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Formulation of avanafil in a solid self-nanoemulsifying drug delivery system for enhanced oral delivery

机译:在固体自纳米乳化药物递送系统中配制阿伐那非以增强口服递送

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摘要

Avanafil was incorporated into solid self-nanoemulsifying systems with the aim of improving its oral bioavailability. Labrafil, Labrafac, and Miglyol 812 N were investigated as oils, Tween 80 and Cremophor EL as surfactants, and Transcutol HP as a co-surfactant. Nine formulations produced clear solutions of 13.89-38.09 nm globules after aqueous dilution. Adsorption of preconcentrate onto Aeroperl 300 Pharma at a 2:1 ratio had no effect on nanoemulsion particle size. Differential scanning calorimetry, X-ray diffraction, and scanning electron microscopy indicated that avanafil was molecularly dispersed within the solid nanosystems. A formulation containing 10% Labrafil, 60% Tween 80, and 30% Transcutol HP had the highest drug loading (44.48 mg/g) and an acceptable in vitro dissolution profile (96.42% within 30 min). This formulation was chemically and physically stable for 6 months under accelerated storage conditions and it produced a 3.2-fold increase in bioavailability in rabbits, as compared to conventional commercially available avanafil tablets (Spedra (R)). (C) 2016 Elsevier B.V. All rights reserved.
机译:为了提高口服生物利用度,将Avanafil掺入固体自纳米乳化系统中。研究了Labrafil,Labrafac和Miglyol 812 N作为油类,研究了Tween 80和Cremophor EL作为表面活性剂,以及Transcutol HP作为辅助表面活性剂。九种制剂在水稀释后产生13.89-38.09 nm小球的澄清溶液。将预浓缩物以2:1的比例吸附到Aeroperl 300 Pharma上对纳米乳液的粒径没有影响。差示扫描量热法,X射线衍射和扫描电子显微镜表明,avanafil分子分散在固体纳米系统中。包含10%Labrafil,60%Tween 80和30%Transcutol HP的制剂具有最高的药物载量(44.48 mg / g)和可接受的体外溶出曲线(30分钟内为96.42%)。与常规的市售avanafil片剂(Spedra)相比,该制剂在加速的储存条件下在化学和物理上稳定了6个月,并且在兔子中产生了3.2倍的生物利用度增加。 (C)2016 Elsevier B.V.保留所有权利。

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