磷脂单分子膜普适状态方程研究

从现有的磷脂单分子膜状态方程入手, 以磷脂临界相变面积(A_c)和相变温度(T_c)为参比, 引入对比面积(A_r), 对比温度(T_r), 并通过分析磷脂分子间作用力和底液分子与磷脂分子间作用力的影响, 提出了第三参数——相对铺展因子的概念, 导出了磷脂单分子膜普适状态方程. 运用1,2-二豆蔻酰基-sn-丙三基-3-磷脂酸, 1,2-二豆蔻酰基-sn-丙三基-3-磷脂酰胆碱, 1,2-二棕榈酰基-sn-丙三基-3-磷脂酰胆碱等磷脂单分子膜的实验数据进行一致性校验的结果表明, 该模型在扩展膜(LE)直至凝聚膜(LC)的整个区域均能较好地描述磷脂单分子膜的π-A曲线. 所获得的各磷脂的相对铺展因子绝对值直接表明了该物质的成膜特性.     

Equation of state for the phase coexistence region of insoluble monolayers under consideration of the entropy nonideality

The equation of state for the monolayer with a fluid (G, LE)/condensed (LC) phase transition derived earlier (Fainerman, V.B.; Vollhardt, D. J. Phys. Chem. B 1999, 103, 145) in the framework of a quasichemical approach is generalized. A term is added that takes into account the entropy nonideality of mixing of the monomers and clusters of amphiphilic molecules. The results calculated from the proposed equations agree well with the experimental Pi-A isotherms obtained for various types of amphiphilic monolayers. The values of molecular areas of the amphiphilic molecules estimated from the fitting of experimental data to the proposed equation are quite similar to the real values. Another equation of state capable of describing the fluid state of insoluble monolayers and based on equations for the chemical potential of the solvent in the bulk phase and in the surface layer (Fainerman, V. B.; Vollhardt, D. J. Phys. Chem. B 2006, 110, 10436) is also generalized to be extended to the fluid/condensed phase transition region (A < A(c)), taking into account entropy nonideality for mixing solvent molecules, monomers, and clusters of amphiphilic molecules. The values calculated on this basis agree also well with the experimental data.     

压缩速度对Surfactin在单分子膜内聚集行为的影响

研究了一种微生物脂肽——Surfactin(表面活性素)在气/液界面形成的单分子膜性质, 测定了压缩速度对其单分子膜的表面压-分子面积(π-A)曲线的影响. 结果表明, Surfactin单分子膜铺展在pH＝2酸性亚相上的过程是一个亚稳过程. 通过原子力显微镜(AFM)观察了不同压缩速度时在25 mN&#8226;m－1下转移的Langmuir-Blodgett (LB)膜. 在中等压缩速度(0.6 nm2&#8226;mol－1&#8226; min－1)时转移的LB膜表面观察到分布均匀、排列规则、类似球形的表面聚集体, 而在其它压缩速度下, 形成了按一定规则分布的表面团簇结构. 结合π-A曲线和AFM图像, 提出了Surfactin表面聚集体在气/液界面上的形成机制.     

Lipolysis of didecanoyl-lecithin/triolein mixed monolayers by phospholipaseA 2

A study of enzyme lipolysis by pancreatic phospholipaseA ₂ and by vipera berus phospholipaseA ₂ on monomolecular mixed films of didecanoyl-lecithin and triolein on an aqueous subphase of pH 8 has been carried out. The influence of the composition of the mixed film, the surface pressure of the film and the amount and type of the injected enzyme on the lipolysis rate were studied.In order to relate the lipolytic activity with the monolayer state, the compression isotherms of the didecanoyl-lecithin/triolein mixed monolayers have also been obtained.The resuls are compared to observations on lipolytic activity of phospholipaseA ₂ on the didecanoyl-lecithin/cholesterol mixed monolayers. Triolein improves the kinetic conditions of the lipolysis of lecithin films in a higher degree than cholesterol. Probably it increases the enzyme penetration by the fluidifying effect exerted on the lecithin monolayers.     

