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Design and evaluation of proniosomes as a carrier for ocular delivery of lomefloxacin HCl
Authors:Rawia M. Khalil  Ghada A. Abdelbary  Mona Basha  Ghada E. A. Awad  Hadeer A. El-Hashemy
Affiliation:1. Department of Pharmaceutical Technology, National Research Centre, Cairo, Egypt,;2. Department of Pharmaceutics, Faculty of Pharmacy, Cairo University, Cairo, Egypt, and;3. Chemistry of Natural and Microbial Product Department, National Research Centre, Cairo, Egypt
Abstract:The current investigation aims to develop and evaluate novel ocular proniosomal gels of lomefloxacin HCl (LXN); in order to improve its ocular bioavailability for the management of bacterial conjunctivitis. Proniosomes were prepared using different types of nonionic surfactants solely and as mixtures with Span 60. The formed gels were characterized for entrapment efficiency, vesicle size, and in vitro drug release. Only Span 60 was able to form stable LXN-proniosomal gel when used individually while the other surfactants formed gels only in combination with Span 60 at different ratios. The optimum proniosomal gel; P-LXN 7 (Span 60:Tween 60, 9:1) appeared as spherical shaped vesicles having high entrapment efficiency (>80%), appropriate vesicle size (187?nm) as well as controlled drug release over 12?h. Differential scanning calorimetry confirmed the amorphous nature of LXN within the vesicles. Stability study did not show any significant changes in entrapment efficiency or vesicle size after storage for 3 months at 4?°C. P-LXN 7 was found to be safe and suitable for ocular delivery as proven by the irritancy test. The antibacterial activity of P-LXN 7 evaluated using the susceptibility test and topical therapy of induced ocular conjunctivitis confirmed the enhanced antibacterial therapeutic efficacy of the LXN-proniosomal gel compared to the commercially available LXN eye drops.
Keywords:Conjunctivitis  lomefloxacin HCl  microbiological evaluation  ocular delivery  proniosomes
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