INHIBITION OF 12-O-TETRADECANOYLPHORBOL-13-ACETATE-INDUCED TUMOR PROMOTION IN MURINE SKIN BY SYSTEMIC EFFECTS OF ULTRAVIOLET IRRADIATION

Systemic effects of UVB irradiation (280-320 nm) have been shown to prevent subsequent chemical tumorigenesis induced by an initiation-promotion protocol. The present investigation was designed to determine whether initiation or promotion is prevented by UV irradiation. Groups of 25 B6D2F1/J mice received 12 weeks of intermittent dorsal UVB radiation treatments administered before, or 3 weeks after, initiation with a single application of 7,12-dimethylbenz[a]anthracene on the ventral skin. All mice were promoted ventrally with 5 micrograms 12-O-tetradecanoylphorbol-13-acetate (TPA) applied three times weekly throughout the experiment. UV irradiation consisted of five 30-min exposures per week to a bank of 6 Westinghouse FS40 sunlamps. UV irradiation applied before or after initiation resulted in a decrease of 18-16 tumors per group of 25 mice, for a reduction of 61 and 50%, respectively, at 24 weeks after the first TPA treatment. Thus, prevention of tumor development was similar whether the UV influence was present or not during initiation. This finding suggests that the UV prevention of promotion could account for UV inhibition of skin tumors induced by an initiation-promotion regimen. Consistent with this concept, pretreatment of mice with dorsal UVB radiation was found to reduce DNA synthesis after exposure to TPA by 46%, although it did not decrease tritiated benzo[a]pyrene binding to DNA, in ventral epidermis. Thus, UVB irradiation systemically reduced TPA-induced tumor promotion in murine skin.     

Effect of mercury(II) on metal complex labilities determined by direct-current anodic stripping voltammetry on a thin mercury film electrode

The labilities of copper, lead and cadmium complexes with fulvic acid, nitrilotriacetic acid and an iron-humic acid colloid were studied on a preplated thin mercury film electrode and with in-situ plating of mercury on a glassy carbon electrode. In the presence of mercury(II) the apparent labilities based on direct-current anodic stripping voltammetric peak-area measurements increased for each of the cadmium and lead species and for the copper iron-humic acid colloid species. In contrast, for the copper complexes with nitrilotriacetic acid and fulvic acid the lability was not measurably altered by mercury(II); it is inferred that they do not undergo rapid metal exchange with mercury(II).     

Iron(III) activation hits a [4 + 4] macrocycle

The tetranuclear complex [Fe(III)2(L')(OH)(CH3O)]2, 1, has been synthesised from the reaction of either ferrous [in excess as 4:1 or stoichiometric 2:1 iron(II) : H4L] or ferric ions [4:1 iron(III) : H4L] with the large macrocycle, H4L, using aerobic conditions in methanol in the presence of triethylamine. The structure of 1 was determined by single-crystal X-ray diffraction. These reaction conditions lead to the modification of the original macrocycle through the incorporation of a methylene group between two amine groups to give an imidazolidine ring in (L')4-. The controlled addition of formaldehyde into the reaction system results in a significantly improved yield of 1, suggesting that it is involved in the reaction mechanism. The (L')4- macrocycle binds to two, well-separated, iron(III) centres [Fe(1)...Fe(1a) > 8 A]. Each iron(III) centre is further linked via hydroxy and methoxy bridges to equivalent iron(iii) centres contained in a second macrocycle. Overall this gives a structure containing two {Fe(OH)(CH(3)O)Fe} dimers [Fe(1)...Fe(2)ca. 3.2 A] sandwiched by two (L')4- macrocycles. The complex was further characterised by SQUID magnetic measurements and can be interpreted in terms of two isolated antiferromagnetically coupled Fe(III) dimers (J=-23.75 K).     

Preparation of iron amido complexes via putative Fe(IV) imido intermediates

The isolation and characterization of monomeric Fe(III) amido complexes with hybrid ureate/amidate ligands is described. An aryl azide serves as the source of the amido ligand in preparing the complexes from trigonal monopyramidal Fe(II) precursors. Aryl azides more commonly react with transition metal complexes by a two-electron oxidation process to yield imido complexes, suggesting that the Fe(III) amido complexes may be formed from high valent species by hydrogen atom abstraction from an external species. The mechanistic basis for formation of the amido complexes is investigated using substrates that readily donate hydrogen atoms. Results from these experiments suggest that the Fe(III) amido complexes are generated from Fe(IV) imido intermediates that can facilitate homolytic X-H bond cleavage. The Fe(III) amido complexes are high spin (S = 5/2) with a strong absorbance band at lambdamax approximately 600 nm and extinction coefficients between 2000 and 3000 M-1 cm-1. These complexes are hygroscopic, reacting with 1 equiv of water to produce the corresponding Fe(III)-OH complexes and p-toluidine.     