Separation and characterization of aggregated species of amyloid-beta peptides

We have investigated the use of isoelectric focusing and immunodetection for the separation of low molecular weight species of amyloid-beta (Aβ) peptides from their aggregates. From solutions of Aβ_1–40 or Aβ_1–42 monomeric peptides, low molecular weight material appeared at a pI value of ca. 5, while the presence of aggregates was detected as bands, observed at a pI of 6–6.5. The formation of Aβ aggregates (protofibrils) was verified by a sandwich ELISA, employing the protofibril conformation-selective antibody mAb158. In order to study the aggregation behavior when using a mixture of the monomers, we utilized the IEF separation combined with Western blot using two polyclonal antisera, selective for Aβ_1–40 and Aβ_1–42, respectively. We conclude that both monomers were incorporated in the aggregates. In a further study of the mixed aggregates, we used the protofibril conformation-selective antibody mAb158 for immunoprecipitation, followed by nanoelectrospray mass spectrometry (IP-MS). This showed that the Aβ_1–42 peptide is incorporated in the aggregate in a significantly larger proportion than its relative presence in the original monomer composition. IP-MS with mAb158 was also performed, and compared to IP-MS with the Aβ-selective antibody mAb1C3, where a monomeric Aβ_1–16 peptide was added to the protofibril preparation. Aβ_1–16 is known for its poor aggregation propensity, and acted therefore as a selectivity marker. The results obtained confirmed the protofibril conformation selectivity of mAb158.     

Interactions of α-Lactalbumin and Cytochrome c with Langmuir Monolayers of Glycerophospholipids

Interaction of cytochrome c (Cyt c), α-lactalbumin III (α-La III) with Langmuir monolayers of pure and mixed glycerophospholipids was investigated using surface pressure-area (Π-A) isotherms. The general trend was that maximum interaction between protein and phospholipid is observed for mixed (1:1 molar ratio) phospholipid monolayers. Interaction between the protein and the charged phospholipid films was found to be independent of global protein charge. Our data indicate that the proteins interact with the phospholipid films by inserting themselves into the monolayer rather than anchoring to the phospholipid head groups.     

Phenomenological theory of the kinetics of ultrasonic emulsification

Summary A working model is given for the rate of ultrasonic emulsification, considering the dispersion at the interface (areaA) and the coagulations in the volumeV of the emulsion. A bimolecular coagulation leads to the equationc=c _∞tanhbt;c _∞=(Aα/Vβ)^1/2;b=(Aαβ/V)^1/2 while a monomolecular coagulation givesc=c _∞{1−exp (−at)};c _∞=Aα/Vβ;a=β. The experiments on the dependence of c_∞,a andb uponA andV favour the bimolecular coagulation. The results are satisfactorily explained on general theoretical grounds.

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Zusammenfassung Ein Arbeitsmodell für die Geschwindigkeit der Ultraschallemulgierung wird entwickelt, das Dispersion in der Grenzfl?che (Fl?cheA) und Koagulation im Volumen (V) der Emulsion annimmt. Eine bimolekulare Koagulation führt zu der Gleichung:c=c _∞ tanhbt;c _∞=(Aα/Vβ)^1/2;b=(Aαβ/V)^1/2, eine monomolekulare dagegen zu:c=c _∞{1−exp (at−)};c _∞=Aα/Vβ;α=β. Die Versuche über die Abh?ngigkeit vonc _∞,a undb vonA undV scheinen für bimolekulare Koagulation zu sprechen. Die Ergebnisse werden auf der Basis dieser einfachen theoretischen Grundlagen befriedigend erkl?rt.

     

Adsorption of TX100 and TX165 at the aqueous solution–air interface: free enthalpy of adsorption and equation of state

Surface tension measurements of aqueous solutions of TX100 and TX165 were made at different temperatures. The thermodynamic parameters of the adsorption calculated from the surface tension measurements, using several methods, have given slightly different values. The equation of state for the TX100 and TX165 monolayers at the solution–air interface was analysed. There is excellent agreement between the modified Volmer equation of state and the experimental π–A isotherms. Received: 13 July 1999/Accepted in revised form: 20 October 1999     

Correlations between chemical structure and chain packing in two- and three-dimensional systems

Phosphatidylcholines (PCs) containing a branched chain fatty acid at the sn-1 position of the glycerol backbone were characterized by calorimetric and X-ray diffraction studies with bilayers as well as by thermodynamic studies with monolayers. Branching leads to altered thermal properties which are connected with a modified structural polymorphism. Gel phases with interdigitated chains or nonbilayer liquid-crystalline phases could be found in dependence on the length of the side branches. The pressure-area isotherms of the monobranched PCs were measured over a wide range of temperature. The critical temperatures T_c of the transition between the liquid-expanded and condensed films were estimated and compared with the main transition temperatures T_m of the bulk phase. T_c was found to be either lower or higher or equal to T_m. The correlations between T_c and T_m are discussed in terms of chain packing in the two- and threedimensional systems.     

