Ligand "noninnocence" in coordination complexes vs. kinetic, mechanistic, and selectivity issues in electrochemical catalysis.

The world of coordination complexes is currently stimulated by the quest for efficient catalysts for the electrochemical reactions underlying modern energy and environmental challenges. Even in the case of a multielectron-multistep process, catalysis starts with uptake or removal of one electron from the resting state of the catalyst. If this first step is an outer-sphere electron transfer (triggering a "redox catalysis" process), the electron distribution over the metal and the ligand is of minor importance. This is no longer the case with "chemical catalysis," in which the active catalyst reacts with the substrate in an inner-sphere manner, often involving the transient formation of a catalyst-substrate adduct. The fact that, in most cases, the ligand is "noninnocent," in the sense that the electron density and charge gained (or removed) from the resting state of the catalyst are shared between the metal and the ligand, has become common-place knowledge over the last half-century. Insistent focus on a large degree of noninnocence of the ligand in the resting state of the catalyst, even robustly validated by spectroscopic techniques, may lead to undermining the essential role of the metal when such essential issues as kinetics, mechanisms, and product selectivity are dealt with. These points are general in scope, but their discussion is eased by adequately documented examples. This is the case for reactions involving metalloporphyrins as well as vitamin B12 derivatives and similar cobalt complexes for which a wealth of experimental data is available.

Traversing the Red-Green-Blue Color Spectrum in Rationally Designed Cupredoxins.

Blue copper proteins have a constrained Cu(II) geometry that has proven difficult to recapitulate outside native cupredoxin folds. Previous work has successfully designed green copper proteins which could be tuned blue using exogenous ligands, but the question of how one can create a self-contained blue copper site within a de novo scaffold, especially one removed from a cupredoxin fold, remained. We have recently reported a red copper protein site within a three helical bundle scaffold which we later revisited and determined to be a nitrosocyanin mimic, with a CuHis2CysGlu binding site. We now report efforts to rationally design this construct toward either green or blue copper chromophores using mutation strategies that have proven successful in native cupredoxins. By rotating the metal binding site, we created a de novo green copper protein. This in turn was converted to a blue copper protein by removing an axial methionine. Following this rational sequence, we have successfully created red, green, and blue copper proteins within an alpha helical fold, enabling comparisons for the first time of their structure and function disconnected from the overall cupredoxin fold.

Rational De Novo Design of a Cu Metalloenzyme for Superoxide Dismutation.

Superoxide dismutases (SODs) are highly efficient enzymes for superoxide dismutation and the first line of defense against oxidative stress. These metalloproteins contain a redox-active metal ion in their active site (Mn, Cu, Fe, Ni) with a tightly controlled reduction potential found in a close range around the optimal value of 0.36 V versus the normal hydrogen electrode (NHE). Rationally designed proteins with well-defined three-dimensional structures offer new opportunities for obtaining functional SOD mimics. Here, we explore four different copper-binding scaffolds: H3 (His3 ), H4 (His4 ), H2 DH (His3 Asp with two His and one Asp in the same plane) and H3 D (His3 Asp with three His in the same plane) by using the scaffold of the de novo protein GRα3 D. EPR and XAS analysis of the resulting copper complexes demonstrates that they are good CuII -bound structural mimics of Cu-only SODs. Furthermore, all the complexes exhibit SOD activity, though three orders of magnitude slower than the native enzyme, making them the first de novo copper SOD mimics.

Development of a Rubredoxin-Type Center Embedded in a de Dovo-Designed Three-Helix Bundle.

