季铵盐型Gemini表面活性剂诱导囊泡结构改变机理研究

用动态光散射技术以及荧光探针方法, 研究了不同连接基长度的季铵盐型Gemini表面活性剂对卵磷脂囊泡结构改变的影响, 并借助理论模型和临界堆积参数理论探索了Gemini表面活性剂诱导囊泡结构改变的机理. 实验结果表明, 表面活性剂诱导囊泡结构改变的主要原因是表面活性剂嵌入到囊泡的双分子层中, 从而改变了囊泡的表面电荷强度以及嵌入后的表面活性剂在囊泡双分子层中分布的不均匀性. 此外, 表面活性剂分子的结构也会对其产生影响, 不同连接基长度的季铵盐型Gemini表面活性剂对囊泡结构改变的影响不完全相同, 但会呈现出一定的规律性.     

阴离子Gemini表面活性剂在油/水界面行为的分子动力学模拟

采用分子动力学方法研究了磺酸盐型阴离子Gemini表面活性剂在油/水界面的吸附行为, 考察了不同长度的连接基(Spacer)对表面活性剂在界面的聚集形态及界面性质的影响. 密度分布和微观结构信息显示, Gemini表面活性剂能在油/水界面形成单层膜结构. Gemini表面活性剂能使油/水界面的厚度显著增大, 并使界面形成能降低. 当连接基为6个碳时, 此类磺酸盐型Gemini表面活性剂的界面厚度最大, 形成的界面最稳定. 连接基长度对Gemini表面活性剂单层膜周围的水分子和Na⁺的吸附结构影响不大, 但是能影响水分子的扩散行为.     

阴离子Gemini表面活性剂和阳离子传统表面活性剂混合体系双水相中囊泡形貌的转变

通过电子显微镜观察了阴离子gemini表面活性剂C₁₁- p-PhCNa和阳离子传统表面活性剂DTAB混合体系双水相中囊泡形貌随体系组成和浓度的转变。结果表明,双水相较浓的一相中形成了多层囊泡,囊泡的大小和壁厚随相的组成和浓度而改变,两组分等电荷混合有利于形成较大且壁较厚的囊泡。分析表明, gemini表面活性剂在聚集体中采取的反式构象可能是其容易形成厚壁多层囊泡的重要原因,C₁₁- p-PhCNa联接链上的苯氧基与DTA⁺之间的p-阳离子相互作用以及两组分相反电性头基之间的静电吸引使囊泡壁的多层结构更加稳定。     

N,N-双十二烷基壳聚糖/胆固醇混合单分子膜及自组装囊泡性质

研究了添加胆固醇对N,N-双十二烷基壳聚糖(N,N-dilauryl chitosan, DLCS)单分子膜以及自组装囊泡性质的影响. 结果表明, 引入少量胆固醇会导致DLCS膜的凝聚性下降; 当胆固醇含量增加到一定程度后, 混合膜的凝聚性增强. 添加胆固醇可显著改变DLCS载药囊泡的药物释放行为, 少量胆固醇可以提高载药囊泡的释放速率和平衡药物释放百分率; 而较高含量胆固醇则可抑制囊泡的释放速率和降低平衡药物释放百分率. 此外, 囊泡平衡药物释放率与其单分子膜压缩模量呈现一定线性关系, 这说明胆固醇的引入导致囊泡分子膜凝聚性的改变, 从而改变囊泡的通透性. 通过调节胆固醇的加入量, 可以制得药物释放行为在一定范围内可控的自组装囊泡.     

表面活性剂混合物水溶液中的囊泡形成

1:1烷基羧酸钠-溴化烷基三甲铵混合水溶液的浓度在cmc以上时, 能自发或超声分散形成一类新型混合表面活性剂囊泡(单层膜), 正负离子表面活性剂的突出囊泡形成能力以及不同表面活性剂结构组合变化所显现的多样特性, 皆预示出混合功能有序组合体研究的广阔前景。     

不含蛋白质的功能泡囊膜及对酶的模拟

本篇综述了模拟生物膜的不含蛋白质的功能泡囊膜的建立过程,并介绍了这类功能泡囊膜所进行的模拟酶的泡囊催化反应。以磷脂或亲水亲油的表面活性剂分子所提供的双分子层泡囊结构为基质,分别在其不同的区域引入活性基团或分子,赋予了泡囊新的功能,由此可实现对一些反应的进程及产物构象的控制。利用这类功能泡囊膜,已成功地模拟了水解酶、还原酶、转氨酶、生物体内的碳单元传递反应等,并为模拟光合作用提供了一个很好的模式。     

