Study of molecular aggregation of artificial amyloid in a langmuir monolayer by infrared spectroscopy

A synthesized peptidolipid (C18IIGLM-NH2) comprised of a single C18-saturated hydrocarbon chain connected to the amino acid sequence IIGLM terminated with the NH2 group was spread on water, which formed a stable Langmuir monolayer. The Langmuir and Langmuir-Blodgett (LB) films have been characterized by measurements of surface pressure-area (pi-A) and surface potential-area (DeltaV-A) isotherms and infrared multiple-angle incidence resolution spectrometry (MAIRS). The Langmuir monolayer had a significantly larger limiting molecular area than that of a similar molecule of C18IIGLM-OH, which was reported in our previous study. The surface dipole moment analysis coupled with the pi-A isotherm suggested that the C18IIGLM-NH2 monolayer was extraordinarily stiff and the fundamental structure of the monolayer was brought about before the monolayer compression. The infrared MAIRS analysis of the C18IIGLM-NH2 LB film revealed that the backbone structure of the monolayer was the 'antiparallel' beta sheet aligned parallel to the substrate. Since the C18IIGLM-OH LB film was made of 'parallel' beta sheet with a random orientation, it has been found that the present C18IIGLM-NH2 Langmuir monolayer has a largely different monolayer structure, although the chemical structures are slightly different from each other by the terminal group only.     

Spectral properties and structure of the J-aggregates of pseudoisocyanine dye in layered silicate films

Monolayer behavior of an ion pair amphiphile (IPA), hexadecyltrimethylammonium-dodecylsulfate (HTMA-DS), with normal long-chain alcohols at the air/water interface was analyzed by the Langmuir trough technique with the Brewster angle microscope (BAM) observations, and the pronounced stability enhancement of a HTMA-DS monolayer with the presence of the alcohol additives was demonstrated. Two normal long-chain alcohols with alkyl chain lengths of C16 and C18, 1-hexadecanol (HD) and 1-octadecanol (OD), were chosen as the additives. The surface pressure-area and surface potential-area isotherms of the monolayers with BAM images of monolayer morphology implied that the addition of either HD or OD with a comparatively small head group in a double-chained HTMA-DS monolayer at the interface led to better molecular packing and attractive interaction between the molecules, showing a similar condensing effect as that observed in mixed phospholipid/cholesterol systems. Moreover, the monolayer hysteresis and relaxation curves indicated that the incorporation of the alcohols into a HTMA-DS monolayer was able to lessen the monolayer hysteresis and to enhance the monolayer stability. In comparison with OD, HD seemed more effective as an additive in stabilizing a HTMA-DS monolayer, most likely due to the relatively better molecular packing of HTMA-DS and HD molecules at the interface. It is inferred that the stability of a monolayer or vesicular bilayer structure composed of IPAs can be improved by adjusting the molecular packing/interaction with a suitable long-chain alcohol as the additive.     

表面活性素单分子膜在空气/水界面的迟滞现象

表面活性素是一类具有较强表面活性的微生物脂肽类化合物,能在空气/水界面形成不溶性单分子膜.利用Langmuir膜天平测定了表面活性素单分子膜的压缩-扩张循环曲线,发现单分子膜在经历了“平台区”后出现较大的迟滞环,迟滞环的形状与亚相pH有关.将“平台区”的单分子膜转移到云母表面后,用原子力显微镜(AFM)和扫描电子显微镜(SEM)均观察到高度达几十至数百纳米的表面聚集体,说明表面活性素在单分子膜的“平台区”伴随着自聚集.研究结果表明,表面活性素单分子膜在空气/水界面的迟滞现象是分子浸入亚相和形成三维表面聚集体共同作用的结果.     