Protein design is a powerful tool for interrogating the basic requirements for the function of a metal site in a way that allows for the selective incorporation of elements that are important for function. Rubredoxins are small electron transfer proteins with a reduction potential centered near 0 mV (vs normal hydrogen electrode). All previous attempts to design a rubredoxin site have focused on incorporating the canonical CXXC motifs in addition to reproducing the peptide fold or using flexible loop regions to define the morphology of the site. We have produced a rubredoxin site in an utterly different fold, a three-helix bundle. The spectra of this construct mimic the ultraviolet-visible, Mössbauer, electron paramagnetic resonance, and magnetic circular dichroism spectra of native rubredoxin. Furthermore, the measured reduction potential suggests that this rubredoxin analogue could function similarly. Thus, we have shown that an α-helical scaffold sustains a rubredoxin site that can cycle with the desired potential between the Fe(II) and Fe(III) states and reproduces the spectroscopic characteristics of this electron transport protein without requiring the classic rubredoxin protein fold.

Nanodiffusion in electrocatalytic films.

In the active interest aroused by electrochemical reactions' catalysis, related to modern energy challenges, films deposited on electrodes are often preferred to homogeneous catalysts. A particularly promising variety of such films, in terms of efficiency and selectivity, is offered by sprinkling catalytic nanoparticles onto a conductive network. Coupled with the catalytic reaction, the competitive occurrence of various modes of substrate diffusion-diffusion toward nanoparticles ('nanodiffusion') against film linear diffusion and solution linear diffusion-is analysed theoretically. It is governed by a dimensionless parameter that contains all the experimental factors, thus allowing one to single out the conditions in which nanodiffusion is the dominant mode of mass transport. These theoretical predictions are illustrated experimentally by proton reduction on a mixture of platinum nanoparticles and carbon dispersed in a Nafion film deposited on a glassy carbon electrode. The density of nanoparticles and the scan rate are used as experimental variables to test the theory.

Clarifying the Copper Coordination Environment in a de Novo Designed Red Copper Protein.

Cupredoxins are copper-dependent electron-transfer proteins that can be categorized as blue, purple, green, and red depending on the spectroscopic properties of the Cu(II) bound forms. Interestingly, despite significantly different first coordination spheres and nuclearity, all cupredoxins share a common Greek Key ß-sheet fold. We have previously reported the design of a red copper protein within a completely distinct three-helical bundle protein, α3DChC2. (1) While this design demonstrated that a ß-barrel fold was not requisite to recapitulate the properties of a native cupredoxin center, the parent peptide α3D was not sufficiently stable to allow further study through additional mutations. Here we present the design of an elongated protein GRANDα3D (GRα3D) with Δ Gu = -11.4 kcal/mol compared to the original design's -5.1 kcal/mol. Diffraction quality crystals were grown of GRα3D (a first for an α3D peptide) and solved to a resolution of 1.34 Å. Examination of this structure suggested that Glu41 might interact with the Cu in our previously reported red copper protein. The previous bis(histidine)(cysteine) site (GRα3DChC2) was designed into this new scaffold and a series of variant constructs were made to explore this hypothesis. Mutation studies around Glu41 not only prove the proposed interaction, but also enabled tuning of the constructs' hyperfine coupling constant from 160 to 127 × 10-4 cm-1. X-ray absorption spectroscopy analysis is consistent with these hyperfine coupling differences being the result of variant 4p mixing related to coordination geometry changes. These studies not only prove that an Glu41-Cu interaction leads to the α3DChC2 construct's red copper protein like spectral properties, but also exemplify the exact control one can have in a de novo construct to tune the properties of an electron-transfer Cu site.

Attempts To Catalyze the Electrochemical CO2-to-Methanol Conversion by Biomimetic 2e(-) + 2H(+) Transferring Molecules.

