Probing the Molecular Structure and Dynamics of Membrane-Bound Proteins during Misfolding Processes by Sum-Frequency Generation Vibrational Spectroscopy.

Protein misfolding and amyloid formation are implicated in the protein dysfunction, but the underlying mechanism remains to be clarified due to the lack of effective tools for detecting the transient intermediates. Sum frequency generation vibrational spectroscopy (SFG-VS) has emerged as a powerful tool for identifying the structure and dynamics of proteins at the interfaces. In this review, we summarize recent SFG-VS studies on the structure and dynamics of membrane-bound proteins during misfolding processes. This paper first introduces the methods for determining the secondary structure of interfacial proteins: combining chiral and achiral spectra of amide A and amide I bands and combining amide I, amide II, and amide III spectral features. To demonstrate the ability of SFG-VS in investigating the interfacial protein misfolding and amyloid formation, studies on the interactions between different peptides/proteins (islet amyloid polypeptide, amyloid ß, prion protein, fused in sarcoma protein, hen egg-white lysozyme, fusing fusion peptide, class I hydrophobin SC3 and class II hydrophobin HFBI) and surfaces such as lipid membranes are discussed. These molecular-level studies revealed that SFG-VS can provide a unique understanding of the mechanism of interfacial protein misfolding and amyloid formation in real time, in situ and without any exogenous labeling.

Orientation of Thiocyanate Ions Tuning the Electron-Phonon Interactions in Pseudohalide Perovskites.

Although the importance of electron-phonon interactions on the optoelectronic properties of perovskites has been well documented, the structural origin of electron-phonon interactions remains largely unexplored. In this study, using pseudohalide perovskites Cs2Pb(SCN)2I2(1-x)Br2x as a model, we have revealed how the orientation of SCN- anions tunes the electron-phonon interactions and the effective charge-carrier mobility by utilizing femtosecond sum frequency generation vibrational spectroscopy, supplemented by photoluminescence spectroscopy and femtosecond optical-pump terahertz-probe spectroscopy. The coupling between neighboring SCN- anions decreases as the Br content (x) increases but does not have a significant effect on the electron-phonon interactions. In contrast, the orientation angle of SCN- anions has a strong correlation with the electron-phonon interaction and effective charge-carrier mobility, that is, a more parallel orientation of SCN- anions leads to a higher electron-phonon interaction and lower effective charge-carrier mobility. This finding provides a molecule-level understanding of the inorganic lattice structure in tuning electron-phonon interactions and may offer valuable guidance for optimizing the optoelectronic properties of perovskites.

Fluoroethylene Carbonate Induces Ordered Electrolyte Interface on Silicon and Sapphire Surfaces as Revealed by Sum Frequency Generation Vibrational Spectroscopy and X-ray Reflectivity.

The cyclability of silicon anodes in lithium ion batteries (LIBs) is affected by the reduction of the electrolyte on the anode surface to produce a coating layer termed the solid electrolyte interphase (SEI). One of the key steps for a major improvement of LIBs is unraveling the SEI's structure-related diffusion properties as charge and discharge rates of LIBs are diffusion-limited. To this end, we have combined two surface sensitive techniques, sum frequency generation (SFG) vibrational spectroscopy, and X-ray reflectivity (XRR), to explore the first monolayer and to probe the first several layers of electrolyte, respectively, for solutions consisting of 1 M lithium perchlorate (LiClO4) salt dissolved in ethylene carbonate (EC) or fluoroethylene carbonate (FEC) and their mixtures (EC/FEC 7:3 and 1:1 wt %) on silicon and sapphire surfaces. Our results suggest that the addition of FEC to EC solution causes the first monolayer to rearrange itself more perpendicular to the anode surface, while subsequent layers are less affected and tend to maintain their, on average, surface-parallel arrangements. This fundamental understanding of the near-surface orientation of the electrolyte molecules can aid operational strategies for designing high-performance LIBs.

