Low-coordinate iridium NHC complexes derived from selective and reversible C–H bond activation of fluoroarenes

Interaction of the reactive 14 VE {Ir(IBioxMe4)3}+ fragment with fluoroarenes results exclusively in ortho-C–H bond oxidative addition and formation of 16 VE Ir(III) derivatives [Ir(IBioxMe4)3(Ar)H]+ (Ar = 2-C6H4F, 2,3-C6H3F2, 2,4,6-C6H2F3). The C–H bond activation reactions occur under mild conditions and are reversible

Biophysical characterization of a protein for structure comparison : methods for identifying insulin structural changes

Although protein structure has been studied for many decades it remains the case that we cannot state with confidence whether two samples have the same molecular structure, particularly in solution. The increasing number of biosimilar biopharmaceutical drugs that are being tested means this is not an academic exercise. In this work we consider how four well-established techniques: dynamic light scattering (DLS), circular dichroism (CD), nuclear magnetic resonance spectroscopy (NMR), and molecular modelling can be combined to provide information about the supposedly well-understood protein insulin. A goal of this work was to establish a systematic means of detecting differences between insulin samples as a function of pH, temperature, and the presence or absence of zinc, all of which are known to change the oligomerisation state and to affect molecular structure. We used the recently developed Secondary Structure Neural Network (SSNN) circular dichroism algorithm to facilitate analysis of the CD spectra

Rhodium(III) and iridium(III) pincer complexes of a neopentyl-substituted PNP pincer ligand which feature agostic interactions

The synthesis and characterization of five-coordinate rhodium(III) and iridium(III) complexes of the form [M(PNP-Np)(biph)][BArF4] are described, where PNP-Np is the neopentyl-substituted pincer ligand 2,6-(Np2PCH2)2C5H3N (Np = CH2tBu), biph = 2,2′-biphenyl, and ArF = 3,5-(CF3)2C6H3. These complexes are notable for the adoption of δ-agostic interactions in the solid state, as evidenced by X-ray crystallography (50–150 K) and ATR-IR spectroscopy, but are structurally dynamic in solution, exhibiting pseudorotation of the biph ligand on the 1H NMR time scale (185–308 K). The strength of the agostic interactions is discussed with reference to the known tert-butyl-substituted analogues [M(PNP-tBu)(biph)][BArF4], probed by reaction with carbon monoxide, and quantified computationally through NBO analysis, from which the conclusion is that 3-center–2-electron bonding increases in the order M = Ir > Rh (cf. 1.5× greater perturbation energy) and pincer ligand = PNP-Np > PNP-tBu (cf. 3.3× greater perturbation energy)

Understanding the enhancement and temperature-dependency of the self-healing and electromechanical properties of dielectric elastomers containing mixed pendant polar groups

High permittivity self-healing dielectric elastomers have the potential to achieve long life, reusability, damage tolerance and enhanced energy density for energy harvesting devices and actuators. The self-healing performance of elastomers and usable temperature range can be affected by the chemical interactions present in the material. Self-healing thermoplastic elastomer styrene-butadiene-styrene (SBS) copolymers were prepared by introducing hydrogen bonding and electrostatic interactions through chemically grafting of polar groups to SBS: methyl thioglycolate (MG) and thioglycolic acid (TG). The mechanical properties were significantly affected by the strength of the hydrogen bonding network in the elastomers, whilst a high relative permittivity of εr ≈ 9.2 with a low loss of tan δ ≈ 0.01 was achieved. In addition, a disorder-to-order phase morphology transition was observed upon increasing the TG content due to the increased hydrogen-bonding network within SBS. At room temperature the self-healed 80/20 MG/TG-SBS exhibited a strain at break of 139% with a recovery ratio of 47.7%, and when healed at 80 °C for 3 hrs exhibited an increased strain at break of 230% with a recovery ratio of 79%. Analysis of FTIR and 1H NMR indicated that the presence of a stronger hydrogen bonding network increased the thermal resistance of the elastomers. The temperature-dependency of the self-healing behaviour was interpreted as the combined effect of hydrogen bonding, electrostatic interactions and chain interdiffusion. This work provides an in-depth understanding of how to tune the electromechanical and self-healing properties of elastomers by tailoring the type and concentration of pendent polar groups. It indicates that intrinsic modification is critical for the development of next generation high performance dielectric elastomers for actuator or energy harvesting devices operating at elevated temperatures