In the context of the electrochemical and photochemical conversion of CO2 to liquid fuels, one of the most important issues of contemporary energy and environmental issues, the possibility of pushing the reduction beyond the CO and formate level and catalytically generate products such as methanol is particularly attractive. Biomimetic 2e(-) + 2H(+) is often viewed as a potential hydride donor. This has been the object of a recent interesting attempt (J. Am. Chem. Soc. 2014, 136, 14007) in which 6,7-dimethyl-4-hydroxy-2-mercaptopteridine was reported as a catalyst of the electrochemical conversion of CO2 to methanol and formate, based on cyclic voltammetric, (13)C NMR, IR, and GC analyses. After checking electrolysis at the reported potential and at a more negative potential to speed up the reaction, it appears, on (1)H NMR and gas chromatographic grounds, that there is neither catalysis nor methanol and nor formate production. (1)H NMR (with H2O presaturation) brings about an unambiguous answer to the eventual production of methanol and formate, much more so than (13)C NMR, which can even be misleading when no internal standard is used as in the above-mentioned paper. IR analysis is even less conclusive. Use of a GC technique with sufficient sensitivity confirmed the lack of methanol formation. The direct or indirect hydride transfer electrochemical reduction of CO2 to formate and to methanol remains an open question. Original ideas and efforts such as those discussed here are certainly worth tempting. However, in view of the importance of the stakes, it appears necessary to carefully check reports in this area.

Breaking bonds with electrons and protons. Models and examples.

Besides its theoretical interest, the attention currently aroused by proton-coupled electron transfers (PCET reactions) has two main motives. One is a better understanding of biological processes in which PCET reactions are involved, Photosystem II as well as a myriad of other natural systems. The other is directed toward synthetic processes, many of which are related to global energy challenges. Until recently, the analyses of the mechanism and reactivity of PCET reactions have focused on outersphere transfers, those in which no bond between heavy atoms (all atoms with the exception of H) is concomitantly formed or broken. Conversely, reactions in which electron transfer triggers the breaking of a heavy-atom bond with no proton transfer have been extensively analyzed, both theoretically and experimentally. In both cases, strategies have been developed to distinguish between stepwise and concerted pathways. In each case, kinetic models have been devised, allowing the relation between activation and thermodynamic driving force to be established by means of parameters pertaining to the initial and final state. Although many natural and artificial processes include electron transfer, proton transfer, and heavy-atom bond breaking (/formation), no means were offered until recently to analyze the mechanism of such reactions, notably to establish the degree of concertedness of the three constitutive events. Likewise, no kinetic models were available to describe reactions where the three events are concerted. In this Account, we discuss the strategies to distinguish stepwise, partially concerted (when two of the three events are concerted), and totally concerted pathways in these reactions that include electron transfer, proton transfer, and heavy-atom bond breaking. These mechanism analysis methods are illustrated and validated by three examples. First we describe the electrochemical cleavage of an O-O bond in an aliphatic peroxide molecule with a pendant carboxylic acid group that can serve as proton donor for electron transfer and bond breaking. In the second example, we examine the breaking of one of the C-O bonds of CO2 within a multistep process where the reduction of CO2 into CO is catalyzed by an electrogenerated iron(0) porphyrin in the presence of various Brönsted acids. In this case, an intramolecular electron transfer triggers proton transfer and bond cleavage. In the first two examples, all three events are concerted. The third example also involves catalysis. It describes the cleavage of a cobalt-carbon bond in the reduction of chloroacetonitrile catalyzed by an electrogenerated cobalt(I) porphyrin. It illustrates the rather common case where the intermediate formed by the reaction of a transition metal complex with the substrate has to be cleaved to close the catalytic cycle. In the first two examples, all three events are concerted, whereas, in the last case, a partially concerted pathway takes place: proton transfer and bond-breaking (Co-C cleavage) are concerted after an initial electron transfer step. The all-concerted cases require a model that connects the kinetics to the thermodynamic driving force of the reaction. Starting from previous models of outersphere electron transfer, concerted proton-electron transfer, and concerted dissociative electron transfer, we describe a model for all-concerted proton-electron-bond breaking reactions. These pathways skip the high-energy intermediates that occur in stepwise pathways, but could introduce kinetic penalties. The all-concerted model allows one to assess these penalties and the way in which they can be fought by the supplement of driving force offered by concerted proton transfer.

