In pure water, zwitterionic lipids form lamellar phases with an equilibrium water gap on the order of 2 to 3 nm as a result of the dominating van der Waals attraction between dipolar bilayers. Monovalent ions can swell those neutral lamellae by a small amount. Divalent ions can adsorb onto dipolar membranes and charge them. Using solution X-ray scattering, we studied how the structure of ions and zwitterionic lipids regulates the charge of dipolar membranes. We found that unlike monovalent ions that weakly interact with all of the examined dipolar membranes, divalent and trivalent ions adsorb onto membranes containing lipids with saturated tails, with an association constant on the order of ∼10 M(-1). One double bond in the lipid tail is sufficient to prevent divalent ion adsorption. We suggest that this behavior is due to the relatively loose packing of lipids with unsaturated tails that increases the area per lipid headgroup, enabling their free rotation. Divalent ion adsorption links two lipids and limits their free rotation. The ion-dipole interaction gained by the adsorption of the ions onto unsaturated membranes is insufficient to compensate for the loss of headgroup free-rotational entropy. The ion-dipole interaction is stronger for cations with a higher valence. Nevertheless, polyamines behave as monovalent ions near dipolar interfaces in the sense that they interact weakly with the membrane surface, whereas in the bulk their behavior is similar to that of multivalent cations. Advanced data analysis and comparison with theory provide insight into the structure and interactions between ion-induced regulated charged interfaces. This study models biologically relevant interactions between cell membranes and various ions and the manner in which the lipid structure governs those interactions. The ability to monitor these interactions creates a tool for probing systems that are more complex and forms the basis for controlling the interactions between dipolar membranes and charged proteins or biopolymers for encapsulation and delivery applications.
X+ is a user‐friendly multi‐core accelerated program that fully analyses solution X‐ray scattering radially integrated images. This software is particularly useful for analysing supramolecular self‐assemblies, often found in biology, and for reconstructing the scattering signal in its entirety. The program enables various ways of subtracting background noise. The user selects a geometric model and defines as many layers of that shape as needed. The thickness and electron density of each layer are the fitting parameters. An initial guess is input by the user and the program calculates the form‐factor parameters that best fit the data. The polydispersity of one size parameter at a time can be taken into account. The program can then address the assembly of those shapes into different lattice symmetries. This is accounted for by fitting the parameters of the structure factor, using various peak line shapes. The models of the program and selected features are presented. Among them are the model‐fitting procedure, which includes both absolute and relative constraints, data smoothing, signal decomposition for separation of form and structure factors, goodness‐of‐fit verification procedures, error estimation, and automatic feature recognition in the data, such as correlation peaks and baseline. The program's intuitive graphical user interface runs on Windows PCs. Using X+, the exact structure of a microtubule in a crowded environment, and the structure, domain size, and elastic and interaction parameters of lipid bilayers, were obtained.
In this paper, the analysis of several involved models, relevant for evaluating solution X-ray scattering form factors of supramolecular self-assembled structures, is presented. Different geometrical models are discussed, and the scattering form factors of several layers of those shapes are evaluated. The thickness and the electron density of each layer are parameters in those models. The models include Gaussian electron density profiles and/or uniform electron density profiles at each layer. Various forms of cuboid, layered, spherical, cylindrical, and helical structures are carefully treated. The orientation-averaged scattering intensities of those form factors are calculated. Similar classes of form factors are examined and compared, and their fit to scattering data of lipid bilayers, capsids of the Simian virus 40 virus-like particle and microtubule is discussed. A more detailed model of discrete helices composed of uniform spheres was derived and compared to solution X-ray scattering data of microtubules. Our analyses show that when high-resolution data are available the more detailed models with Gaussian electron density profiles or helical structures composed of spheres should be used to better capture all the elements in the scattering curves. The models presented in this paper may also be applied, with minor corrections, for the analysis of solution neutron scattering data.
Interactions between charged and neutral self-assembled phospholipid membranes are well understood and take into account temperature dependence. Yet, the manner in which the structure of the membrane is affected by temperature was hardly studied. Here we study the effect of temperature on the thickness, area per lipid, and volume per lipid of charged membranes. Two types of membranes were studied: membranes composed of charged lipids and dipolar (neutral) membranes that adsorbed divalent cations and became charged. Small-angle X-ray scattering data demonstrate that the thickness of charged membranes decreases with temperature. Wide-angle X-ray scattering data show that the area per headgroup increases with temperature. Intrinsically charged membranes linearly thin with temperature, whereas neutral membranes that adsorb divalent ions and become charged show an exponential decrease of their thickness. The data indicate that, on average, the tails shorten as the temperature rises. We attribute this behavior to higher lipid tail entropy and to the weaker electrostatic screening of the charged headgroups, by their counterions, at elevated temperatures. The latter effect leads to stronger electrostatic repulsion between the charged headgroups that increases the area per headgroup and decreases the bilayer thickness.
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