Toxicity of nanomaterials

Nanoscience has matured significantly during the last decade as it has transitioned from bench top science to applied technology. Presently, nanomaterials are used in a wide variety of commercial products such as electronic components, sports equipment, sun creams and biomedical applications. There are few studies of the long-term consequences of nanoparticles on human health, but governmental agencies, including the United States National Institute for Occupational Safety and Health and Japan's Ministry of Health, have recently raised the question of whether seemingly innocuous materials such as carbon-based nanotubes should be treated with the same caution afforded known carcinogens such as asbestos. Since nanomaterials are increasing a part of everyday consumer products, manufacturing processes, and medical products, it is imperative that both workers and end-users be protected from inhalation of potentially toxic NPs. It also suggests that NPs may need to be sequestered into products so that the NPs are not released into the atmosphere during the product's life or during recycling. Further, non-inhalation routes of NP absorption, including dermal and medical injectables, must be studied in order to understand possible toxic effects. Fewer studies to date have addressed whether the body can eventually eliminate nanomaterials to prevent particle build-up in tissues or organs. This critical review discusses the biophysicochemical properties of various nanomaterials with emphasis on currently available toxicology data and methodologies for evaluating nanoparticle toxicity (286 references).     

Side reaction of significance in preparation of peptide- or peptidomimetic-based hydroxamate enzyme inhibitors

Peptidic and peptidomimetic hydroxamates are increasingly being developed as potential pharmaceutical agents in targeting metalloenzymes. For a number of practical considerations, the hydroxamate moiety is often introduced in the synthesis onto valuable advanced synthetic precursors. The approach entails activation of the carboxylate of the synthetic precursor by any number of methods for the preparation of the hydroxamate. We report herein that this widely used approach in preparation of an entire class of enzyme inhibitors is problematic as documented by the formation of an undesirable cyclization product (characterized in this report), which could at times be the exclusive outcome of the carboxylate activation process.     

Interactions of designer antibiotics and the bacterial ribosomal aminoacyl-tRNA site

The X-ray crystal structures for the complexes of three designer antibiotics, compounds 1, 2, and 3, bound to two models for the ribosomal aminoacyl-tRNA site (A site) at 2.5-3.0 Angstroms resolution and that of neamine at 2.8 Angstroms resolution are described. Furthermore, the complex of antibiotic 1 bound to the A site in the entire 30S ribosomal subunit of Thermus thermophilus is reported at 3.8 Angstroms resolution. Molecular dynamics simulations revealed that the designer compounds provide additional stability to bases A1492 and A1493 in their extrahelical forms. Snapshots from the simulations were used for free energy calculations, which revealed that van der Waals and hydrophobic effects were the driving forces behind the binding of designer antibiotic 3 when compared to the parental neamine.     

Temperature-triggered fast-disintegrating polyNIPAM particles via semicontinuous heterophase polymerisation

Crosslinker-free poly(n-isopropylacrylamide) (polyNIPAM) particles produced by conventional emulsifier-free heterophase polymerisations contain gels and do not easily and completely disintegrate in water, if at all. These particles, when cooled below lower critical solution temperature (LCST) swell first and then gradually shrink, due to their slow rate of disintegration. We first show that only particles formed using very low monomer concentration, which have a low molecular weight, are fully soluble in water. Then, we describe a seeded semicontinuous route which was designed in order to be able to maintain a low monomer concentration in water in the course of reaction and control the length and location of growing chains. Nanoparticles produced via semicontinuous approach not only disintegrated in water very quickly but also dissolved in water completely as soon as LCST was reached. This finding may also find applications in technologically important processes for dissolution of macromolecules in solvents.

Enantiomers of a selective gelatinase inhibitor: (R)‐ and (S)‐2‐[(4‐phenoxyphenyl)sulfonylmethyl]thiirane

The compound 2‐[(4‐phenoxyphenyl)sulfonylmethyl]thiirane, C₁₅H₁₄O₃S₂, a selective gelatinase inhibitor, was synthesized and structurally characterized. Two crystals were analyzed, one each for the R and S enantiomers, and the results were compared with the previously reported structure of the racemate. The enantiomerically pure compounds both crystallize with Z′ = 2 in the space group P2₁, while the racemic mixture crystallizes with Z′ = 1 in the space group P2₁/c, with disorder in the position of the thiirane group. This disorder accommodates both molecules for each of the enantiomerically pure crystals, showing good overlap of the molecules of the pure enantiomorphs with the components of the centrosymmetric structure.     