Memory effects of monolayers and vesicles formed by the non-ionic surfactant, 2C(18)E(12)

The behaviour of monolayers and bilayers formed by the dialkyl chain non-ionic surfactant, 1,2-di-O-octadecyl-rac-glycerol-3-omega-methoxydodecaethylene glycol (2C(18)E(12)) in water at 297 K has been investigated. Using a surface film balance (or Langmuir trough) the compression-expansion cycle of the 2C(18)E(12) monolayer was found to be reversible when compressed to surface pressures (pi) less than 42 mN m(-1). Compression of 2C(18)E(12) monolayer to pi greater than 42 mN m(-1) above this resulted in a considerable hysteresis upon expansion with the pi remaining high relative to that obtained upon compression, suggesting a time/pressure dependent re-arrangement of 2C(18)E(12) molecules in the film. Morphology of the 2C(18)E(12) monolayer, investigated using Brewster angle microscopy, was also found to depend upon monolayer history. Bright, randomly dispersed domains of 2C(18)E(12) of approximately 5 mum in size were observed during compression of the monolayer to pi less than 42 mN m(-1). At pi of 42 mN m(-1) and above, the surfactant film appeared to be almost completely 'solid-like.' Regardless of the extent of compression of the monolayer film, expansion of the film caused formation of chains or 'necklaces' of individual surfactant domains, with the extent of chain formation dependent upon pressure of compression of the monolayer and the length of time held at that pressure. Irreversible effects on 2C(18)E(12) vesicle size were also seen upon temperature cycling the vesicles through their liquid-crystalline phase transition temperature with vesicles shrinking in size and not returning to their original size upon standing at 298 K for periods of more than 24 h. No comparable hysteresis, time, pressure or temperature effects were observed with the monolayer or vesicles formed by the corresponding phospholipid, disteaorylphosphatidylcholine, under identical conditions. The effects observed with 2C(18)E(12) are attributed to the ability of the polyoxyethylene head group to dehydrate and intrude into the hydrophobic chain region of the mono- and bilayers. These studies have important implications for the use of the vesicles formed by 2C(18)E(12) as drug delivery vehicles.     

Synthesis and characterization of monolayers and Langmuir-Blodgett films of an amphiphilic oligo(ethylene glycol)-C60-hexadecaaniline conjugate

A novel amphiphilic oligo(ethylene glycol)-C60-hexadecaaniline (A16) tricomponent conjugate, C60>(A16-EG43), possessing a well-defined number of repeating aniline donor units and a hydrophilic ethylene glycol oligomer chain was synthesized. The compound is composed of a covalently bound donor-acceptor chromophore structure. Molecular self-assembly of C60>(A16-EG43) at the air-water interface formed a densely packed Langmuir monolayer with all highly hydrophobic fullerene cages located above the liquid interface. The monolayer can then be transferred onto a glass substrate via Langmuir-Blodgett (LB) deposition. LB multilayered thin films formed by multiple deposition of the monolayer yielded broadened optical absorption peaks extending beyond 600 nm into the 950 nm region, suggesting strong intermolecular interactions among the C60 cages and the A16 moieties. An X-ray reflectometry study clearly reveals that the Langmuir film at the air-water interface consists of a C60 top layer and a bottom layer containing hexcadecaaniline and oligo(ethylene glycol) with gradually decreasing electron density over a distance of approximately 130 A above bulk water. The pressure isotherm shows that the packing density of the C60>(A16-EG43) monolayer, corresponding to a molecular area of approximately 95 A2/molecule, is similar to that of the surface area of the C60 monolayer. This result suggests that C60 packing plays a dominant role in guiding the formation of the monolayer structure. Further photoexcitation of hexadecaaniline moieties of aligned (C60>)-A16 layers by a flash light source induces cross linking between adjacent A16 segments forming an interlinked A16 array. Our results have demonstrated a unique fabrication method for preparing the aligned donor-acceptor array using strong intermolecular interactions between fullerenes as the molecular orientation guiding force in the Langmuir-Blodgett technique.     

Fibril-like aggregate formation of peptide carboxylate Langmuir films analyzed by surface pressure, surface dipole moment, and infrared spectroscopy

The fibril formation process of a synthetic peptidolipid compound in a Langmuir monolayer at the air-water interface has been analyzed by surface pressure and surface dipole moment-area isotherms, followed by infrared spectral analysis of related Langmuir-Blodgett films. Thus far, the analysis of randomly oriented molecular assemblies has been a difficult matter, especially for spectroscopic measurements. In the present study, the Langmuir film isotherms were discussed in detail, and they have readily been correlated to the infrared spectra. For the spectral analysis, infrared multiple-angle incidence resolution spectroscopy (MAIRS) was employed, which was compared to the results by conventional techniques. Since the peptide assemblies greatly responded to a metal surface, the reflection-absorption technique was not useful for our analysis. Instead, MAIRS was found to be powerful to reveal the anisotropic structure of the Langmuir films, and a disordered molecular architecture has been revealed via the molecular orientation analysis. As a result, the fibril-like aggregation formation process during the monolayer compression, which was suggested by previous topographical study, has been found to be due to the stiff domain formation in the Langmuir films.     

