Biosensors designed for environmental and food quality control based on screen-printed graphite electrodes with different configurations

Graphite electrodes fabricated by screen-printing have been used as amperometric detectors in biosensors based on NAD(+)-dependent dehydrogenases, tyrosinase, or genetically modified acetylcholinesterases. The mono-enzyme sensors have been optimized as disposable or reusable devices for detection of a variety of substrates important in the food industry ( D-lactic acid, L-lactic acid, acetaldehyde) or in environmental pollution control (phenols and dithiocarbamate, carbamate and organophosphorus pesticides). The sensors were prepared in four configurations differing in enzyme confinement, enzyme immobilization and location of the immobilization agent in the biosensor assembly. Tests on real samples have been performed with the biosensors; D-lactic acid and acetaldehyde have been detected in wine and phenols in air.     

Viability of the antigen determines whether DNA or urocanic acid act as initiator molecules for UV-induced suppression of delayed-type hypersensitivity

UV radiation suppresses the immune response, and UV-induced immune suppression contributes to UV-induced photocarcinogenesis. For UV-induced immune suppression to occur, electromagnetic energy (i.e. UV radiation) must be converted to a biological signal. Two photoreceptors have been identified in the skin that serves this purpose, epidermal DNA and trans-urocanic acid (UCA). Although compelling evidence exists to support a role for each pathway (UV-induced DNA damage or photoisomerization of UCA) in UV-induced immune suppression, it is not clear what determines which photoreceptor pathway is activated. To address this question, we injected UV-irradiated mice with a monoclonal antibody with specificity for cis-UCA or applied liposomes containing DNA repair enzymes to the skin of UV-irradiated mice. The effect that each had on UV-induced suppression of delayed-type hypersensitivity was measured. We asked whether the light source used (FS-40 sunlamps vs solar-simulated UV radiation) altered whichever pathway of immune suppression was activated. Different doses of UV radiation and the viability of the antigen were also considered. Neither the dose of UV nor the light source had any influence on determining which pathway was activated. Rather, we found that the viability of the antigen was the critical determinant. When live antigens were used, UV-induced immune suppression was blocked with monoclonal anti-cis-UCA but not with T4 endonuclease V-containing liposomes. The reverse was observed when formalin-fixed or killed antigens were used. Our findings indicate that antigen viability dictates which photoreceptor pathway predominates after UV exposure.     

Synthesis of (pyridinyl)-1,2,4-triazolo[4,3-a]pyridines

Methods for the synthesis of (pyridinyl)-1,2,4-triazolo[4,3-a]pyridines were developed. The principal route to the required intermediate 2-chloropyridines was based on rearrangements of mono N-oxides of 2,2′-bipyridine, 2,3′-bipyridine, 3,3′-bipyridine, 2,4′-bipyridine and 4,4′-bipyridine with phosphorus oxychloride. Reaction of 3,3′-bipyridine 1-oxide or 2,2′-bipyridine 1-oxide with phosphorus oxychloride gave mixtures of chloro isomers. Reaction with acetic anhydride, 3,3′-bipyridine 1-oxide and 2,2′-bipyridine 1-oxide gave exclusively [3,3′-bipyridine]-2(1H)-one and [2,2′-bipyridine]-6(1H)-one, respectively. 1,2,4-Triazolo[4,3-a]pyridines with pyridinyl groups at the 5,6,7 and 8 positions were synthesized.     

Glycosylidene Carbenes. Part 18. Insertion of glycosylidene carbenes into the Sn?H bond of tributyl- and triphenylstannane: A synthesis of stannoglycosides

Insertion of the glycosylidene carbenes, derived from the gluco- and the manno-diazirines 1 and 2 , into the Sn? H bond of R₃SnH (R = Bu or Ph) leads to the fully substituted stannoglycosides 3 – 8 (53–77%). The 1,2-cis-configurated products are formed preferentially (α-D /β -D ranges from 2.5:1 to 5.1:1 with 1 , and 1:1.3 to 1:4.2 with 2 ). Relative to CH₂Cl₂, THF favors formation of the equatorial Sn-glycosides. The stannylated (benzyloxy)glucals 9 and 10 were isolated as side products. The reaction of 1 with (Bu₃Sn)₂ yielded 9 (17% in CH₂Cl₂; 36% in CCl₄) together with the azines 11 and the benzyloxyglucal 12 . NMR Data of the Sn-glycosides 3 – 8 show evidence for an anomeric effect, ¹J(C(1),H) being larger in the axial and ¹J(Sn,C(1)) larger in the equatorial anomers.     

