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Arene-Ruthenium(II) Complexes Containing 11H-Indeno[1,2-b]quinoxalin-11-one Derivatives and Tryptanthrin-6-oxime: Synthesis, Characterization, Cytotoxicity, and Catalytic Transfer Hydrogenation of Aryl Ketones.
A series
of novel mono- and binuclear arene–ruthenium(II)
complexes [( p -cym)Ru(L)Cl] containing 11 H -indeno[1,2- b ]quinoxalin-11-one derivatives or tryptanthrin-6-oxime
were synthesized and characterized by X-ray crystallography, IR, NMR
spectroscopy, cyclic voltammetry, and elemental analysis. Theoretical
calculations invoking singlet state geometry optimization, solvation
effects, and noncovalent interactions were done using density functional
theory (DFT). DFT calculations were also applied to evaluate the electronic
properties, and time-dependent DFT was applied to clarify experimental
UV–vis results. Cytotoxicity for cancerous and noncancerous
human cell lines was evaluated with cell viability MTT assay. Complexes
demonstrated a moderate cytotoxic effect toward cancerous human cell
line PANC-1. The catalytic activity of the complexes was evaluated
in transfer hydrogenation of aryl ketones. All complexes exhibited
good catalytic activity and functional group tolerance.
## Introduction
Introduction Chemistry
of half-sandwich arene–ruthenium(II) complexes
has been intensively investigated in the recent years, due to their
applications in different areas such as catalysis and pharmacology.
Such complexes demonstrated high antiviral, 1 − 3 antibiotic, 3 − 6 and antitumor 7 − 17 activity. Ruthenium(II) coordination compounds also have been
extensively
investigated for their catalytic activity in transfer hydrogenation
reactions 18 − 27 and metathesis polymerization. 28 − 30 Arene–ruthenium
complexes have piano-stool type geometry
with pseudo-octahedral symmetry near the ruthenium(II) atom. The arene
fragment stabilizes the complex and protects the Ru(II) metal center
from oxidation to ruthenium(III). Aromatic ligands are relatively
inert in substitution reactions and can be considered as spectator
ligands. The three remaining coordination sites opposite to the arene
ligand can be used to introduce a wide variety of ligands with N-,
O-, S- or P-donor atoms. In the past decade, there has been a surge
of interest in nitrogen-donor ligands for use in catalysis and bidentate
ligands have been very successful in this area. Our group is
involved in the research of polycyclic N-containing
ligands—oximes of 11 H -indeno[1,2- b ]quinoxalin-11-one and its structural analogues. 31 11 H -Indeno[1,2- b ]quinoxalin-11-one
oxime, often denoted in the literature as IQ1, and its sodium salt,
IQ1S, were reported as potent c-Jun N-terminal kinase (JNK3) inhibitors, 31 , 32 anti-inflammatory agents, 33 − 35 neuroprotectors, 36 , 37 and antitumor agents. 38 − 40 Tryptanthrin demonstrates a wide
range of bioactivities, 41 , 42 including antibacterial, 43 , 44 antiviral, 45 anticancer, 46 , 47 and anti-inflammatory 48 activity. However,
the coordination chemistry of such compounds is insufficiently explored.
There are only few examples of nickel(II) and cobalt(II) complexes
with 11 H -indeno[1,2- b ]quinoxalin-11-one
oxime, which to the best of our knowledge has never been employed
before in the synthesis of any noble metal complexes. Such oxime ligands
as 11 H -indeno[1,2- b ]quinoxalin-11-one
oxime in the presence of base (NEt 3 ) can adopt up to eight
different coordination modes, leading to Ni(II) and Co(II) complexes
with nuclearities ranging from 1 to 8. 49 , 50 11 H -Indeno[1,2- b ]quinoxalin-11-one oxime
and its derivatives look promising in terms of stabilizing the complexes
due to π–π stacking interactions and its coordinating
ability. Herein, we report the first examples of arene–Ru(II)
complexes with 11 H -indeno[1,2- b ]quinoxalin-11-one
oximes and tryptanthrin-6-oxime, a derivative of natural alkaloid
tryptanthrin. It was shown that such polycyclic oximes are capable
of acting as chelating ligands, forming mono- and binuclear coordination
compounds.
## Results and Discussion
Results and Discussion Synthesis of the Complexes The ligands
used in this
work and their abbreviations are summarized in Scheme 1 . Scheme 1 Structures of Ligands HL 1 –HL 4 Complexes 1 , 2 , and 4 were
prepared in high yield by the reaction between the commercially available
arene–ruthenium dimer [Ru( p -cym)Cl 2 ] 2 and the appropriate ligand in methanol/dimethylformamide
(DMF) mixture (complexes 1 , 4 ) or methanol
(complexes 2 , 3 ). It was shown that even
in the absence of a base, deprotonation of the oxime group occurs,
and the ligands ( HL 1 , HL 2 , and HL 4 ) are coordinated in anionic form. It is worth noting that
complex 3 could be obtained only in the presence of a
base. Complex 3 was prepared by the reaction between
[Ru( p -cym)Cl 2 ] 2 and HL 3 in methanol in the presence of KOH. Ligands HL 1 and HL 2 form mononuclear complexes of the typical piano-stool
type ( Scheme 2 ). Scheme 2 Synthesis of Complexes 1–2 Ligands HL 3 and HL 4 contain an additional nitrogen
atom; therefore,
they can form both mono- and binuclear complexes. Unexpectedly, the
ratio of the reagents did not affect the product composition: at a
ratio of Ru/ HL 3 2:1, ligand HL 3 forms a binuclear complex 3 of composition [Ru 2 ( p -cym) 2 (L 3 )Cl 3 ], whereas at a ratio of 1:1
instead of a mononuclear complex, the product contains the same complex 3 and the initial ligand ( Scheme 3 ). Scheme 3 Synthesis of Complex 3 Similarly, reaction between HL 4 and [Ru( p -cym)Cl 2 ] 2 is not
affected by reactants ratios. Regardless of the metal–ligand
ratio, only mononuclear complex of the composition [Ru( p -cym) (L 4 )Cl] was obtained ( Scheme 4 ). In this case, the formation of a dinuclear
complex ( via nitrogen donor atom in position 1 of
the tetracyclic system) is probably hindered by the repulsion between
the lone pair of the nitrogen atom in position 11 and bulky Ru(cym)
fragment. Scheme 4 Synthesis of Complex 4 All complexes are air-stable in the solid state; they
are sparingly
soluble in chloroform, acetonitrile, and DMSO and almost insoluble
in water and alcohols. The complexes were fully characterized by elemental
analysis, cyclic voltammetry, IR, NMR spectroscopy methods, and single-crystal
X-ray diffraction. Coordination of anionic forms of the ligands HL 1 –HL 4 with strong electron-withdrawing indeno[1,2- b ]quinoxaline
or tryptanthrin cores may be due to increased acidity of these ligands
compared to the oximes of aliphatic or aromatic ketones, leading to
increased concentration of their anionic forms. Thermochemical density
functional theory (DFT) calculations were carried out in order to
compare the thermodynamic stability of the complex 1 and its hypothetical
form with the neutral coordinated HL 1 ligand. Two reactions of formation of both of the complexes
were considered 1 2 Free-energy
and enthalpy changes were calculated at M062X 6-311+G(2d,p)/LANL2DZ
level of theory, and solvent (DMF) effects were taken into account
using SMD model. It was found that the formation of the complex with
the anionic form is more thermodynamically favorable (Δ G 1 = −94.9 kJ/mol; Δ G 2 = −16.3 kJ/mol; Δ H 1 = −97.6 kJ/mol; Δ H 2 = −10.8 kJ/mol). X-ray Crystal Structures Complexes 1–4 crystallize in a monoclinic crystal system having
a single formula
unit as an asymmetric unit. Phase purity of the obtained products
was confirmed by powder X-ray diffraction analysis (see the Supporting Information ). In mononuclear complexes 1 , 2 , and 4 , ruthenium coordinates
cymene molecule in a η 6 fashion, which is considered
to occupy three coordination sites of a quasi-octahedral arrangement.
The other three sites are occupied by a chlorine atom and two nitrogen
atoms of the deprotonated oximate ligands coordinated in a bidentate
fashion forming a five-membered chelate ring ( Figures 1 – 3 ). It should be noted that in most of the structurally characterized
arene–ruthenium complexes with heterocyclic oximes, the N,N-coordinated
ligands remain neutral 51 − 54 and so far only one example of deprotonated 2-pyridyl cyanoxime
was reported. 51 Figure 1 X-ray molecular structure
of complex 1 . Thermal ellipsoids
are drawn at a 50% probability level. Hydrogen atoms are omitted for
clarity. Selected bond lengths [Å]: Ru1–N1 2.101(1), Ru1–N2
2.147(1), Ru1–Cl1 2.4066(5), Ru1–C16 2.193(2), Ru1–C17
2.175(2), Ru1–C18 2.256(2), Ru1–C19 2.264(2), Ru1–C20
2.186(2), Ru1–C21 2.181(2). Figure 2 X-ray
molecular structure of complex 2 . Thermal ellipsoids
are drawn at a 50% probability level. Hydrogen atoms are omitted for
clarity. Selected bond lengths [Å]: Ru1–N1 2.079(1), Ru1–N2
2.159(1), Ru1–Cl1 2.4041(7), Ru1–C16 2.200(1), Ru1–C17
2.177(2), Ru1–C18 2.255(1), Ru1–C19 2.265(2), Ru1–C20
2.183(2), Ru1–C21 2.180(2). Figure 3 X-ray
molecular structure of complex 4 . Thermal ellipsoids
are drawn at a 50% probability level. Hydrogen atoms and DMF solvent
molecules are omitted for clarity. Selected bond lengths [Å]:
Ru1–N1 2.094(2), Ru1–N2 2.124(2), Ru1–Cl1 2.4031(6),
Ru1–C15 2.212(2), Ru1–C16 2.172(2), Ru1–C17 2.189(2),
Ru1–C18 2.260(2), Ru1–C19 2.249(2), Ru1–C20 2.171(2). The interatomic Ru–N distances involving
oxime and heterocyclic
nitrogen atoms are in the ranges of 2.08–2.10 and 2.12–2.16
Å and somewhat greater than the corresponding values typical
for oxime–ruthenium complexes (1.95–2.04 and 1.95–2.08
Å), probably due to bulkiness of the ligands. The interatomic
Ru–Cl distances of about 2.40 Å and Ru–C distances
in the range 2.17–2.26 Å are close to typically found
in arene–ruthenium complexes. All three complexes have chiral
metal centers, but crystallize in a centrosymmetric space group, and
thus, enantiomer resolution was not possible. Compound 3 is a binuclear complex that crystallizes
in a centrosymmetric monoclinic C 2/ c space group ( Figure 4 ). Arrangement of one of ruthenium atoms is similar to mononuclear
complexes described above—it consists of two nitrogen atoms
of deprotonated oxime ligand HL 3 , chloride ion and p -cymene molecule, interatomic
distances between ruthenium and donor atoms are also close to the
ones observed for mononuclear complexes. The second ruthenium atom
is achiral and coordinates one cymene molecule, two chloride ions,
and a nitrogen atom in position 2 of ligand HL 3 . Figure 4 X-ray molecular structure of 3 . Thermal ellipsoids
are drawn at a 50% probability level. Hydrogen atoms and MeOH solvent
molecules are omitted for clarity. Selected bond lengths [Å]:
Ru1–N1 2.096(2), Ru1–N2 2.124(2), Ru1–Cl1 2.387(2),
Ru1–C15 2.207(5), Ru1–C16 2.146(6), Ru1–C17 2.182(4),
Ru1–C18 2.238(3), Ru1–C19 2.230(3), Ru1–C20 2.189(4),
Ru1–N4 2.134(2), Ru1–Cl2 2.425(1), Ru1–Cl3 2.412(1),
Ru1–C25 2.203(4), Ru1–C26 2.179(5), Ru1–C27 2.153(5),
Ru1–C28 2.187(5), Ru1–C29 2.169(4), Ru1–C30 2.183(3). In complexes 1 and 2 the
heterocyclic
oxime ligands are involved in π–π stacking with
intermolecular distances 3.379(3) and 3.384(2) Å correspondingly
( Figures S1 and S2 ). In compound 4 , the molecules of ligand HL 4 cannot align in parallel planes due to the presence of lattice
DMF molecules. In this case, each of HL 4 molecules is involved in four CH···N short
contacts with interatomic H···N distances of 2.658
and 2.741 Å ( Figure S3 ). In
order to provide a quantum mechanical foundation to the experimental
observations, the analysis of the non-covalent interaction (NCI) isosurfaces
was performed both on monomers and dimers of compounds 1 , 2 , and 4 ( Figure S4 ). The intramolecular interactions that are mainly responsible
for the stabilization of the monomers (blue areas) involve hydrogen
atoms, which are involved in attractive interactions with the two
oxygen atoms, carbon atoms, and with the chlorine atom. Concerning
dimers, the main contribution to the stabilization of 1 2 and 2 2 is a wide π–π interaction between two ligands;
the case of 4 2 is rather different,
by involving four punctual but more attractive interactions between
hydrogen atoms of one ligand and nitrogen atoms of the other ligand
molecule ( Figure S4 ). Thermodynamic
preference of N , N -bidentate over N , O -bidentate coordination
mode of the ligand L 1 was confirmed
by DFT calculations. Both in the gas phase and DMF N,N-coordination
of the deprotonated ligand L 1 with the formation of a five-membered ring is about 19 kJ/mol more
favorable ( Figure S5 ). Two possible
orientations of the cymene ligand—one with
isopropyl group close to the oxime fragment and the other with the
opposite orientation—methyl group facing the oxime were evaluated
by DFT calculations ( Figure S6 ). It was
found that the first orientation is about 8 kJ/mol more stable than
the second one consistent with the X-ray crystal structures. Despite
the proximity of the bulky isopropyl group and the oxime fragment,
this form is more stable probably due to the repulsion of the isopropyl
group and the aromatic part of the HL1 ligand in the structure with
the opposite cymene orientation. Spectroscopic Characterization The IR spectra of free
neutral ligands display broad bands in the range 3200–3250
cm –1 due to OH stretching vibrations and bands in
the range 1640–1630 cm –1 due to C=N
stretching vibrations. Upon coordination OH stretching bands disappear,
whereas C=N stretching bands shift to 1625–1600 cm –1 , in accordance with the deprotonation of the ligands
and their coordination to the metal center in N , N ′-bidentate chelating fashion. The 1 H NMR spectra of complexes 1–4 recorded in DMSO- d 6 display all of the expected signals of the