Real-time investigation of interactions between nanoparticles and cell membrane model.

Understanding the internal cellular processes of micron/nanoparticles will be important for particles toxicity studies or drug-delivery systems designing. The details and mechanisms of the cellular up-take process of micron/nano particles can hardly be described in real-time. In this study, cellular internalization of micron/nanoparticles was investigated by fluorescence spectroscopy, flow cytometry and sum frequency generation vibrational spectroscopy (SFG). Model cell membranes such as substrate supported lipid bilayers and lipid vesicles were used in this research. Especially, SFG was used to examine the behavior of each leaflet of the lipid bilayer while interacting with micron/nanoparticles. Experiments of SFG show direct evidences that micron/nanoparticles attachment lead to the lipid orientation. Vesicle dye-leakage model were used to study long-term interactions on model membrane. Results from this study provide in-depth insight into the molecular interactions between micron/nanoparticles and cell membranes, which will help to understand the particles toxicity and will be useful for the designing of micron/nanoparticles for applications.

Sum Frequency Generation Vibrational Spectroscopy for Characterization of Buried Polymer Interfaces.

Sum frequency generation vibrational spectroscopy (SFG-VS) has become one of the most appealing technologies to characterize molecular structures at interfaces. In this focal point review, we focus on SFG-VS studies at buried polymer interfaces and review many of the recent publications in the field. We also cover the essential theoretical background of SFG-VS and discuss the experimental implementation of SFG-VS.

Reorganization of hydrogen bond network makes strong polyelectrolyte brushes pH-responsive.

Weak polyelectrolytes have found extensive practical applications owing to their rich pH-responsive properties. In contrast, strong polyelectrolytes have long been regarded as pH-insensitive based on the well-established fact that the average degree of charging of strong polyelectrolyte chains is independent of pH. The possible applications of strong polyelectrolytes in smart materials have, thus, been severely limited. However, we demonstrate that almost all important properties of strong polyelectrolyte brushes (SPBs), such as chain conformation, hydration, stiffness, surface wettability, lubricity, adhesion, and protein adsorption are sensitive to pH. The pH response originates from the reorganization of the interchain hydrogen bond network between the grafted chains, triggered by the pH-mediated adsorption-desorption equilibrium of hydronium or hydroxide with the brushes. The reorganization process is firmly identified by advanced sum-frequency generation vibrational spectroscopy. Our findings not only provide a new understanding of the fundamental properties of SPBs but also uncover an extensive family of building blocks for constructing pH-responsive materials.

Dependence of Alamethicin Membrane Orientation on the Solution Concentration.

Alamethicin has been extensively studied as an antimicrobial peptide and is widely used as a simple model for ion channel proteins. It has been shown that the antimicrobial activity of peptides is related to their membrane orientation. In this study, we determined the relationship between the solution concentration of alamethicin and its membrane orientation in lipid bilayers using sum frequency generation (SFG) vibrational spectroscopy. Our SFG results indicated that the alamethicin molecules more or less lay down on the surface of 1-palmitoyl-2-oleoyl-sn-glycero-3-phosphocholine (POPC) lipid bilayers at a low peptide concentration of 0.84 µM; the α-helix segment tilts at about 88°, and 310-helix segment tilts at about 58° versus the surface normal. However, when the peptide concentration was increased to 15.6 µM, we observed that alamethicin molecules further inserted into the lipid bilayers: the α-helical component changes its orientation to make a 37° tilt from the lipid bilayer normal, and the 310-helical component tilts at about 50° versus the surface normal. This is in agreement with the barrel-stave mode for the alamethicin-cell membrane interaction as reported previously. Additionally, we have also studied membrane orientation of alamethicin as a function of peptide concentration with SFG. Our results showed that the membrane orientation of the alamethicin α-helical component changed substantially with the increase of the alamethicin concentration, while the membrane orientation of the 310-helical component remained more or less the same.