Mobile and three-dimensional presentation of adhesion proteins within microwells.

On traditional cell culture substrates cells adhere to a planar 2D surface where ligands are presented immobile. A more realistic presentation of cell adhesion ligands which can account for lateral mobility and a more tissue-like 3D presentation would allow studies addressing fundamental questions of significant importance for applications such as tissue engineering and implant intregration. To study the effect of lateral mobility of cell membrane interaction cues in three dimensions, we have developed and characterized a platform which generically enables patterning of single cells into microwells presenting a cell membrane mimetic interface pre-patterned to its walls.

In vitro expressed GPCR inserted in polymersome membranes for ligand-binding studies.

The dopamine receptor D2 (DRD2), a G-protein coupled receptor is expressed into PBd(22)-PEO(13) and PMOXA(20)-PDMS(54)-PMOXA(20) block copolymer vesicles. The conformational integrity of the receptor is confirmed by antibody- and ligand-binding assays. Replacement of bound dopamine is demonstrated on surface-immobilized polymersomes, thus making this a promising platform for drug screening.

A novel microfluidics-based method for probing weak protein-protein interactions.

We report the use of a novel microfluidics-based method to detect weak protein-protein interactions between membrane proteins. The tight junction protein, claudin-2, synthesised in vitro using a cell-free expression system in the presence of polymer vesicles as membrane scaffolds, was used as a model membrane protein. Individual claudin-2 molecules interact weakly, although the cumulative effect of these interactions is significant.

Proteopolymersomes: in vitro production of a membrane protein in polymersome membranes.

Polymersomes are stable self-assembled architectures which mimic cell membranes. For characterization, membrane proteins can be incorporated into such bio-mimetic membranes by reconstitution methods, leading to so-called proteopolymersomes. In this work, we demonstrate the direct incorporation of a membrane protein into polymersome membranes by a cell-free expression system.

Selective deposition and self-assembly of triblock copolymers into matrix arrays for membrane protein production.

To improve the stability of cell membrane mimics, there has been growing interest in the use of block copolymers. Here, we present an easy approach to create an array of planar polymeric matrices capable of hosting membrane proteins. The array of polymeric matrices was formed by the selective deposition of triblock copolymers onto an array of hydrophilic islands situated within a hydrophobic background.

Single cell 3-D platform to study ligand mobility in cell-cell contact.

Lateral mobility and dimensionality have both been shown to influence cellular behavior, but have yet to be combined and applied in a single in vitro platform to address, e.g., cell adhesion in a setting mimicking the three-dimensional environment of neighboring cells in a reductionist way.

Multicompartmentalized polymersomes for selective encapsulation of biomacromolecules.

Multicompartmentalized polymersomes are formed using block co-polymers PMOXA-PDMS-PMOXA and PS-PIAT, and are subsequently proven to be capable of selective encapsulation of biomacromolecules. This architecture mimics the compartmentalization found in cells and may serve as a simple, albeit robust, model system.