coordinated p -cymene and N,N′-ligand. The
resonances of the N,N′-ligand atoms are shifted upfield with
respect to those of uncoordinated ligands, confirming its coordination
to the ruthenium(II) center. The chirality of ruthenium center in
the complexes induces significant changes to the NMR signals of the p -cymene moiety in complexes 1–4 . The 1 H NMR spectra of 1 , 2 , and 4 exhibit a doublet of doublets for the methyl groups in the
isopropyl moiety, and four doublets attributable to the protons of p -cymene ring in the range of 5.5–6.3 ppm, which
is typical of ruthenium–arene systems with an asymmetric ruthenium
center. 55 , 56 The 1 H NMR spectra of binuclear
complex 3 exhibit two doublets of doublets for the methyl
groups in the isopropyl moiety, and eight doublets attributable to
the p -cymene protons in the range of 5.3–6.2
ppm. There is no signal of the oxime proton in the spectra of all
complexes, which confirms the coordination of the ligand in the anionic
form. All complexes demonstrate resonances in the range typical of
related compounds and in accordance with the existence of only one
species in solution. UV–vis spectrum of complex 1 ( Figure S7 ) in acetonitrile demonstrates
a complex shape that
can be deconvoluted into five Gaussian bands ( Figure S8 ). In order to gain insight into the origin of the
absorption bands, time-dependent DFT calculations were carried out
( Figure S9 ). The main features of the singlet
excited states showing the highest values of oscillator strength ( f ) together with the experimental positions of deconvoluted
Gaussian bands are given in Table 1 . Because of the complexity of the transition nature
in terms of MOs elementary transitions, the natural transition orbital
(NTO) analysis was also carried out. As it can be seen from the transition
diagrams, all of the absorption bands are of mixed character and correspond
to both local and charge transfer excitations. Although the nature
of the longer absorption transitions (500–260 nm) is charge
transfer, calculations performed by employing long-range corrected
hybrid functionals ( viz . CAM-B3LYP and ω-B97X[D])
did not show a significant improvement in the match with the experimental
values with respect to the B3LYP functional; on the contrary, for
the short wavelength region transitions (200–230 nm), ω-B97X[D]
demonstrated a good performance. Table 1 TDA–DFT (B3LYP
6-311+G(2d,p)/LANLDZ
IEFPCM) Calculated Singlet Excited States and Experimental Absorption
Maxima in the UV–Vis Spectrum of Complex 1 a Values
calculated using ω-B97X[D]
6-311+G(2d,p)/LANLDZ IEFPCM method. Cyclic Voltammetry Studies To study the redox properties
of mononuclear and binuclear complexes 1 and 3 in solution, cyclic voltammograms were recorded at room temperature
and a scan rate of 0.1 V/s using a 0.1 M solution of Bu 4 NPF 6 in DMF ( Figures S10 and S11 ). The corresponding values E 1/2 of the
redox potentials are shown in Table 2 . In the positive region, an anodic peak was detected
at +1.30 and +1.37 V (versus Ag/AgCl) for complexes 1 and 3 , respectively. These irreversible processes apparently
correspond to the oxidation of Ru(II) to Ru(III). This is consistent
with the fact that the highest occupied molecular orbital in 1 is partially localized on the ruthenium atom (8,5%, Table S1 ). Sufficiently high oxidation potentials
are consistent with the π-acceptor properties of heterocyclic
oxime and p -cymene ligands. Ru-centered oxidation
in the region from +1.0 to +1.5 V (vs Ag/AgCl) was also found for
similar p -cymene complexes of Ru(II). 57 , 58 The irreversibility of this process is probably due to the instability
of the p -cymene–Ru(III) species and the removing
of the p -cymene fragment. This is evidenced by the
elongation of Ru–C bonds and a loss in energy during the transition
from Ru(II) complex to Ru(III) complex according to DFT calculations. Table 2 Redox Potentials a (V, vs Ag/AgCl)
for Complexes 1 , 3 , and HL 1 compound E p ox E p red 1 +1.30 –1.06, −2.06 3 +1.37 –0.85, −1.82 HL 1 b –1.80, −2.21 a Determined in 0.1 M Bu 4 NPF 6 in DMF at room
temperature and a scan rate of 0.1
V/s. b In CH 3 CN. A number of irreversible processes
were detected in the negative
region both for complexes 1 and 3 , probably
related to the reduction of the heterocyclic oxime ligand. This is
consistent with the composition of lowest unoccupied molecular orbital
in 1 , which mainly consists of the oxime ligand orbitals
(53%, Table S1 ). Similar irreversible reduction
processes shifted to a more cathodic region were also found in the
cyclic voltammogram of the starting HL 1 ligand in acetonitrile ( Figure S12 ). Catalytic Activity Studies We have tested the catalytic
activity of complexes for the selective hydrogenation of aryl ketones
using 2-propanol as both the reducing agent and solvent in the presence
of NaOH as the base. Reaction between isopropyl alcohol and acetophenone
was chosen as a model reaction ( Scheme 5 ). Scheme 5 Ru-Catalyzed Transfer Hydrogenation of Aryl Ketones Reduction of acetophenone did not go to completion
( Table 3 ), which can
be explained by
the reversibility of hydrogen transfer. Conversion versus time plots
for complexes 1–4 are shown in Figure 5 . Complex 1 demonstrated
the best catalytic activity, providing 93% conversion after 1 h. Other
complexes ( 2 – 4 ) gave ∼50%
conversions after 1–2 h, and nearly full conversion for catalysts 2 and 3 was achieved in 6 h. Figure 5 Conversion versus reaction
time for acetophenone transfer hydrogenation. Table 3 Transfer Hydrogenation of Acetophenone
Catalyzed by Complexes 1—4 bomplex yield, % a TON TOF, h –1 1 93 18 18 2 95 19 5 3 93 18 6 4 69 13 2 a Reactions were
carried out in 2-propanol(4.0
mL), in the presence of NaOH (0.1 mmol), acetophenone (1 mmol), and
catalyst (0.05 mmol) at 82 °C during 6 h [Ru]/substrate/NaOH
molar ratio = 1/20/2. Hydrogenated products were determined by gas
chromatography using phenetole as internal standard. TON = turnover number = mol of product/mol of pre-catalyst. TOF
= turnover frequency = mol of product/mol of pre-catalyst/time. Encouraged by the potential
of complex 1 , we were
interested to test this complex for transfer hydrogenation of substituted
aryl ketones ( Scheme 5 ), and complex 1 was found to exhibit good catalytic
activity and functional groups tolerance ( Table 4 ). Table 4 Transfer Hydrogenation
of Aryl Ketones
Catalyzed by Complex 1 a Hydrogenated products
were determined
by gas chromatography using phenetole as internal standard. Conversion versus time plots for
the five ketones ( Table 4 , entries 2–6) are shown
in Figure 6 . It was
shown that ketones with electron-donating groups reacted faster. It
might be due to the increase of the electron density on the carbon
atom of the carbonyl group, which favorably affects the coordination
of the carbonyl group to ruthenium(II) center. In turn, electron-withdrawing
substituents ( Table 4 , entries 6, 7) reduce the electron density on the carbonyl group
of the substrate, which makes coordination to the ruthenium(II) more
difficult, which results in the decrease of the reaction rate. Figure 6 Conversion
versus time plots (entries 2–6 in Table 4 ). High chemoselectivity of the reduction process was noted: nitro
groups ( Table 4 , entries
6, 7) remain unchanged under the hydrogenation conditions. For ketone
with the double C=C bond conjugated to the carbonyl group ( Table 4 , entry 8), only ketone
moiety undergoes transformation. Moreover, high yields can also be
achieved in case of 4-bromooacetophenone hydrogenation ( Table 4 , entry 5), with no evidence
of dehydrobromination or ring reduction. It is worth noting that a
heteroaromatic ketone can also be reduced ( Table 4 , entry 10). Pyridine moiety can potentially
bind to ruthenium center and inhibit the catalytic reaction; however,
2-acetylpyridine ( Table 4 , entry 10) was rapidly hydrogenated. Cytotoxicity Pancreatic
cancer is one of the most aggressive
and deadly types of cancer. The increasing resistance of the pancreatic
cancer to effective chemotherapy has become an urgent problem. 59 Therefore, the obtained complexes were screened
at different concentrations for their ability to affect the cell viability
of human adenocarcinoma cell line PANC-1 over noncancerous human retinal
pigment epithelial cell line ARPE-19. The cytotoxic activity of the
complexes was analyzed by cell viability MTT assay. As it is
shown in Figure 7 ,
complexes 1–3 demonstrate moderate cytotoxic effect
toward PANC-1 but practically no cytotoxic effect ARPE-19 cell lines.
Complex 2 at the concentrations of 30 and 90 μM
decreased cell viability for PANC-1 cell line to 95 and 70%, respectively.
Complex 4 at the concentrations 0.3, 30, and 90 μM
decreased cell viability for PANC-1 cell line to 55, 40, and 55%,
respectively. It can be concluded that complexes 2 and 4 have mild cytotoxic activity for cancer human cell lines.
Nevertheless, the cytotoxicity of the studied complexes is significantly
inferior to the cytotoxicity of drugs widely used in clinical practice
for the chemotherapeutical treatment of pancreatic adeonocarcinoma,
that is, fluorouracil (IC 50 3.85 μM) and gemcitabine
(IC 50 27 nM). 60 It is interesting
to note that at low concentrations of the complexes viability of the
cells increased (relative to control) despite the known cytotoxic
potential of arene–ruthenium core. This is probably due to
the JKN3-inhibitive activity of the oxime ligands discovered recently, 31 which limit the cell apoptosis process. Figure 7 Cell viability
MTT assay results for complexes 1–4 against PANC-1
(top) and ARPE-19 (bottom) cell lines (values are
shown as the mean ± SEM of four experiments, the concentrations
of the complexes on the horizontal axis are given in μM).
## Synthesis of the Complexes
Synthesis of the Complexes The ligands
used in this
work and their abbreviations are summarized in Scheme 1 . Scheme 1 Structures of Ligands HL 1 –HL 4 Complexes 1 , 2 , and 4 were
prepared in high yield by the reaction between the commercially available
arene–ruthenium dimer [Ru( p -cym)Cl 2 ] 2 and the appropriate ligand in methanol/dimethylformamide
(DMF) mixture (complexes 1 , 4 ) or methanol
(complexes 2 , 3 ). It was shown that even
in the absence of a base, deprotonation of the oxime group occurs,
and the ligands ( HL 1 , HL 2 , and HL 4 ) are coordinated in anionic form. It is worth noting that
complex 3 could be obtained only in the presence of a
base. Complex 3 was prepared by the reaction between
[Ru( p -cym)Cl 2 ] 2 and HL 3 in methanol in the presence of KOH. Ligands HL 1 and HL 2 form mononuclear complexes of the typical piano-stool
type ( Scheme 2 ). Scheme 2 Synthesis of Complexes 1–2 Ligands HL 3 and HL 4 contain an additional nitrogen
atom; therefore,
they can form both mono- and binuclear complexes. Unexpectedly, the
ratio of the reagents did not affect the product composition: at a
ratio of Ru/ HL 3 2:1, ligand HL 3 forms a binuclear complex 3 of composition [Ru 2 ( p -cym) 2 (L 3 )Cl 3 ], whereas at a ratio of 1:1
instead of a mononuclear complex, the product contains the same complex 3 and the initial ligand ( Scheme 3 ). Scheme 3 Synthesis of Complex 3 Similarly, reaction between HL 4 and [Ru( p -cym)Cl 2 ] 2 is not
affected by reactants ratios. Regardless of the metal–ligand
ratio, only mononuclear complex of the composition [Ru( p -cym) (L 4 )Cl] was obtained ( Scheme 4 ). In this case, the formation of a dinuclear
complex ( via nitrogen donor atom in position 1 of
the tetracyclic system) is probably hindered by the repulsion between
the lone pair of the nitrogen atom in position 11 and bulky Ru(cym)
fragment. Scheme 4 Synthesis of Complex 4 All complexes are air-stable in the solid state; they
are sparingly
soluble in chloroform, acetonitrile, and DMSO and almost insoluble
in water and alcohols. The complexes were fully characterized by elemental
analysis, cyclic voltammetry, IR, NMR spectroscopy methods, and single-crystal
X-ray diffraction. Coordination of anionic forms of the ligands HL 1 –HL 4 with strong electron-withdrawing indeno[1,2- b ]quinoxaline
or tryptanthrin cores may be due to increased acidity of these ligands
compared to the oximes of aliphatic or aromatic ketones, leading to
increased concentration of their anionic forms. Thermochemical density
functional theory (DFT) calculations were carried out in order to
compare the thermodynamic stability of the complex 1 and its hypothetical
form with the neutral coordinated HL 1 ligand. Two reactions of formation of both of the complexes
were considered 1 2 Free-energy
and enthalpy changes were calculated at M062X 6-311+G(2d,p)/LANL2DZ
level of theory, and solvent (DMF) effects were taken into account
using SMD model. It was found that the formation of the complex with
the anionic form is more thermodynamically favorable (Δ G 1 = −94.9 kJ/mol; Δ G 2 = −16.3 kJ/mol; Δ H 1 = −97.6 kJ/mol; Δ H 2 = −10.8 kJ/mol).
## X-ray Crystal Structures
X-ray Crystal Structures Complexes 1–4 crystallize in a monoclinic crystal system having
a single formula
unit as an asymmetric unit. Phase purity of the obtained products
was confirmed by powder X-ray diffraction analysis (see the Supporting Information ). In mononuclear complexes 1 , 2 , and 4 , ruthenium coordinates
cymene molecule in a η 6 fashion, which is considered
to occupy three coordination sites of a quasi-octahedral arrangement.