Reactions of cisplatin and oxaliplatin with penicillin G : implications for drug inactivation and biological activity

Determination of the toxicity of compounds toward cancer cells is a frequent procedure in drug discovery. For metal complexes, which are often reactive prodrugs, care has to be taken to consider reactions with components of the cell culture medium that might change the speciation of the metal complex before it is taken up by the cells. Here, we consider possible reactions between the clinical platinum drugs cisplatin and oxaliplatin with penicillin G, an antibiotic added routinely to cell culture media to prevent bacterial contamination. Platinum has a high affinity for ligands with sulfur donors. Penicillin G is an unstable thioether that degrades in a range of pathways. Nuclear magnetic resonance (NMR) and UV–Vis absorption spectroscopic studies show that reactions with cisplatin can occur within minutes to hours at 310 K, but more slowly with oxaliplatin. The identities of the Pt- adducts were investigated by mass spectrometry. The marked effect on cytotoxicity of co-incubation of cisplatin with penicillin G was demonstrated for the HeLa human cervical cancer cell line. These studies highlight the possibility that reactions with penicillin G might influence the cytotoxic activity of metal complexes determined in culture media

Enhanced surface passivation of sub-nanometer silicon dioxide films by superacidic treatments

Subnanometer-scale silicon dioxide (SiO2) films are frequently present before, during, and after silicon device processing, yet they offer minimal surface passivation and can detrimentally impact subsequent processing steps. Here we develop a process whereby the surface passivation of nanometer and subnanometer SiO2 films is enhanced by up to 2 orders of magnitude by a simple room temperature treatment using the superacid bis(trifluoromethane)sulfonimide (TFSA, sometimes TFSI). By accurately modeling the effective lifetime curves corresponding to the superacid treated SiO2 samples, we have determined that the enhanced passivation is mainly due to a reduction in the interface defect density (Dit) at the Si/SiO2 interface, with a minor contribution also arising from the presence of negative charge. X-ray photoelectron spectroscopy of the treated SiO2 films reveals the presence of fluorine, and this, along with hydrogen, is a strong candidate for the chemical passivation of defects at the Si/SiO2 interface. Post treatment, the SiO2 films show short time scale electronic instability, whereby a degradation and then recovery are observed over a period of 1–10 h which is attributed to variations in the Dit, as determined from our analysis of the injection-dependent lifetime data. Following the instability period, the surface passivation remains relatively stable for days. Nuclear magnetic resonance measurements of superacid-based solutions reveal that electron-donating solvents should be avoided, as they exacerbate surface passivation instabilities. The results presented demonstrate that simple strategies can be used to enhance the passivation properties of ultrathin films greatly, which in the age of nanotechnology could offer benefits to device performance in a range of applications including solar cells and batteries

NMR studies of group 8 metallodrugs : 187Os-enriched organo-osmium half-sandwich anticancer complex

Synthesis of this 187Os-enriched organo-osmium azopyridine anticancer complex, has allowed determination of 187Os NMR J-couplings to ligand 1H and 13C, and the 187Os chemical shift. The complex was also characterised by X-ray crystallography and MS

Development and application of a poly(acrylic acid)-grafted styrene–butadiene rubber as a binder system for silicon-graphite anodes in Li-Ion batteries

Silicon anodes require polymer binder systems that are both mechanically robust and electrochemically stable, to accommodate the dramatic volume expansion experienced during cycling operation. Herein, we report the use of a poly(acrylic acid)-grafted styrene–butadiene rubber (PAA-g-SBR) with 80% partially neutralized Na-PAA as the binder system for silicon-graphite anodes. The PAA-g-SBR graft copolymer was synthesized by grafting tert-butyl acrylate onto SBR and treating the intermediate with H3PO4. The PAA-g-SBR/Na-PAA binder system was found to provide superior electrochemical performances to that of a Na-PAA/SBR system. The Na-PAA/PAA-g-SBR system had a stable capacity retention of 673 mAh g–1 for 130 cycles, while the capacity retention of the Na-PAA/SBR system was found to decline immediately. The Na-PAA/PAA-g-SBR system also displayed more preferable mechanical properties, with a lower Young’s modulus value and a larger strain at failure compared to that of the Na-PAA/SBR system. Overall, these findings indicate a promising and robust polymer binder system for the application of silicon anodes in the next generation of lithium-ion batteries

