4.7 Article

Design and Optimization of In Situ Gelling Mucoadhesive Eye Drops Containing Dexamethasone

期刊

GELS
卷 8, 期 9, 页码 -

出版社

MDPI
DOI: 10.3390/gels8090561

关键词

corneal-PAMPA; cyclodextrin; factorial design; ophthalmic delivery; penetration; poloxamer 407

资金

  1. Ministry of Innovation and Technology of Hungary from the National Research, Development, and Innovation Fund [TKP2021-EGA-32]
  2. [TKP2021-EGA]

向作者/读者索取更多资源

This study aims to develop in situ gelling mucoadhesive ophthalmic preparations that can improve the bioavailability of eye drops. The results show that formulations based on thermosensitive polymers and mucoadhesive polymers can increase the residence time and penetration of the active pharmaceutical ingredient, thereby enhancing the bioavailability of the eye drops.
Poor bioavailability of eye drops is a well-known issue, which can be improved by increasing the residence time on the eye surface and the penetration of the active pharmaceutical ingredient (API). This study aims to formulate in situ gelling mucoadhesive ophthalmic preparations. To increase the residence time, the formulations were based on a thermosensitive polymer (Poloxamer 407 (P407)) and were combined with two types of mucoadhesive polymers. Dexamethasone (DXM) was solubilized by complexation with cyclodextrins (CD). The effect of the composition on the gel structure, mucoadhesion, dissolution, and permeability was investigated with 3(3) full factorial design. These parameters of the gels were measured by rheological studies, tensile test, dialysis membrane diffusion, and in vitro permeability assay. The dissolution and permeability of the gels were also compared with DXM suspension and CD-DXM solution. The gelation is strongly determined by P407; however, the mucoadhesive polymers also influenced it. Mucoadhesion increased with the polymer concentration. The first phase of drug release was similar to that of the CD-DXM solution, then it became prolonged. The permeability of DXM was significantly improved. The factorial design helped to identify the most important factors, thereby facilitating the formulation of a suitable carrier for the CD-DXM complex.

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