Miscibility of mixed stereoregular PMMA/PVPh monolayers at the air/water interface

The mixed monolayer behavior of stereoregular poly(methyl methacrylate) (PMMA) and poly(vinyl phenol) (PVPh) was investigated from the measurements of surface pressure–area per molecule (π–A) isotherms. The π–A isotherms indicated that isotactic PMMA (iPMMA) and PVPh were miscible at the air/water interface. The miscibility and non-ideality of the mixed monolayers were examined by calculating the excess area as a function of composition, and negative deviations from ideality were observed, which suggest the existence of attractive interactions between iPMMA and PVPh. However, the π–A isotherms of mixed syndiotactic PMMA (sPMMA)/PVPh monolayers showed positive deviation from ideality, which might suggest that non-favorable interactions exist between sPMMA and PVPh.The π–A isotherms of mixed atactic PMMA (aPMMA)/PVPh monolayers exhibited complicated excess area behavior. Both positive and negative deviations from ideality were observed at various surface pressures. These isotherm results of mixed polymers correlate approximately well with the miscibility of the corresponding mixtures in the bulk state. The formation of hydrogen bonding between PMMA and PVPh was substantiated in the bulk state by means of Fourier transform infrared (FTIR). Regardless of tacticity, an increase of hydrogen-bonded carbonyl fraction was observed.     

Effects of Fullerenes on Phospholipid Membranes: A Langmuir Monolayer Study

We investigate two‐component Langmuir monolayers of dipalmitoylphosphatidylcholine (DPPC)/C₆₀ by recording surface pressure/area (π/A) and surface potential/area (ΔV/A) isotherms and by direct Brewster angle microscopy (BAM) imaging. Atomic force microscopy (AFM) is employed to study morphologies of the mixed monolayers transferred to a solid substrate by the Langmuir–Blodgett technique. C₆₀ is shown to have little influence on isotherms of the DPPC/C₆₀ monolayers even at a molar fraction as high as X_C60=0.3. The elastic modulus ( ) versus π curves of the DPPC/C₆₀ monolayers almost overlay each other, as well as that of pure DPPC, that is, the elasticities of pure DPPC monolayers and DPPC/C₆₀ monolayers are remarkably similar. AFM studies reveal that fullerene flocs form at low surface pressures (π≤15 mN m^?1), are gradually disaggregated and dispersed in the DPPC monolayer with increasing surface pressure up to 35 mN m^?1, and are then progressively squeezed out to form protruded islands as the surface pressure increases up to 65 mN m^?1. Our work provides experimental support to the computational result that C₆₀ can dissolve in lipid bilayers without significantly compromising their mechanical properties, a finding which has important implications for the toxicity and development of drug vehicles from fullerene materials.     

Characterizing Methyl‐Bearing Side Chain Contacts and Dynamics Mediating Amyloid β Protofibril Interactions Using 13Cmethyl‐DEST and Lifetime Line Broadening

Many details pertaining to the formation and interactions of protein aggregates associated with neurodegenerative diseases are invisible to conventional biophysical techniques. We recently introduced ¹⁵N dark‐state exchange saturation transfer (DEST) and ¹⁵N lifetime line‐broadening to study solution backbone dynamics and position‐specific binding probabilities for amyloid β (Aβ) monomers in exchange with large (2–80 MDa) protofibrillar Aβ aggregates. Here we use ¹³C_methyl DEST and lifetime line‐broadening to probe the interactions and dynamics of methyl‐bearing side chains in the Aβ‐protofibril‐bound state. We show that all methyl groups of Aβ40 populate direct‐contact bound states with a very fast effective transverse relaxation rate, indicative of side‐chain‐mediated direct binding to the protofibril surface. The data are consistent with position‐specific enhancements of ¹³C_methyl‐${R{{{\rm tethered}\hfill \atop 2\hfill}}}$ values in tethered states, providing further insights into the structural ensemble of the protofibril‐bound state.     

Submonolayer-Deposition of Mass-Selected Au+ and Au n + (n = 3 and 7) on HOPG and Amorphous Carbon

Ions of gold monomer and clusters emitted from a liquid metal ion source were mass-selected, and deposited on cleaved HOPG (highly oriented pyrolytic graphite) surfaces and on amorphous carbon thin films at room temperature with the impinging energy E _i from 0 to 500 eV. The coverage of deposited ions were 1/100 and 1/1000 monolayers on HOPG surfaces and 1/3 monolayers on carbon films. Scanning tunneling microscopy of the HOPG surfaces deposited with low impinging energy (E _i<50 eV) revealed that large clusters with diameters ranging from 2 to 5 nm and height of 1–2 layers were present instead of isolated monomers and original clusters. When E _i was higher than 100 eV, HOPG surfaces were damaged and only bumpy surfaces were observed by STM. Transmission electron microscopy of Au⁺-deposited carbon films showed the formation of clusters with diameter 0.5–20 nm, depending on the E _i and the time elapsed after deposition.     