Mixed monolayers to promote g-protein adsorption: alpha2A-adrenergic receptor-derived peptides coadsorbed with formyl-terminated oligopeptides

Pure and mixed monolayers of a synthetic peptide, GPR-i3n, derived from the third intracellular loop of the alpha2 adrenergic receptor and a shorter inactive oligopeptide, N-formyl-(Gly)3-(Cys) (called 3GC), were prepared on gold surfaces. The mixing ratio of the GPR-i3n and 3GC was used to control G-protein binding capability. The GPR-i3n peptide is specially designed for bovine G-protein selectivity and has been proven to have high affinity to G-proteins [Vahlberg, C.; Petoral, R. M., Jr.; Lindell, C.; Broo, K.; Uvdal, K. Langmuir 2006, 22 (17), 7260-7264]. Pure 3GC monolayers show very low protein adsorption capability. In this study, 3GC is chosen as a coadsorbent, with the aim to induce molecular conformational changes during monolayer formation to enhance G-protein adsorption. A full characterization of the mixed monolayers was done. The monolayer thickness and the mass-related surface coverage for both GPR-i3n and 3GC were investigated using radio labeling. The GPR-i3n was labeled by 125I-targeting tyrosine, and the activity was measured by using radioimmunoassay (RIA). The formation and chemical composition of GPR-i3n and 3GC monolayers were investigated using X-ray photoelectron spectroscopy, and it is shown that both GPR-i3n and 3GC bind chemically to the gold surface. The interaction between the mixed monolayers and G-proteins was investigated by means of real-time surface plasmon resonance. There is a higher protein binding capacity to the monolayer when the GPR-i3n peptide is intermixed with the 3GC coadsorbent, despite the fact that the 3GC itself has a very low G-protein binding capability. This supports a molecular reorientation at the surface, while 3GC is intermixed with GPR-i3n.     

2-烷基-苯并咪唑在硝酸银亚相上的Langmuir膜及LB膜

对不同链长的2-烷基-苯并咪唑衍生物（BzCn,烷基链长从C5到C15）在硝酸银亚相上的成膜行为及形成的LB膜的结构进行了研究.表面压－面积曲线的结果表明，短链(C5～C9)的2-烷基-苯并咪唑可在银离子亚相上形成稳定的单分子膜，而长链(C13和C15)衍生物则形成多层膜.利用LB技术可将上述Langmuir膜转移到固体基板上形成LB膜，其吸收光谱的结果说明了苯并咪唑和银离子配位.利用AFM、XRD及FT-IR等技术研究了烷基链长对LB膜结构的影响.实验结果表明,除了BzC15，其余的衍生物都可形成规整的层状结构.短链衍生物的单层LB膜具有均一、平整的形貌；而对于BzC15，观察到多层结构.     

Effects of lipid chain length on molecular interactions between paclitaxel and phospholipid within model biomembranes

