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首页> 外文期刊>Biomacromolecules >Thermogelling Chitosan-g-(PAF-PEG) Aqueous Solution As an Injectable Scaffold
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Thermogelling Chitosan-g-(PAF-PEG) Aqueous Solution As an Injectable Scaffold

机译:热凝胶壳聚糖-g-(PAF-PEG)水溶液作为可注射支架

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摘要

The present study reports on a thermogelling poly(ethylene glycol)-poly(L-alanine-co-L-phenyl alanine) grafted chitosan (CS-g-(PAF-PEG)) system, focusing on phase diagram, transition mechanism, and in vivo gel duration. The sol-to-gel transition temperature decreased from 27 to 11 °C as the concentration increased from 4.0 wt % to 9.0 wt %. The polymer formed micelles with 10-50 nm in diameter at 10 °C and formed large aggregates ranging from hundreds to thousands of nanometers in size as the temperature increasedfrom 10 to 35 °C, suggesting that an extensive molecular aggregation might be involved in the sol-to-gel transition. To study the transition mechanism on a molecular level, we investigated pH, circular dichroism spectra, and ~(13)C NMR spectra of the CS-g-(PAF-PEG) aqueous solution as a function of temperature. As the temperature increased, deprotonation of the chitosan and dehydration of the PEG were suggested, whereas the α-helical secondary structure of PAF was slightly changed in the sol-to-gel transition temperature range of 10-50 °C. A gel was formed in situ after injecting the CS-g-(PAF-PEG) aqueous solution into the subcutaneous layer of rats. About 60-70% of the gel was eliminated in 1 week, and the remaining gel was completely cleared from the implant site in 14 days. The results indicate the potential of CS-g-(PAF-PEG) as a promising short-term carrier for pharmaceutical agents.
机译:本研究报告了热胶凝聚(乙二醇)-聚(L-丙氨酸-共-L-苯基丙氨酸)接枝的壳聚糖(CS-g-(PAF-PEG))系统,重点研究了相图,过渡机理和体内凝胶持续时间。随着浓度从4.0重量%增加到9.0重量%,溶胶-凝胶转变温度从27℃降低到11℃。聚合物在10°C时形成直径为10-50 nm的胶束,并随着温度从10°C升高到35°C形成大的聚集体,尺寸从数百纳米到数千纳米不等,这表明溶胶中可能涉及广泛的分子聚集。到凝胶的转变。为了在分子水平上研究转变机理,我们研究了CS-g-(PAF-PEG)水溶液的pH,圆二色性光谱和〜(13)C NMR光谱随温度的变化。随着温度的升高,建议壳聚糖去质子化和PEG脱水,而PAF的α-螺旋二级结构在10-50°C的溶胶-凝胶转变温度范围内略有变化。将CS-g-(PAF-PEG)水溶液注入大鼠皮下层后,原位形成凝胶。在1周内消除了大约60-70%的凝胶,并在14天之内从植入部位完全清除了剩余的凝胶。结果表明CS-g-(PAF-PEG)作为药物的有希望的短期载体的潜力。

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