Poloxamer 407-based intranasal thermoreversible gel of zolmitriptan-loaded nanoethosomes: formulation, optimization, evaluation and permeation studies

被引:68
作者
Shelke, Santosh [1 ,4 ]
Shahi, Sadhana [2 ]
Jalalpure, Sunil [3 ,4 ]
Dhamecha, Dinesh [3 ,4 ]
机构
[1] Yash Inst Pharm, Dept Pharmaceut, Aurangabad 431134, Maharashtra, India
[2] Govt Coll Pharm, Dept Pharmaceut, Aurangabad, Maharashtra, India
[3] KLE Univ, Coll Pharm, Belagavi, Karnataka, India
[4] KLE Univ, Dr Prabhakar Kore Basic Sci Res Ctr, Belagavi, Karnataka, India
关键词
Ethosomes; factorial design; intranasal; poloxamer; thermoreversible gel; Zolmitriptan; IN-SITU GEL; DELIVERY; RELEASE;
D O I
10.3109/08982104.2015.1132232
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Zolmitriptan is the drug of choice for migraine, but low oral bioavailability (<50%) and recurrence of migraine lead to frequent dosing and increase in associated side effects. Increase in the residence time of drug at the site of drug absorption along with direct nose to brain targeting of zolmitriptan can be a solution to the existing problems. Hence, in the present investigation, thermoreversible intranasal gel of zolmitriptan-loaded nanoethosomes was formulated by using mucoadhesive polymers to increase the residence of the drug into the nasal cavity. The preparation of ethosomes was optimized by using 3(2) factorial design for percent drug entrapment efficiency, vesicle size, zeta potential, and polydispersity index. Optimized formulation E6 showed the vesicle size (171.67nm) and entrapment efficiency (66%) when compared with the other formulations. Thermoreversible gels prepared by using poloxamer 407 showed the phase transition temperature at 32-33 degrees C which was in line with the nasal physiological temperature. The optimized ethosomes were loaded into the thermoreversible mucoadhesive gel optimized by varying concentrations of poloxamer 407, carbopol 934, HPMC K100, and evaluated for gel strength, gelation temperature, mucoadhesive strength, in vitro drug release, and ex vivo drug permeation, where G3 and G6 were found to be optimized formulations. In vitro drug release was studied by different kinetic models suggested that G3 (n=0.582) and G6 (n=0.648) showed Korsemeyer-Peppas (K-KP) model indicating non-Fickian release profiles. A permeation coefficient of 5.92 and 5.9 mu g/cm(2) for G3 and G6, respectively, revealed very little difference in release rate after 24h between both the formulations. Non-toxic nature of the gels on columnar epithelial cells was confirmed by histopathological evaluation.
引用
收藏
页码:313 / 323
页数:11
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