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来自聚合物微粒系统的贝伐单抗控释作为病理性血管生成疾病的有趣工具

Bevacizumab-Controlled Delivery from Polymeric Microparticle Systems as Interesting Tools for Pathologic Angiogenesis Diseases.

作者信息

De Negri Atanasio Giulia, Ferrari Pier Francesco, Campardelli Roberta, Firpo Giuseppe, Perego Patrizia, Palombo Domenico

机构信息

Department of Civil, Chemical and Environmental Engineering, University of Genoa, via Opera Pia, 15, 16145 Genoa, Italy.

Department of Physics, University of Genoa, via Dodecaneso, 33, 16146 Genoa, Italy.

出版信息

Polymers (Basel). 2022 Jun 26;14(13):2593. doi: 10.3390/polym14132593.

Abstract

This work is a comparative study among three different biocompatible and biodegradable polymers, poly(lactic--glycolic acid), poly(ε-caprolactone), and poly(lactic acid), used to produce microparticles for the encapsulation of bevacizumab for drug delivery purposes. All the formulations were produced using the double emulsion water-oil-water evaporation method and characterized in terms of particle mean diameter, particle size distribution, and bevacizumab entrapment efficiency. Bevacizumab cumulative release was taken into consideration to study the dissolution kinetics from the three different polymeric delivery platforms for a period of 50 days at 37 °C in phosphate buffered saline and mathematical models of the drug release kinetic were attempted in order to describe the release phenomena from the different types of the studied microparticles. Finally, cell viability on human endothelial cell line EA.hy926 was studied to define the maximum cytocompatible concentration for each microsystem, registering the mitochondrial functionality through MTS assay.

摘要

本研究对三种不同的生物相容性和可生物降解聚合物——聚(乳酸-乙醇酸)、聚(ε-己内酯)和聚乳酸进行了比较,这些聚合物用于制备微粒以包裹贝伐单抗用于药物递送目的。所有制剂均采用水包油包水双乳液蒸发法制备,并对其平均粒径、粒径分布和贝伐单抗包封率进行了表征。考虑了贝伐单抗的累积释放情况,以研究在37℃下于磷酸盐缓冲盐水中,三种不同聚合物递送平台在50天内的溶解动力学,并尝试建立药物释放动力学的数学模型,以描述不同类型研究微粒的释放现象。最后,研究了人内皮细胞系EA.hy926的细胞活力,以确定每个微系统的最大细胞相容浓度,并通过MTS法记录线粒体功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bff3/9269115/a1a589cd3d45/polymers-14-02593-g001.jpg

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