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Query: UNIPROT:Q9UIJ5 (
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58,342
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Phenanthrene
and 9 K-region derivatives, most of them potential metabolites of
phenanthrene
, were tested for mutagenicity by the reversion of histidine-dependent Salmonella typhimurium TA1535, TA1537, TA1538, TA98 and TA100 and the
rec
assay with Bacillus subtilis H17 and M45. The strongest mutagenic effects in the reversion assay were observed with
phenanthrene
9,10-oxide, 9-hydroxyphenanthrene and N-benzyl-
phenanthrene
-9,10-imine. Interestingly, the mutagenic potency of the arene imine was similar to that of the corresponding arene oxide. This is the first report on the mutagenicity of arene imine. The mutagenic effects of all these
phenanthrene
derivatives were much weaker than that of the positive control benzo[a]pyrene 4,5-oxide. Even weaker mutagenicty was found with cis-9,10-dihydroxy-9,10-dihydrophenanthrene and with trans-9,10-dihydroxy-9-10-dihydrophenanthrene. The other derivatives were inactive in this test. However, 9-10-dihydroxyphenanthrene and 9,10-phenanthrenequinone were more toxic to the
rec
- B. subtilis M45 strain than to the rec+ H17 strain. This was also true for
phenanthrene
9,10-oxide and 9-hydroxyphenanthrene, but not with the other test compounds that reverted (9,10-dihydroxy-9,10-dihydrophenanthrenes; N-benzyl-
phenanthrene
9,10-imine; benzo[a]pyrene 4,5-oxide) or did not revert (
phenanthrene
, 9,10-bis-(p-chlorophenyl)-
phenanthrene
9,10-oxide, 9-10-diacetoxyphenanthrene) the Salmonella tester strains. Although the K region is a main site of metabolism and although all potential K-region metabolites were mutagenic,
phenanthrene
did not show a mutagenic effect in the presence of mouse-liver microsomes and an NADPH-generating system under standard conditions. However, uhen epoxide hydratase was inhibited,
phenanthrene
was activated to a mutagen that reverted his- S. typhimurium. This shows that demonstration of the mutagenic activity of metabolites together with the knowledge that a major metabolic route proceeds via these metabolites dose not automatically imply a mutagenic hazard of the mother compound, because the metabolites in question may not accumulate in sufficient quantities and therefore the presence and relative activities of enzymes that control the mutagenically active metabolites are crucial. N-Benzyl-
phenanthrene
9.10-imine was mutagenic for the episome-containing S. typhimurium TA98 and TA100 but not for the precursor strains TA1538 and TA1535. This arene imine would therefore be useful as a positive control during routine testing to monitor in the former strains the presence of the episome which is rather easily lost.
...
PMID:Mutagenicity of phenanthrene and phenanthrene K-region derivatives. 37 29
Tricarbonyl chromium complexes of naphthalene derivatives are synthesized by chromium-templated [3 + 2 + 1]-benzannulation and subjected to thermally induced haptotropic rearrangement experiments. Thermodynamic and kinetic parameters for the metal shift demonstrate the influence of the arene substitution pattern. In turn, the chromium template may be tuned as well by phosphorus coligands which allow to accelerate or slow down the isomerization process; this effect quantitatively reflects the steric and electronic properties of the coligand sphere. Proper adjustment of the template allows for a photo-induced reverse migration of the chromium moiety which results in a switchable organometallic device. Experiments with enantiopure arene chromium complexes indicate a stereospecific metal migration. The rearrangement proceeds by an intramolecular mechanism in both directions. Haptotropic isomerization reactions are not limited to bicyclic arenes and can be extended from naphthalenes to
phenanthrene
or tetra- and pentacyclic heteroarene systems.
Chem
Rec
2004
PMID:Tunable haptotropic metal migration in fused arenes: towards organometallic switches. 1507 74
This account summarizes our recent efforts to synthesize numerous important and interesting polycyclic arenes under mild conditions using metal-catalyzed protocols. The palladium-catalyzed annulations of 2-iodobiphenyls or 2,2'-diiodobiphenyls with alkynes efficiently generated
phenanthrene
derivatives. This synthetic method was utilized as the key step when preparing
phenanthrene
-based alkaloids, tetrabenzopyracylenes and persubstituted [8]circulenes. Depending on whether a palladium or nickel catalytic system was used, 1-ethynyl-8-iodonaphthalenes underwent either a cyclodimerization or a nitrile-incorporated cascade reaction to produce zethrenes or pyrroloarenes, respectively. Methylene-bridged polyarenes are generated easily from 2-halo-2'-methylbiaryls through benzylic C-H bond activation and subsequent carbon-carbon bond formation, and palladium complexes promote the arylation of methylene carbons. The palladium-catalyzed annulations of 1,8-bis(arylethynyl)naphthalene derivatives with o-diiodoarenes yielded benzo[k]fluoranthene-based linear acenes, which can be applied to synthesize highly curved fragments of fullerenes. The self-reactions of diarylethynes formed either dihydrocyclopenta[a]indenes or octaaryl-1,3,5,7-octatetraenes through palladium-catalyzed cycloisomerization or nickel-catalyzed tetramerization, respectively. In the presence of palladium catalysts, the hydroalkynylation of terminal arylalkynes directly generated angular trimerization adduct dienynes.
Chem
Rec
2015 Feb
PMID:Metal-catalyzed cascade reactions: useful synthetic tools for the preparation of polycyclic arenes. 2537 30
