• 산업식품공학
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• 제21권3호
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• pp.215-224
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• 2017

Resveratrol was incorporated into various combinations of single- and double-layer nanoemulsions, prepared by self-assembly emulsification and complex coacervation with chitosan, alginate, and ${\beta}$-cyclodextrin, respectively. Resveratrol nanoemulsions were composed of medium-chain trigacylglycerols (MCTs), $Tween^{(R)}$ 80, water, chitosan, alginate, and ${\beta}$-cyclodextrin. The corresponding mixtures were formulated for the purpose of being used as a nutraceutical delivery system. Resveratrol nanoemulsions were obtained with particle sizes of 10-800 nm, with the size variation dependent on the emulsification parameters including the ratio of aqueous phase and surfactant ratio. Resveratrol nanoemulsions were characterized by evaluating particle size, zeta-potential value, stability, and release rate. There were no significant changes in particle size and zeta-potential value of resveratrol nanoemulsions during storage for 28 days at $25^{\circ}C$. The stability of resveratrol in the double-layer nanoemulsions complexed with chitosan or ${\beta}$-cyclodextrin was higher, compared with the single-layer nanoemulsions.

• Biomolecules & Therapeutics
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• 제21권2호
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• pp.173-179
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• 2013

Objective of present study was to prepare and characterize self-nanoemulsifying drug delivery system (SNEDDS) of lutein and to evaluate its effect on bioavailability of warfarin. The SNEDDS was prepared using an oil, a surfactant, and co-surfactants with optimal composition based on pseudo-ternary phase diagram. Effect of the SNEDDS on the bioavailability of warfarin was performed using Sprague Dawley rats. Lutein was successfully formulated as SNEDDS for immediate self-emulsification and dissolution by using combination of Peceol as oil, Labrasol as surfactant, and Transcutol-HP or Lutrol-E400 as co-surfactant. Almost complete dissolution was achieved after 15 min while lutein was not detectable from the lutein powder or intra-capsule content of a commercial formulation. SNEDDS formulation of lutein affected bioavailability of warfarin, showing about 10% increase in $C_{max}$ and AUC of the drug in rats while lutein as non-SNEDDS did not alter these parameters. Although exact mechanism is not yet elucidated, it appears that surfactant and co-surfactant used for SNEDDS formulation caused disturbance in the anatomy of small intestinal microvilli, leading to permeability change of the mucosal membrane. Based on this finding, it is suggested that drugs with narrow therapeutic range such as warfarin be administered with caution to avoid undesirable drug interaction due to large amount of surfactants contained in SNEDDS.

• Food Science and Biotechnology
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• 제18권5호
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• pp.1161-1172
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• 2009

Food nanoemulsion systems consisting of water and oleoresin capsicum (OC), polyoxythylene sorbitan esters (Tween 20, 40, 60, and 80), propylene glycol (PG), sucrose monostearate (SM), and their corresponding mixtures were formulated to use as food vehicles. Tween 80 produced OC nanoemulsions with stable dispersions as one-phase systems, and the dertermined emulsification efficiencies clearly distinguished the ability of the various surfactants to emulsify OC. The nanoemulsions were prepared by both ultrasonication and self-assembly, and the nanoemulsion areas were determined using phase diagrams by measuring the sizes of the emulsions. One-phase nanoemulsions were presented, with a multiple cloudy region and phase separation that were dependent on the particle size of the emulsion. The OC nanoemulsions prepared by ultrasonication using systems of OC/Tween 80/water, OC/Tween 80/water+PG, and OC/Tween 80/water+SM, resulted in particle sizes ranging from 15 to 100 nm. Finally, the nanoemulsions maintained their initial sizes during storage, ranging from 65 to 92 nm.

• Journal of Pharmaceutical Investigation
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• 제37권6호
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• pp.339-347
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• 2007

SMEDDS is mixture of oils, surfactants, and cosurfactants, which are emulsified in aqueous media under conditions of gentle agitation and digestive motility that would be encountered in the gastro-intestinal(GI) tract. The main purpose of this work is to prepare self-microemulsifying drug delivery system(SMEDDS) for oral bioavailability enhancement of a poorly water soluble drug, atorvastatin calcium. Solubility of atorvastatin calcium was determined in various vehicles. Pseudo-ternary phase diagrams were constructed to identity the efficient self-emulsification region and particle size distributions of the resultant micro emulsions were determined using a laser diffraction sizer. Optimized formulations for in vitro dissolution and bioavailability assessment were $Capryol^{(R)}$ 90(50%), Tetraglycol(16%), and $Cremophor^{(R)}$ EL(32%). The release rate of atorvastatin from SMEDDS was significantly higher than the conventional tablet ($Lipitor^{(R)}$), 2-fold. Our studies illustrated the potential use of SMEDDS for the delivery of hydrophobic compounds, such as atorvastatin calcium by the oral route.

