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Ionic liquid crystals (ILCs), that is, ionic liquids exhibiting mesomorphism, liquid crystalline phases, and anisotropic properties, have received intense attention in the past years. Among others, this is due to their special properties arising from the combination of properties stemming from ionic liquids and from liquid crystalline arrangements. Besides interesting fundamental aspects, ILCs have been claimed to have tremendous application potential that again arises from the combination of properties and architectures that are not accessible otherwise, or at least not accessible easily by other strategies. The current review highlights recent developments in ILC research, starting with some key fundamental aspects. Further subjects covered include the synthesis and variations of modern ILCs, including the specific tuning of their mesomorphic behavior. The review concludes with reflections on some applications that may be within reach for ILCs and finally highlights a few key challenges that must be overcome prior and during true commercialization of ILCs.
A directed attractive interaction between predefined "patchy" sites on the surfaces of anisotropic microcolloids can provide them with the ability to self-assemble in a controlled manner to build target structures of increased complexity. An important step toward the controlled formation of a desired superstructure is to identify reversible electrostatic interactions between patches which allow them to align with one another. The formation of bipatchy particles with two oppositely charged patches fabricated using sandwich microcontact printing is reported. These particles spontaneously self-aggregate in solution, where a diversity of short and long chains of bipatchy particles with different shapes, such as branched, bent, and linear, are formed. Calculations show that chain formation is driven by a combination of attractive electrostatic interactions between oppositely charged patches and the charge-induced polarization of interacting particles.
Dual glucagon-like peptide-1/glucagon receptor agonists have emerged as promising candidates for the treatment of diabetes and obesity. Issues of degradation sensitivity and rapid renal clearance are addressed, for example, by the conjugation of peptides to fatty acid chains, promoting reversible albumin binding. We use combined dynamic and static light scattering to directly measure the self-assembly of a set of dual peptide agonists based on the exendin-4 structure with varying fatty acid chain lengths in terms of apparent molecular mass and hydrodynamic radius (R-S). We use NMR spectroscopy to gain an insight into the molecular architecture of the assembly. We investigate conformational changes of the monomeric subunits resulting from peptide self-assembly and assembly stability as a function of the fatty acid chain length using circular dichroism and fluorescence spectroscopy. Our results demonstrate that self-assembly of the exendin-4-derived dual agonist peptides is essentially driven by hydrophobic interactions involving the conjugated acyl chains. The fatty acid chain length affects assembly equilibria and the assembly stability, although the peptide subunits in the assembly retain a dynamic secondary structure. The assembly architecture is characterized by juxtaposition of the fatty acyl side chains and a hydrophobic cluster of the peptide moiety. This cluster experiences local conformational changes in the assembly compared to the monomeric unit leading to a reduction in solvent exposure. The N-terminal half of the peptide and a C-terminal loop are not in contact with neighboring peptide subunits in the assemblies. Altogether, our study contributes to a thorough understanding of the association characteristics and the tendency toward self-assembly in response to lipidation. This is important not only to achieve the desired bioavailability but also with respect to the physical stability of peptide solutions.
Cryo-electron microscopy (cryo-EM) is a powerful structure determination technique that is well-suited to the study of protein and polymer self-assembly in solution. In contrast to conventional transmission electron microscopy (TEM) sample preparation, which often times involves drying and staining, the frozen-hydrated sample preparation allows the specimens to be kept and imaged in a state closest to their native one. Here, we give a short overview of the basic principles of Cryo-EM and review our results on applying it to the study of different protein and polymer self-assembled nanostructures. More specifically, we show how we have applied cryo-electron tomography (cryo-ET) to visualize the internal morphology of self-assembled poly(ionic liquid) nanoparticles and cryo-EM single particle analysis (SPA) to determine the three-dimensional (3D) structures of artificial protein microtubules.
Subdividing space through interfaces leads to many space partitions that are relevant to soft matter self-assembly. Prominent examples include cellular media, e.g. soap froths, which are bubbles of air separated by interfaces of soap and water, but also more complex partitions such as bicontinuous minimal surfaces.
Using computer simulations, this thesis analyses soft matter systems in terms of the relationship between the physical forces between the system's constituents and the structure of the resulting interfaces or partitions. The focus is on two systems, copolymeric self-assembly and the so-called Quantizer problem, where the driving force of structure formation, the minimisation of the free-energy, is an interplay of surface area minimisation and stretching contributions, favouring cells of uniform thickness.
In the first part of the thesis we address copolymeric phase formation with sharp interfaces. We analyse a columnar copolymer system "forced" to assemble on a spherical surface, where the perfect solution, the hexagonal tiling, is topologically prohibited. For a system of three-armed copolymers, the resulting structure is described by solutions of the so-called Thomson problem, the search of minimal energy configurations of repelling charges on a sphere. We find three intertwined Thomson problem solutions on a single sphere, occurring at a probability depending on the radius of the substrate.
