Liquid Lipids Act as Polymorphic Modifiers of Tristearin-Based Formulations Produced by Melting Technologies

被引:24
作者
Bertoni, Serena [1 ]
Passerini, Nadia [1 ]
Albertini, Beatrice [1 ]
机构
[1] Univ Bologna, Dept Pharm & BioTechnol, Via S Donato 19-2, I-40127 Bologna, Italy
关键词
spray congealing; lipid microparticles; triacylglycerol; drug release; stability; polymorphism; SATURATED MONOACID TRIGLYCERIDES; DRUG-RELEASE; BINARY-MIXTURES; MILK-FAT; BEHAVIOR; CRYSTALLIZATION; STABILITY; NANOPARTICLES; NANOSCALE; SYSTEM;
D O I
10.3390/pharmaceutics13071089
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Despite the growing interest in lipid-based formulations, their polymorphism is still a challenge in the pharmaceutical industry. Understanding and controlling the polymorphic behavior of lipids is a key element for achieving the quality and preventing stability issues. This study aims to evaluate the impact of different oral-approved liquid lipids (LL) on the polymorphism, phase transitions and structure of solid lipid-based formulations and explore their influence on drug release. The LL investigated were isopropyl myristate, ethyl oleate, oleic acid, medium chain trigycerides, vitamin E acetate, glyceryl monooleate, lecithin and sorbitane monooleate. Spray-congealing was selected as an example of a melting-based solvent-free manufacturing method to produce microparticles (MPs) of tristearin (Dynasan(R)118). During the production process, tristearin MPs crystallized in the metastable alpha-form. Stability studied evidenced a slow phase transition to the stable beta-polymorph overtime, with the presence of the alpha-form still detected after 60 days of storage at 25 degrees C. The addition of 10% w/w of LL promoted the transition of tristearin from the alpha-form to the stable beta-form with a kinetic varying from few minutes to days, depending on the specific LL. The combination of various techniques (DSC, X-ray diffraction analysis, Hot-stage polarized light microscopy, SEM) showed that the addition of LL significantly modified the crystal structure of tristearin-based formulations at different length scales. Both the polymorphic form and the LL addition had a strong influence on the release behavior of a model hydrophilic drug (caffeine). Overall, the addition of LL can be considered an interesting approach to control triglyceride crystallization in the beta-form. From the industrial viewpoint, this approach might be advantageous as any polymorphic change will be complete before storage, hence enabling the production of stable lipid formulations.
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页数:24
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