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温度触发柠檬酸根 - 磷脂纳米粒中动力学捕获的自组装体。

Temperature triggering of kinetically trapped self-assemblies in citrem-phospholipid nanoparticles.

机构信息

Department of Pharmacy, Faculty of Health and Medical Sciences, University of Copenhagen, Universitetsparken 2, DK-2100 Copenhagen Ø, Denmark.

Laboratory for Biointerfaces, Empa, Swiss Federal Laboratories for Materials Science and Technology, Lerchenfeldstrasse 5, 9014, St. Gallen, Switzerland.

出版信息

Chem Phys Lipids. 2018 Nov;216:30-38. doi: 10.1016/j.chemphyslip.2018.09.003. Epub 2018 Sep 14.

Abstract

Lyotropic non-lamellar liquid crystalline (LLC) nanoparticles are attractive nanocarriers for drug delivery, particularly for the solubilization of poorly water-soluble drugs. Due to the reported problems of complement activation and cytotoxicity of most investigated Pluronic F127-stabilized cubosomes and hexosomes, there is an interest in introducing safe stabilizers for these LLC nanodispersions. Citrem appears to be the stabilizer of choice for the colloidal stabilization of these LLC nano-self-assemblies owing to its hemocompatiblity and poor activation of the complement system. This anionic food-grade emulsifier in combination with soy phosphatidylcholine (SPC) can be used to introduce a library of hemocompatible lamellar and non-lamellar liquid crystalline nanodispersions at different lipid compositions. We found that batch-to-batch variability in citrem composition is associated with slight alterations in the size, structural characteristics, and surface charge of the produced citrem/SPC nanoparticles. Further, we report on the temperature-triggered alterations in these nano-self-assemblies at different lipid compositions by using synchrotron small angle X-ray scattering (SAXS). The addition of citrem at different temperatures induces lamellar to non-lamellar structural transitions as evident from the appearance of inverse bicontinuous cubic Pn3m and discontinuous hexagonal (H) phases, respectively, upon increasing citrem concentration and varying temperature in the range of 5-59 °C. Citrem/SPC nanoparticles are attractive for use in the development of nanocarriers for drug delivery owing to their structural tunability and hemocompatiblity.

摘要

溶致型非层状液晶(LLC)纳米颗粒是药物传递的有吸引力的纳米载体,特别是对于增溶水溶性差的药物。由于报道的大多数研究的 Pluronic F127 稳定的立方纳米囊泡和六方纳米囊泡的补体激活和细胞毒性问题,人们对这些 LLC 纳米分散体引入安全稳定剂感兴趣。由于其血液相容性和补体系统的低激活,Citrem 似乎是这些 LLC 纳米自组装体胶体稳定的首选稳定剂。这种阴离子食品级乳化剂与大豆卵磷脂(SPC)结合使用,可以在不同的脂质组成下引入一系列具有血液相容性的层状和非层状液晶纳米分散体。我们发现,Citrem 组成的批间变异性与所产生的 Citrem/SPC 纳米颗粒的大小、结构特征和表面电荷的轻微变化有关。此外,我们还通过同步加速器小角 X 射线散射(SAXS)报告了在不同脂质组成下这些纳米自组装体在不同温度下的变化。在不同温度下添加 Citrem 会诱导层状到非层状结构转变,这可以从增加 Citrem 浓度和在 5-59°C 的范围内改变温度时分别出现的反向连续立方 Pn3m 和不连续六方(H)相看出。由于其结构可调性和血液相容性,Citrem/SPC 纳米颗粒是用于药物传递的纳米载体开发的有吸引力的选择。

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