Perfluorocyclobutane aromatic ether polymers. III. Synthesis and thermal stability of a thermoset polymer containing triphenylphosphine oxide

The preparation of a novel triaryl phosphine oxide thermoset polymer containing the perfluorocyclobutane linkage is described. The synthetic methodology involves the formation of a Grignard reagent from 4-bromotrifluorovinyloxybenzene and reaction with phosphorous trichloride to form the triaryl phosphine trifluorovinyl ether monomer. Oxidation of the phosphine monomer with hydrogen peroxide in ethanol provides quantitative conversion of the phosphine to the phosphine oxide. Analysis of the thermal decomposition of the resulting polymer in both nitrogen and air indicates improvement in thermal and thermal/oxidative stability with respect to the previously reported polymer prepared from 1,1,1-tris(4-trifluorovinyloxy)phenyl ethane. Differences in thermal and thermal/oxidative performance still exist, indicating that oxidative processes contribute to the polymer decomposition in air. © 1998 John Wiley & Sons, Inc. J Appl Polym Sci 69: 2005–2012, 1998     

Kinetics of trifluorovinyl ether cyclopolymerization via Raman spectroscopy

Polymerization kinetics of tris(trifluorovinyloxyphenyl)ethane (TVE) in the bulk are characterized by measuring the disappearance of the fluoro-olefin Raman signal at 1831cm^-1 normalized to an aromatic ring signal as an internal standard. The nth order kinetic model (dx/dt = k(1 − x)ⁿ) was applied to determine a reaction order of 2·0. Reaction rates below 85% conversion measured for various temperatures ranged from 2·2×10^-3min^-1 (t_1/2 = 454 min) to 3·1×10^-1min^-1 (t_1/2 = 3·3 min) for 130°C and 210°C, respectively. Above 85% olefin conversion, second order rate constants deviated from linearity as gelation ensued. An Arrhenius activation energy of 24·6 kcalmol^-1 was determined. The non-destructive Raman technique was found to be an excellent method for measuring the cure kinetics in the bulk and may be applicable to ‘on-line’ needs for general application of perfluorocyclobutane (PFCB) polyarylether materials. © 1998 SCI.     

Computer‐Guided Design,Synthesis, and Biological Evaluation of Quinoxalinebisarylureas as FLT3 Inhibitors

Activating mutations of FMS‐like tyrosine kinase 3 (FLT3) are present in ～30 % of patients with acute myeloid leukemia (AML) and are associated with poor prognosis. Point mutations in the tyrosine kinase domain (TKD) are observed as primary mutations or are acquired as secondary mutations in FLT3 with internal tandem duplications (ITDs) after treatment with tyrosine kinase inhibitors (TKIs). Although dozens of potent inhibitors against FLT3 ITD have been reported, activating TKD point mutations, especially at residues F691 and D835, remain the leading cause for therapy resistance, highlighting the consistent need for new potent inhibitors. Herein we report the identification and characterization of novel quinoxaline‐based FLT3 inhibitors. We used the pharmacophore features of diverse known inhibitors as a starting point for a new optimization algorithm for type II TKIs, starting from an in silico library pharmacophore search and induced‐fit docking in the known FLT3 structure. This led to the design of a set of diverse quinoxalinebisarylureas, which were profiled in an FLT3 kinase activity assay. The most promising compounds were further evaluated in a zebrafish embryo phenotype assay.     

Antimicrobial properties of commercial annatto extracts against selected pathogenic, lactic acid, and spoilage microorganisms

Annatto preparations are used to impart distinctive flavor and color to foods and are a primary colorant in dairy foods such as cheese and butter. There are several reports indicating that certain fractions of the annatto plant have biological activities against microorganisms of significance in food fermentation, food preservation, and human health. However, little is reported describing the nature of the antimicrobial compound(s) or their potential presence in commercial annatto colorant preparations. This study was conducted to determine whether commonly available annatto extracts are capable of influencing the outgrowth of selected lactic acid, spoilage, and pathogenic microorganisms. Disk diffusion and tube macrodilution techniques were used to determine the MICs and MBCs of double-strength water-soluble annatto extracts. Standard antibiotic disks were used as controls for the disk diffusion assay. The results demonstrate that annatto has an inhibitory effect on Bacillus cereus, Clostridium perfringens, and Staphylococcus aureus, with MICs of 0.08, 0.31, and 0.16% (vol/vol) and diameters of inhibition of 9 to 10, 12 to 13, and 15 to 16 mm, respectively. A concentration of 0.63% (vol/vol) inhibited the growth of Streptococcus thermophilus, Lactobacillus casei subsp. casei, Lactococcus lactis, and Paenibacillus polymyxa. The MICs for Listeria monocytogenes and Enterococcus durans were 1.25 and 2.5% (vol/vol), respectively. No activity was detected against Lactobacillus plantarum, Bifidobacterium bifidum, yeasts, or selected gram-negative bacteria.     

