Functional longevity of intraperioneal drains: an experimental evaluation

Various types of drains were inserted into the peritoneal cavity of twenty-eight dogs. After one to seven days, all drains failed to show the presence of 200 cc of colored fluid injected intraperitoneally. On autopsy, all tubes were surrounded and occluded by omentum.     

Foetal alcohol syndrome in Saskatchewan: unchanged incidence in a 20-year period

Ethers and thioethers of monosaccharides have been synthesised which show potent toxicity to mouse (LD50 > or = 4 g.kg-1 O.W. and 0.2 to 1.5 g.kg-1 I.P.W.). A study of calcium antagonist activity for the full series of compounds indicated that the activity was similar for both O- and S- ethers and maximum activities were observed for monoacetoneglucose ethers possessing carbon chain close to 8 carbons.     

Molecular structure and driving force to metastable states: Janus faces in polymer crystallization

This paper is a retrospective of a past dedicated to research on polymers and a situation sketch of the present and the near future. (Co)polymers discussed are mainly based on ethylene. (Cross‐)fractionation techniques combined with state‐of‐the‐art characterization techniques, like quantitative differential scanning calorimetry, are powerful tools for the study of the links between two main topics: molecular structure and crystallization/melting. These form the two ‘Janus faces’ polymers can show, namely Face 1: the molecular structure resulting from polymerization with the keyword ‘nature’; and Face 2: the driving force of crystallization towards a metastable state, with the keyword ‘nurture’. After all, to meet demands for properties of products, in principle one starts with a given molecular architecture, after which dedicated processing, including application of temperature–time ramps, has to do the job. With new instrumentation, especially fast scanning (chip) calorimetry, for the first time in history the driving force towards crystallization into one of the possible metastable states – via Face 2 – can be controlled, of course within certain limits given by Face 1. This promising outlook of combining the faces to a useful symbiosis of Janus will be a challenge for those working in the science of crystallization of polymers. © 2018 Society of Chemical Industry     

Corrosion protection of AA 2024-T3 aluminium alloys using 3, 4-diaminobenzoic acid chelated zirconium-silane hybrid sol-gels

Organic-inorganic polymers formed by hydrolysis/condensation reactions of alkoxide precursors, such as organically modified silanes (Ormosils) are used for several industrial applications such as electronic, optical and protective anticorrosion coatings. Such materials possess superior chemical stability, physical strength and scratch resistance characteristics when compared to organic polymers. Further performance improvement can be achieved through the incorporation of zirconium and titanium based nanoparticles, also formed through from precursors via the sol-gel process. However due to the inherent reactivity differences of the above precursors, they must be hydrolysed separately before being combined for final condensation. Zirconium precursors are commonly chelated using acetic acid or acetyl acetonate prior to hydrolysis, to lower the hydrolysis rate.In this body of work, 3,4-diaminobenzoic acid (DABA) and acetyl acetonate (acac) were compared as chelating ligands for controlling the hydrolysis reactions of zirconium n-propoxide to form nanoparticles within a silane sol matrix. The sols were applied as coatings on aerospace grade aluminium alloy AA 2024-T3 and characterised by physical, spectroscopical, microscopical, electrochemical and calorimetric techniques. The electrochemical properties of the coatings, as characterised by EIS and PDS, correlated with neutral salt spray evaluations confirming that the use of DABA as a chelating ligand significantly improved the coating performance when compared to the traditional diketone ligand. The data indicates the anticorrosion properties of the nitrogen rich chelate have a key role in protecting the alloy through the formation of smaller zirconium nanoparticles, thus improving the polymer network stability.     

A combination of a common splice site mutation and a frameshift mutation in the COL7A1 gene: absence of functional collagen VII in keratinocytes and skin

Musk xylene (2,4,6-trinitro-1-t-butylxylene; MX) is a synthetic nitromusk perfume ingredient that induces and inhibits mouse cytochrome P4502B (CYP2B) enzymes in vivo. The purpose of the present work was to determine whether amine metabolites of MX contributed to the enzyme inhibition and, if so, to define the nature and kinetics of this inhibition. When dosed orally to phenobarbital (PB)-treated mice, MX (200 mg/kg) inhibited > 90% of the PB-induced O-dealkylation of 7-pentoxyresorufin (PROD), and [14C]MX equivalents bound covalently to microsomal proteins. However, when this experiment was repeated in mice pretreated with antibiotics to eliminate the gastrointestinal flora, no decrease in PB-induced PROD activity and no covalent binding to microsomal proteins were observed. Thus, the ability of antibiotic treatment to eliminate the enzyme inhibition and covalent binding implicated amine metabolites of MX formed by nitroreduction in anaerobic intestinal flora as obligatory for these effects. Two monoamine metabolites of MX were synthesized to study enzyme inhibition directly. These metabolites were 2-amino-4,6-dinitro-1-t-butyl-xylene and 4-amino-2,6-dinitro-1-t-butylxylene, referred to as o-NH2-MX and p-NH2-MX, respectively, reflecting the position of the amine substitution relative to the t-butyl function. In the in vitro studies with PB-induced mouse liver microsomes, both amines inhibited PROD activity when preincubated in the absence of NADPH. However, only p-NH2-MX caused a time- and NADPH-dependent loss of PROD activity, and the inactivation rate was a pseudo-first-order process that displayed saturation kinetics. These results indicate that p-NH2-MX is a mechanism-based inactivator of mouse CYP2B enzymes. From kinetic analyses, the Ki was calculated to be 10.5 microM and the Kinact was 1.2 min-1. As final confirmation of the inhibitory effects of p-NH2-MX on mouse CYP2B enzymes, the amine (0.67 mmol/kg) was dosed orally to PB-induced mice. At 2 hr after dosing, p-NH2-MX inhibited essentially all of the PB-induced PROD activity, whereas an equimolar dosage of parent MX had no effect at this early time. Thus, although MX is an inducer of mouse CYP2B enzymes, an amine metabolite of MX is a mechanism-based inactivator of mouse CYP2B10. Furthermore, it is likely that the amine is responsible for the lack of functional CYP2B enzyme activity associated with induction of this enzyme by MX.