The other three sites are occupied by a chlorine atom and two nitrogen
atoms of the deprotonated oximate ligands coordinated in a bidentate
fashion forming a five-membered chelate ring ( Figures 1 – 3 ). It should be noted that in most of the structurally characterized
arene–ruthenium complexes with heterocyclic oximes, the N,N-coordinated
ligands remain neutral 51 − 54 and so far only one example of deprotonated 2-pyridyl cyanoxime
was reported. 51 Figure 1 X-ray molecular structure
of complex 1 . Thermal ellipsoids
are drawn at a 50% probability level. Hydrogen atoms are omitted for
clarity. Selected bond lengths [Å]: Ru1–N1 2.101(1), Ru1–N2
2.147(1), Ru1–Cl1 2.4066(5), Ru1–C16 2.193(2), Ru1–C17
2.175(2), Ru1–C18 2.256(2), Ru1–C19 2.264(2), Ru1–C20
2.186(2), Ru1–C21 2.181(2). Figure 2 X-ray
molecular structure of complex 2 . Thermal ellipsoids
are drawn at a 50% probability level. Hydrogen atoms are omitted for
clarity. Selected bond lengths [Å]: Ru1–N1 2.079(1), Ru1–N2
2.159(1), Ru1–Cl1 2.4041(7), Ru1–C16 2.200(1), Ru1–C17
2.177(2), Ru1–C18 2.255(1), Ru1–C19 2.265(2), Ru1–C20
2.183(2), Ru1–C21 2.180(2). Figure 3 X-ray
molecular structure of complex 4 . Thermal ellipsoids
are drawn at a 50% probability level. Hydrogen atoms and DMF solvent
molecules are omitted for clarity. Selected bond lengths [Å]:
Ru1–N1 2.094(2), Ru1–N2 2.124(2), Ru1–Cl1 2.4031(6),
Ru1–C15 2.212(2), Ru1–C16 2.172(2), Ru1–C17 2.189(2),
Ru1–C18 2.260(2), Ru1–C19 2.249(2), Ru1–C20 2.171(2). The interatomic Ru–N distances involving
oxime and heterocyclic
nitrogen atoms are in the ranges of 2.08–2.10 and 2.12–2.16
Å and somewhat greater than the corresponding values typical
for oxime–ruthenium complexes (1.95–2.04 and 1.95–2.08
Å), probably due to bulkiness of the ligands. The interatomic
Ru–Cl distances of about 2.40 Å and Ru–C distances
in the range 2.17–2.26 Å are close to typically found
in arene–ruthenium complexes. All three complexes have chiral
metal centers, but crystallize in a centrosymmetric space group, and
thus, enantiomer resolution was not possible. Compound 3 is a binuclear complex that crystallizes
in a centrosymmetric monoclinic C 2/ c space group ( Figure 4 ). Arrangement of one of ruthenium atoms is similar to mononuclear
complexes described above—it consists of two nitrogen atoms
of deprotonated oxime ligand HL 3 , chloride ion and p -cymene molecule, interatomic
distances between ruthenium and donor atoms are also close to the
ones observed for mononuclear complexes. The second ruthenium atom
is achiral and coordinates one cymene molecule, two chloride ions,
and a nitrogen atom in position 2 of ligand HL 3 . Figure 4 X-ray molecular structure of 3 . Thermal ellipsoids
are drawn at a 50% probability level. Hydrogen atoms and MeOH solvent
molecules are omitted for clarity. Selected bond lengths [Å]:
Ru1–N1 2.096(2), Ru1–N2 2.124(2), Ru1–Cl1 2.387(2),
Ru1–C15 2.207(5), Ru1–C16 2.146(6), Ru1–C17 2.182(4),
Ru1–C18 2.238(3), Ru1–C19 2.230(3), Ru1–C20 2.189(4),
Ru1–N4 2.134(2), Ru1–Cl2 2.425(1), Ru1–Cl3 2.412(1),
Ru1–C25 2.203(4), Ru1–C26 2.179(5), Ru1–C27 2.153(5),
Ru1–C28 2.187(5), Ru1–C29 2.169(4), Ru1–C30 2.183(3). In complexes 1 and 2 the
heterocyclic
oxime ligands are involved in π–π stacking with
intermolecular distances 3.379(3) and 3.384(2) Å correspondingly
( Figures S1 and S2 ). In compound 4 , the molecules of ligand HL 4 cannot align in parallel planes due to the presence of lattice
DMF molecules. In this case, each of HL 4 molecules is involved in four CH···N short
contacts with interatomic H···N distances of 2.658
and 2.741 Å ( Figure S3 ). In
order to provide a quantum mechanical foundation to the experimental
observations, the analysis of the non-covalent interaction (NCI) isosurfaces
was performed both on monomers and dimers of compounds 1 , 2 , and 4 ( Figure S4 ). The intramolecular interactions that are mainly responsible
for the stabilization of the monomers (blue areas) involve hydrogen
atoms, which are involved in attractive interactions with the two
oxygen atoms, carbon atoms, and with the chlorine atom. Concerning
dimers, the main contribution to the stabilization of 1 2 and 2 2 is a wide π–π interaction between two ligands;
the case of 4 2 is rather different,
by involving four punctual but more attractive interactions between
hydrogen atoms of one ligand and nitrogen atoms of the other ligand
molecule ( Figure S4 ). Thermodynamic
preference of N , N -bidentate over N , O -bidentate coordination
mode of the ligand L 1 was confirmed
by DFT calculations. Both in the gas phase and DMF N,N-coordination
of the deprotonated ligand L 1 with the formation of a five-membered ring is about 19 kJ/mol more
favorable ( Figure S5 ). Two possible
orientations of the cymene ligand—one with
isopropyl group close to the oxime fragment and the other with the
opposite orientation—methyl group facing the oxime were evaluated
by DFT calculations ( Figure S6 ). It was
found that the first orientation is about 8 kJ/mol more stable than
the second one consistent with the X-ray crystal structures. Despite
the proximity of the bulky isopropyl group and the oxime fragment,
this form is more stable probably due to the repulsion of the isopropyl
group and the aromatic part of the HL1 ligand in the structure with
the opposite cymene orientation.
## Spectroscopic Characterization
Spectroscopic Characterization The IR spectra of free
neutral ligands display broad bands in the range 3200–3250
cm –1 due to OH stretching vibrations and bands in
the range 1640–1630 cm –1 due to C=N
stretching vibrations. Upon coordination OH stretching bands disappear,
whereas C=N stretching bands shift to 1625–1600 cm –1 , in accordance with the deprotonation of the ligands
and their coordination to the metal center in N , N ′-bidentate chelating fashion. The 1 H NMR spectra of complexes 1–4 recorded in DMSO- d 6 display all of the expected signals of the
coordinated p -cymene and N,N′-ligand. The
resonances of the N,N′-ligand atoms are shifted upfield with
respect to those of uncoordinated ligands, confirming its coordination
to the ruthenium(II) center. The chirality of ruthenium center in
the complexes induces significant changes to the NMR signals of the p -cymene moiety in complexes 1–4 . The 1 H NMR spectra of 1 , 2 , and 4 exhibit a doublet of doublets for the methyl groups in the
isopropyl moiety, and four doublets attributable to the protons of p -cymene ring in the range of 5.5–6.3 ppm, which
is typical of ruthenium–arene systems with an asymmetric ruthenium
center. 55 , 56 The 1 H NMR spectra of binuclear
complex 3 exhibit two doublets of doublets for the methyl
groups in the isopropyl moiety, and eight doublets attributable to
the p -cymene protons in the range of 5.3–6.2
ppm. There is no signal of the oxime proton in the spectra of all
complexes, which confirms the coordination of the ligand in the anionic
form. All complexes demonstrate resonances in the range typical of
related compounds and in accordance with the existence of only one
species in solution. UV–vis spectrum of complex 1 ( Figure S7 ) in acetonitrile demonstrates
a complex shape that
can be deconvoluted into five Gaussian bands ( Figure S8 ). In order to gain insight into the origin of the
absorption bands, time-dependent DFT calculations were carried out
( Figure S9 ). The main features of the singlet
excited states showing the highest values of oscillator strength ( f ) together with the experimental positions of deconvoluted
Gaussian bands are given in Table 1 . Because of the complexity of the transition nature
in terms of MOs elementary transitions, the natural transition orbital
(NTO) analysis was also carried out. As it can be seen from the transition
diagrams, all of the absorption bands are of mixed character and correspond
to both local and charge transfer excitations. Although the nature
of the longer absorption transitions (500–260 nm) is charge
transfer, calculations performed by employing long-range corrected
hybrid functionals ( viz . CAM-B3LYP and ω-B97X[D])
did not show a significant improvement in the match with the experimental
values with respect to the B3LYP functional; on the contrary, for
the short wavelength region transitions (200–230 nm), ω-B97X[D]
demonstrated a good performance. Table 1 TDA–DFT (B3LYP
6-311+G(2d,p)/LANLDZ
IEFPCM) Calculated Singlet Excited States and Experimental Absorption
Maxima in the UV–Vis Spectrum of Complex 1 a Values
calculated using ω-B97X[D]
6-311+G(2d,p)/LANLDZ IEFPCM method.
## Cyclic Voltammetry Studies
Cyclic Voltammetry Studies To study the redox properties
of mononuclear and binuclear complexes 1 and 3 in solution, cyclic voltammograms were recorded at room temperature
and a scan rate of 0.1 V/s using a 0.1 M solution of Bu 4 NPF 6 in DMF ( Figures S10 and S11 ). The corresponding values E 1/2 of the
redox potentials are shown in Table 2 . In the positive region, an anodic peak was detected
at +1.30 and +1.37 V (versus Ag/AgCl) for complexes 1 and 3 , respectively. These irreversible processes apparently
correspond to the oxidation of Ru(II) to Ru(III). This is consistent
with the fact that the highest occupied molecular orbital in 1 is partially localized on the ruthenium atom (8,5%, Table S1 ). Sufficiently high oxidation potentials
are consistent with the π-acceptor properties of heterocyclic
oxime and p -cymene ligands. Ru-centered oxidation
in the region from +1.0 to +1.5 V (vs Ag/AgCl) was also found for
similar p -cymene complexes of Ru(II). 57 , 58 The irreversibility of this process is probably due to the instability
of the p -cymene–Ru(III) species and the removing
of the p -cymene fragment. This is evidenced by the
elongation of Ru–C bonds and a loss in energy during the transition
from Ru(II) complex to Ru(III) complex according to DFT calculations. Table 2 Redox Potentials a (V, vs Ag/AgCl)
for Complexes 1 , 3 , and HL 1 compound E p ox E p red 1 +1.30 –1.06, −2.06 3 +1.37 –0.85, −1.82 HL 1 b –1.80, −2.21 a Determined in 0.1 M Bu 4 NPF 6 in DMF at room
temperature and a scan rate of 0.1
V/s. b In CH 3 CN. A number of irreversible processes
were detected in the negative
region both for complexes 1 and 3 , probably
related to the reduction of the heterocyclic oxime ligand. This is
consistent with the composition of lowest unoccupied molecular orbital
in 1 , which mainly consists of the oxime ligand orbitals
(53%, Table S1 ). Similar irreversible reduction
processes shifted to a more cathodic region were also found in the
cyclic voltammogram of the starting HL 1 ligand in acetonitrile ( Figure S12 ).
## Catalytic Activity Studies
Catalytic Activity Studies We have tested the catalytic
activity of complexes for the selective hydrogenation of aryl ketones
using 2-propanol as both the reducing agent and solvent in the presence
of NaOH as the base. Reaction between isopropyl alcohol and acetophenone
was chosen as a model reaction ( Scheme 5 ). Scheme 5 Ru-Catalyzed Transfer Hydrogenation of Aryl Ketones Reduction of acetophenone did not go to completion
( Table 3 ), which can
be explained by
the reversibility of hydrogen transfer. Conversion versus time plots
for complexes 1–4 are shown in Figure 5 . Complex 1 demonstrated
the best catalytic activity, providing 93% conversion after 1 h. Other
complexes ( 2 – 4 ) gave ∼50%
conversions after 1–2 h, and nearly full conversion for catalysts 2 and 3 was achieved in 6 h. Figure 5 Conversion versus reaction
time for acetophenone transfer hydrogenation. Table 3 Transfer Hydrogenation of Acetophenone
Catalyzed by Complexes 1—4 bomplex yield, % a TON TOF, h –1 1 93 18 18 2 95 19 5 3 93 18 6 4 69 13 2 a Reactions were
carried out in 2-propanol(4.0
mL), in the presence of NaOH (0.1 mmol), acetophenone (1 mmol), and
catalyst (0.05 mmol) at 82 °C during 6 h [Ru]/substrate/NaOH
molar ratio = 1/20/2. Hydrogenated products were determined by gas
chromatography using phenetole as internal standard. TON = turnover number = mol of product/mol of pre-catalyst. TOF
= turnover frequency = mol of product/mol of pre-catalyst/time. Encouraged by the potential
of complex 1 , we were
interested to test this complex for transfer hydrogenation of substituted
aryl ketones ( Scheme 5 ), and complex 1 was found to exhibit good catalytic
activity and functional groups tolerance ( Table 4 ). Table 4 Transfer Hydrogenation
of Aryl Ketones
Catalyzed by Complex 1 a Hydrogenated products
were determined
by gas chromatography using phenetole as internal standard. Conversion versus time plots for
the five ketones ( Table 4 , entries 2–6) are shown
in Figure 6 . It was
shown that ketones with electron-donating groups reacted faster. It
might be due to the increase of the electron density on the carbon
atom of the carbonyl group, which favorably affects the coordination
of the carbonyl group to ruthenium(II) center. In turn, electron-withdrawing
substituents ( Table 4 , entries 6, 7) reduce the electron density on the carbonyl group
of the substrate, which makes coordination to the ruthenium(II) more
difficult, which results in the decrease of the reaction rate. Figure 6 Conversion
versus time plots (entries 2–6 in Table 4 ). High chemoselectivity of the reduction process was noted: nitro
groups ( Table 4 , entries
6, 7) remain unchanged under the hydrogenation conditions. For ketone
with the double C=C bond conjugated to the carbonyl group ( Table 4 , entry 8), only ketone
moiety undergoes transformation. Moreover, high yields can also be
achieved in case of 4-bromooacetophenone hydrogenation ( Table 4 , entry 5), with no evidence
of dehydrobromination or ring reduction. It is worth noting that a
heteroaromatic ketone can also be reduced ( Table 4 , entry 10). Pyridine moiety can potentially
bind to ruthenium center and inhibit the catalytic reaction; however,
2-acetylpyridine ( Table 4 , entry 10) was rapidly hydrogenated.
## Cytotoxicity
Cytotoxicity Pancreatic
cancer is one of the most aggressive
and deadly types of cancer. The increasing resistance of the pancreatic
cancer to effective chemotherapy has become an urgent problem. 59 Therefore, the obtained complexes were screened
at different concentrations for their ability to affect the cell viability
of human adenocarcinoma cell line PANC-1 over noncancerous human retinal
pigment epithelial cell line ARPE-19. The cytotoxic activity of the
complexes was analyzed by cell viability MTT assay. As it is
shown in Figure 7 ,
complexes 1–3 demonstrate moderate cytotoxic effect
toward PANC-1 but practically no cytotoxic effect ARPE-19 cell lines.
Complex 2 at the concentrations of 30 and 90 μM
decreased cell viability for PANC-1 cell line to 95 and 70%, respectively.
Complex 4 at the concentrations 0.3, 30, and 90 μM
decreased cell viability for PANC-1 cell line to 55, 40, and 55%,
respectively. It can be concluded that complexes 2 and 4 have mild cytotoxic activity for cancer human cell lines.
Nevertheless, the cytotoxicity of the studied complexes is significantly
inferior to the cytotoxicity of drugs widely used in clinical practice
for the chemotherapeutical treatment of pancreatic adeonocarcinoma,
that is, fluorouracil (IC 50 3.85 μM) and gemcitabine
(IC 50 27 nM). 60 It is interesting
to note that at low concentrations of the complexes viability of the
cells increased (relative to control) despite the known cytotoxic
potential of arene–ruthenium core. This is probably due to
the JKN3-inhibitive activity of the oxime ligands discovered recently, 31 which limit the cell apoptosis process. Figure 7 Cell viability
MTT assay results for complexes 1–4 against PANC-1
(top) and ARPE-19 (bottom) cell lines (values are
shown as the mean ± SEM of four experiments, the concentrations
of the complexes on the horizontal axis are given in μM).
