Silencing Red Blood Cell Recognition toward Anti-A Antibody by Means of Polyelectrolyte Layer-by-Layer Assembly in a Two-Dimensional Model System

Mansouri, Sania; Fatisson, Julien; Miao, Zhi-Mei; Merhi, Yahye; Winnik, Françoise M.; Tabrizian, Maryam

doi:10.1021/la9016799

Cited by 29 publications

(29 citation statements)

References 48 publications

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“…22, 23 The biocompatibility, ready availability and low cost of charged polysaccharides have made them attractive choices for a range of applications, including drug delivery vehicles based on lipid-polyelectrolyte particles, biocompatible surfaces for controlling cell growth and tissue biomimetics. [23][24][25][26][27][28] We have examined the suitability of PEM films constructed from alternating layers of chitosan (CHI) and hyaluronic acid (HA) as polymer cushions for supported lipid bilayers.…”

Section: -21mentioning

confidence: 99%

Supported Lipid Bilayers on Biocompatible Polysaccharide Multilayers

2011

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The formation of supported lipid bilayers on soft polymer cushions is a useful approach to decouple the membrane from the substrate for applications involving membrane proteins. We have prepared biocompatible polymer cushions by the layer-by-layer assembly of two polysaccharide polyelectrolytes, chitosan (CHI) and hyaluronic acid, on glass and silicon substrates. (CHI/HA) 5 films were characterized by atomic force microscopy, giving an average thickness of 57 and roughness of 25 nm in aqueous solution at pH 6.5. Formation of zwitterionic lipid bilayers by the vesicle fusion method was attempted using DOPC vesicles at pH 4 and pH 6.5 on (CHI/HA) 5 films. At higher pH adsorbed lipids had low mobility and large immobile lipid fractions; a combination of fluorescence and AFM indicated that this was attributable to the formation of poor quality membranes with defects and pinned lipids, rather than to a layer of surface adsorbed vesicles. By contrast, more uniform bilayers with mobile lipids were produced at pH 4. Fluorescence recovery after photobleaching gave diffusion coefficients that were similar to those for bilayers on PEG cushions and considerably higher than those measured on other polyelectrolyte films. The results suggest that the polymer surface charge is more important than the surface roughness in controlling the formation of mobile supported bilayers. These results demonstrate that polysaccharides provide a useful alternative to other polymer cushions, particularly for applications where biocompatibility is important.

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Section: -21mentioning

confidence: 99%

Supported Lipid Bilayers on Biocompatible Polysaccharide Multilayers

2011

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“…Recent work with cast films composed of water‐soluble phosphorylcholine‐modified chitosan (Pc‐CHI) has indicated significantly improved bone marrow cellular adhesion properties in comparison to unmodified CHI 19. Meanwhile, initial studies of LbL films composed of Pc‐CHI and HA have demonstrated biocompatibility 20, 21. The more commercially available glycol‐modified chitosan (Glyc‐CHI) also exhibits significantly improved water solubility and biocompatibility, features that have led to its wide deployment in drug delivery systems, as well as in gene therapy and tissue engineering applications 22–25.…”

Section: Introductionmentioning

confidence: 99%

Enhanced MC3T3 preosteoblast viability and adhesion on polyelectrolyte multilayer films composed of glycol‐modified chitosan and hyaluronic acid

Holmes

Tabrizian

2011

J Biomedical Materials Res

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Layer-by-layer polyelectrolyte films made of the naturally derived polysaccharides chitosan (CHI) and hyaluronic acid (HA) constitute a well-studied system for the development of cell-responsive biointerfaces. However, many cell lines exhibit decreased adhesion to CHI/HA multilayer films, particularly as the number of bilayers is increased. Here, our group demonstrates that films composed of glycol-modified chitosan exhibit significantly improved MC3T3 preosteoblast adhesion and viability compared to corresponding films consisting of unmodified CHI. These differences in cellular adhesion are likely due to differences in surface topography and roughness, as measured via atomic force microscopy (AFM), as well as in film chemistry and the water solubility of the cation, since both types of films exhibited similar: thickness, as measured via quartz crystal microbalance and AFM; wettability, as measured via contact angle; and serum protein adsorption, as measured via the bicinchoninic acid assay.

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“…Tabrizian and colleagues [64,97] have recently taken a different polymer film engineering approach to generating a universal RBC. Instead relying on a single polymer layer to form a steric barrier between RBC surface antigens and antibodies, they instead assembled a PEM thin film on the surface of RBCs.…”

Section: Molecular Camouflage and Nano-encapsulationmentioning

confidence: 99%