Nanoemulsion formation by phase inversion emulsification: on the nature of inversion

Emulsification processes are usually characterized by the way they allow the surfactants, as well as the dispersed phase, to be incorporated into emulsions. A model cyclohexane-in-water emulsion using a pair of polyoxyethylene nonylphenyl ether surfactants, one oil-soluble and one water-soluble, was considered. Two surfactant mixing approaches consisting of mixed surfactants (agent-in-oil and agent-in-water) and segregated surfactants (agent in corresponding oil and water phases) were used to produce the model emulsion. Formation of oil-in-water nanodroplets could be only achieved if emulsification was associated with the formation of a three-phase microemulsion structure (transitional phase inversion) across the path. This occurred only if segregated surfactants were used in a process in which water was added to oil. With decreasing surfactant concentration, a point was reached below which the inversion mechanism transformed from transitional to catastrophic, leading to the formation of large droplets. The transformation was also accompanied by a shift in the evolution of the drop size. Drop size variations showed a minimum at the inversion point for the transitional phase inversion, whereas they showed a maximum for the catastrophic phase inversion. The agent-in-oil technique followed a catastrophic phase inversion mechanism and ranked second in terms of drop size.     

A method for protein accessibility prediction based on residue types and conformational states

Prediction of protein accessibility from sequence, as prediction of protein secondary structure is an intermediate step for predicting structures and consequently functions of proteins. Most of the currently used methods are based on single residue prediction, either by statistical means or evolutionary information, and accessibility state of central residue in a window predicted. By expansion of databases of proteins with known 3D structures, we extracted information of pairwise residue types and conformational states of pairs simultaneously. For solving the problem of ambiguity in state prediction by one residue window sliding, we used dynamic programming algorithm to find the path with maximum score. The three state overall per-residue accuracy, Q₃, of this method in a Jackknife test with dataset of known proteins is more than 65% which is an improvement on results of methods based on evolutionary information.     

Nanoparticle formation by monomer-starved semibatch emulsion polymerization

Latexes with very small particle size are usually manufactured by microemulsion polymerization. This article explains the preparation of nanolatexes by monomer-starved nucleation in a conventional semibatch emulsion polymerization with a low surfactant/monomer ratio and with no need for a cosurfactant. The semibatch emulsion polymerization reactions started with an aqueous solution of a surfactant and a water soluble initiator. Monomer was added at a fixed rate. The size of particles decreased with decreasing rate of monomer addition. High solids content nanolatexes with particles as small as 25 nm in diameter were produced. Several monomers with different water solubilities were compared. The order of the number of particles in terms of the rate of monomer addition was found to depend on the type of monomer. Water soluble monomers produced more particles due to associated chain transfer to monomer and radical exit. The monodispersity of particles at the end of nucleation increased as the rate of monomer addition decreased. The technique seems to be preferable to microemulsion polymerization, which uses a high concentration of surfactant/cosurfactant and is limited to low monomer holdup.     

Determination of Copper by Adsorptive Stripping Voltammetry in the Presence of Calcein Blue

An electrochemical adsorptive stripping approach is presented for the trace measurement of copper in some real samples. The method is based on the reduction of Cu²⁺ at pH 5.5 calcein blue (CB) containing solution at ?250 mV (vs. Ag/AgCl), adsorption of Cu? CB complex on hanging mercury drop electrode (HMDE) and the voltammetric determination by further reduction to Cu⁺ at HMDE. Experimental optimum conditions were determined in the fundamental studies. At the experimental optimum conditions the adsorbed complex of Cu²⁺ and calcein blue gives a well defined cathodic stripping peak current at ?0.135 V, which has been used for the determination of copper in the concentration range of 0.02 to 15 ng/mL with accumulation time of 90 s. The relative standard deviation (RSD) for the determination of 0.5 and 6.0 ng mL^?1 were 2.60 and 1.94% respectively. (n=10). The method has been applied to the analysis of copper in analytical reagent grade salts and tap water, mineral water and drug samples with satisfactory results.     

A practical synthesis of nitrocefin

Nitrocefin is a key reagent for high and low throughput assays of the activities of penicillin-binding proteins (PBPs) and beta-lactamases, the former used for discovery of antibiotics and the latter for inhibitors of resistance determinants for beta-lactam antibiotics. This compound is commercially available but is prohibitively expensive because of the circuitous routes to its synthesis. We describe herein a three-step synthesis of nitrocefin that gives an overall yield of 44%. This is a practical route to the synthesis of this key reagent for drug discovery.