Development of a salmon protein hydrolysate that lowers blood pressure

A salmon protein hydrolysate (SPH) was developed containing several angiotensin I-converting enzyme (ACE) inhibitory tripeptides the most abundant of which were Val-Leu-Trp, Val-Phe-Tyr, and Leu-Ala-Phe. Simulated digestion experiments showed that active constituents of SPH would survive in the digestive tract and be available for absorption into the bloodstream. In fact, ACE inhibitory activity was improved following simulated digestion suggesting that there were larger peptides in SPH that might contribute to bioactivity in vivo. A single oral dose (1,500 mg/kg body mass) of SPH significantly lowered blood pressure in spontaneously hypertensive rats (SHR). The treatment of SHR with either SPH fraction (<3,000 Da) or SPH fraction (>3,000 Da) reduced blood pressure. We conclude that the ability of SPH to lower blood pressure is due to a combination of ACE inhibitory tripeptides as identified, as well as additional unknown, peptide species that are generated during digestion of SPH in the gastrointestinal tract.     

Effect of meat ingredients (sodium nitrite and erythorbate) and processing (vacuum storage and packaging atmosphere) on germination and outgrowth of Clostridium perfringens spores in ham during abusive cooling

The effect of nitrite and erythorbate on Clostridium perfringens spore germination and outgrowth in ham during abusive cooling (15 h) was evaluated. Ham was formulated with ground pork, NaNO₂ (0, 50, 100, 150 or 200 ppm) and sodium erythorbate (0 or 547 ppm). Ten grams of meat (stored at 5 °C for 3 or 24 h after preparation) were transferred to a vacuum bag and inoculated with a three-strain C. perfringens spore cocktail to obtain an inoculum of ca. 2.5 log spores/g. The bags were vacuum-sealed, and the meat was heat treated (75 °C, 20 min) and cooled within 15 h from 54.4 to 7.2 °C. Residual nitrite was determined before and after heat treatment using ion chromatography with colorimetric detection. Cooling of ham (control) stored for 3 and 24 h, resulted in C. perfringens population increases of 1.46 and 4.20 log CFU/g, respectively. For samples that contained low NaNO₂ concentrations and were stored for 3 h, C. perfringens populations of 5.22 and 2.83 log CFU/g were observed with or without sodium erythorbate, respectively. Residual nitrite was stable (p > 0.05) for both storage times. Meat processing ingredients (sodium nitrite and sodium erythorbate) and their concentrations, and storage time subsequent to preparation of meat (oxygen content) affect C. perfringens spore germination and outgrowth during abusive cooling of ham.     

Comparative analysis of CRISPR loci in lactic acid bacteria genomes

Clustered regularly interspaced short palindromic repeats (CRISPR) are hypervariable loci widely distributed in bacteria and archaea, that provide acquired immunity against foreign genetic elements. Here, we investigate the occurrence of CRISPR loci in the genomes of lactic acid bacteria (LAB), including members of the Firmicutes and Actinobacteria phyla. A total of 102 complete and draft genomes across 11 genera were studied and 66 CRISPR loci were identified in 26 species. We provide a comparative analysis of the CRISPR/cas content and diversity across LAB genera and species for 37 sets of CRISPR loci. We analyzed CRISPR repeats, CRISPR spacers, leader sequences, and cas gene content, sequences and architecture. Interestingly, multiple CRISPR families were identified within Bifidobacterium, Lactobacillus and Streptococcus, and similar CRISPR loci were found in distant organisms. Overall, eight distinct CRISPR families were identified consistently across CRISPR repeats, cas gene content and architecture, and sequences of the universal cas1 gene. Since the clustering of the CRISPR families does not correlate with the classical phylogenetic tree, we hypothesize that CRISPR loci have been subjected to horizontal gene transfer and further evolved independently in select lineages, in part due to selective pressure resulting from phage predation. Globally, we provide additional insights into the origin and evolution of CRISPR loci and discuss their contribution to microbial adaptation.     