Complexing processes in M(II)-dithiomalonamide-diacetyl triple systems (M= Ni,Cu) in ethanol solution and in a metal(II)hexacyanoferrate(II) gelatin-immobilized matrix materials

The complexing processes in the M ^II -dithiomalonamide-diacetyl triple system (M=Ni, Cu) occuring in the nickel(II)- and copper(II)hexacyanoferrate(II) gelatin-immobilized matrix in contact with aqueous alkaline solutions (pH~12) containing dithiomalonamide and diacetyl at room temperature, and between MCl₂, dithiomalonamide and diacetyl in EtOH solutions upon heating to$80°C, have been studied. In the Ni ^II -dithiomalonamide-diacetyl system, template synthesis occurs in EtOH solution but does not occur in the gelatin-immobilized matrix, whereas in the Cu ^II -dithiomalonamide-diacetyl system, template synthesis occurs in the gelatin-immobilized matrix but not in EtOH solution. Dithiomalonamide and diacetyl are the ligand synthons in the processes indicated.     

<Emphasis Type="Italic">In vitro</Emphasis> inhibitory effect of polyoxometalates on human tumor cells

H₇[NiV₁₃O₃₈] was synthesized from K₇[NiV₁₃O₃₈] using an ion exchange method. Then Pr₂H[NiV₁₃O₃₈] was obtained by double decomposition of H₇[NiV₁₃O₃₈] with Pr₂(CO₃)₃. The actual amount of praseodymium measured by elemental analysis coincides with the designed amount of praseodymium in Pr₂H[NiV₁₃O₃₈]. The i.r. spectra suggested that the [NiV₁₃O₃₈]^7– anion did not collapse after the ion exchange and double decomposition. The ⁵¹V n.m.r. spectrum of Pr₂H[NiV₁₃O₃₈] showed four peaks and their ratio of the relative intensity was 4:4:4:1. This result agrees with the chemical environment of V atoms in the [NiV₁₃O₃₈]^7– anion. In vitro antitumor activities of polyoxometalates on several human tumor cells have been investigated using the MTT method. Pr₂H[NiV₁₃O₃₈] is the most effective polyoxometalate tested in this study for inhibiting KB cell. Pr₂H[NiV₁₃O₃₈] also showed remarkable inhibitory effect on some other tumor cells: HCT, Bel, B₁₆, BCAP and ESCL cells. These results indicate that Pr₂H[NiV₁₃O₃₈] is a potent broad spectrum antitumor agent. The structure type of polyoxometalates greatly influences their antitumor activity: the order of structure type for inhibiting KB cell is: [NiV₁₃O₃₈]^7–>[Mo₇O₂₄]^6–>Anderson structure Keggin structure Dawson structure. Moreover, the nature of the polyatom in the polyoxometalates also greatly influences their antitumor activity: the polyatom order for inhibiting KB cell is: V>Mo W. On the other hand, the nature of the counter cation and the heteroatom in the polyoxometalates exerted a relatively small influence on the inhibitory effect against the KB cell, although the praseodymium salt of [NiV₁₃O₃₈]^7– showed a higher antitumor activity than its potassium salt.     

Influence of branch length asymmetry on the electrophoretic mobility of rigid rod-like DNA

The electrophoretic mobility of three-arm asymmetric star DNA molecules, produced by incorporating a short DNA branch at the midpoint of rigid-rod linear DNA fragments, is investigated in polyacrylamide gels. We determine how long the added branch must be to separate asymmetric star DNA from linear DNA with the same total molecular weight. This work focuses on two different geometric progressions of small DNA molecules. First, branches of increasing length were introduced at the center of a linear DNA fragment of constant length. At a given gel concentration, we find that relatively small branch lengths are enough to cause a detectable reduction in electrophoretic mobility. The second geometric progression starts with a small branch on a linear DNA fragment. As the length of this branch is increased, the DNA backbone length is decreased such that the total molar mass of the molecule remains constant. The branch length was then increased until the asymmetric branched molecule becomes a symmetric three-arm star polymer, allowing the effect of molecular topology on mobility to be studied independent of size effects. DNA molecules with very short branches have a mobility smaller than linear DNA of identical molar mass. The reason for this change in mobility when branching is introduced is not known, however, we explore two possible explanations in this article. (i) The branched DNA could have a greater interaction with the gel than linear DNA, causing it to move slower; (ii) the linear DNA could have modes of motion or access to pores that are unavailable to the branched DNA.     

