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Evaluation of in vitro wound adhesion characteristics of composite film and wafer based dressings using texture analysis and FTIR spectroscopy: a chemometrics factor analysis approach

机译:用纹理分析和FTIR光谱评价复合膜和晶片基敷料的体外缠绕粘附特性:化学计量因子分析方法

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摘要

The adhesive properties of two dressing types, solvent cast films and freeze-dried wafers have been determined and compared using two analytical techniques, combined with chemometrics data analysis. Films and wafers were prepared from gels containing polyox (POL) combined with carrageenan (CAR) or sodium alginate (SA), glycerol (GLY) as plasticiser (films) with streptomycin and diclofenac as model drugs. The gels were dried in an oven at 40 degrees C or freeze-dried to obtain films and wafers respectively. The adhesive performance of the films and wafers was assessed with 6.67% w/v gel using a texture analyser to measure the stickiness, work of adhesion and cohesiveness. The effect of viscosity of simulated wound fluid [containing (2% w/w or 5% w/w bovine serum albumin)] and mucin solution (2% w/w) present on the gelatin surface on texture analyser profiles was investigated. Furthermore, the adhesive properties were estimated and evaluated using attenuated total reflectance Fourier transform infrared spectroscopy by monitoring the diffusion of mucin solution [2% w/w in phosphate buffered saline (PBS) pH 7.4] through the formulations. The diffusion data was analysed using target factor analysis (chemometrics approach) to establish proof of concept for predicting adhesion by measuring mucin interaction and its diffusion through films and wafers. There was a significant effect of simulated wound fluid, viscosity, plasticizer (for films) and drug loading on the adhesive performance of both films and wafers. POL-SA films showed higher mucoadhesive performance in the presence of viscous simulated wound fluid containing 5% bovine serum albumin. Wafers and plasticised films demonstrated high detachment force indicating strong interactions between the chains of the polymers (POL, SA and CAR) and the model wound surface (gelatin). ATR-FTIR spectroscopy showed that mucin diffused independently through the solvent and across the films and wafers. POL-CAR films generally showed slower diffusion of mucin when compared with POL-SA films whilst the opposite effect was observed for diffusion through POL-CAR wafers and POL-SA wafers. Generally, diffusion through wafers was faster than the corresponding films.
机译:已经确定并使用两种分析技术确定了两种敷料类型,溶剂铸膜和冷冻干燥晶片的粘合性能,与化学计量数据分析相结合。从含有Polyox(Pol)的凝胶制备薄膜和晶片,所述聚合物(POL)与藻属(CAR)或藻酸钠(SA),甘油(GLY)作为增塑剂(薄膜),用链霉素和双氯芬酸作为模型药物。将凝胶在40℃下在烘箱中干燥或冷冻干燥,以分别获得薄膜和晶片。使用质地分析仪评估薄膜和晶片的粘合性能,用纹理分析仪测量粘性,粘合性和粘合性的粘性。研究了模拟伤口流体粘度的影响[含有(2%w / w或5%w / w / w牛血清白蛋白)]和存在于明胶表面上的明胶表面上的粘膜溶液(2%w / w)。此外,通过通过制剂监测粘合蛋白溶液的扩散[2%w / w]通过制剂,使用衰减的总反射率傅里叶变换红外光谱估计和评估粘合性能。使用目标因子分析(化学计量方法)分析扩散数据,以建立通过测量粘膜相互作用及其通过薄膜和晶片的扩散来预测粘附的概念证明。模拟伤口流体,粘度,增塑剂(薄膜)和药物负载对两种薄膜和晶片的粘合性能产生显着影响。 POL-SA薄膜在存在含有5%牛血清白蛋白的粘性模拟伤口流体的情况下表现出更高的粘液性能。晶片和塑料薄膜展示了高脱离力,表明聚合物链(POL,SA和CAR)链之间的强相互作用和模型伤口表面(明胶)。 ATR-FTIR光谱显示粘蛋白通过溶剂和穿过薄膜和晶片独立地扩散。与Pol-SA薄膜相比,POL-CAR膜通常表现出粘膜的较慢扩散,而通过POL-CAR晶片和POL-SA晶片观察到相反的效果。通常,通过晶片的扩散比相应的薄膜更快。

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  • 来源
    《RSC Advances》 |2015年第129期|共12页
  • 作者单位

    Univ Greenwich Medway Fac Sci &

    Engn Dept Pharmaceut Chem &

    Environm Sci Chatham ME4 4TB Kent England;

    Univ Greenwich Medway Fac Sci &

    Engn Dept Pharmaceut Chem &

    Environm Sci Chatham ME4 4TB Kent England;

    Univ Greenwich Medway Fac Sci &

    Engn Dept Pharmaceut Chem &

    Environm Sci Chatham ME4 4TB Kent England;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学;
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