We then investigate the formation of amorphous and crystalline structures in the Quantizer system, a particulate model with an energy functional without surface tension that favours spherical cells of equal size. We find that quasi-static equilibrium cooling allows the Quantizer system to crystallise into a BCC ground state, whereas quenching and non-equilibrium cooling, i.e. cooling at slower rates then quenching, leads to an approximately hyperuniform, amorphous state. The assumed universality of the latter, i.e. independence of energy minimisation method or initial configuration, is strengthened by our results. We expand the Quantizer system by introducing interface tension, creating a model that we find to mimic polymeric micelle systems: An order-disorder phase transition is observed with a stable Frank-Caspar phase.
The second part considers bicontinuous partitions of space into two network-like domains, and introduces an open-source tool for the identification of structures in electron microscopy images. We expand a method of matching experimentally accessible projections with computed projections of potential structures, introduced by Deng and Mieczkowski (1998). The computed structures are modelled using nodal representations of constant-mean-curvature surfaces. A case study conducted on etioplast cell membranes in chloroplast precursors establishes the double Diamond surface structure to be dominant in these plant cells. We automate the matching process employing deep-learning methods, which manage to identify structures with excellent accuracy.
Die herausragenden mechanischen Eigenschaften natürlicher anorganisch-organischer Kompositmaterialien wie Knochen oder Muschelschalen entspringen ihrer hierarchischen Struktur, die von der nano- bis hinauf zur makroskopischen Ebene reicht, und einer kontrollierten Verbindung entlang der Grenzflächen der anorganischen und organischen Komponenten.
Ausgehend von diesen Schlüsselprinzipien des biologischen Materialdesigns wurden in dieser Arbeit zwei Konzepte für die bioinspirierte Strukturbildung von Kompositen untersucht, die auf dem Verkleben von Nano- oder Mesokristallen mit funktionalisierten Poly(2-oxazolin)-Blockcopolymeren beruhen sowie deren Potenzial zur Herstellung bioinspirierter selbstorganisierter hierarchischer anorganisch-organischer Verbundstrukturen ohne äußere Kräfte beleuchtet. Die Konzepte unterschieden sich in den verwendeten anorganischen Partikeln und in der Art der Strukturbildung.
Über einen modularen Ansatz aus Polymersynthese und polymeranaloger Thiol-En-Funktionalisierung wurde erfolgreich eine Bibliothek von Poly(2-oxazolin)en mit unterschiedlichen Funktionalitäten erstellt. Die Blockcopolymere bestehen aus einem kurzen partikelaffinen "Klebeblock", der aus Thiol-En-funktionalisiertem Poly(2-(3-butenyl)-2-oxazolin) besteht, und einem langen wasserlöslichen, strukturbildenden Block, der aus thermoresponsivem und kristallisierbarem Poly(2-isopropyl-2-oxazolin) besteht und hierarchische Morphologien ausbildet. Verschiedene analytische Untersuchungen wie Turbidimetrie, DLS, DSC, SEM oder XRD machten das thermoresponsive bzw. das Kristallisationsverhalten der Blockcopolymere in Abhängigkeit vom eingeführten Klebeblock zugänglich. Es zeigte sich, dass diese Polymere ein komplexes temperatur- und pH-abhängiges Trübungsverhalten aufweisen. Hinsichtlich der Kristallisation änderte der Klebeblock nicht die nanoskopische Kristallstruktur; er beeinflusste jedoch die Kristallisationszeit, den Kristallisationsgrad und die hierarchische Morphologie. Dieses Ergebnis wurde auf das unterschiedliche Aggregationsverhalten der Polymere in Wasser zurückgeführt.
Für die Herstellung von Kompositen nutzte Konzept 1 mikrometergroße Kupferoxalat-Mesokristalle, die eine innere Nanostruktur aufweisen. Die Strukturbildung über den anorganischen Teil wurde durch das Verkleben und Anordnen dieser Partikel erstrebt. Konzept 1 ermöglichte homogene freistehende stabile Kompositfilme mit einem hohen anorganischen Anteil. Die Partikel-Polymer-Kombination vereinte jedoch ungünstige Eigenschaften in sich, d. h. ihre Längenskalen waren zu unterschiedlich, was die Selbstassemblierung der Partikel verhinderte. Aufgrund des geringen Aspektverhältnisses von Kupferoxalat blieb auch die gegenseitige Ausrichtung durch äußere Kräfte erfolglos. Im Ergebnis eignet sich das Kupferoxalat-Poly(2-oxazolin)-Modellsystem nicht für die Herstellung hierarchischer Kompositstrukturen.