• Journal of Pharmaceutical Investigation
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• 제32권4호
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• pp.267-275
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• 2002

A self-microemulsifying drug delivery system (SMEDDS) was developed to increase the dissolution rate, solubility, and ultimately bioavailability of a poorly water soluble drug, lovastatin. SMEDDS was thε mixtures of oils, surfactants, and cosurfactants, which emulsify under conditions of gentle agitation, similar to those which would be encountered in the gastro-intestinal (GI) tract. Various types of self-emulsifying formulations were prepared using four types of oil (Capryol 90, Lauroglycol 90, Labrafil M 1944 CS and Labrafil M 2125), two surfactants (Cremophor EL and Tween 80), and three cosurfactants (Carbitol, PEG 400 and propylene glycol). Thε efficiency of emulsification was studied using a laser diffraction size analyzer to determine particle size distributions of the resultant emulsions. Optimized formulations selected for bioavailability assessment were Carpryol 90 (40%), Cremophor EL (30%) and Carbitol (30%). SMEDDS containing lovastatin (20 mg and 5 mg) were compared to a conventional lovastatin tablet $(Mevacor^{\circledR},\;20\;mg/tab)$ by the oral administration as prefilled hard gelatin capsules to fasted beagle dogs for in vivo study. The arεa under the serum concentration-time curve from time zero to the last measured time in serum, $AUC_{0{\rightarrow}24h}$, was significantly greater in SMEDDS, suggesting that bioavailability increase 130% and 192% by the SMEDDS, respectively. The self-emulsifying formulations of lovastatin afforded the improvement in absolute oral bioavailability relative to previous data of lovastatin tablet formulation. These data indicate the utility of dispersed self-emulsifying formulations for the oral delivery of lovastatin and potentially other poorly absorbed drugs.

• 대한화학회지
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• 제50권6호
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• pp.464-470
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• 2006

약물인 덱사메타손은 효과적인 염증치료제이다. 그러나 난용성 약물로써 수용액에서 주사제로 가용화가 어렵다. 따라서 º ¿±¸에서는 ¸Þ¸손을 수용액상에서 주사제로 가용화하기 §Ø¼­ 지질로 만들어진 나노입자에 ¸Þ¸손을 봉입하여 체내투여 시 약물을 서서히 방출할 수 ´ 약물전달체를 제조하고자 ¿´´. 지질나노입자는 인지질, 콜레스테롤 ±×¸?簾? 양이온성 지질을 사용하여 자발 유화 ¿매확산법에 의해 제조하였다. ³ª노입자는 다양한 지질 종류와 지질의 함량에 따라서 봉입효율, 기 그리고 표면전하와 °°º ¹°리적 특성을 평가하였다. 기는 80~120 nm ¿´¸¸, 봉입효율은 80% 이상의 높은 효율을 보였다. 질의 지방쇄의 길이가 ±æ¼· 봉입효율은 증가하였고, 콜레스테롤의 량과 봉입효율은 반비례하였다. 나노지질입자는 양이온성 지질 없이는 형성되지 않았으며 ¾온성 지질의 ·?閻?¡ 따라서 봉입효율은 °¡하였다. 덱사메타손이 봉입된 지질나노입자는 난용성 약물을 주사제로 가용화 수 ´ 새로운 약물전달체로써의 가능성을 기대하는 바이다.

• 대한화장품학회지
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• 제32권3호
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• pp.149-152
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• 2006

천연물 유래의 잇꽃 oleosomes은 미래 에너지 자원으로 사용되며 씨 안쪽에 트리그리세라이드를 저장한 작고($1{\sim}3{\mu}m$) 둥근 모양의 저장소이다. Oleosome의 표면은 고분자의($20{\sim}24$ KDa) oleosin 단백질로 덮여 있으며 유화 특성을 나타낸다. 전통적으로, 잇꽃처럼 오일을 내포하고 있는 씨앗의 Oleosomes은 내부에 있는 오일을 분리하기 위하여 단순히 분쇄하는 방법을 사용하였다. 특허 받은 DermaSphere 기술은 손상되지 않은 상태의 oleosomes의 분리가 가능하다. 분리된, 이 원료는 일반적으로 잇꽃 오일과 관련된 피부 유연제, 보습제, 산화 방지제들을 전달하는 제형에 사용될 수 있다. 그러나, 현재의 에멀젼화된 oleosin 단백질이 둥근 오일 바디를 덮고 있기 때문에, oleosomes은 전형적인 oil-in-water (O/W) 유상액에서 다른 oil phase를 에멀젼화할 뿐만 아니라 자기 유화 특성도 가지고 있다. Oleosomes은 화장품 제형에서 유상의 비 활성 부분으로 역할을 하고 있다. 천연 oleosomes은 다양한 유상 활성 성분들을 포집할 수 있으며 화장품 효능 증진을 위한 전달 시스템으로 사용 될 수 있다. 또한, Oleosomes은 방향제, 비타민, 방충제, UV chromophores 같은 다양한 물질들을 포집 할 수 있었다. 이러한 oleosomes은 제품내에 있는 활성물질들을 보호하거나, 시간이 경과에 따른 활성물질의 적절한 방출을 제어하는데 사용 될 수 있다.

