar. Particle size of SLM increased with time, while the pH was almost constant. The SLMs had maximum EE% of 80.6% and sustained the release of artesunate more than the reference tablet. In vivo pharmacodynamic studies showed that the SLMs had significant (p50.05) reduction in parasitaemia compared with reference tablet. Conclusion: Artesunate-loaded SLMs could be used once daily in the treatment of malaria.

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Solid lipid microparticles: formulation, preparation, characterisation, drug release and applications

Cited by 162 publications

References 44 publications

A New Approach to Drug Therapy: Fc-Fusion Technology

A New Approach to Drug Therapy: Fc-Fusion Technology

Encapsulation Techniques

Formulation development and evaluation of the anti-malaria properties of sustained release artesunate-loaded solid lipid microparticles based on phytolipids

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