Role of medium-chain fatty acids in the emulsification mechanistics of self-micro-emulsifying lipid formulations

Hasan, Naser M. Y.

doi:10.1016/j.jsps.2014.02.005

Cited by 19 publications

(31 citation statements)

References 23 publications

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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%

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Role of Hydrophilic Surfactants in the Emulsification Mechanistics of Type Iii Self-Micro-Emulsifying Drug Delivery Systems (Smedds)

Hasan

2019

Int J App Pharm

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Objective: Evaluation of the self-emulsifying behaviour of type III lipid systems comprising mixed medium chain glycerides (Miglyol 812-Imwitor 988) and wide range of hydrophilic surfactants in an attempt to identify self-emulsifying microemulsion formulations, prevaricate the crystallization tendency of Cremophor RH40 in the pre-microemulsion concentrate, to shed some light on the mechanistic behavior of these systems after aqueous dispersion. Methods: Non-ionic surfactants with HLB in the range 14 to 16.5 are investigated amongst these are; Cremophor RH40, Cremophor EL, Crillet 4 (polysorbate 80), Crillet 1 (polysorbate 20) and Tagat O2. Optimum oil blends of Miglyol 812-Imwitor 988 and various non-ionic surfactant systems were verified using self-emulsification performance studies, oil droplet diameter measurements and dynamic equilibrium phase studies. Results: Oil blends of Miglyol 812 as an oil and Imwitor 988 as a cosurfactant were optimized for microemulsion systems at ratios of 1:1 in the case of Cremophor RH40 or EL, and at 2:3 in the case of Crillet 4 or Tagat O2. In order to obtain small droplet size and fast dispersion rate for type III lipid systems, hydrophilic surfactants with HLB values between 13 and 15 were found to be the optimum. Conclusion: Spontaneous micro-emulsification in type III lipid system was attributed to the “diffusion and stranding” theory. Yet, the formation of liquid crystalline phases as intermediate phases during dilution of the oil formulation with water appears to be quintessential for the mechanistics of emulsification regardless type of lipid class system.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Role of Hydrophilic Surfactants in the Emulsification Mechanistics of Type Iii Self-Micro-Emulsifying Drug Delivery Systems (Smedds)

Hasan

2019

Int J App Pharm

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“…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%

“…In order to facilitate formulation design of lipid systems, they were classified by Pouton [10] into type I, II and III and IV according to the hydrophilicity of oil mixture, oil droplet size after aqueous dispersion and digestion by bile salts. One advantage which, both SEDDS and SMEDDS have over solid dosage formulations is, the avoidance of slow and incomplete drug dissolution as they can facilitate the formation of solubilised phases from which absorption may occur [11,12]. Nonetheless, formulation design of self-emulsifying lipid technology has some disadvantages including; possible interaction between the filling and the capsule shell, precipitation of either active ingredient and/or oil constituents as influenced by storage temperature, besides high manufacturing cost [13,14].…”

Section: Introductionmentioning

confidence: 99%

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Smedds Tablet: Compatability of Solid Smedds Using Various Pharmaceutical Tablet Excipients

Hasan

Almalki

Althuwaybi

et al. 2016

Int J Pharm Pharm Sci

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Objective: There are many successful products on the market which are the culmination of the self-micro-emulsification lipid technology applications. Despite the importance of lipid-based formulations, these systems have some limitations including; stability, complexity during large scale manufacturing process and limited dosage forms to such as soft gelatin capsule. In order to overcome these limitations, the prospect of converting self-micro-emulsifying drug delivery systems (SMEDDS) into tablet dosage form was investigated in this study. Methods:A self-micro-emulsifying oil formulation representing type III A lipid class composed of glycerox 767HC/croduret 40 ss at ratios of (80/20) was converted into solid SMEDDS using solid carrier adsorption method. Powder blends containing magnesium trisilicate hydrate (MTSH) or magnesium lluminum silicate (MAS) at various oil loading factors were mixed with MCC with and without various binders and compressed into tablets using a fixed loading force of approximately of 5 KN. Hardness profiles of these oil loaded tablets were then analyzed. Results:Powder compacts which contained MTSH with and without SMEDDS oil had shown relatively better compaction properties than MAS. Adding SMEDDS oil solution to either MTSH or MAS at ratios of 1:9 has relatively reduced tablets hardness by almost 2 or 4 folds, respectively. Conclusion:Progressive inclusion of increasing amounts of SMEDDS oil solution adsorbed unto the solid carrier has incurred a further reduction in the hardness of SMEDDS tablets. It appears that manufacturing of tablet SMEDDS can only be attainable for highly potent drugs as minimal amounts of oil solution added to the powder blends can adversely affect the mechanical strength of compressed tablet.

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Nanolipid Materials for Drug Delivery Systems

Negi

2019

Characterization and Biology of Nanomaterials for Drug Delivery

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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.

Cited by 19 publications

References 23 publications

Role of Hydrophilic Surfactants in the Emulsification Mechanistics of Type Iii Self-Micro-Emulsifying Drug Delivery Systems (Smedds)

Role of Hydrophilic Surfactants in the Emulsification Mechanistics of Type Iii Self-Micro-Emulsifying Drug Delivery Systems (Smedds)

Smedds Tablet: Compatability of Solid Smedds Using Various Pharmaceutical Tablet Excipients

Nanolipid Materials for Drug Delivery Systems

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