Surface anchoring mode‐dependent hydrolysis reactions of hydrazone groups on gold examined by pH‐dependent Raman spectroscopy

We conducted a comparative study of the pH‐dependent anchoring behaviors of 3‐methyl‐2‐benzothiazolinone hydrazone (3M2BH) and benzophenone hydrazone (BPH) on gold nanoparticles (AuNPs) by means of interfacial Raman spectroscopy. We found that several bands of 3M2BH in the highly alkaline pH region disappeared as the colloidal conditions became more neutral and acidic. The vibrational band at 919, 1174, and 1222 cm⁻¹ at pH 10.0 disappeared below pH 9.2, which may be because of the hydrolysis reactions that cleave the labile N―NH₂ group of 3M2BH, indicating a rather perpendicular orientation via the sulfur atom at the surfaces. A fairly high transition pH value was assumed to be because of the interaction of the N―NH₂ group in the vicinity of the surfaces. Several characteristic bands, including 1584 and 1617 cm⁻¹, also exhibited different intensities, suggesting that the adsorbates on Au surfaces underwent structural transformations of the N―NH₂ group after the pH value became neutral or acidic. These changes were not observed for BPH, presumably because of the direct and robust binding of the hydrazone onto Au surfaces. Our results revealed that the pH‐dependent cleavage reactions may vary depending on the surface anchoring modes of the adsorbates. Copyright © 2015 John Wiley & Sons, Ltd.     

Hydrosilylation Induced by N→Si Intramolecular Coordination: Spontaneous Transformation of Organosilanes into 1‐Aza‐Silole‐Type Molecules in the Absence of a Catalyst

Our attempts to synthesize the N→Si intramolecularly coordinated organosilanes Ph₂L¹SiH ( 1 a ), PhL¹SiH₂ ( 2 a ), Ph₂L²SiH ( 3 a ), and PhL²SiH₂ ( 4 a ) containing a CH?N imine group (in which L¹ is the C,N‐chelating ligand {2‐[CH?N(C₆H₃‐2,6‐iPr₂)]C₆H₄}^? and L² is {2‐[CH?N(tBu)]C₆H₄}^?) yielded 1‐[2,6‐bis(diisopropyl)phenyl]‐2,2‐diphenyl‐1‐aza‐silole ( 1 ), 1‐[2,6‐bis(diisopropyl)phenyl]‐2‐phenyl‐2‐hydrido‐1‐aza‐silole ( 2 ), 1‐tert‐butyl‐2,2‐diphenyl‐1‐aza‐silole ( 3 ), and 1‐tert‐butyl‐2‐phenyl‐2‐hydrido‐1‐aza‐silole ( 4 ), respectively. Isolated organosilicon amides 1 – 4 are an outcome of the spontaneous hydrosilylation of the CH?N imine moiety induced by N→Si intramolecular coordination. Compounds 1–4 were characterized by NMR spectroscopy and X‐ray diffraction analysis. The geometries of organosilanes 1 a – 4 a and their corresponding hydrosilylated products 1 – 4 were optimized and fully characterized at the B3LYP/6‐31++G(d,p) level of theory. The molecular structure determination of 1 – 3 suggested the presence of a Si?N double bond. Natural bond orbital (NBO) analysis, however, shows a very strong donor–acceptor interaction between the lone pair of the nitrogen atom and the formal empty p orbital on the silicon and therefore, the calculations show that the Si?N bond is highly polarized pointing to a predominantly zwitterionic Si⁺N^? bond in 1 – 4 . Since compounds 1 – 4 are hydrosilylated products of 1 a – 4 a , the free energies (ΔG₂₉₈), enthalpies (ΔH₂₉₈), and entropies (ΔH₂₉₈) were computed for the hydrosilylation reaction of 1 a – 4 a with both B3LYP and B3LYP‐D methods. On the basis of the very negative ΔG₂₉₈ values, the hydrosilylation reaction is highly exergonic and compounds 1 a – 4 a are spontaneously transformed into 1 – 4 in the absence of a catalyst.     

Dormant versus Evolving Aminopalladated Intermediates: Toward a Unified Mechanistic Scenario in PdII‐Catalyzed Aminations

Pd^II‐catalyzed alkene aminopalladation and allylic C?H activation are two competing reaction sequences sharing the same reaction conditions. This study aimed at understanding the factors that bias one or the other path in the intramolecular oxidative cyclization of two types of N‐tosyl amidoalkenes. The results obtained are in accord with the initial generation of a high‐energy cyclic (5‐ or 6‐membered) aminopalladated intermediate. However, this latter species can evolve only if the following specific conditions are met: the availability of distocyclic β‐H elimination pathway, the presence of a strong terminal oxidant, or the availability of a carbopalladation pathway. Conversely, the cyclic alkylpalladium complex is only a latent species in equilibrium with the initial substrate and cannot evolve. Such a reactivity hurdle leaves the way open for alternative reactivities such as allylic C?H activation of the olefinic substrate to generate a η³‐allyl complex followed by its interception by the nitrogen nucleophile, [3,3]‐sigmatropic rearrangement, or decomposition. This study proposes a unifying mechanistic picture that connects these competing mechanisms.     