## Conclusions
Conclusions Ruthenium(II)–arene
complexes containing 11 H -indeno[1,2- b ]quinoxalin-11-one derivatives and
tryptanthrin-6-oxime were prepared and their catalytic, biological,
and electrochemical properties were evaluated. The crystal structures
of all complexes display a typical piano-stool geometry with ligands
N,N′-coordinated to the ruthenium in each case. Our research
also shows that arene–ruthenium(II) complexes
with 11 H -indeno[1,2- b ]quinoxalin-11-one
derivatives and tryptanthrin-6-oxime are effective catalysts for the
transfer hydrogenation reaction. These complexes tolerate a range
of functional groups and catalyze the reaction, giving target alcohols
in high yields. Ruthenium complexes with tryptanthrin-6-oxime and
6 H -indeno[1,2- b ]pyrido[3,2- e ]pyrazin-6-one oxime demonstrated mild cytotoxic activity
for human adenocarcinoma cell line PANC-1.
## Experimental Section
Experimental Section Materials
and Methods The dimer [Ru( p -cym)Cl 2 ] 2 was purchased from Alfa Aesar. The
ligands 11 H -indeno[1,2- b ]quinoxalin-11-one
oxime ( HL 1 ), 6-(hydroxyimino)indolo[2,1- b ]quinazolin-12(6 H )-one (tryptanthrin-6-oxime, HL 2 ), 10 H -indeno[1,2- b ]pyrido[3,4- e ]pyrazin-10-one oxime ( HL 3 ), and 6 H -indeno[1,2- b ]pyrido[3,2- e ]pyrazin-6-oneoxime ( HL 4 ) were prepared as previously described. 36 All other materials were obtained from commercial
sources and were used as received. IR spectra were recorded
on an Agilent Cary 630 FTIR spectrometer quipped with a diamond attenuated
total reflectance tool from 700 to 3500 cm –1 . NMR
spectroscopic data were recorded with a Brucker AVANCE III 400 spectrometer
(400.13 MHz for 1 H and 100.61 MHz for 13 C) and
were referenced to residual solvent signal. Chromato-mass spectrometric
analysis was carried out using Agilent
7890A gas chromatograph with Agilient 5975C mass-selective detector
with quadrupole mass-analyzer (electron impact ionization energy 70
eV). The injector temperature was maintained at 300 °C, and the
injection volume was 1 μL (split 40:1). The instrument was equipped
with a HP-5 ms capillary column of 30 m length, 0.25 mm i.d., and
0.25 μm film thickness. The carrier gas was helium at a constant
flow rate of 1 mL/min. The GC oven program started at 79 °C (1.0
min hold) ramped up to 300 °C (heating rate 13 °C/min) for
10 min, total chromatogram time was 28 min. Transfer line temperature
was 300 °C, MS Source—230 °C and MS Quadrouple—150
°C. The electron energy was 70 eV. From 0 to 4 min, the MS was
switched off (solvent delay). Data analysis and instrument control
was carried out with MSD 5975C software. Cyclic Voltammetry Cyclic voltammograms were recorded
with a 797 VA Computrace system (Metrohm, Switzerland). All measurements
were carried out at room temperature with a conventional three-electrode
configuration consisting of glassy carbon working electrode, platinum
auxiliary electrode, and Ag/AgCl/KCl reference electrode. The solvent
(DMF or CH 3 CN) was deoxygenated before use. The solution
of tetra- n -butylammonium hexafluorophosphate Bu 4 NPF 6 (0.1 M) was used as a supporting electrolyte.
The concentrations of the compounds were 10 –3 M. X-ray Crystallography Single-crystal X-ray diffraction
(XRD) data for the compounds were collected by a Bruker Apex DUO diffractometer
using the graphite-monochromated Mo Kα radiation (λ =
0.71073 Å). Absorption corrections were applied with the use
of the SADABS program. 61 The crystal structures
were solved and refined by means of the SHELXT 62 and SHELXL 63 programs using
OLEX2 GUI. 64 Atomic thermal displacement
parameters for nonhydrogen atoms except for some solvate molecules
were refined anisotropically. The positions of H atoms were calculated
corresponding to their geometrical conditions and refined using the
riding model. In 3 , O atoms of one of solvate methanol
molecules was disordered over three positions with restrained C–O
distances (DFIX) and occupancy of 0.33. H atoms of hydroxyl group
of methanol molecules were not located but included in the formula
of 3 . The crystallographic data and details of the structure
refinements are summarized in Table 5 . Crystallographic data for the structures 1–4 have been deposited with the Cambridge Crystallographic Data Centre
(CCDC) as Supporting Information nos. 1974048–1974051.
Copies of the data can be obtained free of charge on application to
CCDC ( http://www.ccdc.cam.ac.uk/data_request/cif ). Table 5 Crystallographic Data of the Complexes 1–4 compound 1 2 3 4 empirical formula C 25 H 22 ClN 3 ORu C 25 H 22 ClN 3 O 2 Ru C 35.5 H 41 Cl 3 N 4 O 2.5 Ru 2 C 25.5 H 24.5 ClN 4.5 O 1.5 Ru formula weight 516.97 532.97 872.23 554.51 temperature/K 200(2) 298(2) 298(2) 150(2) crystal system monoclinic monoclinic monoclinic monoclinic space group P 2 1 / n P 2 1 / n C 2/ c P 2 1 / c a /Å 15.3365(10) 15.601(4) 34.0106(13) 18.414(2) b /Å 8.0892(6) 8.0342(18) 12.5712(5) 16.071(2) c /Å 17.0781(14) 17.108(4) 20.0181(8) 7.6248(11) β/deg 93.968(2) 93.210(7) 123.3950(10) 97.453(4) volume/Å 3 2113.6(3) 2140.9(8) 7145.7(5) 2237.4(5) Z 4 4 8 4 ρ calc /g/cm 3 1.625 1.654 1.619 1.646 μ/mm –1 0.891 0.886 1.109 0.852 F(000) 1048.0 1080.0 3516.0 1128.0 crystal size/mm 3 0.15 × 0.1 × 0.08 0.3 × 0.25 × 0.25 0.3 × 0.2 × 0.1 0.33 × 0.17 × 0.05 2Θ range for data collection/deg 3.452 to 57.452 3.438 to 57.468 3.544 to 51.466 3.376 to 57.46 index ranges –20 ≤ h ≤ 13, –10 ≤ k ≤ 10, –23 ≤ l ≤ 23 –21 ≤ h ≤ 21, –10 ≤ k ≤ 10, –23 ≤ l ≤ 23 –38 ≤ h ≤ 41, –10 ≤ k ≤ 15, –24 ≤ l ≤ 23 –23 ≤ h ≤ 24, –21 ≤ k ≤ 21, –7 ≤ l ≤ 10 reflections
collected 28,954 31,935 26,579 15,991 independent
reflections 5460 [ R int = 0.0304, R sigma = 0.0221] 5550 [ R int = 0.0243, R sigma = 0.0142] 6810 [ R int = 0.0351, R sigma = 0.0354] 5678 [ R int = 0.0336, R sigma = 0.0442] restraints/parameters 0/283 0/292 4/426 12/330 goodness-of-fit on F 2 1.026 1.069 1.020 1.023 final R indexes [ I >≥ 2σ ( I )] R 1 = 0.0224, wR 2 = 0.0540 R 1 = 0.0190, wR 2 = 0.0508 R 1 = 0.0313, wR 2 = 0.0724 R 1 = 0.0296, wR 2 = 0.0597 final R indexes [all data] R 1 = 0.0273, wR 2 = 0.0565 R 1 = 0.0211, wR 2 = 0.0525 R 1 = 0.0447, wR 2 = 0.0788 R 1 = 0.0424, wR 2 = 0.0639 largest diff. peak/hole/e Å –3 0.58/–0.34 0.36/–0.43 0.78/–0.40 0.51/–0.78 Catalytic Activity Determination A typical transfer
hydrogenation reaction was carried out under air as follows: to 0.05
mmol of catalyst precursor contained in the reaction flask were added
isopropyl alcohol (4 mL), NaOH (0.2 mmol) and acetophenone (1 mmol),
in that order. The reaction mixture was stirred for 6 h at 82 °C.
After that, reaction mass was analyzed by GC and GC–MS. The
performed blank experiments confirmed that no products of reaction
were obtained unless the catalyst and NaOH were added. Cytotoxicity
Determination PANC-1 (pancreatic adenocarcinoma)
were obtained from Russian Cell Culture Collection (Institute of Cytology
RAS). ARPE-19 (ATCC CRL-2302 retinal pigment epithelial) cells were
obtained from the American Type Culture Collection (ATCC) (Manassas,
VA). PANC-1 and ARPE-19 cells were cultured in DMEM-F12 medium supplemented
with 10% fetal bovine serum, 100 units/mL penicillin, and 100 μg/mL
streptomycin, at 37 °C in a humidified atmosphere containing
95% air and 5% CO 2 . The cytotoxicity of tested compounds
was studied using 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium
bromide (MTT) reduction assay as described previously. 65 MTT-formazan crystals formed by metabolically
active cells were dissolved in dimethyl sulfoxide, and absorbance
was measured at 540 and 690 nm in Varioskan LUX Multimode Microplate
Reader (Thermo Scientific, USA). Values measured at 540 nm were subtracted
for background values at 690 nm, and the data were shown as a percent
of control untreated samples. Computational Chemistry
Details The calculations were
performed using Gaussian 09 package. 66 Experimental
X-ray structures of complex 1 was used as a starting
point for DFT geometry optimizations. Singlet state geometry optimizations
were carried out at the DFT level of theory employing the three-parameter
hybrid B3LYP functional 67 − 70 and 6-311+G(2d,p) basis set 71 − 74 for the first and second-row
atoms, while LanL2DZ 75 , 76 was used for the ruthenium atoms.
Solvation effects were taken into account using the IEFPCM model 77 and acetonitrile as solvent. Frequency calculations
were performed for the optimized geometries in order to establish
the nature of the stationary points. Lack of imaginary vibration modes
for the optimized structures indicate that the stationary points found
corresponded to minima on the potential energy surface. Time-dependent
DFT calculations with Tamm–Dancoff approximation 78 were carried out using the same basis sets and
B3LYP, 67 − 70 CAM-B3LYP, 79 and ω-B97X[D] 80 functionals. The nature of electronic transitions
was analyzed using the NTOs approach. 81 The energies of the coordination isomers of complex 1 were compared after geometry optimization and calculation of vibrational
frequencies using M062X 82 functional and
6-311+G(2d,p)/LanL2DZ 75 , 76 basis sets; solvation effects
in dimethylformamide were taken into account using the SMD model. 83 NCI Analysis by means of the Reduced Density
Gradient 84 − 88 was Performed on the Density of the Optimized Structures Using a
Homemade Code Synthesis and Characterization [Ru( p -cym) (L 1 )Cl] ( 1 ) HL 1 (24.7 mg, 0.1
mmol) was dissolved in DMF (1.5 mL), [Ru( p -cym)Cl 2 ] 2 (30.6 mg, 0.05 mmol) was dissolved in MeOH (1.5
mL), and the resulting solution was added to the initial one. After
24 h, red crystals formed were filtered off and washed twice with
MeOH. Yield 43 mg (83%). 1 H NMR (400 MHz, DMSO- d 6 ): δ 0.99 (d, 3H, Me- i Pr, J = 8 Hz), 1.05 (d, 3H, Me- i Pr, J = 8 Hz), 2.15 (s, 3H, Me-Ar), 2.64 (m, 1H,
CH-Ar), 2.73 (s, Me- i Pr), 5.76 (d, 1H, CH ( p -cym), J = 4 Hz), 5.99 (d, 1H, CH ( p -cym), J = 4 Hz), 6.03 (d, 1H, CH ( p -cym), J = 8 Hz), 6.08 (d, 1H, CH ( p -cym), J = 8 Hz), 7.53 (t, 1H, H2-L 1 , J = 8 Hz), 7.65 (t, 1H, H3-L 1 , J = 8 Hz), 7.93 (t, 1H, H1-L 1 , J = 4 Hz), 8.02 (t, 1H, H4-L 1 , J = 8 Hz), 8.08 (d, 1H, H9-L 1 , J = 8 Hz),
8.18 (d, 1H, H8-L 1 , J = 8 Hz), 8.33 (d,
1H, H10-L 1 , J = 2 Hz), 8.40 (d, 1H, H7-L 1 , J = 8 Hz) ppm. 13 C NMR (100
MHz, CDCl 3 ): δ 22.1 (Me-Ar), 22.5 (Me- i Pr), 24.1 (Me- i Pr), 31.2 (CH- i Pr),
80.9 ( p -cym), 81.3 ( p -cym), 83.7
( p -cym), 84.1 ( p -cym), 89.5 ( p -cym), 103.7 ( p -cym), 123.0 (L 1 ), 123.4 (L 1 ), 124.1 (L 1 ), 126.3 (L 1 ) 128.0 (L 1 ), 128.4 (L 1 ), 128.9 (L 1 ), 130.3 (L 1 ), 131.3 (L 1 ), 132.0 (L 1 ), 134.4 (L 1 ), 140.2 (L 1 ), 141.6 (L 1 ), 148.0 (L 1 ), 157.4 (L 1 ) ppm. IR: 3075 (w),
3059 (w), 3030 (w), 2963 (w), 2867 (w), 1604 (w), 1596 (m), 1497 (s),
1468 (s), 1447 (m), 1420 (m), 1383 (m), 1356 (m), 1327 (m), 1303 (m),
1244 (s), 1212 (m), 1199 (m), 1164 (m), 1140 (m), 1124 (s), 1092 (m),
1068 (m), 1052 (m), 1034 (m), 1012 (m), 970 (m), 946 (m), 871 (s),
794 (s), 765 (s), 749 (s), 725 (s). Found, %: C, 58.40; H, 4.41; N,
8.32. C 25 H 22 N 3 OClRu. Calcd, %: C,
58.08; H, 4.29; N, 8.13. [Ru( p -cym) (L 2 )Cl] ( 2 ) HL 2 (53 mg, 0.2 mmol)
was dissolved in MeOH (1.5 mL). [Ru( p -cym)Cl 2 ] 2 (61.2 mg, 0.1 mmol) was dissolved in MeOH (1.5
mL), and the resulting solution was added to the initial one. After
24 h, red crystals formed were filtered off and washed twice with
MeOH. Yield 80 mg (75%). 1 H NMR (400 MHz, CDCl 3 ): δ 1.08 (d, 3H, Me- i Pr, J = 8 Hz), 1.11 (d, 3H, Me- i Pr, J = 8 Hz), 2.16 (s, 3H, Me-Ar), 2.70 (m, 1H, CH-Ar), 5.74 (d, 1H,
CH ( p -cym), J = 8 Hz), 5.925 (d,
1H, CH ( p -cym), J = 4 Hz), 5.98
(d, 1H, CH ( p -cym), J = 8 Hz), 6.03
(d, 1H, CH ( p -cym), J = 8 Hz), 7.45
(t, 1H, H-8, J = 8 Hz), 7.52 (td, 1H, H-9, J = 8 Hz, J = 1.2 Hz), 7.65 (td, 1H, H-2, J = 8 Hz, J = 2.4 Hz), 7.98 (d, 1H, H-4, J = 8 Hz), 8.02 (t, 1H, H-3, J = 4H), 8.03
(dd, 1H, H-7, J = 8 Hz, J = 0.8
Hz), 8.37 (d, 1H, H-1, J = 4 Hz), 8.39 (d, 1H, H-10, J = 4 Hz) ppm. 13 C NMR (100 MHz, CDCl 3 ): δ 19.2 (Me-Ar), 22.1 (Me- i Pr), 22.6 (Me- i Pr), 31.2 (CH- i Pr), 83.1 ( p -cym), 83.4 ( p -cym), 83.9 ( p -cym),
88.6 ( p -cym), 102.5 ( p -cym), 103.7
( p -cym), 116.9 (L 2 ), 117.7 (L 2 ), 120.2 (L 2 ), 121.7 (L 2 ) 122.9 (L 2 ), 125.8 (L 2 ), 127.4 (L 2 ), 128.1 (L 2 ), 128.2 (L 2 ), 128.9 (L 2 ), 136.2 (L 2 ), 137.9 (L 2 ) 146.3 (L 2 ), 157.0 (L 2 ), 157.6 (L 2 ) ppm. IR: 3083 (w), 3062 (w), 3033 (w), 2971
(w), 2873 (w), 1692 (s), 1625 (m), 1593 (m), 1561 (m), 1540 (w), 1495
(s), 1460 (s), 1441 (s), 1404 (m), 1356 (m), 1330 (m), 1316 (m), 1303
(m), 1242 (s), 1191 (m), 1159 (m), 1146 (m), 1124 (m), 1111 (m), 1095
(m), 1055 (m), 1039 (m), 1026 (m), 1007 (m), 940 (m), 868 (m), 807
(s), 794 (m), 759 (s), 743 (s), 727 (m), 709 (m), 687 (s), 674 (m).
