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Enhanced ocular bioavailability of fluconazole from niosomal gels and microemulsions: formulation, optimization, and in vitro-in vivo evaluation

机译:从憩室凝胶和微乳液中增强氟康唑的眼部生物利用度:配方,优化和体内体内评价

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摘要

Fungal keratitis may cause vision loss if it is not treated. Methods other than ocular delivery exhibited several limitations. No previous studies investigated and compared ocular bioavailability of fluconazole (FLZ) from niosomal gels and microemulsions. Niosomal gels of FLZ (0.3% w/w) based on Span((R)) 60 and cholesterol (CH) using 1% w/w carbopol((R)) 934 (CP) were evaluated. FLZ microemulsions (0.3% w/v) containing isopropyl myristate (IPM, as oil phase) and a 3:1 mixture of Tween((R)) 80 (as surfactant) and polyethylene glycol 400 (PEG 400, as cosurfactant) were characterized. Optimized formulations were compared for their ocular bioavailability in rabbit's. Nanoscopic niosomes (63.67-117.13 nm) and microemulsions (57.05-59.93 nm) showed respective negative zeta potential ranges of -45.37 to -61.40 and -20.50 to -31.90 mV and sustained release up to 12 h. Entrapment efficiency (EE%) of niosomes ranged from 56.48% to 70.67%. Niosomal gels were more sustainable than niosomes and microemulsions. The most stable niosomal gel based on Span((R)) 60 and CH at a molar ratio of 5:5 and microemulsion containing 45% w/w IPM and 40% w/w of 3:1 Tween((R)) 80-PEG 400 mixture significantly (p 0.0001) enhanced FLZ ocular bioavailability compared with its solution. Niosomal gel showed higher bioavailability than microemulsion by approximate to 2-fold.
机译:如果未治疗,真菌角膜炎可能会导致视力损失。除眼部输送以外的方法表现出几个限制。没有先前的研究,并从憩室凝胶和微乳液中研究了氟康唑(FLZ)的眼部生物利用度。评价基于跨度((R))60和使用1%w / w carbopol((r))934(cp)的跨度((r))60和胆固醇(ch)的Flz(0.3%w / w)的憩室凝胶。含有异丙基myristate(IPM,作为油相)的FLZ微乳液(0.3%w / v)和吐温((r))80(作为表面活性剂)和聚乙二醇400(PEG 400,作为含有含有含量活性剂)的3:1混合物。比较优化的制剂以兔子的眼部生物利用度进行比较。纳米镜综合征(63.67-117.13nm)和微乳液(57.05-59.93nm)显示相应的负Zeta电位范围-45.37至-61.40和-20.50至-31.90 mV,持续释放至12小时。梭效率(EE%)定位率为56.48%至70.67%。憩室凝胶比憩室和微乳液更具可持续性。基于跨度((R))60和Ch的最稳定的脊髓质凝胶,其摩尔比为5:5和含有45%w / w的微乳液和40%w / w的3:1吐温((r))80 -PEG 400混合物显着(P <0.0001)与其溶液相比增强了FLZ眼生物利用度。通过近似为2倍,Niatomal凝胶显示比微乳液更高的生物利用度。

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