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水凝胶作为软质隐形眼镜材料的应用 被引量:4
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作者 彭志明 陈晓明 《武汉工程大学学报》 CAS 2009年第7期76-80,共5页
介绍了用作软质隐形眼镜(SCL)的水凝胶材料;分析了材料的性能要求,包括生物相容性、光学性能、透氧性、对蛋白质和酯类吸附、脱水速率、机械性能、加工性能等;综述了SCL的研究进展,包括抛弃型眼镜(DDCL)、可长期佩戴隐形眼镜、眼药控释.
关键词 软质隐形眼镜 水凝胶 透氧性 眼药释放
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Preparation and evaluation of ophthalmic thermosensitive in situ gels of penciclovir 被引量:7
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作者 李桂玲 李眉 《Journal of Chinese Pharmaceutical Sciences》 CAS 2007年第2期90-95,共6页
Aim To develop pluronic F127 (PF127) based formulations of penciclovir (PCV) aimed at enhancing its ocular bioavailability. Methods Thermosensitive in situ gels of penciclovir were prepared through combination of ... Aim To develop pluronic F127 (PF127) based formulations of penciclovir (PCV) aimed at enhancing its ocular bioavailability. Methods Thermosensitive in situ gels of penciclovir were prepared through combination of HPMC K4M or carbopol 934P and pluronic F127. Optimized formulations were examined through measuring gelation temperature, rheology speciality, drug release behavior, pharmacokinetics and ocular irritation. Results The gelation temperature was reduced by adding HPMC K4M or carbopol 934P, and the viscosity was enhanced slightly. Either HPMC K4M or carbopol 934P delayed the release of PCV from in situ gel. PCV was released by non-Fickian diffusion. The study of ocular irritation for different PCV formulations did not show any irritation or damage for the cornea. PCV bioavailability from combination of carbopol 934P and pluronic F127 gels was higher than that obtained from any other gels. Conclusion Pluronic F127 formulations of PCV can be used as liquid for administration by instilling into the eye. Facilitated by the appropriate eye temperature, the formulations were transformed to gel phase. On the basis of in vitro and in vivo results, PCV formulations containing HPMC K4M or carbopol 934P and low concentration of pluronic F127 (12%) showed potential for use as a drug delivery system with improved ocular bioavailability. 展开更多
关键词 PENCICLOVIR Thermosensitive in situ forming gel PLURONIC Rbeology Drug release Ocular irritation PHARMACOKINETICS
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