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Michal Swierczewski, Plinio Maroni, Alexis Chenneviere, Mohammad M. Dadras, Lay-Theng Lee, Thomas Bürgi

Nanoscale particles attract much attention due to their size-dependent optical, electrical and chemical properties. Of particular interest are ultrasmall metal nanoclusters which experience strong quantum confinement effect leading to profound changes in the atomic packing structure. The synthesis of these atomically precise metal clusters, typically with metal cores smaller than 2 nm in diameter, makes use of stabilizing functional molecules such as thiol ligands, hence deriving the common name – monolayer-protected clusters (MPCs). The next stage toward applications and at the same time a challenge in the field, is the manipulation and controlled organization of MPCs into two dimensional (2D) superlattices which would exhibit a collective response of the desired kind. Multiple examples of deposition techniques have been extensively studied, including droplet evaporation, spin-coating and chemical vapor deposition. However, a common drawback of all these methods is the failure to form large-scale structures of closely packed particles. Here, we study the formation and deposition of extended thin films of Au38(SC2H4Ph)24 nanoclusters onto solid supports by the Langmuir-Blodgett (LB) method. A combination of techniques, atomic force microscopy (AFM), high magnification transmission electron microscopy (TEM), X-ray reflectivity (XRR), and grazing incidence wide-angle X-ray scattering (GIWAXS) is applied to reveal the morphology and the degree of vertical and in-plane ordering of the transferred films. We find that while a degree of order is initially obtained between the clusters, temporal annealing of the compressed films successfully removes mesoscopic defects between islands of nanoclusters but that it does so at the cost of reducing the local order within the domains. To our knowledge, this is the first reported example of the deposition on an extended scale (several cm2) of ordered gold nanoclusters in the small size regime of 1 – 2 nm.

https://doi.org/10.1002/smll.202005954

Li Shi, Florent Carn, Arsen Goukassov, Eric Buhler, and François Boué

Mixing negatively charged polyelectrolyte (PEL) with positively charged gold nanoparticles (Au NPs) in aqueous solution results in electrostatics complexes of different shapes and compactness. Here, when complexing with a semirigid PEL hyaluronic acid (HA), we obtain crystals made of nanoparticles in a new region of the phase diagram, as evidenced by small-angle Xray scattering (SAXS). The Au NPs were initially well dispersed in solution; their size distribution is well controlled but does not need to be extremely narrow. The bacterial hyaluronic acid, polydispersed, is commercially available. Such rather simple materials and mixing preparation produce a highly ordered crystalline phase of electrostatic complexes. The details of the interactions between spherical nanoparticles and linear polymer chains remain to be investigated. In practice, it opens a completely new and unexpected method of complexation. It has high potential, in particular because one can take advantage of the versatility of Au NPs associated with the specificity of biopolymers, varied due to natural biodiversity.

https://dx.doi.org/10.1021/acs.langmuir.0c01064

Aline Maire du Poset, Mikaela Börjesson, Céline Rameau, Claire Madeleine-Perdrillat, Adrien Lerbret, Camille Loupiac, Fabrice Cousin, Ali Assifaoui

We show here how the structure of polygalacturonate (polyGalA) hydrogels cross-linked by Ca2+ cations via external gelation controls the loading and release rate of beta-lactoglobulin (BLG), a globular protein. Hydrogels prepared from a polyGalA/BLG solution are found to be similar to those obtained from a polyGalA solution in our previous study (Maire du Poset et al. Biomacromolecules 2019, 20 (7), 2864–2872): they exhibit similar transparencies and gradients of mechanical properties and polyGalA concentrations. The nominal BLG/polyGalA ratio of the mixtures is almost recovered within the whole mixed hydrogel despite such strong concentration gradients, except in the part of the hydrogels with the largest mesh size, where more BLG proteins are present. This gradient enables one to tune the amount of protein loaded within the hydrogel. At a local scale, the proteins are distributed evenly within the hydrogel network, as shown by small-angle neutron scattering (SANS). The release of proteins from hydrogels is driven by Fickian diffusion, and the release rate increases with the mesh size of the network, with a characteristic time of a few hours. The specific structure of these polysaccharide-based hydrogels allows for control of both the dosage and the release rate of the loaded protein and makes them good candidates for use as oral controlled-delivery systems.

https://dx.doi.org/10.1021/acs.biomac.9b01722

 

 

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