Interaction of acetone, hydroxyacetone, acetaldehyde and benzaldehyde with the surface of water ice and HNO3·3H2O ice

Oxygenated volatile organic compounds (OVOCs) influence the oxidative properties of the atmosphere, and their transport from the ground may occur by scavenging by the HNO(3)-rich supercooled water droplets found in polluted convective air masses. With infrared spectroscopy, we have studied the interactions of four typical atmospheric OVOCs (acetone, hydroxyacetone, acetaldehyde and benzaldehyde) with model surfaces of water ice and of trihydrated nitric acid (NAT) ice. We show that these molecules weakly adsorb on water ice and NAT by hydrogen bonding. No chemical reaction occurs between the molecules and the NAT substrate, the OVOCs remaining intact when in contact with hydrated HNO(3) in atmospheric ice clouds.     

In vitro inhibitory properties of ferrocene-substituted chalcones and aurones on bacterial and human cell cultures

Two series of ten chalcones and ten aurones, where ferrocene replaces the C ring and with diverse substituents on the A ring were synthesized. The compounds were tested against two antibiotic-sensitive bacterial strains, E. coli ATCC 25922 and S. aureus ATCC 25923, and two antibiotic-resistant strains, S. aureus SA-1199B and S. epidermidis IPF896. The unsubstituted compound and those with methoxy substitution showed an inhibitory effect on all bacterial strains at minimum inhibitory concentrations ranging between 2 and 32 mg L(-1). For four of these compounds, the effect was bactericidal, as opposed to bacteriostatic. The corresponding organic aurones did not show growth inhibition, underscoring the role of the ferrocene group. The methoxy-substituted aurones and the unsubstituted aurone also showed low micromolar (IC(50)) activity against MRC-5 non-tumoral lung cells and MDA-MB-231 breast cancer cells, suggesting non-specific toxicity.     

Structure of sodiated polyglycines

The intrinsic folding of peptides about a sodium ion has been investigated in detail by using infrared multiple photon dissociation (IRMPD) spectroscopy and a combination of theoretical methods. IRMPD spectroscopy was carried out on sodiated polyglycines G(n)-Na(+) (n=2-8), in both the fingerprint and N-H/O-H stretching regions. Interplay between experimental and computational approaches (classical and quantum) enables us to decipher most structural details. The most stable structures of the small peptides up to G(6)-Na(+) maximize metal-peptide interactions with all peptidic C=O groups bound to sodium. In addition, direct interactions between peptide termini are possible for G(6)-Na(+) and larger polyglycines. The increased flexibility of larger peptides leads to more complex folding and internal peptide structuration through γ or β turns. A structural transition is found to occur between G(6)-Na(+) and G(7)-Na(+), leading to a structure with sodium coordination that becomes tri-dimensional for the latter. This transition was confirmed by H/D exchange experiments on G(n)-Na(+) (n=3-8). The most favorable hydrogen-bonding pattern in G(8)-Na(+) involves direct interactions between the peptide termini and opens the way to salt-bridge formation; however, there is only good agreement between experimental and computational data over the entire spectral range for the charge solvation isomer.     

K2Re(NCS)6: A weak ferromagnet

The preparation of the potassium salt of hexathiocyanate Re(IV) as a pure and crystalline solid is described. The crystal structure for [{K(H₂O)₂}₂{Re(NCS)₆}] (P2₁/c, a = 8.29132(8) Å, b = 15.0296(2) Å, c = 8.5249(1) Å, β = 90.885(1)°, V = 1062.21(2) Å³) revealed the formation of a 3-D coordination polymer based on K-S linkages. This organization leads to rather short intermolecular S···S contacts. The magnetic behavior for the compound is characterized by substantial antiferromagnetic interactions (with Curie-Weiss parameters C = 1.93 cm³mol⁻¹ and θ = −171 K) that in turn lead to a weak ferromagnet with T_C = 13 K.     