De novo design and characterization of copper metallopeptides inspired by native cupredoxins.

Using de novo protein design, we incorporated a copper metal binding site within the three-helix bundle α3D (Walsh et al. Proc. Natl. Acad. Sci. U.S.A. 1999, 96, 5486-5491) to assess whether a cupredoxin center within an α-helical domain could mimic the spectroscopic, structural, and redox features of native type-1 copper (CuT1) proteins. We aimed to determine whether a CuT1 center could be realized in a markedly different scaffold rather than the native ß-barrel fold and whether the characteristic short Cu-S bond (2.1-2.2 Å) and positive reduction potentials could be decoupled from the spectroscopic properties (ε600 nm = 5000 M(-1) cm(-1)) of such centers. We incorporated 2HisCys(Met) residues in three distinct α3D designs designated core (CR), chelate (CH), and chelate-core (ChC). XAS analysis revealed a coordination environment similar to reduced CuT1 proteins, producing Cu-S(Cys) bonds ranging from 2.16 to 2.23 Å and Cu-N(His) bond distances of 1.92-1.99 Å. However, Cu(II) binding to the CR and CH constructs resulted in tetragonal type-2 copper-like species, displaying an intense absorption band between 380 and 400 nm (>1500 M(-1) cm(-1)) and A|| values of (150-185) × 10(-4) cm(-4). The ChC construct, which possesses a metal-binding site deeper in its helical bundle, yielded a CuT1-like brown copper species, with two absorption bands at 401 (4429 M(-1) cm(-1)) and 499 (2020 M(-1) cm(-1)) nm and an A|| value ∼30 × 10(-4) cm(-4) greater than its native counterparts. Electrochemical studies demonstrated reduction potentials of +360 to +460 mV (vs NHE), which are within the observed range for azurin and plastocyanin. These observations showed that the designed metal binding sites lacked the necessary rigidity to enforce the appropriate structural constraints for a Cu(II) chromophore (EPR and UV-vis); however, the Cu(I) structural environment and the high positive potential of CuT1 centers were recapitulated within the α-helical bundle of α3D.

Proton-coupled electron transfer in azobenzene/hydrazobenzene couples with pendant acid-base functions. Hydrogen-bonding and structural effects.

Electron transfer in azobenzene derivatives bearing two carboxylic acid groups is coupled with intramolecular proton transfer in a stepwise manner in the title 2e(-) + 2H(+) redox couple. The presence of the pendant acid-base functions pushes the redox chemistry of the azo/hydrazo couple toward positive potentials by as much as 0.75 V. This is essentially the result of H-bonding of one of the nitrogen atoms by the neighboring carboxylic group and H-bonding of one carboxylate by the neighboring protonated nitrogen atom. The two electron-transfer reactions, particularly the second one, are accompanied by strong structural changes, which results in the occurrence of a square scheme mechanism in which electron transfer and structural change are not concerted. These are typical phenomena that are likely to be encountered when attempting to boost proton-coupled electron-transfer stoichiometric or catalytic processes by installing pendant acid-base functionalities in the close vicinity of the reacting center.

Concerted heavy-atom bond cleavage and proton and electron transfers illustrated by proton-assisted reductive cleavage of an O-O bond.

Electron transfer may be concerted with proton transfer. It may also be concerted with the cleavage of a bond between heavy atoms. All three events may also be concerted. A model is presented to analyze the kinetics of these all-concerted reactions for homogeneous or electrochemical reduction or oxidation processes. It allows the estimation of the kinetic advantage that derives from the increase of the bond-breaking driving force resulting from the concerted proton transfer. Application of the model to the electrochemical reductive cleavage of the O-O bond of an organic peroxide in the presence of a proximal acid group illustrates the applicability of the model and provides an example demonstrating that electron transfer, heavy-atom bond breaking, and proton transfer may be all concerted. Such analyses are expected to be useful for the invention, analysis, and optimization of reactions involved in contemporary energy challenges as well as for the comprehension of major biochemical processes, a number of which involve electron and proton transfer together with cleavage of bonds between heavy atoms.

