Claire Fave

Tunable electrochemical switch of the optical properties of metallic nanoparticles.

Control of the optical properties of oblate metallic nanoparticles (NP) is realized using an electrochemical switch consisting of a thin layer of conducting polymer (CP). Reversible modulation, moderate damping, and almost total quenching of the localized surface plasmon (LSP) resonance is achieved as a function of the thickness of the CP layer and the potential applied to the electrochemical systems, that is, the charge carrier density injected into the CP layer. These experimental results can be qualitatively reproduced using the single-particle model in the electrostatic approximation. We believe that combining an electroactive conducting polymer and NP will prove to be a general strategy for controlling the properties of various types of NP (fluorescent, magnetic, semiconducting) in many fields.

Active Plasmonic Devices with Anisotropic Optical Response: A Step Toward Active Polarizer

Control of the optical properties of metallic nanoparticles (NP) is realized using an electrochemical switch consisting of a thin layer of conducting polymer (CP). It is shown that the quenching of localized surface plasmon (LSP) sustained by oblate particles depends of the frequency of the LSP resonance. This effect is attributed to the variation of the CP dielectric function with wavelength. As a consequence, prolate arrays show total quenching of the LSP resonance along the major axis of the particles whereas modulation and moderate damping are observed along the minor axis. Combining electroactive conducting polymer and prolate NP makes it possible to design active plasmonic devices with anisotropic optical response upon CP switching. In the present case, such devices can be used as active filters or polarizers.

Simple and Highly Enantioselective Electrochemical Aptamer-Based Binding Assay for Trace Detection of Chiral Compounds

A new electrochemical methodology is reported for monitoring in homogeneous solution the enantiospecific binding of a small chiral analyte to an aptamer. The principle relies on the difference of diffusion rates between the targeted molecule and the aptamer/target complex, and thus on the ability to more easily electrochemically detect the former over the latter in a homogeneous solution. This electrochemical detection strategy is significant because, in contrast to the common laborious and time-consuming heterogeneous binding approaches, it is based on a simple and fast homogeneous binding assay which does not call for an aptamer conformational change upon ligand binding. The methodology is here exemplified with the specific chiral recognition of trace amounts of l- or d-tyrosinamide by a 49-mer d- or l-deoxyribooligonucleotide receptor. Detection as low as 0.1% of the minor enantiomer in a nonracemic mixture can be achieved in a very short analysis time (<1 min). The assay finally combines numerous attractive features including simplicity, rapidity, low cost, flexibility, low volume samples (few microliters), and homogeneous format.

Hydroxynaphthoquinone ultrathin films obtained by diazonium electroreduction: toward design of biosensitive electroactive interfaces.

Electroactive 2-(phenylsulfanyl)-8-hydroxy-1,4-naphthoquinone has been electrodeposited via the reduction of the corresponding diazonium salt on Au electrodes. Surface characterizations by X-ray photoelectron spectroscopy (XPS) and infrared reflection-absorption spectroscopy (IRRAS) reveal that the mechanism of film deposition follows an aryl radical formation and its immobilization on the electrode surface. Electrochemical study shows that the surface coverage can be finely tuned (thickness between one and four layers) by adjusting the potential and the deposition time. By managing the potential applied when reducing diazonium in potentiostatic mode, the formed layer could mediate or not charge transfer. This is the first time that the films obtained by diazonium process are demonstrated to act as mediators in the growth process. Hence, with potentials higher than the formal potential of quinone group, very thin and homogeneous layers are obtained, whereas thicker films are formed when more cathodic potentials than that of quinone are applied. The possibility to manage the charge-transfer kinetics, the thickness, and the homogeneity of electroactive deposits is interesting in the scope of designing electrochemical transducers.

Atomic contacts via electrochemistry in water/cyclodextrin media: a step toward protected atomic contacts.

Atomic contacts are nanoscience devices proposed for applications such as single-atom switches in nanoelectronic circuits or one-molecule sensing devices. The conductance of such contacts varies in a stepwise fashion with a tendency to quantize near integer multiples of the conductance quantum (G0) but can also deviate significantly from integer values upon molecular adsorption. However, for sensing applications it is first necessary to coat the contact permanently to avoid nonspecific adsorption. Here, we show that marked differences are observed between atomic contacts generated in water, and in water/beta-CD. In this latter medium, atomic contacts with unusual properties can be generated. They have below 1 G0 conductance, low conductance fluctuation with time, and appear to be protected or partially protected from salicylate external molecular probes. Such contacts are not obtained in water, in water/glucose, or when beta-CD is added after 1 G0 contacts have been generated in water. These results indicate specific adsorption of beta-cyclodextrin on the atomic contacts and are compatible with the formation of encapsulated atomic contacts. However, direct independent structural evidence is still needed to confirm or infirm this interpretation.

Directed synthesis of a halogen-bonded open porphyrin network†

A strategy for the elaboration of a halogen-bonded porphyrin network is reported. The progressive introduction of geometric constraints via the modulation of building blocks and self-assembly via strong and directional halogen bonding led successfully to the construction of an open porphyrin network with nano-sized tubular channels.

Rational Design of a Redox-Labeled Chiral Target for an Enantioselective Aptamer-Based Electrochemical Binding Assay

A series of redox-labeled L-tyrosinamide (L-Tym) derivatives was prepared and the nature of the functional group and the chain length of the spacer were systematically varied in a step-by-step affinity optimization process of the tracer for the L-Tym aptamer. The choice of the labeling position on L-Tym proved to be crucial for the molecular recognition event, which could be monitored by cyclic voltammetry and is based on the different diffusion rates of free and bound targets in solution. From this screening approach an efficient electroactive tracer emerged. Comparable dissociation constants Kd were obtained for the unlabeled and labeled targets in direct or competitive binding assays. The enantiomeric tracer was prepared and its enantioselective recognition by the corresponding anti-D-Tym aptamer was demonstrated. The access to both enantiomeric tracer molecules opens the door for the development of one-pot determination of the enantiomeric excess when using different labels with well-separated redox potentials for each enantiomer.

Optimization of Experimental Parameters to Explore Small-Ligand/Aptamer Interactions through Use of (1) H NMR Spectroscopy and Molecular Modeling.

Aptamers constitute an emerging class of molecules designed and selected to recognize any given target that ranges from small compounds to large biomolecules, and even cells. However, the underlying physicochemical principles that govern the ligand-binding process still have to be clarified. A major issue when dealing with short oligonucleotides is their intrinsic flexibility that renders their active conformation highly sensitive to experimental conditions. To overcome this problem and determine the best experimental parameters, an approach based on the design-of-experiments methodology has been developed. Here, the focus is on DNA aptamers that possess high specificity and affinity for small molecules, L-tyrosinamide, and adenosine monophosphate. Factors such as buffer, pH value, ionic strength, Mg(2+) -ion concentration, and ligand/aptamer ratio have been considered to find the optimal experimental conditions. It was then possible to gain new insight into the conformational features of the two ligands by using ligand-observed NMR spectroscopic techniques and molecular mechanics.