Tuning of the emission efficiency and HOMO-LUMO band gap for ester-functionalized {Al(salophen)(H2O)2}+ blue luminophors

A series of [AlL(H(2)O)(2)(NO(3))] complexes, with L standing for an ester substituted salophen-type ligand, has been synthesized, and the luminescence properties have been investigated. These derivatives differ by the nature of the ester-R group introduced at the C5 position of their salicylidene rings (i.e., phenyl, 7a,a'; naphthyl, 7b,b'; pentafluorophenyl, 7c,c'; and p-nitrophenyl, 7d) and by the bis-imino bridge (i.e., 1,2- phenylene, 7a-d; and 1,2-naphthalene, 7a'-c'). All the complexes are characterized by luminescence in the blue range, the chemical diversity having no effect on the emission wavelength (480-485 nm). However, the emission efficiency was found to be strongly dependent on the Schiff-base ligand with quantum yields ranging from ? = 22% to 44%, the highest values being for the salophen derivatives with the electron-withdrawing ester-R groups (7a, 34%; 7a', 23%; 7b, 31%; 7b', 22%; 7c, 40%; 7c', 29%, and 7d, 44%). Both the electrochemical data and DFT calculations show that the HOMO-LUMO band gap is modified as a function of the ester R group (from 2.92 to 3.16 eV, based on the redox potentials). The crystal structures for the N,N'-bis(5-(phenoxycarbonyl)salicylidene)-1,2-phenylenediamine and the N,N'-bis(5-(p-nitrophenoxycarbonyl)salicylidene)-1,2-phenylenediamine aluminum complexes (7a and 7d) are reported.     

Versatile reactivity of 3-chloro-2-phenyl-isoindole-1-carbaldehyde: hydrolysis and alkylating rearrangement to 1-amino-4-isochromanones

3-Chloro-2-phenyl-isoindole-1-carbaldehyde has been prepared from N-phenylisoindolinone under Vilsmeier–Hack conditions. This electrophilic isoindole proved to be stable under the basic conditions used in the final treatment (KOH/MeOH), and for weeks under air in the solid state. Nevertheless, the C–Cl bond proved highly sensitive to any treatment with reducing or alkylating agents targeted towards the pendant carbaldehyde group, giving various phthalimide derivatives. This unique reactivity is exploited for the selective synthesis of new aminoisochromanones.     

Design, synthesis and biological activity of new CDK4-specific inhibitors, based on fascaplysin

We present the design, synthesis, and biological activity of three classes of tryptamine derivatives, which are non-planar analogues of the toxic anti-cancer agent fascaplysin. We show these compounds to be selective inhibitors of CDK4 over CDK2, the most active compound has an IC50 for the inhibition of CDK4 of 6 microM.     

Structure and bonding in a cyclobutyl tris(pyrazolyl)boratoniobium complex and the variation in agostic behaviour with ring size in the series Tp(Me2)NbCl(c-C(n)H(2n-1))(MeC[triple bond]CMe), n = 3-6

The synthesis and characterisation of the cyclobutyl complex Tp(Me2)NbCl(c-C4H7)(MeC[triple bond]CMe) completes the family of cycloalkyl complexes Tp(Me2)NbCl(c-C(n)H(2n-1)), n = 3-6. The properties of the cyclobutyl complex are qualitatively similar to those of its cyclopentyl and cyclohexyl analogues, and dramatically different from those of the cyclopropyl derivative. Most conspicuously, the cyclobutyl system has an alpha-C-H agostic interaction in the dominant isomer, with no evidence for the alpha-C-C agostic character found for the smaller ring. C-C agostic character therefore seems to be unique to the cyclopropyl complex, where the acute C-C-C angles destabilise the C-C bonding orbitals.     

Gd(III) polyaminocarboxylate chelate: realistic many-body molecular dynamics simulations for molecular imaging applications

Realistic molecular dynamics simulations of polyaminocarboxylate complexes of gadolinium (III) ion in water are performed, providing coordination numbers and average residence times in quantitative agreement with available experimental data. A theoretical analysis, based on fitting a fluctuating charges model on ab initio data, also indicates that charge transfer between the ion and the ligand is significant.     

Rh soaked in polyionic gel: an effective catalyst for dehydrogenative silylation of ketones

[Structure: see text] A polyionic gel-soaked Rh catalyst allows the formation of synthetically useful diphenylsilyl (DPS) enols under mild conditions. The reaction proceeds through dehydrogenative silylation of ketones, affording the kinetic silyl enol ether in good to excellent yields. The in situ formed DPS enols were directly involved, without purification, in one-pot aldol and Mannich condensations.