TY - JOUR
T1 - Reactions of potent antitumor complex trans-[RuIIICl 4(indazole)2]- with a DNA-relevant nucleobase and thioethers: Insight into biological action
AU - Egger, Alexander
AU - Arion, Vladimir
AU - Reisner, Erwin
AU - Cebrian, Berta
AU - Shova, Sergiu
AU - Trettenhahn, Günter
AU - Keppler, Bernhard
N1 - Coden: INOCA
Affiliations: Inst. Inorg. Chem. Univ. Vienna, Währingerstrasse 42, A-1090 Vienna, Austria; Inst. of Phys. Chem. Univ. Vienna, Währingerstrasse 42, A-1090 Vienna, Austria; Department of Chemistry, Moldova State University, A. Mateevici Street 60, 2009 Chisinau, Moldova
Adressen: Arion, V.B.; Inst. Inorg. Chem. Univ. Vienna; Währingerstrasse 42 A-1090 Vienna, Austria; email: [email protected]
Source-File: PhysChemieScopus.csv
Import aus Scopus: 2-s2.0-11244291325
Importdatum: 21.12.2006 12:06:24
12.02.2008: Datenanforderung 2112 (Import Sachbearbeiter)
09.02.2010: Datenanforderung UNIVIS-DATEN-DAT.RA-2 (Import Sachbearbeiter)
PY - 2005
Y1 - 2005
N2 - Reactions of the complex trans-[RuCl4(Hind)2]- (Hind ) indazole), which is of clinical relevance today, with both
the DNA model nucleobase 9-methyladenine (made) and the thioethers R2S (R ) Me, Et), as models of the
methionine residue in biological molecules possibly acting as nitrogen-competing sulfur-donor ligands for ruthenium
atom, have been investigated to get insight into details of mechanism leading to antitumor activity. Three novel
ruthenium complexes, viz., [RuIIICl3(Hind)2(made)], 1, [RuIICl2(Hind)2(Me2S)2], 2, and [RuIICl2(Hind)2(Et2S)2], 3, have
been isolated as solids. Oxidation of 2 and 3 with hydrogen peroxide in the presence of 12 M HCl in chloroform
afforded the monothioether adducts, viz., [RuIIICl3(Hind)2(Me2S)], 4, and [RuIIICl3(Hind)2(Et2S)], 5. By dissolution of
2 or 3 in DMSO, replacement of both R2S ligands by DMSO molecules occurred with isolation of trans,trans,trans-
[RuIICl2(Hind)2(DMSO)2], 6. The products were characterized by elemental analysis, IR, UV-vis, electrospray mass
spectrometry, cyclic voltammetry, and X-ray crystallography (1âCH2Cl2âCH3OH and 1â1.1H2Oâ0.9CH3OH, 2, and
5). The first crystallographic evidence for the monofunctional coordination of the 9-methyladenine ligand to ruthenium
via N7 and the self-pairing of the complex molecules via H-bonding, using the usual Watson-Crick pairing donor
and acceptor sites of two adjacent 9-methyladenine ligands, is reported. The electrochemical behavior of 1-5 has
been studied in DMF and DMSO by cyclic voltammetry. The redox potential values have been interpreted on the
basis of the Lever¿s parametrization method. The EL parameter was estimated for 9-methyladenine at 0.18 V,
showing that this ligand behaves as a weaker net electron donor than imidazole (EL ) 0.12 V). The kinetics of the
reductively induced stepwise replacement of chlorides by DMF in 4 and 5 were studied by digital simulation of the
cyclic voltammograms. The rate constant k1 has been determined as 0.9 ± 0.1 s-1, which obeys the first-order rate
law, while k2 is concentration dependent (0.2 ± 0.1 M1-nâs-1 with n > 1 for 4 mM solutions of 4 and 5), indicating
higher-order reactions mechanism.
AB - Reactions of the complex trans-[RuCl4(Hind)2]- (Hind ) indazole), which is of clinical relevance today, with both
the DNA model nucleobase 9-methyladenine (made) and the thioethers R2S (R ) Me, Et), as models of the
methionine residue in biological molecules possibly acting as nitrogen-competing sulfur-donor ligands for ruthenium
atom, have been investigated to get insight into details of mechanism leading to antitumor activity. Three novel
ruthenium complexes, viz., [RuIIICl3(Hind)2(made)], 1, [RuIICl2(Hind)2(Me2S)2], 2, and [RuIICl2(Hind)2(Et2S)2], 3, have
been isolated as solids. Oxidation of 2 and 3 with hydrogen peroxide in the presence of 12 M HCl in chloroform
afforded the monothioether adducts, viz., [RuIIICl3(Hind)2(Me2S)], 4, and [RuIIICl3(Hind)2(Et2S)], 5. By dissolution of
2 or 3 in DMSO, replacement of both R2S ligands by DMSO molecules occurred with isolation of trans,trans,trans-
[RuIICl2(Hind)2(DMSO)2], 6. The products were characterized by elemental analysis, IR, UV-vis, electrospray mass
spectrometry, cyclic voltammetry, and X-ray crystallography (1âCH2Cl2âCH3OH and 1â1.1H2Oâ0.9CH3OH, 2, and
5). The first crystallographic evidence for the monofunctional coordination of the 9-methyladenine ligand to ruthenium
via N7 and the self-pairing of the complex molecules via H-bonding, using the usual Watson-Crick pairing donor
and acceptor sites of two adjacent 9-methyladenine ligands, is reported. The electrochemical behavior of 1-5 has
been studied in DMF and DMSO by cyclic voltammetry. The redox potential values have been interpreted on the
basis of the Lever¿s parametrization method. The EL parameter was estimated for 9-methyladenine at 0.18 V,
showing that this ligand behaves as a weaker net electron donor than imidazole (EL ) 0.12 V). The kinetics of the
reductively induced stepwise replacement of chlorides by DMF in 4 and 5 were studied by digital simulation of the
cyclic voltammograms. The rate constant k1 has been determined as 0.9 ± 0.1 s-1, which obeys the first-order rate
law, while k2 is concentration dependent (0.2 ± 0.1 M1-nâs-1 with n > 1 for 4 mM solutions of 4 and 5), indicating
higher-order reactions mechanism.
M3 - Article
SN - 0020-1669
VL - 44
SP - 122
EP - 132
JO - Inorganic Chemistry
JF - Inorganic Chemistry
IS - 1
ER -