E‐64c‐Hydrazide: A Lead Structure for the Development of Irreversible Cathepsin C Inhibitors

Cathepsin C is a papain‐like cysteine protease with dipeptidyl aminopeptidase activity that is thought to activate various granule‐associated serine proteases. Its exopeptidase activity is structurally explained by the so‐called exclusion domain, which blocks the active‐site cleft beyond the S2 site and, with its Asp 1 residue, provides an anchoring point for the N terminus of peptide and protein substrates. Here, the hydrazide of (2S,3S)‐trans‐epoxysuccinyl‐L ‐leucylamido‐3‐methylbutane (E‐64c) (k₂/K_i=140±5 M ^?1 s^?1) is demonstrated to be a lead structure for the development of irreversible cathepsin C inhibitors. The distal amino group of the hydrazide moiety addresses the acidic Asp 1 residue at the entrance of the S2 pocket by hydrogen bonding while also occupying the flat hydrophobic S1′–S2′ area with its leucine‐isoamylamide moiety. Furthermore, structure–activity relationship studies revealed that functionalization of this distal amino group with alkyl residues can be used to occupy the conserved hydrophobic S2 pocket. In particular, the n‐butyl derivative was identified as the most potent inhibitor of the series (k₂/K_i=56 000±1700 M ^?1 s^?1).     

Cardiac and vascular structure and function are related to lipid peroxidation and metabolism

The present study investigated possible relationships between left ventricular mass, intima-media thickness of the carotid artery (IMT), total arterial compliance, and lipid status in a population sample of 58 apparently healthy subjects aged 20 to 69. By stepwise multiple regression analysis, including age, blood pressure, and smoking, left ventricular mass index, measured by M-mode echocardiography, increased by 13.0 g/m² for each 1 standard deviation (SD=0.11 μM, r=0.60, P<0.01) increase in plasma malondialdehyde and 9.50 g/m² per SD increase in plasma 8-iso-prostaglandin F_2α in women only (SD=8.88 ng/L, r=0.44, P=0.01). Each 1-SD (SD=0.27 g/L) increase in apolipoprotein B was associated with a 63 μm increase in IMT (r=0.47, P=0.01) and a 0.27 mL/min/m²/mm Hg (r=−0.60, P<0.01) decrease in stroke index/pulse pressure ratio, reflecting total arterial compliance in women. In men, each 1-SD increase in the proportion of stearic acid (18∶0) in serum cholesterol esters (SD=0.12 percent units) reduced the transmitral E/A ratio, measured by Doppler echocardiography, reflecting left ventricular diastolic function, by 0.10 units (r=−0.29, P<0.05). Thus, important cardiovascular characteristics, such as left ventricular mass, left ventricular diastolic function, carotid IMT, and total arterial compliance, were independently predicted by indices of lipid metabolism and peroxidation in apparently healthy subjects.     

In situ gasification and CO2 separation using chemical looping with a Cu-based oxygen carrier: Performance with bituminous coals

This paper is concerned with the chemical looping combustion of coal in a technique whereby the fuel is gasified in situ using CO₂ in the presence of a batch of supported copper oxide (the “oxygen carrier”) in a single reactor. As the metal oxide becomes depleted, the feed of fuel is discontinued, the inventory of fuel is reduced by further gasification and then the contents are re-oxidised by the admission of air to the reactor, to begin the cycle again. A catalyst support, impregnated with a saturated solution of copper and aluminium nitrates, acted as a durable oxygen carrier over numerous cycles of reduction and oxidation, using air as the oxidant. Two bituminous coals (Taldinskaya, Russia, and Illinois No. 5, USA) were investigated and compared with a lignite (Hambach, Germany). The lignite was highly reactive and was gasified completely by 15 mol% CO₂ in N₂ at 1203 K and 1 bar, so that there was no build up of char in the bed. The bituminous coals produced chars much less reactive than the lignite char, so that there was a steady accumulation of char in the bed with number of cycles, with the degree of accumulation being dependent on the reactivity of the char. Since the kinetics of gasification by CO₂ of the chars from either bituminous coal were slow, their rates were controlled by intrinsic chemical kinetics and were not affected by the ability of the oxygen carrier to alter the rates of external mass transfer when gasification is rapid. However, it is likely that rates of gasification in the presence of the carrier are still larger than in its absence, owing to the overall lower [CO] present in the bulk of the fluidised bed during chemical looping. At the temperature used, the carrier was cycling between Cu and Cu₂O, since CuO is only stable if the partial pressure of O₂ exceeds 0.03 bar at 1203 K. The CuO decomposes to Cu₂O and O₂ relatively rapidly at these temperatures, once the oxygen concentration is effectively zero. It was impossible to ascertain in our experiments whether the oxygen so generated, after the switching of the air for nitrogen before the start of the succeeding cycle of gasification, made any substantial difference to the reactivity of the char present in the bed. The rate of oxidation of the carrier was found to be much more rapid than the rate of oxidation of the inventory of char. This allows a preferential oxidation of the carrier and most likely accounts for why progressively less CO and CO₂ is produced during successive cycles with short periods of oxidation: the increasingly reduced carrier reacts more rapidly than the char. There was no obvious impact from the sulphur contained in the fuels, but longer-term testing is needed. No agglomeration between the carrier particles and the ash was observed, despite the high temperatures during oxidation.