Molecular complexation of some amino acids and triglycine with 18-crown-6 ether in H2O-EtOH solvents at 298.15 K

The influence of composition of H₂O-EtOH solvent on the reaction of formation of a molecular complex of 18-crown-6 ether (18C6) with triglycine (3Gly) has been studied at 298.15 K by a thermochemical method. The standard thermodynamic parameters (Δ_r G°, Δ_r H°, and TΔ_r S°) of the reaction of [3Gly18C6] complex formation in water-ethanol (H₂O-EtOH) solvents having an EtOH mole fraction of 0.0, 0.1, 0.15, 0.2, 0.25, 0.30, and 0.50 have been calculated from the data of calorimetric measurements performed on a TAM III titration microcalorimeter. It has been found that an increase in EtOH concentration in the mixed solvent results in an increase in stability of [3Gly18C6] and in an enhancement in exothermicity of its formation reaction. The water-ethanol solvent has an analogous effect on the stability and energetics of the reactions of formation of molecular complexes of 18C6 with glycine, D,L-alanine, and L-phenylalanine.     

Reduction of N‐Nitrosaminoquinolinediones with LiAlH4 – an Easy Path to New Tricyclic Benzoxadiazocines

3‐Butylaminoquinolinediones ( 1 ) react with NaNO₂ in AcOH to give the corresponding N‐nitrosoderivatives ( 2 ). The analogous reactions of 4‐hydroxy‐3‐butylaminoquinolinediones ( 5 ), prepared by the reduction of 1 with NaBH₄, produce the corresponding nitrosamines ( 4 ). The reduction of both 2 and 4 with Zn under different conditions was non‐productive, but the reduction of both compounds with LiAlH₄ at the oxo and lactame groups yielded impure products, generating new tricyclic benzoxadiazocines ( 9 ) by a reaction with HNCO. All compounds were characterized by IR, ¹H‐, and ¹³C‐NMR (in some cases, ¹⁵N‐NMR also) spectroscopy and EI and/or ESI mass spectrometry. The X‐ray structure of compound 9g was determined.     

Assay of diazinon pesticides in cucumber juice and in the deep brain cells of a live carp

An electrochemical assay for diazinon pesticides was developed using cyclic voltammetry and square-wave anodic and cathodic stripping voltammetry. The method has a linear working range from 6 to 62 ng L^?1. The detection limit is 0.5 ng L^?1 (1.64 pM), and the relative standard deviation at a diazinon concentration of 6.0 mg L^?1 was 0.06% (n?=?15) in an 0.1 M ammonium phosphate electrolyte solution. The results of the application of the sensor were compared with those of other common spectrometric and electrochemical methods. The method was also applied to cucumber juice and the deep brain cells of a live carp in real conditions.     

Diagnosis of copper ions in vascular tracts using a fluorine-doped carbon nanotube sensor

The voltammetric assay of Cu(II) was investigated using a carbon nanotube electrode (CNE) and fluorine immobilized onto a carbon nanotube electrode (FCNE) in cyclic voltammetry (CV), square-wave (SW) stripping voltammetry, and chronoamperometry. Optimum SW conditions were attained at working ranges of 0.01–0.11 ng L⁻¹ Cu(II) (11 points), and a relative standard deviation of 1.68% (RSD, n = 15) was observed at 10.0 μg L⁻¹ Cu(II). Within a 200 s accumulation time, detection limit of 0.006 μg L⁻¹ was attained. The life span of each electrode was more than 1 month. The sensor was applied to tap water, blood, and rat tail vascular (in vivo). It was found that the sensor could be used with an interface system in the assay of live cells and non-treated blood.     

Residue-specific radical-directed dissociation of whole proteins in the gas phase

The rapid identification of proteins from biological samples is critical for extracting useful information in proteomics studies. Mass spectrometry is one among the various methods of choice for achieving this task; however, current approaches are limited by a lack of chemical control over proteins in the gas phase. Herein, it is shown that modification of tyrosine to iodo-tyrosine followed by UV photodissociation of the carbon-iodine bond can be used to generate a radial site specifically at the modified residue. The subsequent dissociation of the protein is largely dominated by radical-directed reactions, including dominant backbone fragmentation at the modified tyrosine. If iodination of the protein is carried out under natively folded conditions, the modification and ultimate fragmentation can typically be isolated to a single tyrosine residue. Some secondary backbone cleavage in the immediate vicinity of the modified tyrosine also occurs, especially if proline is present. In the absence of a reactive tyrosine residue, similar chemistry occurs via iodination at histidine. Possible mechanisms which would lead to the observed a-type fragments at tyrosine and the secondary fragments at proline are discussed. A method for using this type of site-specific information to reduce database searching times in proteomics experiments by several orders of magnitude is outlined.