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Article

Synthesis and Characterization of Novel Cu(II), Pd(II) and Pt(II) Complexes with 8-Ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone: Antimicrobial and in Vitro Antiproliferative Activity

1
Inorganic Chemistry Department, Faculty of Pharmacy, University of Medicine and Pharmacy ”Carol Davila”, 6 Traian Vuia Street, Bucharest 020956, Romania
2
Organic Chemistry Department, Faculty of Chemistry, University of Bucharest, 90-92 Panduri Street, Bucharest 050663, Romania
3
Organic Chemistry Department, Faculty of Pharmacy, University of Medicine and Pharmacy ”Carol Davila”, 6 Traian Vuia Street, Bucharest 020956, Romania
4
Oncology and Molecular Endocrinology Research Center CHUL, Research Center and Universite Laval, CHUQ-CHUL, 2705 Boulevard Laurier, Quebec City, QC G1V 4G2, Canada
5
Pharmaceutical Chemistry Department, Faculty of Pharmacy, University of Medicine and Pharmacy “Victor Babeş”, Timişoara 300041, Romania
6
Functional Sciences Department, Faculty of Medicine, University of Medicine and Pharmacy “Victor Babeş”, 2 Eftimie Murgu Square, Timişoara 300041, Romania
7
Coordination Chemistry Department, Moldova State University, 60 Mateevici Street, Chisinau 2009, Moldova
8
Inorganic Chemistry Department, Faculty of Chemistry, University of Bucharest, 23 Dumbrava Rosie Street, Bucharest 020462, Romania
9
Clinic of Urology, Universitary Emergency Central Military Hospital, Clinical Departament 3, University of Medicine and Pharmacy “Carol Davila”, 6 Traian Vuia Street, Bucharest 020956, Romania
*
Authors to whom correspondence should be addressed.
Submission received: 21 March 2016 / Revised: 30 April 2016 / Accepted: 16 May 2016 / Published: 21 May 2016
(This article belongs to the Special Issue ECSOC-19)

Abstract

:
New Cu(II), Pd(II) and Pt(II) complexes, (Cu(L)(H2O)2(OAc)) (1), (Cu(HL)(H2O)2(SO4)) (2), (Cu(L)(H2O)2(NO3)) (3), (Cu(L)(H2O)2(ClO4)) (4), (Cu(L)2(H2O)2) (5), (Pd(L)(OAc))H2O (6), and (Pt(L)2) (7) were synthesized from 8-ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one thiosemicarbazone (HL). The ligand and its metal complexes were characterized by IR, 1H-NMR, 13C-NMR, UV-Vis, FAB, EPR, mass spectroscopy, elemental and thermal analysis, magnetic susceptibility measurements and molar electric conductivity. The free ligand and the metal complexes have been tested for their antimicrobial activity against E. coli, S. enteritidis, S. aureus, E. faecalis, C. albicans and cytotoxicity against the NCI-H1573 lung adenocarcinoma, SKBR-3 human breast, MCF-7 human breast, A375 human melanoma and HL-60 human promyelocytic leukemia cell lines. Copper complex 2 exhibited the best antiproliferative activities against MCF-7 human breast cancer cells. A significant inhibition of malignant HL-60 cell growth was observed for copper complex 2, palladium complex 6 and platinum complex 7, with IC50 values of 1.6 µM, 6.5 µM and 6.4 µM, respectively.

Graphical Abstract

1. Introduction

Thiosemicarbazones represents a class of N,S-donor ligands important in coordination chemistry. These ligands have great versatility, manifested by the existence of two forms (thione-thiol), and the ability to bind metal ions in the neutral or anionic form, acting as monodentate or bidentate ligands [1,2,3,4,5,6]. Metal thiosemicarbazone complexes are of interest due their bioinorganic applications. Research in recent years has demonstrated the ability of thiosemicarbazones and their complexes to be antifungal, antibacterial, antiviral, anti-inflammatory and chemotherapeutic agents, potentially useful for inhibiting the activities of cancer cells [7,8,9,10,11,12,13,14,15,16,17]. The cytotoxicity of these ligands is enhanced by coordination to metal ions such as copper, zinc, platinum and palladium. This activity is explained not only by the metals’ ability to influence lipophilicity but also the mechanism of action within the cell [18,19,20,21,22,23,24,25,26]. Substitution on the C2 position can also affect the coordination and biological properties. The introduction of different groups at the C2 position was made to vary the hydrophilic-lipophilic character of the compounds in order to increase the cell absorption [27].
In a previous paper [28] we presented the synthesis of Cu(II) and Pd(II) complexes with 8-propyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone and 8-furyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone. This paper is a continuation of our previous research and it presents the synthesis and characterization of complexes of Cu(II), Pd(II) and Pt(II) with the new ligand 8-ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone, a less voluminous substituent. The anti-proliferative activity of the ligand and its synthesized complexes in NCI-H1573 lung adenocarcinoma, SKBR-3 human breast, MCF-7 human breast, A375 human melanoma cancer cells and human HL-60 promyelocytic leukemia cells were investigated. The complexes and ligand were also tested for their in vitro antibacterial activity against Escherichia coli, Salmonella enteritidis, Staphylococcus aureus, Enterococcus faecalis and Candida albicans strains using the paper disc diffusion method [29] (for the qualitative determination) and the serial dilutions in liquid broth method [30] (for determination of MIC).