Dynamic Behaviors and Morphology Change of Anionic Phospholipid DPPG Monolayer Caused by Bovine Serum Albumin at Air-Water Interface

The interaction between bovine serum albumin (BSA) and the anionic 1.2-dipalmitoyl-snglycero- 3-(phospho-rac-(1-glycerol)) (sodium salt) (DPPG) phospholipid at different subphase pH values was investigated at air-water interface through surface pressure measurements and atomic force microscopy (AFM) observation. By analyzing surface pressure-mean molecular area (π-A) isotherms, the limiting molecular area in the closed packing state-the concentration of BSA (A_lim-[BSA]) curves, the compressibility coefficient-surface pressure (C_S^-1-π) curves and the difference value of mean molecular area-the concentration of BSA (ΔA-[BSA]) curves, we obtained that the mean molecular area of DPPG monolayer became much larger when the concentration of BSA in the subphase increased at pH=3 and 5. But the isotherms had no significant change at different amount of BSA at pH=10. In addition, the amount of BSA molecules adsorbed onto the lipid monolayer reached a threshold value when [BSA]>5×10^-8 mol/L for all pHs. From the surface pressure-time (π-t) data, we obtained that desorption and adsorption processes occurred at pH=3, however, there was only desorption process occurring at pH=5 and 10. These results showed that the interaction mechanism between DPPG and BSA molecules was affected by the pH of subphase. BSA molecules were adsorbed onto the DPPG monolayers mainly through the hydrophobic interaction at pH=3 and 5, and the strength of hydrophobic interaction at pH=3 was stronger than the case of pH=5. At pH=10, a weaker hydrophobic interaction and a stronger electrostatic repulsion existed between DPPG and BSA molecules. AFM images revealed that the pH of subphase and [BSA] could affect the morphology features of the monolayers, which was consistent with these curves. The study provides an important experimental basis and theoretical support to understand the interaction between lipid and BSA at the air-water interface.     

Interfacial behaviour of wheat puroindolines: monolayers of puroindolines at the air–water interface

Puroindolines are among the major basic and cysteine-rich lipid binding proteins of wheat seeds. The interfacial properties of puroindoline-a (PIN-a) and puroindoline-b (PIN-b) are important both from a biological and a technological point of view. In the work reported here, the interfacial characteristics of spread monolayers of wheat puroindolines at the air–water interface were studied at varying subphase compositions using a Langmuir–Blodgett film balance. The compression isotherms (π–A _Sp) were recorded at constant barrier speed (3.3 cm/min). It was observed that both PIN-a and PIN-b form stable monolayers at the air–water interface. The stability of the monolayers was found to be dependent on the subphase composition as well as on the concentration of protein in the spreading solution. When the ionic strength of the subphase is below 0.50, the compression isotherms of both PIN-a and PIN-b remains unaffected with the change in the ionic strength of the subphase; however, when the ionic strength is above 0.50, the compression isotherms of both PIN-a and PIN-b undergo significant change with an increase in the ionic strength of the subphase. A gradual increase in the values of the collapse pressure (π_C) and the limiting area (A ₀) was observed due to an increase in the ionic strength of the subphase from 0.5 to 4.0, which may be correlated with the salt-induced conformational changes of the protein molecule. The presence of NaCl and KCl (ionic strength 1.0) in the subphase has a comparable effect on the compression isotherms of both PIN-a and PIN-b; however, the presence of CaCl₂ (ionic strength 1.0) in the subphase leads to an increase in the values of π_C and A ₀. A change in the pH of the subphase from 3.0 to 7.2 was to have a significant effect on the values of π_C and A ₀, which may be due to the pH-induced alteration of the protein conformation. Received: 8 August 2000 Accepted: 15 December 2000     

Penetration of dissolved amphiphiles into two-dimensional aggregating lipid monolayers