Found, %: C, 56.58; H, 4.22; N, 7.95. C 25 H 22 N 3 O 2 ClRu. Calcd, %: C, 56.34; H, 4.16; N, 7.88. [Ru 2 ( p -cym) 2 (L 3 )Cl 2 ]·1.5MeOH ( 3 ) HL 3 (24.8 mg, 0.1 mmol) was suspended in MeOH
(5 mL) and 1 mL of 0.1 M solution KOH in MeOH was added. Reaction
mixture was stirred for 1 h to afford pale yellow precipitate of potassium
salt. [Ru( p -cym)Cl 2 ] 2 (30.6
mg, 0.1 mmol) was dissolved in MeOH (2 mL), and solution was added
to the initial suspension. The resulting red crystals were filtered,
washed with MeOH, and dried at room temperature. Yield 47 mg (55%). 1 H NMR (400 MHz, CDCl 3 ): δ 1.08 (dd, 6H, Me- i Pr (assymm. p -cym), J 1 = 24 Hz, J 2 = 4 Hz), 1.41
(dd, 6H, Me- i Pr (symm. p -cym), J 1 = 16 Hz, J 2 =
8 Hz), 2.20 (s, 3H, Me-Ar (assymm. p -cym)), 2.34
(s, 3H, Me-Ar (symm. p -cym)), 2.72 (m, 1H, CH-Ar
(assymm. p -cym)), 3.10 (m, 1H, CH-Ar (symm. p -cym)), 5.30 (d, 1H, CH (symm. p -cym), J = 4 Hz), 5.40 (d, 1H, CH (symm. p -cym), J = 8 Hz), 5.55 (d, 1H, CH (symm. p -cym), J = 4 Hz), 5.58 (d, 1H, CH (symm. p -cym), J = 8 Hz), 5.79 (d, 1H, CH (assymm. p -cym), J = 8 Hz), 5.96 (d, 1H, CH (assymm. p -cym),
8 Hz), 6.02 (d, 1H, CH (assymm. p -cym), 4 Hz), 6.19
(d, 1H, CH (assymm. p -cym), 8 Hz), 7.51 (t, 1H, H8-L3, J = 8 Hz), 7.67 (t, 1H, H7-L3, J = 8 Hz),
8.10 (d, 1H, H4-L3, J = 4 Hz), 8.23 (t, 2H, H9-L3, J = 8 Hz), 9.23 (d, 1H, H3-L3, J = 8 Hz),
10.10 (s, 1H, H1-L3) ppm. 13 C NMR (100 MHz, DMSO- d 6 ): δ 18.3 (Me-Ar), 18.9 (Me-Ar), 22.9
(Me- i Pr), 22.2 (Me- i Pr), 22.3 (Me- i Pr), 30.4 (CH- i Pr) 31.1 (CH- i Pr), 83.3 ( p -cym), 84.1 ( p -cym),
85.2 ( p -cym), 85.9 ( p -cym), 86.8
( p -cym), 90.0 ( p -cym), 100.5 ( p -cym), 103.3 ( p -cym), 103.7 (L 3 ), 106.8 (L 3 ), 121.9 (L 3 ), 123.2 (L 3 ), 124.9 (L 3 ), 128.3 (L 3 ), 132.5 (L 3 ), 134.0 (L 3 ), 144.4 (L 3 ), 146.7 (L 3 ), 146.9 (L 3 ), 148.8 (L 3 ), 151.8 (L 3 ), 157.9 (L 3 ) ppm. IR: 3051 (w), 2955 (m), 2926 (w), 2873
(w), 1604 (m), 1593 (w), 1561 (w), 1497 (s), 1473 (s), 1412 (s), 1394
(s), 1359 (m), 1316 (s), 1250 (s), 1204 (m), 1154 (s), 1132 (m), 1116
(m), 1068 (m), 1028 (m), 978 (m), 874 (m), 826 (s), 802 (s), 773 (s),
757 (s), 730 (s). Found, %: C, 49.11; H, 4.54; N, 6.43. C 35.5 H 41 Cl 3 N 4 O 2.5 Ru 2 . Calcd, %: C, 48.90; H, 4.74; N, 6.42. [Ru( p -cym) 2 (L 4 )Cl 2 ]·0.5DMF ( 4 ) HL 4 (24.8 mg, 0.1
mmol) was suspended in DMF (2.5
mL). [Ru( p -cym)Cl 2 ] 2 (30.6
mg, 0.05 mmol) and was dissolved in MeOH (2.5 mL), and the resulting
solution was added to the initial suspension. The mixture was stirred
until the ligand was completely dissolved. The resulting red precipitate
was filtered, washed with MeOH, and dried at room temperature. Yield
42 mg (81%). 1 H NMR (400 MHz, DMSO- d 6 ): δ 1.005 (d, 3H, Me- i Pr, J = 4 Hz), 1.075 (d, 3H, Me- i Pr, J = 4 Hz), 2.15 (s, 3H, Me-Ar), 2.68 (m, 1H, CH-Ar), 5.805
(d, 1H, CH ( p -cym), J = 4 Hz), 6.03
(d, 1H, CH ( p -cym), J = 8 Hz), 6.045
(d, 1H, CH ( p -cym), J = 4 Hz), 6.105
(d, 1H, CH ( p -cym), J = 4 Hz), 7.57
(t, 1H, H8-L 3 , J = 8 Hz), 7.70 (t, 1H,
H3-L 3 , J = 8 Hz), 8.015 (dd, 1H, H9-L 3 , J = 12 Hz, J = 4 Hz),
8.09 (d, 1H, H7-L 3 , J = 8 Hz), 8.26 (d,
1H, H10-L 3 , J = 8 Hz), 8.795 (dd, 1H,
H4-L 3 , J = 10 Hz, J =
1.6 Hz), 9.195 (dd, 1H, H2-L 3 , J = 4 Hz, J = 1.6 Hz) ppm. 13 C NMR (100 MHz, CDCl 3 ): δ 21.9 (Me-Ar), 24.1 (Me- i Pr), 30.9 (Me- i Pr), 31.2 (CH- i Pr), 83.6 ( p -cym), 83.9 ( p -cym), 85.9 ( p -cym),
87.0 ( p -cym), 89.3 ( p -cym), 100.6
( p -cym), 122.8 (L 4 ), 124.2 (L 4 ), 124.6 (L 4 ), 124.6 (L 4 ) 126.0 (L 4 ), 126.2 (L 4 ), 127.3 (L 4 ), 128.9 (L 4 ), 132.9 (L 4 ), 133.9 (L 4 ), 136.3 (L 4 ), 138.7 (L 4 ), 139.7 (L 4 ), 156.4 (L 4 ) ppm. IR: 3056 (w), 2971 (w), 2923 (w), 2873 (w), 1679 (s), 1620
(m), 1604 (m), 1569 (m), 1511 (m), 1495 (s), 1476 (s), 1460 (s), 1417
(s), 1380 (m), 1359 (m), 1308 (s), 1282 (m), 1242 (s), 1204 (m), 1175
(m), 1154 (m), 1149 (m), 1111 (m), 1076 (m), 1036 (m), 1007 (m), 996
(m), 959 (m), 911 (m), 890 (m), 876 (m), 820 (m), 797 (m), 775 (s),
762 (s), 738 (m), 690 (m). Found, %: C, 55.03; H, 4.48; N, 11.53.
C 25.5 H 24.5 ClN 4.5 O 1.5 Ru.
Calcd, %: C, 55.23; H, 4.45; N, 11.37.
## Materials
and Methods
Materials
and Methods The dimer [Ru( p -cym)Cl 2 ] 2 was purchased from Alfa Aesar. The
ligands 11 H -indeno[1,2- b ]quinoxalin-11-one
oxime ( HL 1 ), 6-(hydroxyimino)indolo[2,1- b ]quinazolin-12(6 H )-one (tryptanthrin-6-oxime, HL 2 ), 10 H -indeno[1,2- b ]pyrido[3,4- e ]pyrazin-10-one oxime ( HL 3 ), and 6 H -indeno[1,2- b ]pyrido[3,2- e ]pyrazin-6-oneoxime ( HL 4 ) were prepared as previously described. 36 All other materials were obtained from commercial
sources and were used as received. IR spectra were recorded
on an Agilent Cary 630 FTIR spectrometer quipped with a diamond attenuated
total reflectance tool from 700 to 3500 cm –1 . NMR
spectroscopic data were recorded with a Brucker AVANCE III 400 spectrometer
(400.13 MHz for 1 H and 100.61 MHz for 13 C) and
were referenced to residual solvent signal. Chromato-mass spectrometric
analysis was carried out using Agilent
7890A gas chromatograph with Agilient 5975C mass-selective detector
with quadrupole mass-analyzer (electron impact ionization energy 70
eV). The injector temperature was maintained at 300 °C, and the
injection volume was 1 μL (split 40:1). The instrument was equipped
with a HP-5 ms capillary column of 30 m length, 0.25 mm i.d., and
0.25 μm film thickness. The carrier gas was helium at a constant
flow rate of 1 mL/min. The GC oven program started at 79 °C (1.0
min hold) ramped up to 300 °C (heating rate 13 °C/min) for
10 min, total chromatogram time was 28 min. Transfer line temperature
was 300 °C, MS Source—230 °C and MS Quadrouple—150
°C. The electron energy was 70 eV. From 0 to 4 min, the MS was
switched off (solvent delay). Data analysis and instrument control
was carried out with MSD 5975C software.
## Cyclic Voltammetry
Cyclic Voltammetry Cyclic voltammograms were recorded
with a 797 VA Computrace system (Metrohm, Switzerland). All measurements
were carried out at room temperature with a conventional three-electrode
configuration consisting of glassy carbon working electrode, platinum
auxiliary electrode, and Ag/AgCl/KCl reference electrode. The solvent
(DMF or CH 3 CN) was deoxygenated before use. The solution
of tetra- n -butylammonium hexafluorophosphate Bu 4 NPF 6 (0.1 M) was used as a supporting electrolyte.
The concentrations of the compounds were 10 –3 M.
## X-ray Crystallography
X-ray Crystallography Single-crystal X-ray diffraction
(XRD) data for the compounds were collected by a Bruker Apex DUO diffractometer
using the graphite-monochromated Mo Kα radiation (λ =
0.71073 Å). Absorption corrections were applied with the use
of the SADABS program. 61 The crystal structures
were solved and refined by means of the SHELXT 62 and SHELXL 63 programs using
OLEX2 GUI. 64 Atomic thermal displacement
parameters for nonhydrogen atoms except for some solvate molecules
were refined anisotropically. The positions of H atoms were calculated
corresponding to their geometrical conditions and refined using the
riding model. In 3 , O atoms of one of solvate methanol
molecules was disordered over three positions with restrained C–O
distances (DFIX) and occupancy of 0.33. H atoms of hydroxyl group
of methanol molecules were not located but included in the formula
of 3 . The crystallographic data and details of the structure
refinements are summarized in Table 5 . Crystallographic data for the structures 1–4 have been deposited with the Cambridge Crystallographic Data Centre
(CCDC) as Supporting Information nos. 1974048–1974051.
Copies of the data can be obtained free of charge on application to
CCDC ( http://www.ccdc.cam.ac.uk/data_request/cif ). Table 5 Crystallographic Data of the Complexes 1–4 compound 1 2 3 4 empirical formula C 25 H 22 ClN 3 ORu C 25 H 22 ClN 3 O 2 Ru C 35.5 H 41 Cl 3 N 4 O 2.5 Ru 2 C 25.5 H 24.5 ClN 4.5 O 1.5 Ru formula weight 516.97 532.97 872.23 554.51 temperature/K 200(2) 298(2) 298(2) 150(2) crystal system monoclinic monoclinic monoclinic monoclinic space group P 2 1 / n P 2 1 / n C 2/ c P 2 1 / c a /Å 15.3365(10) 15.601(4) 34.0106(13) 18.414(2) b /Å 8.0892(6) 8.0342(18) 12.5712(5) 16.071(2) c /Å 17.0781(14) 17.108(4) 20.0181(8) 7.6248(11) β/deg 93.968(2) 93.210(7) 123.3950(10) 97.453(4) volume/Å 3 2113.6(3) 2140.9(8) 7145.7(5) 2237.4(5) Z 4 4 8 4 ρ calc /g/cm 3 1.625 1.654 1.619 1.646 μ/mm –1 0.891 0.886 1.109 0.852 F(000) 1048.0 1080.0 3516.0 1128.0 crystal size/mm 3 0.15 × 0.1 × 0.08 0.3 × 0.25 × 0.25 0.3 × 0.2 × 0.1 0.33 × 0.17 × 0.05 2Θ range for data collection/deg 3.452 to 57.452 3.438 to 57.468 3.544 to 51.466 3.376 to 57.46 index ranges –20 ≤ h ≤ 13, –10 ≤ k ≤ 10, –23 ≤ l ≤ 23 –21 ≤ h ≤ 21, –10 ≤ k ≤ 10, –23 ≤ l ≤ 23 –38 ≤ h ≤ 41, –10 ≤ k ≤ 15, –24 ≤ l ≤ 23 –23 ≤ h ≤ 24, –21 ≤ k ≤ 21, –7 ≤ l ≤ 10 reflections
collected 28,954 31,935 26,579 15,991 independent
reflections 5460 [ R int = 0.0304, R sigma = 0.0221] 5550 [ R int = 0.0243, R sigma = 0.0142] 6810 [ R int = 0.0351, R sigma = 0.0354] 5678 [ R int = 0.0336, R sigma = 0.0442] restraints/parameters 0/283 0/292 4/426 12/330 goodness-of-fit on F 2 1.026 1.069 1.020 1.023 final R indexes [ I >≥ 2σ ( I )] R 1 = 0.0224, wR 2 = 0.0540 R 1 = 0.0190, wR 2 = 0.0508 R 1 = 0.0313, wR 2 = 0.0724 R 1 = 0.0296, wR 2 = 0.0597 final R indexes [all data] R 1 = 0.0273, wR 2 = 0.0565 R 1 = 0.0211, wR 2 = 0.0525 R 1 = 0.0447, wR 2 = 0.0788 R 1 = 0.0424, wR 2 = 0.0639 largest diff. peak/hole/e Å –3 0.58/–0.34 0.36/–0.43 0.78/–0.40 0.51/–0.78
## Catalytic Activity Determination
Catalytic Activity Determination A typical transfer
hydrogenation reaction was carried out under air as follows: to 0.05
mmol of catalyst precursor contained in the reaction flask were added
isopropyl alcohol (4 mL), NaOH (0.2 mmol) and acetophenone (1 mmol),
in that order. The reaction mixture was stirred for 6 h at 82 °C.