Hydrogen-bond relays in concerted proton-electron transfers.

Reaction mechanisms in which electron and proton transfers are coupled are central to a huge number of processes, both natural and synthetic. Moreover, most of the new approaches to address modern energy challenges involve proton-coupled electron transfer (PCET). Recent research has focused on the possibility that the two steps are concerted, that is, concerted proton-electron transfer (CPET) reactions, rather than stepwise pathways in which proton transfer precedes (PET) or follows (EPT) electron transfer. CPET pathways have the advantage of bypassing the high-energy intermediates of stepwise pathways, although this thermodynamic benefit may have a kinetic cost. Concerted processes require short distances between the group being oxidized and the proton acceptor (and vice versa for a reduction process), which usually involves the formation of a hydrogen bond. Unlike the electron in outer-sphere electron-transfer reactions, the distance a proton may travel in a CPET is therefore rather limited. The idea has recently emerged, however, that this distance may be substantially increased via a H-bond relay located between the electron-transfer-triggered proton source and the proton acceptor. Generally speaking, the relay is a group bearing a H atom able to accept a H-bond from the moiety being oxidized and, at the same time, to form a H-bond with the proton-accepting group without going through a protonated intermediate. Although these molecules do not retain all the properties of chains of water molecules engaged in Grotthuss-type transport of a proton, the OH group in these molecules does possess a fundamental property of water molecules: namely, it is both a hydrogen-bond acceptor and a hydrogen-bond donor. Despite centuries of study, the mechanisms of proton movement in water remain active experimental and theoretical research areas, but so far with no connection to CPET reactions. In this Account, we bring together recent results concerning (i) the oxidative response of molecules containing a H-bond relay and (ii) the oxidation of phenol with water (in water) as the proton acceptor. In the first case, a nondestructive electrochemical method (cyclic voltammetry) was used to investigate the oxidation of phenol molecules containing one H-bond relay and an amine proton acceptor compared with a similar amino phenol deprived of relay. In the second, the kinetics of phenol oxidation with water (in water) as proton acceptor is contrasted with that of conventional proton acceptors (such as hydrogen phosphate and pyridine) to afford evidence of the concerted nature of Grotthuss-type proton displacement with electron transfer. First indications were provided by the same electrochemical method, whereas a more complete kinetic characterization was obtained from laser flash photolysis. Older electrochemical results concerning the reduction of superoxide ion in the presence of water are also examined. The result is a timely picture of current insight into concerted mechanisms involving electron transfer coupled with proton transport over simple H-bond relays and over H-bond networks.

Coupling of α-bromoamides and unactivated alkenes to form γ-lactams through EDA and photocatalysis.

γ-Lactams are prevalent in small-molecule pharmaceuticals and provide useful precursors to highly substituted pyrrolidines. Despite numerous methods for the synthesis of this valuable motif, previous redox approaches to γ-lactam synthesis from α-haloamides and olefins require additional electron withdrawing functionality as well as N-aryl substitution to promote electrophilicity of the intermediate radical and prevent competitive O-nucleophilicity about the amide. Using α-bromo imides and α-olefins, our strategy enables the synthesis of monosubstituted protected γ-lactams in a formal [3 + 2] fashion. These species are poised for further derivatization into more complex heterocyclic scaffolds, complementing existing methods. C-Br bond scission occurs through two complementary approaches, the formation of an electron donor-acceptor complex between the bromoimide and a nitrogenous base which undergoes photoinduced electron transfer, or triplet sensitization with photocatalyst, to furnish an electrophilic carbon-centered radical. The addition of Lewis acids allows for further increased electrophilicity of the intermediate carbon-centered radical, enabling tertiary substituted α-Br-imides to be used as coupling partners as well as internal olefins.

