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四臂嵌段共聚物的胶束化、凝胶化及药物增溶作用:pH值和离子强度的影响

Tetronic micellization, gelation and drug solubilization: Influence of pH and ionic strength.

作者信息

Alvarez-Lorenzo Carmen, Gonzalez-Lopez Jaime, Fernandez-Tarrio Marta, Sandez-Macho Isabel, Concheiro Angel

机构信息

Departamento de Farmacia y Tecnología Farmacéutica, Universidad de Santiago de Compostela, Santiago de Compostela, Spain.

出版信息

Eur J Pharm Biopharm. 2007 May;66(2):244-52. doi: 10.1016/j.ejpb.2006.10.010. Epub 2006 Oct 20.

Abstract

The aim of this work was to gain an insight into the self-associative processes and drug solubilization ability of a Tetronic variety, T904 (4 x 15 EO units; 4 x 17 PO units; HLB 15), in aqueous media covering the physiological range of pH and ionic strength, applying isoperibol microcalorimetry, transmission electronic microscopy (TEM), dynamic light scattering (DLS), oscillatory rheometry, and drug diffusion experiments. T904 shows two pK(a) (pK(a1)=4.0 and pK(a2)=7.9) and, at pH<5.8, the diprotonated form predominates over the non-protonated one. Deprotonization of the central diamine group is a required condition for micellization, which is an endothermic entropy-driven process owing to hydrophobic interactions between the PPO chains. As the pH of the solutions decreases, the coulombic repulsions among the positively charged amine groups make the aggregation more difficult, raising the critical micellar concentration (CMC) and decreasing the size of the micelles. The changes in the conformation and hydrophilicity of the Tetronic were reflected in its gelation temperature (around 30 degrees C at neutral-alkaline pH; no gelation at pH<2) and solubilization capacity for griseofulvin (2-fold greater at neutral-alkaline pH than at pH<2) and rate of diffusion (slower at pH 7.4). Such alterations in self-assembly are relevant when using Tetronic in the design of drug delivery systems.

摘要

本研究旨在通过等温微量热法、透射电子显微镜(TEM)、动态光散射(DLS)、振荡流变学和药物扩散实验,深入了解Tetronic品种T904(4×15个环氧乙烷单元;4×17个环氧丙烷单元;HLB 15)在覆盖生理pH和离子强度范围的水性介质中的自缔合过程和药物增溶能力。T904显示出两个pK(a)(pK(a1)=4.0和pK(a2)=7.9),并且在pH<5.8时,双质子化形式比非质子化形式占优势。中央二胺基团的去质子化是胶束化的必要条件,由于PPO链之间的疏水相互作用,胶束化是一个吸热的熵驱动过程。随着溶液pH值的降低,带正电荷的胺基团之间的库仑排斥使得聚集更加困难,提高了临界胶束浓度(CMC)并减小了胶束的尺寸。Tetronic的构象和亲水性变化反映在其凝胶化温度(中性至碱性pH下约为30℃;pH<2时不凝胶化)、灰黄霉素的增溶能力(中性至碱性pH下比pH<2时大2倍)和扩散速率(pH 7.4时较慢)上。在药物递送系统设计中使用Tetronic时,这种自组装的改变是相关的。

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