Synthesis, characterization, solid-state molecular structures, and deprotonation reactions of cationic alcohol complexes of osmium nitrosyl porphyrins

New alkoxide (OEP)Os(NO)(OR) (OEP = 2,3,7,8,12,13,17,18-octaethylporphyrinato dianion; R = ethyl, isopropyl, hexyl, cyclohexyl) compounds and alcohol [(OEP)Os(NO)(HOR)]+ complexes (R = methyl, ethyl, isopropyl, hexyl, cyclohexyl) have been prepared in high yields and have been fully characterized by IR, 1H NMR, and UV-vis spectroscopy, and by elemental analyses. The (OEP)Os(NO)(OEt) compound was characterized by single-crystal X-ray crystallography. The cationic aqua and alcohol [(OEP)Os(NO)(HOR)]+ complexes (R = ethyl, isopropyl, hexyl) complexes were also characterized by single-crystal X-ray crystallography, and the latter represent the first osmium alcohol structures to be reported. The electrophilic [(OEP)Os(NO)]+ cation in the [(OEP)Os(NO)(HOR)]+ complexes renders the coordinated alcohol ligands susceptible to deprotonation by pyridine to produce the corresponding alkoxide (OEP)Os(NO)(OR) derivatives. A one-pot reaction sequence for the preparation of new (OEP)Os(NO)(OR) complexes from (OEP)Os(NO)(OEt) was developed, which was based on (i) initial protonation of the ethoxide compound to give [(OEP)Os(NO)(HOEt)]+, (ii) alcohol substitution by ROH to give [(OEP)Os(NO)(HOR)]+, and (iii) deprotonation of the latter by pyridine to give (OEP)Os(NO)(OR).     

Ternary-column system for high-throughput direct-injection bioanalysis by liquid chromatography/tandem mass spectrometry

As a continuation of our efforts to improve our high-flow on-line bioanalytical approach for high-throughput quantitation of drugs and metabolites in biological matrices by high-performance liquid chromatography (LC) and tandem mass spectrometry (MS/MS), we have developed a ternary-column on-line LC/MS/MS system with dual extraction columns used in parallel for purification and an analytical column for analysis. The advantage of the dual extraction column system is that sample analysis can take place in one of the extraction columns while the other column is being equilibrated. Thus, the equilibration time does not add to the run time, hence shortening the injection cycle time and increasing the sample throughput. Moreover, the use of two extraction columns in parallel increases the number of samples that can be injected before the system fails due to an overused extraction column. Such a system has successfully been used to develop and validate a positive ion electrospray LC/MS/MS bioanalytical method for the quantitative determination of a guanidine-containing drug candidate in rat plasma. The system used for this work utilized two Oasis HLB extraction columns (1 x 50 mm, 30 microm), one C18 analytical column (3.9 x 50 mm, 5 microm), a ten-port switching value and a tandem mass spectrometer. The on-line analysis was accomplished by the direct injection of 10 microL of the sample, obtained by mixing a rat plasma sample 1:1 with an aqueous internal standard solution. Selected reaction monitoring (SRM) was utilized for the detection of the analyte and internal standard. The standard curve range was 1.00-200 ng/mL. The intra- and inter-day precision and accuracy were within 6.6%. The on-line purification step lasted for only 0.3 min and total run time was only 1.6 min.     

Conformation and vibrational spectra of 1-bromo-1,5-hexadiyne (bromobipropargyl)

The IR spectra of 1-bromo-1,5-hexadiyne (bromobipropargyl) as a vapour, liquid and crystalline solid and in several solvents have been recorded. Raman spectra were obtained for the liquid (including polarization measurements) and the crystal.The data were interpreted in terms of two conformers, trans and gauche, in the vapour and liquid states and one, trans, in the crystal. The conclusion that the trans conformer was the one present in the crystal was based on several independent pieces of evidence. Vibrational assignments were made, supported by normal coordinate calculations.     