After that, reaction mass was analyzed by GC and GC–MS. The
performed blank experiments confirmed that no products of reaction
were obtained unless the catalyst and NaOH were added.
## Cytotoxicity
Determination
Cytotoxicity
Determination PANC-1 (pancreatic adenocarcinoma)
were obtained from Russian Cell Culture Collection (Institute of Cytology
RAS). ARPE-19 (ATCC CRL-2302 retinal pigment epithelial) cells were
obtained from the American Type Culture Collection (ATCC) (Manassas,
VA). PANC-1 and ARPE-19 cells were cultured in DMEM-F12 medium supplemented
with 10% fetal bovine serum, 100 units/mL penicillin, and 100 μg/mL
streptomycin, at 37 °C in a humidified atmosphere containing
95% air and 5% CO 2 . The cytotoxicity of tested compounds
was studied using 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium
bromide (MTT) reduction assay as described previously. 65 MTT-formazan crystals formed by metabolically
active cells were dissolved in dimethyl sulfoxide, and absorbance
was measured at 540 and 690 nm in Varioskan LUX Multimode Microplate
Reader (Thermo Scientific, USA). Values measured at 540 nm were subtracted
for background values at 690 nm, and the data were shown as a percent
of control untreated samples.
## Computational Chemistry
Details
Computational Chemistry
Details The calculations were
performed using Gaussian 09 package. 66 Experimental
X-ray structures of complex 1 was used as a starting
point for DFT geometry optimizations. Singlet state geometry optimizations
were carried out at the DFT level of theory employing the three-parameter
hybrid B3LYP functional 67 − 70 and 6-311+G(2d,p) basis set 71 − 74 for the first and second-row
atoms, while LanL2DZ 75 , 76 was used for the ruthenium atoms.
Solvation effects were taken into account using the IEFPCM model 77 and acetonitrile as solvent. Frequency calculations
were performed for the optimized geometries in order to establish
the nature of the stationary points. Lack of imaginary vibration modes
for the optimized structures indicate that the stationary points found
corresponded to minima on the potential energy surface. Time-dependent
DFT calculations with Tamm–Dancoff approximation 78 were carried out using the same basis sets and
B3LYP, 67 − 70 CAM-B3LYP, 79 and ω-B97X[D] 80 functionals. The nature of electronic transitions
was analyzed using the NTOs approach. 81 The energies of the coordination isomers of complex 1 were compared after geometry optimization and calculation of vibrational
frequencies using M062X 82 functional and
6-311+G(2d,p)/LanL2DZ 75 , 76 basis sets; solvation effects
in dimethylformamide were taken into account using the SMD model. 83
## NCI Analysis by means of the Reduced Density
Gradient
NCI Analysis by means of the Reduced Density
Gradient 84 − 88 was Performed on the Density of the Optimized Structures Using a
Homemade Code Synthesis and Characterization [Ru( p -cym) (L 1 )Cl] ( 1 ) HL 1 (24.7 mg, 0.1
mmol) was dissolved in DMF (1.5 mL), [Ru( p -cym)Cl 2 ] 2 (30.6 mg, 0.05 mmol) was dissolved in MeOH (1.5
mL), and the resulting solution was added to the initial one. After
24 h, red crystals formed were filtered off and washed twice with
MeOH. Yield 43 mg (83%). 1 H NMR (400 MHz, DMSO- d 6 ): δ 0.99 (d, 3H, Me- i Pr, J = 8 Hz), 1.05 (d, 3H, Me- i Pr, J = 8 Hz), 2.15 (s, 3H, Me-Ar), 2.64 (m, 1H,
CH-Ar), 2.73 (s, Me- i Pr), 5.76 (d, 1H, CH ( p -cym), J = 4 Hz), 5.99 (d, 1H, CH ( p -cym), J = 4 Hz), 6.03 (d, 1H, CH ( p -cym), J = 8 Hz), 6.08 (d, 1H, CH ( p -cym), J = 8 Hz), 7.53 (t, 1H, H2-L 1 , J = 8 Hz), 7.65 (t, 1H, H3-L 1 , J = 8 Hz), 7.93 (t, 1H, H1-L 1 , J = 4 Hz), 8.02 (t, 1H, H4-L 1 , J = 8 Hz), 8.08 (d, 1H, H9-L 1 , J = 8 Hz),
8.18 (d, 1H, H8-L 1 , J = 8 Hz), 8.33 (d,
1H, H10-L 1 , J = 2 Hz), 8.40 (d, 1H, H7-L 1 , J = 8 Hz) ppm. 13 C NMR (100
MHz, CDCl 3 ): δ 22.1 (Me-Ar), 22.5 (Me- i Pr), 24.1 (Me- i Pr), 31.2 (CH- i Pr),
80.9 ( p -cym), 81.3 ( p -cym), 83.7
( p -cym), 84.1 ( p -cym), 89.5 ( p -cym), 103.7 ( p -cym), 123.0 (L 1 ), 123.4 (L 1 ), 124.1 (L 1 ), 126.3 (L 1 ) 128.0 (L 1 ), 128.4 (L 1 ), 128.9 (L 1 ), 130.3 (L 1 ), 131.3 (L 1 ), 132.0 (L 1 ), 134.4 (L 1 ), 140.2 (L 1 ), 141.6 (L 1 ), 148.0 (L 1 ), 157.4 (L 1 ) ppm. IR: 3075 (w),
3059 (w), 3030 (w), 2963 (w), 2867 (w), 1604 (w), 1596 (m), 1497 (s),
1468 (s), 1447 (m), 1420 (m), 1383 (m), 1356 (m), 1327 (m), 1303 (m),
1244 (s), 1212 (m), 1199 (m), 1164 (m), 1140 (m), 1124 (s), 1092 (m),
1068 (m), 1052 (m), 1034 (m), 1012 (m), 970 (m), 946 (m), 871 (s),
794 (s), 765 (s), 749 (s), 725 (s). Found, %: C, 58.40; H, 4.41; N,
8.32. C 25 H 22 N 3 OClRu. Calcd, %: C,
58.08; H, 4.29; N, 8.13. [Ru( p -cym) (L 2 )Cl] ( 2 ) HL 2 (53 mg, 0.2 mmol)
was dissolved in MeOH (1.5 mL). [Ru( p -cym)Cl 2 ] 2 (61.2 mg, 0.1 mmol) was dissolved in MeOH (1.5
mL), and the resulting solution was added to the initial one. After
24 h, red crystals formed were filtered off and washed twice with
MeOH. Yield 80 mg (75%). 1 H NMR (400 MHz, CDCl 3 ): δ 1.08 (d, 3H, Me- i Pr, J = 8 Hz), 1.11 (d, 3H, Me- i Pr, J = 8 Hz), 2.16 (s, 3H, Me-Ar), 2.70 (m, 1H, CH-Ar), 5.74 (d, 1H,
CH ( p -cym), J = 8 Hz), 5.925 (d,
1H, CH ( p -cym), J = 4 Hz), 5.98
(d, 1H, CH ( p -cym), J = 8 Hz), 6.03
(d, 1H, CH ( p -cym), J = 8 Hz), 7.45
(t, 1H, H-8, J = 8 Hz), 7.52 (td, 1H, H-9, J = 8 Hz, J = 1.2 Hz), 7.65 (td, 1H, H-2, J = 8 Hz, J = 2.4 Hz), 7.98 (d, 1H, H-4, J = 8 Hz), 8.02 (t, 1H, H-3, J = 4H), 8.03
(dd, 1H, H-7, J = 8 Hz, J = 0.8
Hz), 8.37 (d, 1H, H-1, J = 4 Hz), 8.39 (d, 1H, H-10, J = 4 Hz) ppm. 13 C NMR (100 MHz, CDCl 3 ): δ 19.2 (Me-Ar), 22.1 (Me- i Pr), 22.6 (Me- i Pr), 31.2 (CH- i Pr), 83.1 ( p -cym), 83.4 ( p -cym), 83.9 ( p -cym),
88.6 ( p -cym), 102.5 ( p -cym), 103.7
( p -cym), 116.9 (L 2 ), 117.7 (L 2 ), 120.2 (L 2 ), 121.7 (L 2 ) 122.9 (L 2 ), 125.8 (L 2 ), 127.4 (L 2 ), 128.1 (L 2 ), 128.2 (L 2 ), 128.9 (L 2 ), 136.2 (L 2 ), 137.9 (L 2 ) 146.3 (L 2 ), 157.0 (L 2 ), 157.6 (L 2 ) ppm. IR: 3083 (w), 3062 (w), 3033 (w), 2971
(w), 2873 (w), 1692 (s), 1625 (m), 1593 (m), 1561 (m), 1540 (w), 1495
(s), 1460 (s), 1441 (s), 1404 (m), 1356 (m), 1330 (m), 1316 (m), 1303
(m), 1242 (s), 1191 (m), 1159 (m), 1146 (m), 1124 (m), 1111 (m), 1095
(m), 1055 (m), 1039 (m), 1026 (m), 1007 (m), 940 (m), 868 (m), 807
(s), 794 (m), 759 (s), 743 (s), 727 (m), 709 (m), 687 (s), 674 (m).
Found, %: C, 56.58; H, 4.22; N, 7.95. C 25 H 22 N 3 O 2 ClRu. Calcd, %: C, 56.34; H, 4.16; N, 7.88. [Ru 2 ( p -cym) 2 (L 3 )Cl 2 ]·1.5MeOH ( 3 ) HL 3 (24.8 mg, 0.1 mmol) was suspended in MeOH
(5 mL) and 1 mL of 0.1 M solution KOH in MeOH was added. Reaction
mixture was stirred for 1 h to afford pale yellow precipitate of potassium
salt. [Ru( p -cym)Cl 2 ] 2 (30.6
mg, 0.1 mmol) was dissolved in MeOH (2 mL), and solution was added
to the initial suspension. The resulting red crystals were filtered,
washed with MeOH, and dried at room temperature. Yield 47 mg (55%). 1 H NMR (400 MHz, CDCl 3 ): δ 1.08 (dd, 6H, Me- i Pr (assymm. p -cym), J 1 = 24 Hz, J 2 = 4 Hz), 1.41
(dd, 6H, Me- i Pr (symm. p -cym), J 1 = 16 Hz, J 2 =
8 Hz), 2.20 (s, 3H, Me-Ar (assymm. p -cym)), 2.34
(s, 3H, Me-Ar (symm. p -cym)), 2.72 (m, 1H, CH-Ar
(assymm. p -cym)), 3.10 (m, 1H, CH-Ar (symm. p -cym)), 5.30 (d, 1H, CH (symm. p -cym), J = 4 Hz), 5.40 (d, 1H, CH (symm. p -cym), J = 8 Hz), 5.55 (d, 1H, CH (symm. p -cym), J = 4 Hz), 5.58 (d, 1H, CH (symm. p -cym), J = 8 Hz), 5.79 (d, 1H, CH (assymm. p -cym), J = 8 Hz), 5.96 (d, 1H, CH (assymm. p -cym),
8 Hz), 6.02 (d, 1H, CH (assymm. p -cym), 4 Hz), 6.19
(d, 1H, CH (assymm. p -cym), 8 Hz), 7.51 (t, 1H, H8-L3, J = 8 Hz), 7.67 (t, 1H, H7-L3, J = 8 Hz),
8.10 (d, 1H, H4-L3, J = 4 Hz), 8.23 (t, 2H, H9-L3, J = 8 Hz), 9.23 (d, 1H, H3-L3, J = 8 Hz),
10.10 (s, 1H, H1-L3) ppm. 13 C NMR (100 MHz, DMSO- d 6 ): δ 18.3 (Me-Ar), 18.9 (Me-Ar), 22.9
(Me- i Pr), 22.2 (Me- i Pr), 22.3 (Me- i Pr), 30.4 (CH- i Pr) 31.1 (CH- i Pr), 83.3 ( p -cym), 84.1 ( p -cym),
85.2 ( p -cym), 85.9 ( p -cym), 86.8
( p -cym), 90.0 ( p -cym), 100.5 ( p -cym), 103.3 ( p -cym), 103.7 (L 3 ), 106.8 (L 3 ), 121.9 (L 3 ), 123.2 (L 3 ), 124.9 (L 3 ), 128.3 (L 3 ), 132.5 (L 3 ), 134.0 (L 3 ), 144.4 (L 3 ), 146.7 (L 3 ), 146.9 (L 3 ), 148.8 (L 3 ), 151.8 (L 3 ), 157.9 (L 3 ) ppm. IR: 3051 (w), 2955 (m), 2926 (w), 2873
(w), 1604 (m), 1593 (w), 1561 (w), 1497 (s), 1473 (s), 1412 (s), 1394
(s), 1359 (m), 1316 (s), 1250 (s), 1204 (m), 1154 (s), 1132 (m), 1116
(m), 1068 (m), 1028 (m), 978 (m), 874 (m), 826 (s), 802 (s), 773 (s),
757 (s), 730 (s). Found, %: C, 49.11; H, 4.54; N, 6.43. C 35.5 H 41 Cl 3 N 4 O 2.5 Ru 2 . Calcd, %: C, 48.90; H, 4.74; N, 6.42. [Ru( p -cym) 2 (L 4 )Cl 2 ]·0.5DMF ( 4 ) HL 4 (24.8 mg, 0.1
mmol) was suspended in DMF (2.5
mL). [Ru( p -cym)Cl 2 ] 2 (30.6
mg, 0.05 mmol) and was dissolved in MeOH (2.5 mL), and the resulting
solution was added to the initial suspension. The mixture was stirred
until the ligand was completely dissolved. The resulting red precipitate
was filtered, washed with MeOH, and dried at room temperature. Yield
42 mg (81%). 1 H NMR (400 MHz, DMSO- d 6 ): δ 1.005 (d, 3H, Me- i Pr, J = 4 Hz), 1.075 (d, 3H, Me- i Pr, J = 4 Hz), 2.15 (s, 3H, Me-Ar), 2.68 (m, 1H, CH-Ar), 5.805
(d, 1H, CH ( p -cym), J = 4 Hz), 6.03
(d, 1H, CH ( p -cym), J = 8 Hz), 6.045
(d, 1H, CH ( p -cym), J = 4 Hz), 6.105
(d, 1H, CH ( p -cym), J = 4 Hz), 7.57
(t, 1H, H8-L 3 , J = 8 Hz), 7.70 (t, 1H,
H3-L 3 , J = 8 Hz), 8.015 (dd, 1H, H9-L 3 , J = 12 Hz, J = 4 Hz),
8.09 (d, 1H, H7-L 3 , J = 8 Hz), 8.26 (d,
1H, H10-L 3 , J = 8 Hz), 8.795 (dd, 1H,
H4-L 3 , J = 10 Hz, J =
1.6 Hz), 9.195 (dd, 1H, H2-L 3 , J = 4 Hz, J = 1.6 Hz) ppm. 13 C NMR (100 MHz, CDCl 3 ): δ 21.9 (Me-Ar), 24.1 (Me- i Pr), 30.9 (Me- i Pr), 31.2 (CH- i Pr), 83.6 ( p -cym), 83.9 ( p -cym), 85.9 ( p -cym),
87.0 ( p -cym), 89.3 ( p -cym), 100.6
( p -cym), 122.8 (L 4 ), 124.2 (L 4 ), 124.6 (L 4 ), 124.6 (L 4 ) 126.0 (L 4 ), 126.2 (L 4 ), 127.3 (L 4 ), 128.9 (L 4 ), 132.9 (L 4 ), 133.9 (L 4 ), 136.3 (L 4 ), 138.7 (L 4 ), 139.7 (L 4 ), 156.4 (L 4 ) ppm. IR: 3056 (w), 2971 (w), 2923 (w), 2873 (w), 1679 (s), 1620
(m), 1604 (m), 1569 (m), 1511 (m), 1495 (s), 1476 (s), 1460 (s), 1417
(s), 1380 (m), 1359 (m), 1308 (s), 1282 (m), 1242 (s), 1204 (m), 1175
(m), 1154 (m), 1149 (m), 1111 (m), 1076 (m), 1036 (m), 1007 (m), 996
(m), 959 (m), 911 (m), 890 (m), 876 (m), 820 (m), 797 (m), 775 (s),
762 (s), 738 (m), 690 (m). Found, %: C, 55.03; H, 4.48; N, 11.53.