Green synthesis of water splitting electrocatalysts: IrO2 nanocages via Pearson's chemistry.

Highly porous iridium oxide structures are particularly well-suited for the preparation of porous catalyst layers needed in proton exchange membrane water electrolyzers. Herein, we report the formation of iridium oxide nanostructured cages, via a water-based process performed at room temperature, using cheap Cu2O cubes as the template. In this synthetic approach, based on Pearson's hard and soft acid-base theory, the replacement of the Cu2O core by an iridium shell is permitted by the difference in hardness/softness of cations and anions of the two reactants Cu2O and IrCl3. Calcination followed by acid leaching allow the removal of residual copper oxide cores and leave IrO2 hierarchical porous structures with outstanding activity toward the oxygen evolution reaction. Fundamental understanding of the reaction steps and identification of the intermediates are permitted by coupling a set of ex situ and in situ techniques including operando time-resolved X-ray absorption spectroscopy during the synthesis.

Thermochromic luminescence of copper iodide clusters: the case of phosphine ligands.

Three copper(I) iodide clusters coordinated by different phosphine ligands formulated [Cu(4)I(4)(PPh(3))(4)] (1), [Cu(4)I(4)(Pcpent(3))(4)] (2), and [Cu(4)I(4)(PPh(2)Pr)(4)] (3) (PPh(3) = triphenylphosphine, Pcpent(3) = tricyclopentylphosphine, and PPh(2)Pr = diphenylpropylphosphine) have been synthesized and characterized by (1)H and (31)P NMR, elemental analysis and single crystal X-ray diffraction analysis. They crystallize in different space groups, namely, monoclinic P21/c, cubic Pa ̅3, and tetragonal I ̅42m for 1, 2, and 3, respectively. The photoluminescence properties of clusters 1 and 3 show reversible luminescence thermochromism with two highly intense emission bands whose intensities are temperature dependent. In accordance to Density Functional Theory (DFT) calculations, these two emission bands have been attributed to two different transitions, a cluster centered (CC) one and a mixed XMCT/XLCT one. Cluster 2 does not exhibit luminescence variation in temperature because of the lack of the latter transition. The absorption spectra of the three clusters have been also rationalized by time dependent DFT (TDDFT) calculations. A simplified model is suggested to represent the luminescence thermochromism attributed to the two different excited states in thermal equilibrium. In contrast with the pyridine derivatives, similar excitation profiles and low activation energy for these phosphine-based clusters reflect high coupling of the two emissive states. The effect of the Cu-Cu interactions on the emission properties of these clusters is also discussed. Especially, cluster 3 with long Cu-Cu contacts exhibits a controlled thermochromic luminescence which is to our knowledge, unknown for this family of copper iodide clusters. These phosphine-based clusters appear particularly interesting for the synthesis of original emissive materials.

H-bond relays in proton-coupled electron transfers. Oxidation of a phenol concerted with proton transport to a distal base through an OH relay.

Four molecules comprising a phenol moiety and a distal pyridine base connected by an intermediary H-bonding and an H-bonded alcohol group have been synthesized and their electrochemistry has been investigated by means of cyclic voltammetry. The molecules differ by the substituent at the alcohol functional carbon and by methyl groups on the pyridine. The reaction follows a concerted proton-electron transfer pathway as confirmed by the observation of a significant H/D kinetic isotope effect in all four cases. The standard rate constants characterizing each of the four compounds are analyzed in terms of reorganization energy and pre-exponential factor. Intramolecular and solvent reorganization energies appear as practically constant in the series, in which a previously investigated aminophenol is included, whereas significantly different pre-exponential factors are observed. That the latter, which is a measure of the efficiency of proton tunneling concerted with electron transfer, be substantially smaller with the H-bond relay molecules than with the aminophenol is related to the fact that two protons are moved in the first case instead of one in the second. Within the H-bond relay molecules, the pre-exponential factor varies with the substituent present at the alcohol functional carbon in the order CF(3) > H > CH(3), presumably as the result of a fine tuning of the balance between the H-bond accepting and H-bond donating properties of the central OH group. The kinetic H/D kinetic isotope effect increases accordingly in the same order.