• 대한화장품학회지
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• 제39권1호
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• pp.55-63
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• 2013

경피흡수 증진의 수단으로 나노에멀젼의 화장품 응용이 관심의 대상이 되고 있다. 본 연구에서는 저에너지 유화법으로 제조된 나노에멀젼 구성 원료들의 조성을 달리하여 안정성을 확인해 보고자 하였다. 시간 경과에 따른 나노에멀젼의 입자 크기 측정을 통한 안정성 실험 결과, 폴리올을 수상에 첨가한 경우 에탄올상 첨가에 비해 안정성이 크게 증가하였다. 에탄올상의 수상에 대한 첨가속도는 입자 크기나 안정성에 큰 영향이 없었다. 오일의 종류에 따라서도 안정성에는 영향이 없었으나 초기에 형성되는 입자 크기는 오일의 분자량과 polarity에 상관관계를 보이는 것으로 생각되었다. 폴리올의 종류에 따른 안정성과 초기 입자 크기는 1,2 헥산디올을 제외하고는 유사한 경향을 보였다. 오일과 계면활성제 농도 변화는 제조된 나노에멀젼의 초기 입자 크기에는 영향을 주었으나 시간 경과에 따른 변화는 없었다. 에탄올의 농도 변화는 초기 입자 크기와 안정성에 큰 영향을 미치는 것으로 관찰되었다.

• Journal of Pharmaceutical Investigation
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• 제41권2호
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• pp.103-109
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• 2011

The objective of the study was to prepare self-microeulsifying drug delivery system (SMEDDS) incorporating atorvastatin calcium and evaluate its properties and oral bioavailability. Solubility of atorvastatin in various vehicles was determined. Pseudo-ternary phase diagrams were constructed to identify the good self-emulsification region. The droplet size distributions of the resultant emulsions were determined by dynamic light scattering measurement. The mean droplet size of chosen formulation (20% ethyl oleate, 40% tween-80, 40% Carbitol$^{(R)}$) was $23.4{\pm}1.3$ nm. The SMEDDS incorporating atorvastatin calcium appeared to be associated with better performance in dissolution and pharmacokinetic studies, compared with raw atorvastatin calcium. In dissolution test, the release percentage of atorvastatin from SMEDDS mixture could rapidly reach more than 95% within 3 min. Oral $AUC_{0{\rightarrow}8hr}$ values in SD rats was $1994{\pm}335\;ng{\cdot}hr/mL$, which significantly increased (P<0.05) compared with raw atorvastatin calcium. The SMEDDS formulation was relatively stable when stored at $4^{\circ}C$ during 3 months. Our studies illustrated the potential use of SMEDDS for the delivery of hydrophobic compounds, such as atorvastatin, by the oral route.

• 대한화장품학회지
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• 제38권3호
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• pp.201-207
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• 2012

Oil-in-ethanol (O/E) 마이크로에멀젼을 물에 희석하여 얻은 O/W 나노에멀젼의 성질에 대하여 다른 희석 과정의 영향을 연구하였다. 물/에탄올/비이온성계면활성제/실리콘 오일 계를 모델 계로 선택하였다. 희석과정은 물(또는 마이크로에멀젼)을 마이크로에멀젼(또는 물)에 단계별로 첨가하는 방법으로 구성되었다. O/E 마이크로에멀젼을 물에 첨가하여 혼합하면 30 nm 정도의 입경을 가진 나노에멀젼을 얻을 수 있었다. 반면에 물을 O/E 마이크로에멀젼에 첨가하면 400 nm의 입경을 가진 에멀젼을 얻을 수 있다. 희석 방법이 얻어지는 에멀젼의 성질에 중요한 역할을 하였다. 시간에 따른 나노에멀젼의 입자 변화는 관찰되지 않았으나 입자가 큰 에멀젼은 시간에 따라 입경이 증가하였으며 불안정화 기작은 오스트왈드 라이퍼닝으로 추정되었다.