C 25.5 H 24.5 ClN 4.5 O 1.5 Ru.
Calcd, %: C, 55.23; H, 4.45; N, 11.37.
## Synthesis and Characterization
Synthesis and Characterization [Ru( p -cym) (L 1 )Cl] ( 1 ) HL 1 (24.7 mg, 0.1
mmol) was dissolved in DMF (1.5 mL), [Ru( p -cym)Cl 2 ] 2 (30.6 mg, 0.05 mmol) was dissolved in MeOH (1.5
mL), and the resulting solution was added to the initial one. After
24 h, red crystals formed were filtered off and washed twice with
MeOH. Yield 43 mg (83%). 1 H NMR (400 MHz, DMSO- d 6 ): δ 0.99 (d, 3H, Me- i Pr, J = 8 Hz), 1.05 (d, 3H, Me- i Pr, J = 8 Hz), 2.15 (s, 3H, Me-Ar), 2.64 (m, 1H,
CH-Ar), 2.73 (s, Me- i Pr), 5.76 (d, 1H, CH ( p -cym), J = 4 Hz), 5.99 (d, 1H, CH ( p -cym), J = 4 Hz), 6.03 (d, 1H, CH ( p -cym), J = 8 Hz), 6.08 (d, 1H, CH ( p -cym), J = 8 Hz), 7.53 (t, 1H, H2-L 1 , J = 8 Hz), 7.65 (t, 1H, H3-L 1 , J = 8 Hz), 7.93 (t, 1H, H1-L 1 , J = 4 Hz), 8.02 (t, 1H, H4-L 1 , J = 8 Hz), 8.08 (d, 1H, H9-L 1 , J = 8 Hz),
8.18 (d, 1H, H8-L 1 , J = 8 Hz), 8.33 (d,
1H, H10-L 1 , J = 2 Hz), 8.40 (d, 1H, H7-L 1 , J = 8 Hz) ppm. 13 C NMR (100
MHz, CDCl 3 ): δ 22.1 (Me-Ar), 22.5 (Me- i Pr), 24.1 (Me- i Pr), 31.2 (CH- i Pr),
80.9 ( p -cym), 81.3 ( p -cym), 83.7
( p -cym), 84.1 ( p -cym), 89.5 ( p -cym), 103.7 ( p -cym), 123.0 (L 1 ), 123.4 (L 1 ), 124.1 (L 1 ), 126.3 (L 1 ) 128.0 (L 1 ), 128.4 (L 1 ), 128.9 (L 1 ), 130.3 (L 1 ), 131.3 (L 1 ), 132.0 (L 1 ), 134.4 (L 1 ), 140.2 (L 1 ), 141.6 (L 1 ), 148.0 (L 1 ), 157.4 (L 1 ) ppm. IR: 3075 (w),
3059 (w), 3030 (w), 2963 (w), 2867 (w), 1604 (w), 1596 (m), 1497 (s),
1468 (s), 1447 (m), 1420 (m), 1383 (m), 1356 (m), 1327 (m), 1303 (m),
1244 (s), 1212 (m), 1199 (m), 1164 (m), 1140 (m), 1124 (s), 1092 (m),
1068 (m), 1052 (m), 1034 (m), 1012 (m), 970 (m), 946 (m), 871 (s),
794 (s), 765 (s), 749 (s), 725 (s). Found, %: C, 58.40; H, 4.41; N,
8.32. C 25 H 22 N 3 OClRu. Calcd, %: C,
58.08; H, 4.29; N, 8.13. [Ru( p -cym) (L 2 )Cl] ( 2 ) HL 2 (53 mg, 0.2 mmol)
was dissolved in MeOH (1.5 mL). [Ru( p -cym)Cl 2 ] 2 (61.2 mg, 0.1 mmol) was dissolved in MeOH (1.5
mL), and the resulting solution was added to the initial one. After
24 h, red crystals formed were filtered off and washed twice with
MeOH. Yield 80 mg (75%). 1 H NMR (400 MHz, CDCl 3 ): δ 1.08 (d, 3H, Me- i Pr, J = 8 Hz), 1.11 (d, 3H, Me- i Pr, J = 8 Hz), 2.16 (s, 3H, Me-Ar), 2.70 (m, 1H, CH-Ar), 5.74 (d, 1H,
CH ( p -cym), J = 8 Hz), 5.925 (d,
1H, CH ( p -cym), J = 4 Hz), 5.98
(d, 1H, CH ( p -cym), J = 8 Hz), 6.03
(d, 1H, CH ( p -cym), J = 8 Hz), 7.45
(t, 1H, H-8, J = 8 Hz), 7.52 (td, 1H, H-9, J = 8 Hz, J = 1.2 Hz), 7.65 (td, 1H, H-2, J = 8 Hz, J = 2.4 Hz), 7.98 (d, 1H, H-4, J = 8 Hz), 8.02 (t, 1H, H-3, J = 4H), 8.03
(dd, 1H, H-7, J = 8 Hz, J = 0.8
Hz), 8.37 (d, 1H, H-1, J = 4 Hz), 8.39 (d, 1H, H-10, J = 4 Hz) ppm. 13 C NMR (100 MHz, CDCl 3 ): δ 19.2 (Me-Ar), 22.1 (Me- i Pr), 22.6 (Me- i Pr), 31.2 (CH- i Pr), 83.1 ( p -cym), 83.4 ( p -cym), 83.9 ( p -cym),
88.6 ( p -cym), 102.5 ( p -cym), 103.7
( p -cym), 116.9 (L 2 ), 117.7 (L 2 ), 120.2 (L 2 ), 121.7 (L 2 ) 122.9 (L 2 ), 125.8 (L 2 ), 127.4 (L 2 ), 128.1 (L 2 ), 128.2 (L 2 ), 128.9 (L 2 ), 136.2 (L 2 ), 137.9 (L 2 ) 146.3 (L 2 ), 157.0 (L 2 ), 157.6 (L 2 ) ppm. IR: 3083 (w), 3062 (w), 3033 (w), 2971
(w), 2873 (w), 1692 (s), 1625 (m), 1593 (m), 1561 (m), 1540 (w), 1495
(s), 1460 (s), 1441 (s), 1404 (m), 1356 (m), 1330 (m), 1316 (m), 1303
(m), 1242 (s), 1191 (m), 1159 (m), 1146 (m), 1124 (m), 1111 (m), 1095
(m), 1055 (m), 1039 (m), 1026 (m), 1007 (m), 940 (m), 868 (m), 807
(s), 794 (m), 759 (s), 743 (s), 727 (m), 709 (m), 687 (s), 674 (m).
Found, %: C, 56.58; H, 4.22; N, 7.95. C 25 H 22 N 3 O 2 ClRu. Calcd, %: C, 56.34; H, 4.16; N, 7.88. [Ru 2 ( p -cym) 2 (L 3 )Cl 2 ]·1.5MeOH ( 3 ) HL 3 (24.8 mg, 0.1 mmol) was suspended in MeOH
(5 mL) and 1 mL of 0.1 M solution KOH in MeOH was added. Reaction
mixture was stirred for 1 h to afford pale yellow precipitate of potassium
salt. [Ru( p -cym)Cl 2 ] 2 (30.6
mg, 0.1 mmol) was dissolved in MeOH (2 mL), and solution was added
to the initial suspension. The resulting red crystals were filtered,
washed with MeOH, and dried at room temperature. Yield 47 mg (55%). 1 H NMR (400 MHz, CDCl 3 ): δ 1.08 (dd, 6H, Me- i Pr (assymm. p -cym), J 1 = 24 Hz, J 2 = 4 Hz), 1.41
(dd, 6H, Me- i Pr (symm. p -cym), J 1 = 16 Hz, J 2 =
8 Hz), 2.20 (s, 3H, Me-Ar (assymm. p -cym)), 2.34
(s, 3H, Me-Ar (symm. p -cym)), 2.72 (m, 1H, CH-Ar
(assymm. p -cym)), 3.10 (m, 1H, CH-Ar (symm. p -cym)), 5.30 (d, 1H, CH (symm. p -cym), J = 4 Hz), 5.40 (d, 1H, CH (symm. p -cym), J = 8 Hz), 5.55 (d, 1H, CH (symm. p -cym), J = 4 Hz), 5.58 (d, 1H, CH (symm. p -cym), J = 8 Hz), 5.79 (d, 1H, CH (assymm. p -cym), J = 8 Hz), 5.96 (d, 1H, CH (assymm. p -cym),
8 Hz), 6.02 (d, 1H, CH (assymm. p -cym), 4 Hz), 6.19
(d, 1H, CH (assymm. p -cym), 8 Hz), 7.51 (t, 1H, H8-L3, J = 8 Hz), 7.67 (t, 1H, H7-L3, J = 8 Hz),
8.10 (d, 1H, H4-L3, J = 4 Hz), 8.23 (t, 2H, H9-L3, J = 8 Hz), 9.23 (d, 1H, H3-L3, J = 8 Hz),
10.10 (s, 1H, H1-L3) ppm. 13 C NMR (100 MHz, DMSO- d 6 ): δ 18.3 (Me-Ar), 18.9 (Me-Ar), 22.9
(Me- i Pr), 22.2 (Me- i Pr), 22.3 (Me- i Pr), 30.4 (CH- i Pr) 31.1 (CH- i Pr), 83.3 ( p -cym), 84.1 ( p -cym),
85.2 ( p -cym), 85.9 ( p -cym), 86.8
( p -cym), 90.0 ( p -cym), 100.5 ( p -cym), 103.3 ( p -cym), 103.7 (L 3 ), 106.8 (L 3 ), 121.9 (L 3 ), 123.2 (L 3 ), 124.9 (L 3 ), 128.3 (L 3 ), 132.5 (L 3 ), 134.0 (L 3 ), 144.4 (L 3 ), 146.7 (L 3 ), 146.9 (L 3 ), 148.8 (L 3 ), 151.8 (L 3 ), 157.9 (L 3 ) ppm. IR: 3051 (w), 2955 (m), 2926 (w), 2873
(w), 1604 (m), 1593 (w), 1561 (w), 1497 (s), 1473 (s), 1412 (s), 1394
(s), 1359 (m), 1316 (s), 1250 (s), 1204 (m), 1154 (s), 1132 (m), 1116
(m), 1068 (m), 1028 (m), 978 (m), 874 (m), 826 (s), 802 (s), 773 (s),
757 (s), 730 (s). Found, %: C, 49.11; H, 4.54; N, 6.43. C 35.5 H 41 Cl 3 N 4 O 2.5 Ru 2 . Calcd, %: C, 48.90; H, 4.74; N, 6.42. [Ru( p -cym) 2 (L 4 )Cl 2 ]·0.5DMF ( 4 ) HL 4 (24.8 mg, 0.1
mmol) was suspended in DMF (2.5
mL). [Ru( p -cym)Cl 2 ] 2 (30.6
mg, 0.05 mmol) and was dissolved in MeOH (2.5 mL), and the resulting
solution was added to the initial suspension. The mixture was stirred
until the ligand was completely dissolved. The resulting red precipitate
was filtered, washed with MeOH, and dried at room temperature. Yield
42 mg (81%). 1 H NMR (400 MHz, DMSO- d 6 ): δ 1.005 (d, 3H, Me- i Pr, J = 4 Hz), 1.075 (d, 3H, Me- i Pr, J = 4 Hz), 2.15 (s, 3H, Me-Ar), 2.68 (m, 1H, CH-Ar), 5.805
(d, 1H, CH ( p -cym), J = 4 Hz), 6.03
(d, 1H, CH ( p -cym), J = 8 Hz), 6.045
(d, 1H, CH ( p -cym), J = 4 Hz), 6.105
(d, 1H, CH ( p -cym), J = 4 Hz), 7.57
(t, 1H, H8-L 3 , J = 8 Hz), 7.70 (t, 1H,
H3-L 3 , J = 8 Hz), 8.015 (dd, 1H, H9-L 3 , J = 12 Hz, J = 4 Hz),
8.09 (d, 1H, H7-L 3 , J = 8 Hz), 8.26 (d,
1H, H10-L 3 , J = 8 Hz), 8.795 (dd, 1H,
H4-L 3 , J = 10 Hz, J =
1.6 Hz), 9.195 (dd, 1H, H2-L 3 , J = 4 Hz, J = 1.6 Hz) ppm. 13 C NMR (100 MHz, CDCl 3 ): δ 21.9 (Me-Ar), 24.1 (Me- i Pr), 30.9 (Me- i Pr), 31.2 (CH- i Pr), 83.6 ( p -cym), 83.9 ( p -cym), 85.9 ( p -cym),
87.0 ( p -cym), 89.3 ( p -cym), 100.6
( p -cym), 122.8 (L 4 ), 124.2 (L 4 ), 124.6 (L 4 ), 124.6 (L 4 ) 126.0 (L 4 ), 126.2 (L 4 ), 127.3 (L 4 ), 128.9 (L 4 ), 132.9 (L 4 ), 133.9 (L 4 ), 136.3 (L 4 ), 138.7 (L 4 ), 139.7 (L 4 ), 156.4 (L 4 ) ppm. IR: 3056 (w), 2971 (w), 2923 (w), 2873 (w), 1679 (s), 1620
(m), 1604 (m), 1569 (m), 1511 (m), 1495 (s), 1476 (s), 1460 (s), 1417
(s), 1380 (m), 1359 (m), 1308 (s), 1282 (m), 1242 (s), 1204 (m), 1175
(m), 1154 (m), 1149 (m), 1111 (m), 1076 (m), 1036 (m), 1007 (m), 996
(m), 959 (m), 911 (m), 890 (m), 876 (m), 820 (m), 797 (m), 775 (s),
762 (s), 738 (m), 690 (m). Found, %: C, 55.03; H, 4.48; N, 11.53.