Gemini表面活性剂对疏水缔合聚丙烯酰胺界面吸附膜扩张流变性质的影响

采用小幅低频振荡和界面张力弛豫技术, 考察了疏水缔合水溶性聚丙烯酰胺(HMPAM)在正癸烷-水界面上的扩张黏弹性质, 研究了不对称Gemini表面活性剂C₁₂COONa-p-C₉SO₃Na对其界面扩张性质的影响. 研究发现, 疏水链段的存在, 使HMPAM在界面层中具有较快的弛豫过程, 扩张弹性显示出明显的频率依赖性. 表面活性剂分子可以通过疏水相互作用与聚合物的疏水嵌段在界面上形成类似于混合胶束的特殊聚集体. 表面活性剂分子与界面聚集体之间存在快速交换过程, 可以大大降低聚合物的扩张弹性. 同时, 聚合物分子链能够削弱表面活性剂分子长烷基链之间的强相互作用, 导致混合吸附膜的扩张弹性远低于单独表面活性剂吸附膜.     

界面扩张流变法研究C_(12)mimBr对Gemini12-2-12在空气/水界面聚集行为的影响

采用界面扩张流变技术研究了季铵盐偶联表面活性剂C12-(CH2)2-C12·2Br(Gemini12-2-12)及其与离子液体表面活性剂溴化1-十二烷基-3-甲基咪唑(C12mim Br)复配体系的动态界面张力、扩张流变性质和界面弛豫过程等,探讨了C12mim Br对C12mim Br/Gemini12-2-12混合体系界面性质的影响及C12mim Br对Gemini12-2-12界面聚集行为影响的机制.结果表明,随着离子液体表面活性剂的不断引入,体系界面吸附达到平衡所需的时间逐渐缩短,扩张模量和相角明显降低,界面吸附膜由粘弹性膜转变为近似纯弹性膜;同时,界面及其附近的弛豫过程也发生显著变化,慢弛豫过程消失,快弛豫过程占主导地位,且离子液体浓度越高,快弛豫的贡献越大.这些界面性质的变化主要归因于离子液体表面活性剂C12mim Br参与界面形成及两表面活性剂在界面竞争吸附的结果.少量离子液体表面活性剂C12mim Br的加入可以填补疏松的Gemini12-2-12界面上的空位,形成混合界面吸附膜.随着C12mim Br含量的增加,嵌入界面的C12mim Br分子数不断增多,导致界面上相互缠绕的Gemini12-2-12烷基链"解缠",在体相和界面分子扩散交换的过程中"解缠"的Gemini12-2-12分子从界面上解吸回到体相,与此同时,C12mim Br分子相对较小的空间位阻及较强的疏水作用促使其优先扩散至界面进而取代Gemini12-2-12分子,最终界面几乎完全被C12mim Br分子所占据.     

表面活性剂体系中电荷诱导的层状相向囊泡相的转化

向一种非离子表面活性剂LA070(英文名AlcoholC12-C16Poly(1-6)Ethoxylate)复配体系LA070/C8H17OH/H2O形成的层状相中加入离子型表面活性剂使其电荷化,在电荷诱导下,双分子层的曲率发生变化,闭合形成具有黏弹性的囊泡相.离子型表面活性剂的加入量增大到一定程度时,由于反离子的屏蔽作用,囊泡结构被破坏,溶液的黏弹性消失,澄清的溶液逐渐变混浊,然后分为两相.     

新型阴离子Gemini表面活性剂与非离子表面活性剂C10E6混合溶液的胶团化的研究

研究了烷基苯磺酸盐Gemini表面活性剂Ia与非离子表面活性剂C10E6溶液混合胶团中分子间的相互作用. 通过表面张力法测定了Ia 和C10E6不同比例不同温度下的临界胶束浓度(cmc). 结果表明, 两种表面活性剂以任何比例复配的cmc比单一表面活性剂的cmc都低, 表现出良好的协同效应. 传统型非离子表面活性剂C10E6、Gemini表面活性剂Ia及混合物的cmc都随着温度升高而降低. 而且, 任何配比的混合胶团中两种表面活性剂分子间的相互作用参数β都是负值, 这说明两种表面活性剂在混合胶团中产生了相互吸引的作用. 混合表面活性剂体系的胶团聚集数比单一Ia的大, 但比单一C10E6的小. 向Gemini表面活性剂Ia胶束中加入非离子表面活性剂C10E6会使胶束的微观极性变小.     

