Poly-ß-(1→6)-N-acetyl-D-glucosamine mediates surface attachment, biofilm formation, and biocide resistance in Cutibacterium acnes.

Background: The commensal skin bacterium Cutibacterium acnes plays a role in the pathogenesis of acne vulgaris and also causes opportunistic infections of implanted medical devices due to its ability to form biofilms on biomaterial surfaces. Poly-ß-(1→6)-N-acetyl-D-glucosamine (PNAG) is an extracellular polysaccharide that mediates biofilm formation and biocide resistance in a wide range of bacterial pathogens. The objective of this study was to determine whether C. acnes produces PNAG, and whether PNAG contributes to C. acnes biofilm formation and biocide resistance in vitro. Methods: PNAG was detected on the surface of C. acnes cells by fluorescence confocal microscopy using the antigen-specific human IgG1 monoclonal antibody F598. PNAG was detected in C. acnes biofilms by measuring the ability of the PNAG-specific glycosidase dispersin B to inhibit biofilm formation and sensitize biofilms to biocide killing. Results: Monoclonal antibody F598 bound to the surface of C. acnes cells. Dispersin B inhibited attachment of C. acnes cells to polystyrene rods, inhibited biofilm formation by C. acnes in glass and polypropylene tubes, and sensitized C. acnes biofilms to killing by benzoyl peroxide and tetracycline. Conclusion: C. acnes produces PNAG, and PNAG contributes to C. acnes biofilm formation and biocide resistance in vitro. PNAG may play a role in C. acnes skin colonization, biocide resistance, and virulence in vivo.

Planar multilayer assemblies containing block copolymer aggregates.

The design, preparation, and properties of planar multilayer structures composed of various combinations of sequentially deposited polyelectrolyte (PE) chains and self-assembled layers of individual block copolymer aggregates (vesicles, micelles, or large compound micelles (LCMs)) are described. The aggregates contain negatively or positively charged corona chains while the PE multilayers contain alternating polyanionic or polycationic chains deposited on silicon wafers. The final structures consist of combinations of layers of various charged species: multilayers of alternating PEs of poly(allyl hydrochloride) (PAH) and poly(acrylic acid) (PAA) as well as vesicles, micelles, or large compound micelles of ionized poly(styrene)-b-poly(4-vinylpyridine) (PS-b-P4VP) or of poly(styrene)-b-poly(acrylic acid) (PS-b-PAA). Two types of layer-by-layer (LbL) multilayer structures were studied: individual aggregate layers sandwiched between PE multilayers and layers of individual aggregates of various morphologies and of different corona chain charges, deposited on top of each other without intermediate multilayers or individual layers of PEs. The strong interactions between the successive layers are achieved mainly by electrostatic attraction between the oppositely charged layers. The planar LbL multilayers containing block copolymer aggregates could, potentially, be used as carriers for multiple functional components; each aggregate layer could be loaded with hydrophobic (in the core of the micelles, LCMs, or vesicle walls) or hydrophilic functional molecules (in the vesicular cavities). The overall thickness of such planar LbL multilayers can be controlled precisely and can vary from tens of nanometers to several micrometers depending on the number of layers, the sizes of the aggregates, and the complexity of the structure.

High levels of molecular orientation of surface azo chromophores can be optically induced even in a wet biological environment.

We have developed polyelectrolyte multilayer bio-films containing azobenzene chromophores that enhance reversible photo-orientation upon irradiation with linearly polarized light, to effect surface photo-switching of adjacent biological systems. When conditions of film preparation and irradiation were optimized, we could observe the highest measured birefringence to date in amorphous systems (Δn > 0.2). This birefringence change to probe orientation was also for the first time measured and determined to be stable completely underwater, permitting optimization for in situ applications immersed in biological conditions.

High-throughput cellular screening of engineered ECM based on combinatorial polyelectrolyte multilayer films.

The capacity to engineer the extracellular matrix is critical to better understand cell function and to design optimal cellular environments to support tissue engineering, transplantation and repair. Stacks of adsorbed polymers can be engineered as soft wet three dimensional matrices, with properties tailored to support cell survival and growth. Here, we have developed a combinatorial method to generate coatings that self assemble from solutions of polyelectrolytes in water, layer by layer, to produce a polyelectrolyte multilayer (PEM) coating that has enabled high-throughput screening for cellular biocompatibility. Two dimensional combinatorial PEMs were used to rapidly identify assembly conditions that promote optimal cell survival and viability. Conditions were first piloted using a cell line, human embryonic kidney 293 cells (HEK 293), and subsequently tested using primary cultures of embryonic rat spinal commissural neurons. Cell viability was correlated with surface energy (wettability), modulus (matrix stiffness), and surface charge of the coatings.Our findings indicate that the modulus is a crucial determinant of the capacity of a surface to inhibit or support cell survival.