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了解鲑鱼降钙素、抗菌肽 AP114 和多粘菌素 B 吸附到脂质纳米囊上的情况。

Understanding the adsorption of salmon calcitonin, antimicrobial peptide AP114 and polymyxin B onto lipid nanocapsules.

机构信息

INSERM U1066, Micro et Nanomédecines Biomimétiques, IBS-CHU, 4 Rue Larrey, F-49933, Angers, France.

INSERM U1066, Micro et Nanomédecines Biomimétiques, IBS-CHU, 4 Rue Larrey, F-49933, Angers, France.

出版信息

Int J Pharm. 2016 Jun 15;506(1-2):191-200. doi: 10.1016/j.ijpharm.2016.04.028. Epub 2016 Apr 22.

Abstract

The adsorption of therapeutic molecules, e.g., peptides, onto nanocarriers is influenced by the properties of the carrier, adsorbed molecule and continuous phase. Hence, through changes in the composition of the nanocarrier and the medium, it should be possible to tune the system to make it capable of efficiently adsorbing peptides. The adsorption of calcitonin, antimicrobial peptide AP114 and polymyxin B onto lipid nanocapsules was investigated. The adsorption data were fitted to a Langmuir isotherm. Dynamic light scattering and laser Doppler velocimetry were used to investigate the changes in the hydrodynamic diameter and zeta potential, respectively, of the nanocarrier. The peptide adsorption was primarily governed by electrostatic forces; however, even without the presence of an ionisable surfactant, a significant amount of each tested molecule was adsorbed due to the enormous surface area of the nanocarriers and to peptide-nanocarrier interactions. The addition of an ionisable lipophilic surfactant, lecithin, improved the adsorption yield, which reached values of up to 100%. The adsorption yield and the properties of the nanocarrier, particularly the zeta potential, depended on the carrier and peptide concentrations and their mixing ratio. The adsorption of all tested molecules obeyed the Langmuir model over a limited concentration range.

摘要

治疗分子(例如肽)吸附到纳米载体上受载体、吸附分子和连续相的性质影响。因此,通过改变纳米载体和介质的组成,应该可以调节系统使其能够有效地吸附肽。本文研究了降钙素、抗菌肽 AP114 和多粘菌素 B 吸附到脂质纳米囊泡上的情况。将吸附数据拟合到 Langmuir 等温线。动态光散射和激光多普勒速度计分别用于研究纳米载体的流体力学直径和 ζ 电位的变化。肽的吸附主要受静电力控制;然而,即使没有可离子化的表面活性剂存在,由于纳米载体的巨大表面积和肽-纳米载体相互作用,仍有相当数量的每种测试分子被吸附。添加可离子化的亲脂性表面活性剂(如卵磷脂)可提高吸附产率,最高可达 100%。吸附产率和纳米载体的性质(特别是 ζ 电位)取决于载体和肽的浓度及其混合比。所有测试分子的吸附都在有限的浓度范围内遵循 Langmuir 模型。

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