Transdermal Film Loaded with Avanafil Ultra-deformable Nanovesicles to Enhance its Percutaneous Absorption and Bioavailability

被引:3
作者
Al-hejaili, Omar D. [1 ]
Alamoudi, Abdullah A. [1 ]
Ahmed, Osama A. A. [1 ]
El-Say, Khalid M. [1 ]
机构
[1] King Abdulaziz Univ, Fac Pharm, Dept Pharmaceut, Jeddah 21589, Saudi Arabia
关键词
avanafil; transfersomes; transdermal delivery; skin permeation; pharmacokinetic parameters; ERECTILE DYSFUNCTION; IN-VITRO; LIPID VESICLES; DELIVERY; VIVO; OPTIMIZATION; SYSTEMS; FORMULATION; EFFICACY; CARRIERS;
D O I
10.1208/s12249-021-02195-4
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
The in vitro dissolution of Avanafil (AVA) is the rate-limiting step for its bioavailability. Also, it undergoes the first-pass metabolism, and its absorption is altered significantly in the presence of food. So, our study aimed to overcome the previous hurdles and improve the AVA bioavailability by its incorporation in the ultra-deformable nanovesicles, transfersomes (TRF), then loading these nanovesicles in transdermal films. The AVA-loaded TRF formulation was optimized using Draper-Lin small composite design (D-LSCD). The optimized AVA-loaded TRF was evaluated for quality attributes and assessed for skin permeation using a fluorescence laser microscope and for pharmacokinetic parameters after topical application on the rats. The optimized AVA-loaded TRF showed a vesicle size of 97.75 nm, a zeta potential of -28.83 mV, and entrapment efficiency of 95.14% with good deformability and release profile. The intense discoloration in the deep skin layers of the rats indicated the permeation efficiency of AVA-loaded TRF films. The pharmacokinetic parameters specified the augmented absorption extent with C-max of 254.66 +/- 8.02 ng/mlversus 7033 +/- 3.05 ng/ml which reflected on the AUC(0-inf) that has a value of 2050.45 +/- 159.14 ng/ml h versus 49734 +/- 102.61 ng/ml h for the optimized AVA-loaded TRF film and raw AVA-loaded film, respectively. These promising results wide open the field for broader clinical application of this alternative delivery pathway for superior bioavailability, efficacy, and patient compliance and satisfaction.
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页数:14
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