2014
DOI: 10.1016/j.jsps.2014.02.005
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Role of medium-chain fatty acids in the emulsification mechanistics of self-micro-emulsifying lipid formulations

Abstract: Potential SMEDDS formulations for the bioavailability enhancement of poorly water-soluble compounds were developed by mixing blends of {Miglyol 812/Imwitor 988} and Tagat TO as a non-ionic surfactant. 'Diffusion and stranding' appears to be the dominant mechanism of emulsification.

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Cited by 19 publications
(31 citation statements)
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“…These systems upon mild agitation in aqueous media form fine oil-in-water emulsions of droplet size of<5 µm in the case of SEDDS [1] or droplets with diameters between 5 and 140 nm in the case of SMEDDS [2]. It is proposed that enhancement in the water solubilisation region (L2) and the formation of interfacial liquid crystal on dilution with water are important to the mechanistic processes [3][4]. Furthermore, it is important in order to maximize the rate of absorption and thus bioavailability of oily formulations; one must maintain the drug in solution and avoid crystallization of the drug on dilution in the lumen of the gut [3,5,6].…”
Section: Introductionmentioning
confidence: 99%
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“…These systems upon mild agitation in aqueous media form fine oil-in-water emulsions of droplet size of<5 µm in the case of SEDDS [1] or droplets with diameters between 5 and 140 nm in the case of SMEDDS [2]. It is proposed that enhancement in the water solubilisation region (L2) and the formation of interfacial liquid crystal on dilution with water are important to the mechanistic processes [3][4]. Furthermore, it is important in order to maximize the rate of absorption and thus bioavailability of oily formulations; one must maintain the drug in solution and avoid crystallization of the drug on dilution in the lumen of the gut [3,5,6].…”
Section: Introductionmentioning
confidence: 99%
“…Self-emulsifying technology for oral delivery use has recently witnessed the introduction of many self-emulsifying microemulsion formulations [7] including; Neoral ® , originally marketed as 'Sandimmune™' (Cyclosporin A, calcineurin inhibitor; new drug application year NDA 1999), Norvir ® (Ritonavir, protease inhibitor; NDA 1996), Targretin ® (Bexarotene, protease inhibitor; NDA 1999), Rapamune ® (Sirolimus, mTOR kinase inhibitor: NDA 1999), Avodart ® (Dutasteride, 5 alpha-reductase inhibitor; NDA 2001, Aptivus ® (Tipranavir, protease inhibitor; NDA 2005), Amitiza ® (Lubiprostone, chloride channel activator; NDA 2006), Xtandi ® (Enzalutamide, androgen receptor inhibitor; NDA 2012) and Rayaldee ® (Calcifediol, vitamin D analog; NDA 2016). However, the design for effective selfmicro-emulsifying drug delivery systems (SMEDDS) needs through an understanding of the various key elements which influence emulsification and how these factors interplay to affect absorption [3][4]. Pouton [8][9] has suggested a classification system for lipidic formulations based on their dispersions characteristics, digestibility and the physicochemical characteristics of the formulation components; principally the HLB of the surfactants and % glycerides content.…”
Section: Introductionmentioning
confidence: 99%
“…According to the method developed by Hasan et al, [11,12], blends of various oils, co-surfactants and surfactants were accurately weighed into glass test tubes and then wrapped by cling film. Test tubes were heated in a water bath at 50 °C for 2 min before lipid mixtures were thoroughly vortexed.…”
Section: Self-emulsification Profiles Of Lipid Mixturesmentioning
confidence: 99%
“…In order to maximize the bioavailability of lipophilic drugs, key elements in the lipid composite have to be optimized which include; type of oil (LCT or MCT), oil-cosurfactant ratio and type of surfactant (HLB value) [11,37]. Fig.…”
Section: Self-micro-emulsifying Lipid Systemmentioning
confidence: 99%
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