Directed Evolution and Biocatalysis

This review describes the current state of biocatalysis in the chemical industry. Although we recognize the advantages of chemical approaches, we suggest that the use of biological catalysis is about to expand dramatically because of the recent developments in the artificial evolution of genes that code for enzymes. For the first time it is possible to consider the rapid development of an enzyme that is designed for a specific chemical reaction. This technology offers the opportunity to adapt the enzyme to the needs of the process. We describe herein the development of enzyme evolution technology and particularly DNA shuffling. We also consider several classes of enzymes, their current applications, and the limitations that should be addressed. In a review of this length it is impossible to describe all the enzymes with potential for industrial exploitation; there are other classes, which given appropriate activity, selectivity, and robustness, could become useful tools for the industrial chemist. This is an exciting era for biocatalysis and we expect great progress in the future.     

Generation of AuPd22/Au2Pd21 analogues of the high-nuclearity Pd23(CO)20(PEt3)10 cluster containing 19-atom centered hexacapped-cuboctahedral (nu 2-octahedral) metal fragment: structural-to-synthesis approach concerning formation of Au2Pd21(CO)20(PEt3)10

Reactions of Pd(PEt(3))(2)Cl(2) and Au(PPh(3))Cl in DMF with NaOH under CO atmosphere gave rise to the unique capped three-shell homopalladium Pd(145)(CO)(x)(PEt(3))(30)(x approximately 60) and two neutral Au-Pd clusters: Au(2)Pd(21)(CO)(20)(PEt(3))(10) (1) and Au(2)Pd(41)(CO)(27)(PEt(3))(15)(following article). Similar reactions with Pd(PMe(3))(2)Cl(2) being used in place of Pd(PEt(3))(2)Cl(2) afforded Au(2)Pd(21)(CO)(20)(PMe(3))(10) (2), the trimethylphosphine analogue of, and the electronically equivalent [AuPd(22)(CO)(20)(PPh(3))(4)(PMe(3))(6)](-) monoanion (3) as the [PPh(4)](+) salt. Each of these three air-sensitive 23-atom heterometallic Au-Pd clusters was obtained in low yields (7-25%); however, their geometrical similarities with the known cuboctahedral-based homopalladium Pd(23)(CO)(20)(PEt(3))(10) (4), recently obtained in good yields from Pd(10)(CO)(12)(PEt(3))(6), suggested an alternative preparative route for obtaining. This "structure-to-synthesis" approach afforded 1 in 60-70% yields from reactions of Pd(10)(CO)(12)(PEt(3))(6) and Au(PPh(3))Cl in DMF with NaOH under N(2) atmosphere. Both the compositions and atomic arrangements for 1, 2 and 3 were unambiguously established from low-temperature single-crystal CCD X-ray crystallographic determinations in accordance with their nearly identical IR carbonyl frequencies. Cluster 1 was also characterized by (31)P[(1)H] NMR, cyclic voltammetry (CV) and elemental analysis. The virtually identical Au(2)Pd(21) core-architectures of 1 and 2 closely resemble that of 4, which consists of a centered hexa(square capped)-cuboctahedral Pd(19) fragment of pseudo-O(h) symmetry that alternatively may be viewed as a centered Pd(19)nu(2)-octahedron (where nu(n) designates (n + 1) equally spaced atoms along each edge). [AuPd(22)(CO)(20)(PPh(3))(4)(PMe(3))(6)](-) (3) in the crystalline state ([PPh(4)](+) salt) consists of two crystallographically independent monoanions 3A and 3B; a superposition analysis ascertained that their geometries are essentially equivalent. A CV indicates that reversibly undergoes two one-electron reductions and two one-electron oxidations; these reversible redox processes form the basis for an integrated structural/electronic picture that is compatible with the existence of the electronically-equivalent 1-3 along with the electronically-nonequivalent 4 (with two fewer CVEs) and other closely related species.     

Practical synthesis of 1-aryl-6-(hydroxymethyl)-2-ketopiperazines via a 6-exo amide-epoxide cyclization

[reaction: see text] Chiral 1-aryl-6-(hydroxymethyl)-2-ketopiperazines can be prepared via an operationally simple, 6-exo epoxide ring-opening cyclization to form the ketopiperazine C6-N1 bond in high yields and with excellent enantiomeric purity.