Molecular interactions between an anticancer drug, paclitaxel, and phosphatidylcholine (PC) of various chain lengths were investigated in the present work by the Langmuir film balance technique and differential scanning calorimetry (DSC). Both the lipid monolayer at the air-water interface and lipid bilayer vesicles (liposomes) were employed as model biological cell membranes. Measurement and analysis of the surface pressure versus molecular area curves of the mixed monolayers of phospholipids and paclitaxel under various molar ratio showed that phospholipids and paclitaxel formed a nonideal miscible system at the interface. Paclitaxel exerted an area-condensing effect on the lipid monolayer at small molecular surface areas and an area-expanding effect at large molecular areas, which could be explained by the intermolecular forces and geometric accommodation between the two components. Paclitaxel and phospholipids could form thermodynamically stable monolayer systems: the stability increased with the chain length in the order DMPC (C14:0)>DPPC (C16:0)>DSPC (C18:0). Investigation of paclitaxel penetration into the pure lipid monolayer showed that DMPC had a higher ability to incorporate paclitaxel and the critical surface pressure for paclitaxel penetration also increased with the chain length in the order DMPC>DPPC>DSPC. A similar trend was testified by DSC studies on vesicles of the mixed paclitaxel/phospholipids bilayer. Paclitaxel showed the greatest interaction with DMPC while little interaction could be measured in the paclitaxel/DSPC liposomes. Paclitaxel caused broadening of the main phase transition without significant change at the peak melting temperature of the phospholipid bilayers, which demonstrated that paclitaxel was localized in the outer hydrophobic cooperative zone of the bilayer. The interaction between paclitaxel and phospholipid was nonspecific and the dominant factor in this interaction was the van der Waals force or hydrophobic force. As the result of the lower net van der Waals interaction between hydrocarbon chains for the shorter acyl chains, paclitaxel interacted more readily with phospholipids of shorter chain length, which also increased the bilayer intermolecular spacing.     

Phase transition in an adsorption layer of a soluble surfactant at the air-water interface

In this paper we provide experimental evidence for a phase transition between a liquid- and gas-like phase occurring in an adsorption layer of a soluble surfactant at the air-water interface. The equilibrium surface tension sigma(e) versus bulk concentration sigma(e) (c) isotherm of surface chemically pure sodium 2-[4-(4-trifluoromethyl-phenylazo) phenoxy]-ethane sulfonate was measured at a temperature of 295 K up to the solubility limit of the amphiphile. The sigma(e) (c) isotherm could be fitted by Frumkin's equation of state. The lateral interaction energy is just above the limit for which Frumkin's model predicts a phase transition. The corresponding surface pressure pi versus surface area A isotherm possesses striking similarities to first-order phase transitions in the Langmuir monolayer. The fact that the difference in the two-dimensional density is only a factor of 2 indicates that the system is very close to the critical point. The surface phases were further characterized by surface second harmonic generation. The major structural difference between the two surface phases is the amphiphile's molecular orientation. A mean orientation of the amphiphile of about 80 degrees was found in the gas analogous phase, whereas a molecular tilt of 38 degrees has been identified in the liquid-like phase.     

Effect of alkanethiol chain length on gold nanoparticle monolayers at the air-water interface

In this study, we report the effects of the alkyl chain length on alkanethiol-capped gold nanoparticle Langmuir films. Gold nanoparticles (2-3 nm) capped with C(n)H(2n+1)SH (n = 5-12, 14-16, 18) were prepared via a two-phase synthesis. The films were sampled by Langmuir-Schaefer horizontal transfer at various points in the pressure-area isotherm and monitored with transmission electron microscopy. Changes in surface pressure, temperature, and alkyl chain length did not lead to observable differences in the mesoscale film morphology. Pressure-area isotherms at 22 °C, however, revealed that the work of compression and the collapse pressure are directly dependent on alkyl chain lengths of 14 carbons or greater. Variable temperature isotherms suggest that the work of compression is strongly affected by the phase state (i.e., crystalline vs liquid-like) of the gold-thiolate self-assembled monolayer (SAM) capping the nanoparticles.     

Molecular Dynamic Studies on Langmuir Monolayers of Stearic Acid

Compression isotherm for stearic acid was obtained by means of molecular dynamic simulation and compared to experimentally measured values for the Langmuir monolayers. Compared to the previous simulation, the present simulation has provided a method to reproduce the compression of the monolayer. The result is consistent with other experimental results. By analyzing the alkyl tails, the configuration of stearic acid molecules during the compression process was studied and a uniform monolayer was obtained after compression. Stearic acid molecules were observed to form fine organized monolayer from completely random structure. Hexatic order of the arrangement has been identified for the distribution of stearic acid molecules in the monolayer. At the end of the compression, the stearic acid molecules were tightly packed in the gap of two other molecules. At last, the hydrogen bonds in the system were analyzed. The main hydrogen bonds were from stearic acid-water interaction and their intensities constantly decreased with the decreased of surface area per molecule. The weak hydrogen bond interaction between stearic acid molecules may be the reason of easy collapse.     