Synthesis of the H-cluster framework of iron-only hydrogenase.

The metal-sulphur active sites of hydrogenases catalyse hydrogen evolution or uptake at rapid rates. Understanding the structure and function of these active sites--through mechanistic studies of hydrogenases, synthetic assemblies and in silico models--will help guide the design of new materials for hydrogen production or uptake. Here we report the assembly of the iron-sulphur framework of the active site of iron-only hydrogenase (the H-cluster), and show that it functions as an electrocatalyst for proton reduction. Through linking of a di-iron subsite to a {4Fe4S} cluster, we achieve the first synthesis of a metallosulphur cluster core involved in small-molecule catalysis. In addition to advancing our understanding of the natural biological system, the availability of an active, free-standing analogue of the H-cluster may enable us to develop useful electrocatalytic materials for application in, for example, reversible hydrogen fuel cells. (Platinum is currently the preferred electrocatalyst for such applications, but is expensive, limited in availability and, in the long term, unsustainable.).

The origin of the high electrochemical activity of pseudo-amorphous iridium oxides.

Combining high activity and stability, iridium oxide remains the gold standard material for the oxygen evolution reaction in acidic medium for green hydrogen production. The reasons for the higher electroactivity of amorphous iridium oxides compared to their crystalline counterpart is still the matter of an intense debate in the literature and, a comprehensive understanding is needed to optimize its use and allow for the development of water electrolysis. By producing iridium-based mixed oxides using aerosol, we are able to decouple the electronic processes from the structural transformation, i.e. Ir oxidation from IrO2 crystallization, occurring upon calcination. Full characterization using in situ and ex situ X-ray absorption spectroscopy, X-ray photoelectron spectroscopy, X-ray diffraction and transmission electron microscopy allows to unambiguously attribute their high electrochemical activity to structural features and rules out the iridium oxidation state as a critical parameter. This study indicates that short-range ordering, corresponding to sub-2nm crystal size for our samples, drives the activity independently of the initial oxidation state and composition of the calcined iridium oxides.

Effect of base pairing on the electrochemical oxidation of guanine.

The effect of base pairing by cytosine on the electrochemical oxidation of guanine is examined by means of cyclic voltammetry on carefully purified reactants in a solvent, CHCl(3), which strongly favors the formation of an H-bonded pair. The thermodynamics and kinetics of the oxidation reaction are not strongly influenced by the formation of the pair. They are actually similar to those of the reaction in which 2,6-lutidine, an encumbered base that cannot form a pair with guanine, replaces cytosine. The reaction does not entail a concerted proton-electron mechanism, as attested by the absence of H/D isotope effect. It rather involves the rate-determining formation of the cation radical, followed by its deprotonation and dimerization of the resulting neutral radical in competition with its further oxidation.

Coherent nonlinear emission from a single KTP nanoparticle with broadband femtosecond pulses.

We demonstrate that the intensity of the second harmonic (SH) generated in KTiOPO(4) nanoparticles excited with femtosecond laser pulses increases with decreasing duration of the infrared pump pulses. The SH intensity scales, approximately, as the inverse of the laser pulse duration ranging between 13 fs and 200 fs. The SH intensity enhancement requires careful compensation of the high-order spectral phase, being achieved with a genetic algorithm. Using ultrashort laser pulses improves the signal-to-noise ratio and will allow the detection of 10-nm size particles. Finally, we demonstrate that the spectrum of broadband (100 nm) pulses can be shaped to generate non-degenerate sum-frequency mixing. This opens up access to the polarization degrees of freedom of this second-order nonlinear process at the nanoscale.