C 25.5 H 24.5 ClN 4.5 O 1.5 Ru.
Calcd, %: C, 55.23; H, 4.45; N, 11.37.
## [Ru(
[Ru( p -cym) (L 1 )Cl] ( 1 ) HL 1 (24.7 mg, 0.1
mmol) was dissolved in DMF (1.5 mL), [Ru( p -cym)Cl 2 ] 2 (30.6 mg, 0.05 mmol) was dissolved in MeOH (1.5
mL), and the resulting solution was added to the initial one. After
24 h, red crystals formed were filtered off and washed twice with
MeOH. Yield 43 mg (83%). 1 H NMR (400 MHz, DMSO- d 6 ): δ 0.99 (d, 3H, Me- i Pr, J = 8 Hz), 1.05 (d, 3H, Me- i Pr, J = 8 Hz), 2.15 (s, 3H, Me-Ar), 2.64 (m, 1H,
CH-Ar), 2.73 (s, Me- i Pr), 5.76 (d, 1H, CH ( p -cym), J = 4 Hz), 5.99 (d, 1H, CH ( p -cym), J = 4 Hz), 6.03 (d, 1H, CH ( p -cym), J = 8 Hz), 6.08 (d, 1H, CH ( p -cym), J = 8 Hz), 7.53 (t, 1H, H2-L 1 , J = 8 Hz), 7.65 (t, 1H, H3-L 1 , J = 8 Hz), 7.93 (t, 1H, H1-L 1 , J = 4 Hz), 8.02 (t, 1H, H4-L 1 , J = 8 Hz), 8.08 (d, 1H, H9-L 1 , J = 8 Hz),
8.18 (d, 1H, H8-L 1 , J = 8 Hz), 8.33 (d,
1H, H10-L 1 , J = 2 Hz), 8.40 (d, 1H, H7-L 1 , J = 8 Hz) ppm. 13 C NMR (100
MHz, CDCl 3 ): δ 22.1 (Me-Ar), 22.5 (Me- i Pr), 24.1 (Me- i Pr), 31.2 (CH- i Pr),
80.9 ( p -cym), 81.3 ( p -cym), 83.7
( p -cym), 84.1 ( p -cym), 89.5 ( p -cym), 103.7 ( p -cym), 123.0 (L 1 ), 123.4 (L 1 ), 124.1 (L 1 ), 126.3 (L 1 ) 128.0 (L 1 ), 128.4 (L 1 ), 128.9 (L 1 ), 130.3 (L 1 ), 131.3 (L 1 ), 132.0 (L 1 ), 134.4 (L 1 ), 140.2 (L 1 ), 141.6 (L 1 ), 148.0 (L 1 ), 157.4 (L 1 ) ppm. IR: 3075 (w),
3059 (w), 3030 (w), 2963 (w), 2867 (w), 1604 (w), 1596 (m), 1497 (s),
1468 (s), 1447 (m), 1420 (m), 1383 (m), 1356 (m), 1327 (m), 1303 (m),
1244 (s), 1212 (m), 1199 (m), 1164 (m), 1140 (m), 1124 (s), 1092 (m),
1068 (m), 1052 (m), 1034 (m), 1012 (m), 970 (m), 946 (m), 871 (s),
794 (s), 765 (s), 749 (s), 725 (s). Found, %: C, 58.40; H, 4.41; N,
8.32. C 25 H 22 N 3 OClRu. Calcd, %: C,
58.08; H, 4.29; N, 8.13.
## [Ru(
[Ru( p -cym) (L 2 )Cl] ( 2 ) HL 2 (53 mg, 0.2 mmol)
was dissolved in MeOH (1.5 mL). [Ru( p -cym)Cl 2 ] 2 (61.2 mg, 0.1 mmol) was dissolved in MeOH (1.5
mL), and the resulting solution was added to the initial one. After
24 h, red crystals formed were filtered off and washed twice with
MeOH. Yield 80 mg (75%). 1 H NMR (400 MHz, CDCl 3 ): δ 1.08 (d, 3H, Me- i Pr, J = 8 Hz), 1.11 (d, 3H, Me- i Pr, J = 8 Hz), 2.16 (s, 3H, Me-Ar), 2.70 (m, 1H, CH-Ar), 5.74 (d, 1H,
CH ( p -cym), J = 8 Hz), 5.925 (d,
1H, CH ( p -cym), J = 4 Hz), 5.98
(d, 1H, CH ( p -cym), J = 8 Hz), 6.03
(d, 1H, CH ( p -cym), J = 8 Hz), 7.45
(t, 1H, H-8, J = 8 Hz), 7.52 (td, 1H, H-9, J = 8 Hz, J = 1.2 Hz), 7.65 (td, 1H, H-2, J = 8 Hz, J = 2.4 Hz), 7.98 (d, 1H, H-4, J = 8 Hz), 8.02 (t, 1H, H-3, J = 4H), 8.03
(dd, 1H, H-7, J = 8 Hz, J = 0.8
Hz), 8.37 (d, 1H, H-1, J = 4 Hz), 8.39 (d, 1H, H-10, J = 4 Hz) ppm. 13 C NMR (100 MHz, CDCl 3 ): δ 19.2 (Me-Ar), 22.1 (Me- i Pr), 22.6 (Me- i Pr), 31.2 (CH- i Pr), 83.1 ( p -cym), 83.4 ( p -cym), 83.9 ( p -cym),
88.6 ( p -cym), 102.5 ( p -cym), 103.7
( p -cym), 116.9 (L 2 ), 117.7 (L 2 ), 120.2 (L 2 ), 121.7 (L 2 ) 122.9 (L 2 ), 125.8 (L 2 ), 127.4 (L 2 ), 128.1 (L 2 ), 128.2 (L 2 ), 128.9 (L 2 ), 136.2 (L 2 ), 137.9 (L 2 ) 146.3 (L 2 ), 157.0 (L 2 ), 157.6 (L 2 ) ppm. IR: 3083 (w), 3062 (w), 3033 (w), 2971
(w), 2873 (w), 1692 (s), 1625 (m), 1593 (m), 1561 (m), 1540 (w), 1495
(s), 1460 (s), 1441 (s), 1404 (m), 1356 (m), 1330 (m), 1316 (m), 1303
(m), 1242 (s), 1191 (m), 1159 (m), 1146 (m), 1124 (m), 1111 (m), 1095
(m), 1055 (m), 1039 (m), 1026 (m), 1007 (m), 940 (m), 868 (m), 807
(s), 794 (m), 759 (s), 743 (s), 727 (m), 709 (m), 687 (s), 674 (m).
Found, %: C, 56.58; H, 4.22; N, 7.95. C 25 H 22 N 3 O 2 ClRu. Calcd, %: C, 56.34; H, 4.16; N, 7.88.
## [Ru
[Ru 2 ( p -cym) 2 (L 3 )Cl 2 ]·1.5MeOH ( 3 ) HL 3 (24.8 mg, 0.1 mmol) was suspended in MeOH
(5 mL) and 1 mL of 0.1 M solution KOH in MeOH was added. Reaction
mixture was stirred for 1 h to afford pale yellow precipitate of potassium
salt. [Ru( p -cym)Cl 2 ] 2 (30.6
mg, 0.1 mmol) was dissolved in MeOH (2 mL), and solution was added
to the initial suspension. The resulting red crystals were filtered,
washed with MeOH, and dried at room temperature. Yield 47 mg (55%). 1 H NMR (400 MHz, CDCl 3 ): δ 1.08 (dd, 6H, Me- i Pr (assymm. p -cym), J 1 = 24 Hz, J 2 = 4 Hz), 1.41
(dd, 6H, Me- i Pr (symm. p -cym), J 1 = 16 Hz, J 2 =
8 Hz), 2.20 (s, 3H, Me-Ar (assymm. p -cym)), 2.34
(s, 3H, Me-Ar (symm. p -cym)), 2.72 (m, 1H, CH-Ar
(assymm. p -cym)), 3.10 (m, 1H, CH-Ar (symm. p -cym)), 5.30 (d, 1H, CH (symm. p -cym), J = 4 Hz), 5.40 (d, 1H, CH (symm. p -cym), J = 8 Hz), 5.55 (d, 1H, CH (symm. p -cym), J = 4 Hz), 5.58 (d, 1H, CH (symm. p -cym), J = 8 Hz), 5.79 (d, 1H, CH (assymm. p -cym), J = 8 Hz), 5.96 (d, 1H, CH (assymm. p -cym),
8 Hz), 6.02 (d, 1H, CH (assymm. p -cym), 4 Hz), 6.19
(d, 1H, CH (assymm. p -cym), 8 Hz), 7.51 (t, 1H, H8-L3, J = 8 Hz), 7.67 (t, 1H, H7-L3, J = 8 Hz),
8.10 (d, 1H, H4-L3, J = 4 Hz), 8.23 (t, 2H, H9-L3, J = 8 Hz), 9.23 (d, 1H, H3-L3, J = 8 Hz),
10.10 (s, 1H, H1-L3) ppm. 13 C NMR (100 MHz, DMSO- d 6 ): δ 18.3 (Me-Ar), 18.9 (Me-Ar), 22.9
(Me- i Pr), 22.2 (Me- i Pr), 22.3 (Me- i Pr), 30.4 (CH- i Pr) 31.1 (CH- i Pr), 83.3 ( p -cym), 84.1 ( p -cym),
85.2 ( p -cym), 85.9 ( p -cym), 86.8
( p -cym), 90.0 ( p -cym), 100.5 ( p -cym), 103.3 ( p -cym), 103.7 (L 3 ), 106.8 (L 3 ), 121.9 (L 3 ), 123.2 (L 3 ), 124.9 (L 3 ), 128.3 (L 3 ), 132.5 (L 3 ), 134.0 (L 3 ), 144.4 (L 3 ), 146.7 (L 3 ), 146.9 (L 3 ), 148.8 (L 3 ), 151.8 (L 3 ), 157.9 (L 3 ) ppm. IR: 3051 (w), 2955 (m), 2926 (w), 2873
(w), 1604 (m), 1593 (w), 1561 (w), 1497 (s), 1473 (s), 1412 (s), 1394
(s), 1359 (m), 1316 (s), 1250 (s), 1204 (m), 1154 (s), 1132 (m), 1116
(m), 1068 (m), 1028 (m), 978 (m), 874 (m), 826 (s), 802 (s), 773 (s),
757 (s), 730 (s). Found, %: C, 49.11; H, 4.54; N, 6.43. C 35.5 H 41 Cl 3 N 4 O 2.5 Ru 2 . Calcd, %: C, 48.90; H, 4.74; N, 6.42.
## [Ru(
[Ru( p -cym) 2 (L 4 )Cl 2 ]·0.5DMF ( 4 ) HL 4 (24.8 mg, 0.1
mmol) was suspended in DMF (2.5
mL). [Ru( p -cym)Cl 2 ] 2 (30.6
mg, 0.05 mmol) and was dissolved in MeOH (2.5 mL), and the resulting
solution was added to the initial suspension. The mixture was stirred
until the ligand was completely dissolved. The resulting red precipitate
was filtered, washed with MeOH, and dried at room temperature. Yield
42 mg (81%). 1 H NMR (400 MHz, DMSO- d 6 ): δ 1.005 (d, 3H, Me- i Pr, J = 4 Hz), 1.075 (d, 3H, Me- i Pr, J = 4 Hz), 2.15 (s, 3H, Me-Ar), 2.68 (m, 1H, CH-Ar), 5.805
(d, 1H, CH ( p -cym), J = 4 Hz), 6.03
(d, 1H, CH ( p -cym), J = 8 Hz), 6.045
(d, 1H, CH ( p -cym), J = 4 Hz), 6.105
(d, 1H, CH ( p -cym), J = 4 Hz), 7.57
(t, 1H, H8-L 3 , J = 8 Hz), 7.70 (t, 1H,
H3-L 3 , J = 8 Hz), 8.015 (dd, 1H, H9-L 3 , J = 12 Hz, J = 4 Hz),
8.09 (d, 1H, H7-L 3 , J = 8 Hz), 8.26 (d,
1H, H10-L 3 , J = 8 Hz), 8.795 (dd, 1H,
H4-L 3 , J = 10 Hz, J =
1.6 Hz), 9.195 (dd, 1H, H2-L 3 , J = 4 Hz, J = 1.6 Hz) ppm. 13 C NMR (100 MHz, CDCl 3 ): δ 21.9 (Me-Ar), 24.1 (Me- i Pr), 30.9 (Me- i Pr), 31.2 (CH- i Pr), 83.6 ( p -cym), 83.9 ( p -cym), 85.9 ( p -cym),
87.0 ( p -cym), 89.3 ( p -cym), 100.6
( p -cym), 122.8 (L 4 ), 124.2 (L 4 ), 124.6 (L 4 ), 124.6 (L 4 ) 126.0 (L 4 ), 126.2 (L 4 ), 127.3 (L 4 ), 128.9 (L 4 ), 132.9 (L 4 ), 133.9 (L 4 ), 136.3 (L 4 ), 138.7 (L 4 ), 139.7 (L 4 ), 156.4 (L 4 ) ppm. IR: 3056 (w), 2971 (w), 2923 (w), 2873 (w), 1679 (s), 1620
(m), 1604 (m), 1569 (m), 1511 (m), 1495 (s), 1476 (s), 1460 (s), 1417
(s), 1380 (m), 1359 (m), 1308 (s), 1282 (m), 1242 (s), 1204 (m), 1175
(m), 1154 (m), 1149 (m), 1111 (m), 1076 (m), 1036 (m), 1007 (m), 996
(m), 959 (m), 911 (m), 890 (m), 876 (m), 820 (m), 797 (m), 775 (s),
762 (s), 738 (m), 690 (m). Found, %: C, 55.03; H, 4.48; N, 11.53.
C 25.5 H 24.5 ClN 4.5 O 1.5 Ru.
Calcd, %: C, 55.23; H, 4.45; N, 11.37.