Characteristics and Transdermal Drug Delivery of Triamcinolone-Acetonide-Acetate-Loaded Solid Lipid Nanoparticles Carbomer Gel

Aim To prepare triamcinolone-acetonide-acetate (TAA)-loaded solid lipidnanoparticles (SLN) carbomer gel with tripalmitin glyceride (TPG), and investigate theircharacteristics and transdermal drug delivery. Methods SLN suspension was prepared by high-pressurehomogenization technique, and then mixed with carbomer gel matrix to get SLN gel. The morphology,particle size with polydispersi-ty index (PI) and zeta potential were examined by atomic forcemicroscopy (AFM) and photon correlation spectroscopy (PCS). The entrapment efficiency, stability andin vitro drug release were also studied. The transdermal drug delivery through porcine ear skin wasevaluated using modified Franz diffusion cells. Results The SLN had a spherical shape with theaverage size of (95.5 - 186.2) nm, the zeta potential of (-26.3- -15.7) mV and the entrapmentefficiency of 67.4%-90.3% for different TAA encapsulated compounds. TAA-SLN carbomer gel had goodstability, the release profile in vitro fitted Higuchi equation. In comparison with conventionalhydrogels, TAA-SLN carbomer gel resulted in higher drug permeation amount and drug deposition withinporcine ear skin after 24 h penetration experiment. Conclusion TAA-SLN carbomer gel is preparedwith stable physicochemical properties. The release profile and improved drug permeation into skinmake it be a promising vehicle for transdermal drug delivery.

黄白温敏型原位凝胶的处方筛选与评价

目的筛选并优化黄白温敏型原位凝胶的处方,并考察其经皮渗透性能。方法以泊洛沙姆407(P407)、泊洛沙姆188(P188)、聚乙二醇6000(PEG6000)作为凝胶基质材料,以胶凝温度为考察指标,采用Box-Behnken效应面法优化温敏凝胶处方;对制备的温敏凝胶进行理化表征,并采用Franz透皮扩散池法考察黄白温敏凝胶的经皮渗透性能。结果黄白温敏型原位凝胶的最佳处方为P407 20.10%,P188 2.54%,PEG6000 2.00%,胶凝温度为(34.2±0.2)℃,24 h内欧前胡素、盐酸小檗碱的累积渗透量分别为(14.07±1.34)、(395.72±35.04)μg/cm^(2),均符合Higuchi动力学方程。结论制备的凝胶具有温敏、缓释作用,为临床提供治疗蛇虫咬伤的制剂奠定基础。