The action of polysilicic acid on mixed monolayers of cholesterol and lecithins

Silicic acid produces marked expansion in dipalmitoyl lecithin films and in mixed cholesterol-dipalmitoyl lecithin films with more than 50 % phospholipid. In the presence of silicic acid, these films no longer exhibit a transition region between the liquid-expanded and liquid-condensed states. Mixed cholesterol-dilauroyl lecithin.films are also expanded by silicic acid. In the absence of silicic acid, the addition of cholesterol produces greater condensation in dilauroyl lecithin films than in films of dipalmitoyl lecithin, but the reverse is the case if the substrate contains silicic acid. These results have been interpreted in terms of a possible electrostatic interaction between negatively charged dissociated silicate ions and the positively charged trimethyl ammonium group of the choline fragment.     

A photo-responsive cholesterol capable of inducing a morphological transformation of the liquid-ordered microdomain in lipid bilayers

An azobenzene-modified cholesterol was designed and synthesized for photo-induced domain transformation in lipid bilayer membranes. Upon UV-light irradiation, the cholesterol derivative changes the conformation through photoisomerization of the azobenzene moiety from trans- to cis-form. The photoisomerization effectively occurred both in liquid-ordered (L_o) and liquid-disordered (L_d) phases. Phase-contrast and fluorescence microscopic observation revealed that photoisomerization of the azobenzene-modified cholesterol induced the shape transformation of giant unilamellar vesicle (GUV) and the reorganization of L_o domain structure. Such a photo-induced transformation of lipid domain gave two different pathways dependent on the lipid composition of GUV; disappearance of the L_o domain or appearance of a small L_d domain with in the L_o domain.     

Effect of cholesterol or phospholipids incorporation on vesicle formation of muramyldipeptide derivative B30-MDP

Summary The muramyldipeptide derivative B30-MDP has immunoadjuvant activity and vesicleforming ability in aqueous solutions. To assist in the clinical application of B30-MDP to liposomal vaccine, we investigated the physicochemical properties including membrane fluidity, surface charge and particle size of B30-MDP vesicles containing cholesterol, dipalmitoylphosphatidyl-choline (DPPC) or dipalmitoylphosphatidylglycerol (DPPG).The membrane fluidity of B30-MDP/cholesterol vesicles was slightly influenced by cholesterol concentration and temperature. The membrane fluidity of B30-MDP/phospholipid vesicle was dependent on temperature. ESR spectra clearly showed the good miscibility of cholesterol with B30-MDP and the occurrence of phase separation between B30-MDP and phospholipid.The surface charge and particle size of B30-MDP/cholesterol vesicles were hardly influenced by cholesterol concentration in the membrane because the membrane surface was covered with the hydrophilic region of B30-MDP. The effect of this hydrophilic region of B30-MDP on the surface charge and particle size of B30-MDP/phospholipid vesicle was greater than that of phospholipid.This study showed that the membrane structure of B30-MDP/cholesterol vesicle differed from that of B30-MDP/phospholipid vesicle. Further, the hydrophilic region of B30-MDP is considered to play an important role in the physicochemical properties and formation of the vesicle.     

Dynamic interaction between oppositely charged vesicles: aggregation, lipid mixing, and disaggregation

We investigated dynamic interactions between oppositely charged small unilamellar vesicles using positively charged vesicles containing 1,2-dioleoyl-3-trimethylammonium-propane or 3beta-[N-(N('),N(')-dimethylaminoethane)-carbamoyl] cholesterol and negatively charged vesicles containing L-alpha-phosphatidyl-DL-glycerol. Aggregation, lipid bilayer mixing, contents mixing and contents leakage were systematically examined using optical density measurements, fluorescence resonance energy transfer assays, fluorescence quenching assays, light-scattering analyses, and freeze-fracture transmission electron microscopy. The oppositely charged vesicles aggregated immediately. Lipid mixing was observed, but there was no mixing of the contents. The vesicle aggregates disaggregated spontaneously after several minutes. The surface potential of the disaggregated vesicles was neutralized. From these results, we infer that the lipids in the external monolayers were exchanged between the oppositely charged vesicles while the internal monolayers remained intact. The two types of cationic lipids used exhibited different speeds of disaggregation.     