Investigation of the Electrochemical Reduction of Benzophenone in Aprotic Solvents Using the Method of Cyclic Voltammetry

The reduction of benzophenone (Bzph) in 3-pentanone (PEN), acetone (ACE), N,N-dimethylacetamide (DMA), N,N-dimethylformamide (DMF), tetrahydrofuran (THF), acetonitrile (ACN) and dimethyl sulfoxide (DMSO) with n-tetrabutylammonium hexafluorophosphate (TBAPF₆) as background electrolyte was studied using the technique of cyclic voltammetry at the temperature of 263.15 K. The half-wave potentials (E _1/2) were extracted. The reduction of Bzph occurs in two successive one-electron steps to produce first the free radical anion Bzph⁻ and then the dianion Bzph²⁻. The results indicated that the radical anion Bzph⁻ is reoxidized to Bzph in all investigated solvent media whereas the dianion Bzph²⁻ is reoxidized to Bzph⁻ only in THF. The heterogeneous electron-transfer rate constants (k _s ) were evaluated by employing the electrochemical rate equation proposed by Nicholson. The rate of electron transfer for the Bzph/Bzph⁻ couple was found to be relatively slow in all investigated solvent media. Consequently, the electron-transfer processes can be recognized as quasi-reversible. The diffusion coefficients (D) of Bzph in the investigated solvent media have been calculated using the modified Randles-Sevcik equation. The effect of the physical and chemical properties of the solvent medium on the electrochemical behavior of Bzph has been examined.     

Synthesis and electronic characterization of bipyridine dithiolate rhodium(III) complexes

Five new mixed diimine 1,1'-dithiolate or dithiocarbamate ligand complexes of the form [Rh(bpy)2(SS)][PF6]n, where bpy = 2,2'-bipyridine and SS = various substituted dialkyldithiocarbamates or 1,1'-dithiolates, were synthesized from cis-[Rh(bpy)2(OTf)2][OTf]. The triflate ligands are easily displaced by other ligands and allow these syntheses to proceed in high yields (80-90% overall) under relatively mild reaction conditions and to give high purity products. Electrochemistry shows irreversible two-electron reduction of Rh(III) to Rh(I) and a concomitant loss of one bipyridine ligand; this is followed by reversible one-electron reduction of the remaining 2,2'-bipyridine ligand. The electronic characterizations of these complexes are consistent with significant delocalization of the sulfur electron density onto the empty metal d orbitals. The 1,1'-dithiolate ligands induce larger red shifts in the absorption and emission spectra than the dithiocarbamates as the 1,1'-dithiolates have a more extensive conjugation system.     

Determination of airborne isocyanates as di-n-butylamine derivatives using liquid chromatography and tandem mass spectrometry

A method for the determination of isocyanates as di-n-butyl amine (DBA) derivatives using tandem mass spectrometry (MS/MS) and electrospray ionisation (ESI) is presented. Multiple-reaction monitoring (MRM) of the protonated molecular ions and corresponding deuterium-labelled d₉-DBA derivatives resulted in selective quantifications with correlation coefficients >0.998 for the DBA derivatives of isocyanic acid (ICA), methyl isocyanate (MIC), ethyl isocyanate (EIC), propyl isocyanate (PIC), phenyl isocyanate (PhI), 1,6-hexamethylene diisocyanate (HDI), 2,4-, 2,6-toluene diisocyanate (TDI), isophorone diisocyanate (IPDI), 4,4′-methylenediphenyl diisocyanate (MDI), 3-ring MDI, 4-ring MDI, HDI-isocyanurate, HDI-diisocyanurate, HDI-biuret and HDI-dibiuret. The instrumental precision for 10 repeated injections of a solution containing 0.1 μg ml⁻¹ of the studied derivatives was <2%. Performing MRM of the product ion [DBA + H]⁺ (m/z = 130) from the protonated molecular ion resulted in the lowest detection limits, down to 10 amol (for TDI). Quantification of concentrations below 10⁻⁶ of the occupational exposure limit (OEL) for TDI during 10 min of air sampling was made possible. In an effort to control the formation of alkali adducts, addition of lithium acetate to the mobile phase and monitoring of lithium adducts was evaluated. Having lithium present in the mobile phase resulted in complete domination of [M + Li]⁺ adducts, but detection limits for the studied compounds were not improved. Different deuterium-labelled derivatives as internal standards were evaluated. (1) DBA derivatives of deuterium-labelled isocyanates (d₄-HDI, d₃-2,4-TDI, d₃-2,6-TDI and d₂-MDI), (2) d₉-DBA derivatives of the corresponding isocyanates and (3) d₁₈-DBA derivatives of the corresponding isocyanates. An increase in number of deuterium in the molecule of the internal standard resulted in an increase in instrumental precision and a decrease in correlation within calibration series.