Im Gegensatz dazu verwendet Konzept 2 scheibenförmige Laponit®-Nanopartikel und kristallisierbare Blockcopolymere zur Strukturbildung über die organische Komponente durch polymervermittelte Selbstassemblierung. Komplementäre Analysemethoden (Zeta-Potenzial, DLS, SEM, XRD, DSC, TEM) zeigten sowohl eine kontrollierte Wechselwirkung zwischen den Komponenten in wässriger Umgebung als auch eine kontrollierte Strukturbildung, die in selbstassemblierten Nanokompositen resultiert, deren Struktur sich über mehrere Längenskalen erstreckt. Es wurde gezeigt, dass die negativ geladenen Klebeblöcke spezifisch und selektiv an den positiv geladenen Rändern der Laponit®-Partikel binden und so Polymer-Laponit®-Nanohybridpartikel entstehen, die als Grundbausteine für die Kompositbildung dienen. Die Hybridpartikel sind bei Raumtemperatur elektrosterisch stabilisiert - sterisch durch ihre langen, mit Wasser wechselwirkenden Poly(2-isopropyl-2-oxazolin)-Blöcke und elektrostatisch über die negativ geladenen Laponit®-Flächen. Im Ergebnis ließ sich Konzept 2 und damit die Strukturbildung über die organische Komponente erfolgreich umsetzten. Das Laponit®-Poly(2-oxazolin)-Modellsystem eröffnete den Weg zu selbstassemblierten geschichteten quasi-hierarchischen Nanokompositstrukturen mit hohem anorganischen Anteil. Abhängig von der frei verfügbaren Polymerkonzentration bei der Kompositbildung entstanden zwei unterschiedliche Komposit-Typen. Darüber hinaus entwarf die Arbeit einen Erklärungsansatz für den polymervermittelten Bildungsprozess der Komposit-Strukturen.
Insgesamt legt diese Arbeit Struktur-Prozess-Eigenschafts-Beziehungen offen, um selbstassemblierte bioinspirierte Kompositstrukturen zu bilden und liefert neue Einsichten zu einer geeigneten Kombination an Komponenten und Herstellungsbedingungen, die eine kontrollierte selbstassemblierte Strukturbildung mithilfe funktionalisierter Poly(2-oxazolin)-Blockcopolymere erlauben.
Bottom-up strategies for fabricating SEIRA substrates are presented. For this purpose, wet-chemically prepared gold nanoparticles are coated with a polystyrene shell and subsequently self-assembled into different nanostructures such as quasi-hexagonally ordered gold nanoparticle monolayers, double layers, and honeycomb structures. Furthermore elongated gold nanostructures are obtained by sintering of gold nanoparticle double layers. The optical properties of these different gold nanostructures are directly connected to their morphology and geometrical arrangement - leading to surface plasmon resonances from the visible to the infrared wavelength range. Finally, SEIRA enhancement factors are determined. Gold nanoparticle double layers show the best performance as SEIRA substrates.
The aqueous self-assembly behavior of a series of poly(ethylene glycol)-poly(l-/d-lactide) block copolymers and corresponding stereocomplexes is examined by differential scanning calorimetry, dynamic light scattering, and transmission electron microscopy. Block copolymers assemble into spherical micelles and worm-like aggregates at room temperature, whereby the fraction of the latter seemingly increases with decreasing lactide weight fraction or hydrophobicity. The formation of the worm-like aggregates arises from the crystallization of the polylactide by which the spherical micelles become colloidally unstable and fuse epitaxically with other micelles. The self-assembly behavior of the stereocomplex aggregates is found to be different from that of the block copolymers, resulting in rather irregular-shaped clusters of spherical micelles and pearl-necklace-like structures.
Dual glucagon-like peptide-1/glucagon receptor agonists have emerged as promising candidates for the treatment of diabetes and obesity. Issues of degradation sensitivity and rapid renal clearance are addressed, for example, by the conjugation of peptides to fatty acid chains, promoting reversible albumin binding. We use combined dynamic and static light scattering to directly measure the self-assembly of a set of dual peptide agonists based on the exendin-4 structure with varying fatty acid chain lengths in terms of apparent molecular mass and hydrodynamic radius (R-S). We use NMR spectroscopy to gain an insight into the molecular architecture of the assembly. We investigate conformational changes of the monomeric subunits resulting from peptide self-assembly and assembly stability as a function of the fatty acid chain length using circular dichroism and fluorescence spectroscopy. Our results demonstrate that self-assembly of the exendin-4-derived dual agonist peptides is essentially driven by hydrophobic interactions involving the conjugated acyl chains. The fatty acid chain length affects assembly equilibria and the assembly stability, although the peptide subunits in the assembly retain a dynamic secondary structure. The assembly architecture is characterized by juxtaposition of the fatty acyl side chains and a hydrophobic cluster of the peptide moiety. This cluster experiences local conformational changes in the assembly compared to the monomeric unit leading to a reduction in solvent exposure. The N-terminal half of the peptide and a C-terminal loop are not in contact with neighboring peptide subunits in the assemblies. Altogether, our study contributes to a thorough understanding of the association characteristics and the tendency toward self-assembly in response to lipidation. This is important not only to achieve the desired bioavailability but also with respect to the physical stability of peptide solutions.
Racemic and highly enantioenriched 3-methoxycarbonyl, 3-carboxy, and 3-hydroxymethyl derivatives of dibenzo[6]helicene were prepared. The Langmuir layers of these helicenes were formed at the air-water interface and transferred onto solid substrates to afford Langmuir-Blodgett films, which were then studied by ambient atomic force microscopy and (chir)optical spectroscopy. Significant differences were found in the behaviour of the Langmuir layers as well as in the morphology, UV/Vis, electronic circular dichroism (ECD), and fluorescence spectra of the Langmuir-Blodgett thin films depending on the molecular chirality and nature of the polar group. The experimental results were supported by molecular dynamics simulations.