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Self-assembled multicompartment liquid crystalline lipid carriers for protein, peptide, and nucleic acid drug delivery.

TLDR
It is demonstrated how high-resolution structural investigations of bicontinuous cubic templates made from lyotropic thermosensitive liquid-crystalline (LC) materials have initiated the development of innovative lipidopolymeric self-assembled nanocarriers.
Abstract
Lipids and lipopolymers self-assembled into biocompatible nano- and mesostructured functional materials offer many potential applications in medicine and diagnostics. In this Account, we demonstrate how high-resolution structural investigations of bicontinuous cubic templates made from lyotropic thermosensitive liquid-crystalline (LC) materials have initiated the development of innovative lipidopolymeric self-assembled nanocarriers. Such structures have tunable nanochannel sizes, morphologies, and hierarchical inner organizations and provide potential vehicles for the predictable loading and release of therapeutic proteins, peptides, or nucleic acids. This Account shows that structural studies of swelling of bicontinuous cubic lipid/water phases are essential for overcoming the nanoscale constraints for encapsulation of large therapeutic molecules in multicompartment lipid carriers. For the systems described here, we have employed time-resolved small-angle X-ray scattering (SAXS) and high-resolution freeze-fracture electronic microscopy (FF-EM) to study the morphology and the dynamic topological transitions of these nanostructured multicomponent amphiphilic assemblies. Quasi-elastic light scattering and circular dichroism spectroscopy can provide additional information at the nanoscale about the behavior of lipid/protein self-assemblies under conditions that approximate physiological hydration. We wanted to generalize these findings to control the stability and the hydration of the water nanochannels in liquid-crystalline lipid nanovehicles and confine therapeutic biomolecules within these structures. Therefore we analyzed the influence of amphiphilic and soluble additives (e.g. poly(ethylene glycol)monooleate (MO-PEG), octyl glucoside (OG), proteins) on the nanochannels' size in a diamond (D)-type bicontinuous cubic phase of the lipid glycerol monooleate (MO). At body temperature, we can stabilize long-living swollen states, corresponding to a diamond cubic phase with large water channels. Time-resolved X-ray diffraction (XRD) scans allowed us to detect metastable intermediate and coexisting structures and monitor the temperature-induced phase sequences of mixed systems containing glycerol monooleate, a soluble protein macromolecule, and an interfacial curvature modulating agent. These observed states correspond to the stages of the growth of the nanofluidic channel network. With the application of a thermal stimulus, the system becomes progressively more ordered into a double-diamond cubic lattice formed by a bicontinuous lipid membrane. High-resolution freeze-fracture electronic microscopy indicates that nanodomains are induced by the inclusion of proteins into nanopockets of the supramolecular cubosomic assemblies. These results contribute to the understanding of the structure and dynamics of functionalized self-assembled lipid nanosystems during stimuli-triggered LC phase transformations.

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Nanoarchitectonics for mesoporous materials

TL;DR: In this article, the authors introduce examples of recent developments in mesoporous materials involving innovations in their components and structural designs and concentrate on their own recent progress, as well as various film preparations, pore alignments, and hierarchic structures.
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Lyotropic liquid crystal engineering–ordered nanostructured small molecule amphiphile self-assembly materials by design

TL;DR: This critical review discusses recent key findings regarding (i) what drives amphiphile self- assembly, (ii) what governs the self-assembly structures that are formed, and (iii) how can amphiphiles self-Assembly materials be used to enhance product formulations, including drug delivery vehicles, medical imaging contrast agents, and integral membrane protein crystallisation media.
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Nature-Inspired Emerging Chiral Liquid Crystal Nanostructures: From Molecular Self-Assembly to DNA Mesophase and Nanocolloids.

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Computational and experimental approaches for investigating nanoparticle-based drug delivery systems

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References
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Journal ArticleDOI

Drug Delivery Systems: Entering the Mainstream

TL;DR: There is considerable interest in exploiting the advantages of DDS for in vivo delivery of new drugs derived from proteomics or genomics research and for their use in ligand-targeted therapeutics.
Journal ArticleDOI

An inverted hexagonal phase of cationic liposome-DNA complexes related to DNA release and delivery

TL;DR: Optical microscopy revealed that the LalphaC complexes bind stably to anionic vesicles (models of cellular membranes), whereas the more transfectant HIIC complexes are unstable and rapidly fuse and release DNA upon adhering to anionics.
Journal ArticleDOI

Cubic phases of lipid-containing systems. Structure analysis and biological implications.

TL;DR: The structures of Q230, Q224, Q229 and of Q212, Q227, Q223 are shown to provide topological generalizations of the two paradigms of lipid organization; namely, the bilayer and the monolayer.
Journal ArticleDOI

Novel Process for Producing Cubic Liquid Crystalline Nanoparticles (Cubosomes)

TL;DR: A novel process for producing cubic liquid crystalline nanoparticles (cubosomes) has been developed in this article, which involves simple mixing of two water-like solutions with a minimal input of energy.
Journal ArticleDOI

Submicron Particles of Reversed Lipid Phases in Water Stabilized by a Nonionic Amphiphilic Polymer

TL;DR: In this article, the formation and structure of aqueous dispersions of lipid-based liquid crystalline phases, namely reversed types of hexagonal and bicontinious cubic phases, were investigated.
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