The review demonstrates the recent theoretical and experimental progress in the understanding of penetration systems at the air-water interface in which a dissolved amphiphile (surfactant, protein) penetrates into a Langmuir monolayer. The critical review of the existing theoretical models which describe the thermodynamics of the penetration are critically reviewed. Although a rigorous thermodynamic analysis of penetration systems is unavailable due to their complexity, some model assumptions, e.g. the invariability of the activity coefficient of the insoluble component of the monolayer during the penetration of the soluble component results in reasonable solutions. New theoretical models describing the equilibrium behaviour of the insoluble monolayers which undergo the 2D aggregation in the monolayer, and the equations of state and adsorption isotherms which assume the existence of multiple states (conformations) of a protein molecule within the monolayer and the non-ideality of the adsorbed monolayers are now available. The theories which describe the penetration of a soluble surfactant into the main phases of Langmuir monolayers were presented first for the case of the mixture of the molecules possessing equal partial molar surfaces (the mixture of homologues), with further extension of the models to include the interesting process of the protein penetration into the monolayer of 2D aggregating phospholipid. This extension was based on a concept which subdivides the protein molecules into independent fragments with areas equal to those of the phospholipid molecule. Various mechanisms for the effect of the soluble surfactant on the aggregation of the insoluble component were considered in the theoretical models: (i) no effect on the aggregate formation process; (ii) formation of mixed aggregates; and (iii) the influence on the aggregating process via the change of aggregation constant, but without any formation of mixed aggregates. Accordingly depending on the mechanism, different forms of the equations of state of the monolayer and of the adsorption isotherms of soluble surfactant are predicted. Based on the shape of the experimental pi-A isotherms, interesting conclusions can be drawn on the real mechanism. First experimental evidence has been provided that the penetration of different proteins and surfactants into a DPPC monolayer in a fluid-like state induces a first order main phase transition of pure DPPC. The phase transition is indicated by a break point in the pi(t) penetration kinetics curves and the domain formation by BAM. Mixed aggregates of protein with phospholipid are not formed. These results agree satisfactorily with the predictions of the theoretical models. New information on phase transition and phase properties of Langmuir monolayers penetrated by soluble amphiphiles are obtained by coupling of the pi(t) penetration kinetics curves with BAM and GIXD measurements. The GIXD results on the penetration of beta-lactoglobulin into DPPC monolayers have shown that protein penetration occurs without any specific interactions with the DPPC molecules and the condensed phase consists only of DPPC.     

Saturation spectroscopy of NH2 using a CW dye laser

Hyperfine structure in the electronic spectrum of NH₂ has been resolved using the technique of intermodulated fluorescence with CW dye laser excitation. From the observed spacings values for the ¹⁴N Fermi contact and dipole-dipole coupling terms have been estimated for both the ground state and the Π(0,10,0) vibrational level of the à ²A₁ excited electronic state.     

Simulation of first- and second-order transitions in asymmetric polymer mixtures

The critical properties of dense asymmetric binary polymer mixtures are studied by grand canonical simulations within the framework of the 3-dimensional bond fluctuation lattice model. The monomers interact with each other via a potential ranging over the entire first peak of the pair distribution. An asymmetry is realized by giving the ratio of interactions λ = ∈_AA/∈_BB between monomers of the A-species and of the B-species a value different from 1. Using multiple histogram extrapolation techniques for the data analysis, the two phase region, which is a line of first-order transitions driven by the chemical potential difference, and the critical point are determined for a mixture of chains with 32 monomers each. At a critical potential difference Δμ_c unmixing occurs below a critical temperature T_c. It is found that Δμ_c is proportional to the asymmetry (1 - λ) and that the quantity 4k_BT_c/(3 + λ)∈ is independent of the asymmetry, consistent with the prediction of the Flory theory.     

Glycoprotein adsorption into bilirubin/cholesterol mixed monolayers at the air-water interface

The adsorption of α₁-acid glycoprotein into bilirubin/cholesterol mixed monolayers with various component molar ratios is investigated using surface pressure-area (π-A) isotherms and (dπ/dA)-A curves. The results showed that the surface area per molecule increased after the adsorption/insertion of glycoprotein molecules into the monolayers. The compressibility of mixed monolayers increased as a result of hydrogen bonding between bilirubin and glycoprotein molecules, while the interactions between bilirubin and cholesterol are weakened. The adsorption of glycoprotein into a monolayer induced changes in molecular surface area depending on the surface pressure and molar fraction of bilirubin. The transmission electron microscopy of mixed monolayers confirmed the insertion of glycoprotein particles of spherical shape with an average diameter of about 80 nm into the monolayer. The text was submitted by the authors in English.