The interaction of an antiparasitic peptide active against African Sleeping Sickness with cell membrane models

Zwitterionic peptides with trypanocidal activity are promising lead compounds for the treatment of African Sleeping Sickness, and have motivated research into the design of compounds capable of disrupting the protozoan membrane. In this study, we use the Langmuir monolayer technique to investigate the surface properties of an antiparasitic peptide, namely S-(2,4-dinitrophenyl)glutathione di-2-propyl ester, and its interaction with a model membrane comprising a phospholipid monolayer. The drug formed stable Langmuir monolayers, whose main feature was a phase transition accompanied by a negative surface elasticity. This was attributed to aggregation upon compression due to intermolecular bond associations of the molecules, inferred from surface pressure and surface potential isotherms, Brewster angle microscopy (BAM) images, infrared spectroscopy and dynamic elasticity measurements. When co-spread with dipalmitoyl phosphatidyl choline (DPPC), the drug affected both the surface pressure and the monolayer morphology, even at high surface pressures and with low amounts of the drug. The results were interpreted by assuming a repulsive, cooperative interaction between the drug and DPPC molecules. Such repulsive interaction and the large changes in fluidity arising from drug aggregation may be related to the disruption of the membrane, which is key for the parasite killing property.     

Nonionic surfactant sorption onto the bacterial cell surface: a multi-interaction isotherm

The adsorption of linear polyoxyethylene (POE) alcohol surfactants of the form CxEy onto the surface of a Sphingomonas sp. has been examined. For this study, the alkyl chain length (x) was fixed at 12 and the POE chain length (y) was varied, with y = 4, 7, 9, 10, and 23 ethylene oxide units. Langmuirian isotherms were observed for C12E4 and C12E23, and more complex isotherms were observed for the three intermediate POE chain length surfactants, with C12E7 and C12E9 exhibiting strong S-shaped isotherms. All isotherms showed plateaus near the critical micelle concentration (CMC) with the plateau decreasing with increasing POE chain length. A simple multi-interaction isotherm is proposed that models the sorption isotherm as the sum of two interactions. The first interaction describes monolayer adsorption, whereas the second interaction describes lateral interactions between sorbed surfactant molecules and the formation of surface aggregates. Varying ratios of these two interactions as a function of POE chain length gives rise to the variety of observed isotherm shapes. Results of the isotherm analysis suggest that lateral interactions dominate for surfactants with low POE chain lengths, and the lateral interactions decrease as the POE chain length is increased.     

Interaction of the antimicrobial peptide dicynthaurin with membrane phospholipids at the air-liquid interface

This paper reports the first study on the interaction of the antimicrobial peptide dicynthaurin with 1,2-dipalmitoyl-glycerophosphatidyl-glycerol investigated in monolayers at the air-liquid interface. The influence of the peptide on the two-dimensional phase behavior of the negatively charged lipid was elucidated by means of pressure-area isotherm measurements, fluorescence microscopy, and grazing incidence X-ray diffraction measurements. The pure peptide forms a stable monolayer at the air-liquid interface up to 30 mN/m as shown for both the monomeric and the dimeric cynthaurins. The peptide lipid interaction was monitored in isotherm measurements showing a strong adsorption of the peptide and stabilization at the interface promoted by the lipid monolayer. The X-ray diffraction measurements in agreement with fluorescence microscopy studies showed that the peptide destabilizes the condensed chain lattice, leading to a complete fluidization of the condensed lipid phase on physiological buffer. The adsorption of the peptide to the negatively charged lipid monolayer and the fluidization of the condensed chain lattice suggest a direct link to the peptides' ability to expand the bacterial membrane that would be relevant for the in vivo mode of action.     