New activation mechanism for half-sandwich organometallic anticancer complexes

The Cpx C–H protons in certain organometallic RhIII half-sandwich anticancer complexes [(η5-Cpx)Rh(N,N′)Cl]+, where Cpx = Cp*, phenyl or biphenyl-Me4Cp, and N,N′ = bipyridine, dimethylbipyridine, or phenanthroline, can undergo rapid sequential deuteration of all 15 Cp* methyl protons in aqueous media at ambient temperature. DFT calculations suggest a mechanism involving abstraction of a Cp* proton by the Rh–hydroxido complex, followed by sequential H/D exchange, with the Cp* rings behaving like dynamic molecular ‘twisters’. The calculations reveal the crucial role of pπ orbitals of N,N′-chelated ligands in stabilizing deprotonated Cpx ligands, and also the accessibility of RhI–fulvene intermediates. They also provide insight into why biologically-inactive complexes such as [(Cp*)RhIII(en)Cl]+ and [(Cp*)IrIII(bpy)Cl]+ do not have activated Cp* rings. The thiol tripeptide glutathione (γ-L-Glu-L-Cys-Gly, GSH) and the activated dienophile N-methylmaleimide, (NMM) did not undergo addition reactions with the proposed RhI–fulvene, although they were able to control the extent of Cp* deuteration. We readily trapped and characterized RhI–fulvene intermediates by Diels–Alder [4+2] cyclo-addition reactions with the natural biological dienes isoprene and conjugated (9Z,11E)-linoleic acid in aqueous media, including cell culture medium, the first report of a Diels–Alder reaction of a metal-bound fulvene in aqueous solution. These findings will introduce new concepts into the design of organometallic Cp* anticancer complexes with novel mechanisms of action

Effect of cysteine thiols on the catalytic and anticancer activity of Ru(ii) sulfonyl-ethylenediamine complexes

We have synthesized a series of novel substituted sulfonyl ethylenediamine (en) RuII arene complexes 1–8 of [(η6-arene)Ru(R1-SO2-EnBz)X], where the arene is benzene, HO(CH2)2O-phenyl or biphenyl (biph), X = Cl or I, and R1 is phenyl, 4-Me-phenyl, 4-NO2-phenyl or dansyl. The ‘piano-stool’ structure of complex 3, [(η6-biph)Ru(4-Me-phenyl-SO2-EnBz)I], was confirmed by X-ray crystallography. The Image ID:d1dt03856g-t1.gif values of their aqua adducts were determined to be high (9.1 to 9.7). Complexes 1–8 have antiproliferative activity against human A2780 ovarian, and A549 lung cancer cells with IC50 values ranging from 4.1 to >50 μM, although, remarkably, complex 7 [(η6-biph)Ru(phenyl-SO2-EnBz)Cl] was inactive towards A2780 cells, but as potent as the clinical drug cisplatin towards A549 cells. All these complexes also showed catalytic activity in transfer hydrogenation (TH) of NAD+ to NADH with sodium formate as hydride donor, with TOFs in the range of 2.5–9.7 h−1. The complexes reacted rapidly with the thiols glutathione (GSH) and N-acetyl-L-cysteine (NAC), forming dinuclear bridged complexes [(η6-biph)2Ru2(GS)3]2− or [(η6-biph)2Ru2(NAC-H)3]2−, with the liberation of the diamine ligand which was detected by LC-MS. In addition, the switching on of fluorescence for complex 8 in aqueous solution confirmed release of the chelated DsEnBz ligand in reactions with these thiols. Reactions with GSH hampered the catalytic TH of NAD+ to NADH due to the decomposition of the complexes. Co-administration to cells of complex 2 [(η6-biph)Ru(4-Me-phenyl-SO2-EnBz)Cl] with L-buthionine sulfoximine (L-BSO), an inhibitor of GSH synthesis, partially restored the anticancer activity towards A2780 ovarian cancer cells. Complex 2 caused a concentration-dependent G1 phase cell cycle arrest, and induced a significant level of reactive oxygen species (ROS) in A2780 human ovarian cancer cells. The amount of induced ROS decreased with increase in GSH concentration, perhaps due to the formation of the dinuclear Ru-SG complex