Characterization of lecithin-based microemulsions used as media for a cholesterol oxidase-catalyzed reaction

Microemulsions stabilized by soybean lecithin and ethanol have been characterized with respect to phase behavior, distribution of the ethanol cosolvent, conductivities, viscosities, and volume fractions of the different phases in Winsor III systems. The conductivities and viscosities of the surfactant-rich phase in the Winsor III system indicate that this phase exhibits a bicontinuous structure. The reaction yield at 298.2K for the enzymatic conversion of cholesterol to cholestenone by cholesterol oxidase performed in a Winsor III system containing water, lecithin, hexadecane, and ethanol is low.     

Adsorption of lipids on silicalite-1

Russian Journal of Physical Chemistry A - The adsorption of egg lecithin and cholesterol from chloroform solutions onto silicalite-1 (hydrophobic silica with MFI zeolite structure) is investigated....     

Membrane binding and structure of de novo designed alpha-helical cationic coiled-coil-forming peptides.

We introduce a de novo designed peptide model system that enables the systematic study of 1) the role of a membrane environment in coiled-coil peptide folding, 2) the impact of different domains of an alpha-helical coiled-coil heptad repeat on the interaction with membranes, and 3) the dynamics of coiled-coil peptide-membrane interactions depending on environmental conditions. Starting from an ideal alpha-helical coiled-coil peptide sequence, several positively charged analogues were designed that exhibit a high propensity toward negatively charged lipid membranes. Furthermore, these peptides differ in their ability to form a stable alpha-helical coiled-coil structure. The influence of a membrane environment on peptide folding is studied. All positively charged peptides show strong interactions with negatively charged membranes. This interaction induces an alpha-helical structure of the former random-coil peptides, as revealed by circular dichroism measurements. Furthermore, vesicle aggregation is induced by a coiled-coil interaction of vesicle-bound peptides. Dynamic light scattering experiments show that the strength of vesicle aggregation increases with the peptide's intrinsic ability to form a stable alpha-helical coiled coil. Thus, the peptide variant equipped with the strongest inter- and intra-helical coiled-coil interactions shows the strongest effect on vesicle aggregation. The secondary structure of this peptide in the membrane-bound state was studied as well as its effect on the phospholipids. Peptide conformation within the peptide-lipid aggregates was analyzed by (13)C cross-polarization magic-angle spinning NMR experiments. A uniformly (13)C- and (15)N-labeled Leu residue was introduced at position 12 of the peptide chain. The (13)C chemical shift and torsion angle measurements support the finding of an alpha-helical structure of the peptide in its membrane-bound state. Neither membrane leakage nor fusion was observed upon peptide binding, which is unusual for amphiphatic peptide structures. Our results lay the foundation for a systematic study of the influence of the alpha-helical coiled-coil folding motif in membrane-active events on a molecular level.     

Destabilisation of liposomes by bovine serum albumin; Sepharose 2B-Cl experiment

Summary The stability of liposomes (2∶1 egg yolk lecithin:cholesterol, mole ratio; diameter about 100 nm) at increasing bovine serum albumin (BSA) concentration was study. The influence of introducing positive or negative charge to the liposomal bilayers was tested. The results indicated appreciable destructive effects of serum albumin on the liposomal membranes of neutral and negatively charged liposomes. Near-physiological concentration (30 mg mL⁻¹) of albumin dissolved more then 50% of liposomes. Presented at the 21^st ISC held in Stuttgart, Germany, 15th–20th September, 1996     

Effect of the structure of ethylene oxide-propylene oxide block copolymers on their interaction with biological membranes

Partition coefficients of ethylene oxide-propylene oxide block copolymers between the lipid phase and water have been estimated via equilibrium dialysis. It has been shown that for the triblock copolymer (Pluronic L61), the partition coefficient is 45 ± 9, while for the diblock copolymer (REP), this parameter is as high as 78 ± 17. The effect of the copolymers on the permeation of the charged organic ion carboxyfluorescein across the lecithin bilayer membrane changes in the same direction. Even though the triblock copolymer binding is weaker, it shows a stronger effect on the rate of transbilayer migration of lipids and on the permeation of the uncharged substance (doxorubicin). The incorporation of cholesterol into the membrane decreases its sensitivity to the action of copolymers; however, the character of changes induced by both copolymers remains invariable. The experimental data of this study indicate that the triblock structure of amphiphilic macromolecules is responsible for their higher ability to disturb lipid bilayer membranes.