The interaction between G-quadruplex-forming oligonucleotide and cationic surfactant monolayer at the air/water interface

We report on the interactions between a 21-mer quadruplex-forming oligonucleotide bearing human telomere sequence of dG(3)(T(2)AG(3))(3) (G4 DNA) and a positively charged dioctadecyldimethylammonium bromide (DODAB) monolayer at the air-aqueous interface, studied by surface film balance measurements. In the presence of G4 DNA, the π-A isotherm of the cationic Langmuir film shifted to lower molecular areas when compared with the reference isotherm recorded on the subphase containing only 50 mM triethylamine-acetate (TEAA) buffer. The presence of quadruplex-stabilizing metal cations (K(+) or Na(+)) further affected profiles of π-A isotherms. Further insight into processes related to the G4 DNA-monolayer interactions was provided by recording time profiles of the surface pressure of monolayer at a constant mean molecular area. In these experiments G4 DNA and/or metal ions were sequentially injected under the monolayer surface. Results indicated that multistranded assemblies of G4 DNA were formed at the monolayer interface even in the absence of metal ions, which suggested that the charged cationic surface of Langmuir monolayer induced aggregation of guanine-rich DNA strands. The presence of sodium and potassium ions inhibited formation of multi-stranded assemblies through the competitive G-quadruplex formation but to different extent that might be related to the differences in stability and topology of both quadruplexes.     

髓鞘碱性蛋白对细胞膜脂质分子DPPC、DPPE单层膜影响机理研究

本文通过Langmuir单层膜的表面压力-平均分子面积(π-A)曲线的测定与分析,分别对髓鞘碱性蛋白(MBP)与细胞膜中不同头部基团脂质分子二棕榈酰基磷脂胆碱(DPPC)和二棕榈酰基磷脂酰乙醇胺(DPPE)在空气/液体界面上的相互作用过程进行了系统研究.实验结果表明:(1)当界面上脂质含量一定时,亚相中随着MBP浓度的增大,DPPC、DPPE单层膜的等温线向平均分子面积较大的方向移动;(2)在单层膜表面压力为10 mN/m时,一个MBP分子分别结合140±3个DPPC分子和100±3个DPPE分子,随着表面压力增大,当MBP分子分别与两种磷脂分子相互作用时,MBP插入到磷脂单层界面的个数逐渐减少;(3)随着蛋白质浓度的增加,脂分子形成的单层膜变得较为疏松,且MBP分子易于插入到分子头部较小的DPPE单层膜中;(4)蛋白质的存在使DPPC单层膜的表面压力逐渐减小,且蛋白质浓度越大表面压力降低越多,DPPC被MBP带入到亚相中越多;(5)对于DPPE单层膜,蛋白质通过与DPPE相互作用插入到界面膜中,引起表面压力增大,且蛋白质浓度越高,压力变化量越大.     

Adsorption studies of acetic acid dimers on activated charcoal from organic solvents

Acetic acid exists as dimers in organic solvents like benzene, toluene and xylene. Adsorption of dimeric acetic acid on activated charcoal (AC) at various temperatures from benzene, toluene and xylene solutions have been studied. The system obeys Langmuir isotherm, thus signifying a monolayer adsorption of dimers. Corrections on AC-solvent pore volume fillings, molecular cross sectional surface area of acetic acid dimers, the adsorption equilibrium constants, the free energy change and the enthalpy change values are computed at different temperatures for the three solvents. The adsorption process has been found to be physisorption type. The FTIR measurements show that the adsorbed acetic acid dimer seems to retain the cyclic structure against the open chain non-cyclic structure.     

Restructuring of hydrophobic surfaces created by surfactant adsorption to mica surfaces

Hydrophobic surfaces created by the adsorption of a monolayer of surfactants, such as CTAB or DODAB, to mica display long-range mutual attraction when placed in water. Initially, this attraction was considered to be due to hydrophobic interaction, but more careful measurements using AFM showed that the surfactant monolayer undergoes rearrangements to produce charged patches on the surface; therefore, the nature of the long-range interaction is due to the electrostatic interaction between patches. The monolayer rearrangement depends on the nature of the surfactant and its counterion. To study possible monolayer rearrangements in molecular detail, we performed detailed molecular dynamics computer simulations on systems containing a monolayer of surfactants RN(CH(3))(3)(+)Cl(-) (R indicates a saturated hydrocarbon chain) adsorbed on a mica surface and immersed in water. We observe that when chain R is 18 carbons long the monolayer rearranges into a micelle but it remains a monolayer when the chain contains 24 carbons.