2. Results and Discussion

2.1. Chemistry

The tiosemicarbazone HL was synthesized by refluxing equimolar amounts of thiosemicarbazide and β-cyclocetol in methanol according to the experimental protocol described in [28] (Scheme 1). The structure of the ligand was established by IR, 1H-NMR, 13C-NMR and mass spectroscopy data.
For the preparation of complexes 17 were used the metal salts Cu(OAc)2·(H2O), CuSO4·5H2O, Cu(NO3)2·3 H2O, Cu(ClO4)2·6 H2O, CuCl2·2H2O, Pd(OAc)2 and K2(PtCl4) which were refluxed with stirring in a hot clear solution of the ligand in methanol (1:1 and 1:2 metal–ligand ratio). All complexes are microcrystalline solids, which are stable in air. The melting point values are greater than 220 °C. The complexes are insoluble in organic solvents such as methanol, ethanol, chloroform and acetone, but soluble in DMF and DMSO.
The proposed molecular formulas for thiosemicarbazone HL and complexes 17 (Figure 1) are in agreement with the stoichiometries obtained based on analytical data (see Experimental). The molar conductance values of the soluble complexes in DMF (8–15 ohm−1∙cm2∙mol−1) showed that all complexes are non-electrolytes [31].

2.1.1. 1H-NMR and 13C-NMR Spectra

The 1H-NMR (DMSO-d6) spectra of diamagnetic Pd(II) and Pt(II) complexes showed the disappearance of the signal due to the =N-NH proton, indicating the deprotonation of this group, while the signals of the other NH (NH2) protons were observed at 10.42 and 10.44 ppm, respectively. The signal due to the OH proton remained unchanged as observed in the free ligand. In the 13C-NMR (DMSO-d6) spectra of the two complexes was observed that imine C=N carbon atoms signal is shifted downfield and appeared at 173.274 and 175.208 ppm, respectively. This information indicates the coordination of the metal center to the azomethine nitrogen and the sulfur in the thiol form and the NH2 group is not coordinated to the metal ion [32].

2.1.2. Infrared Spectra and Coordination Mode

The thiosemicarbazone group can exhibit thione-thiol tautomerism, because it contains a thioamide functional group. The presence of the band υ(N2′-H) at 3214 cm−1 and the absence of the one from 2570 cm−1 specific to υ(SH), indicates the ligand’s existence in thione form in a solid state [33]. In all IR spectra of the complexes the band at 3214 cm−1 is shifted to lower wavenumbers by 38 cm−1 and the presence of new band at 1617–1631 cm−1 (except for 2), due to the υ(N2′=C) group, indicates the C=S thioenolisation followed by deprotonation and complexation with the metal ions. The band at 3360 attributed to the υ(N4′-H) stretching mode in the spectra of the ligand did not present any considerable change in the complexes and thus ruled out the possibility of metal ion bonding in this area [34]. Also, in the spectrum of ligand HL two bands appear at 1276, 815 cm−1 assigned to the υ(C=S) + υ(C=N) frequencies, respectively, and the υ(C=S) (tioamide IV) frequency. In the complexes’ spectra these bands are shifted towards lower frequencies indicating the coordination of the thione/thiol sulphur [35,36]. On the other hand, in the spectra of all complexes (except 2) the emergence of a new band in the 581–628 cm−1 range, due to υ(C-S) vibration is also a sign of sulphur coordination in the thiol form.
The presence of υas(COO) and υs(COO) absorption bands at 1648, 1533 cm−1 and 1565, 1473 cm−1, respectively, in the IR spectra of complexes 1 and 6 suggests that bidentate behavior of the acetate group [37].
Three bands, which appeared at 1211, 1118, 1089 cm−1 in the IR spectrum of complex 2 are assignable to ʋ3 of the bidentate coordinated sulfato group. Further, the presence of the medium bands (ʋ1) at 931 cm−1 confirm the bidentate behaviour of the sulfato group [38].
The nitrate complex 3 has two bands at 1404 and 1210 cm−1 corresponding to υ5 and υ1, with a separation of 194 cm−1, and a medium band at 934 cm−1 assigned to υ2 of the nitrate group. The separation υ5–υ1 can be used as a criterion to distinguish between the degree of covalence of the nitrate coordination. These values indicate the presence of a terminal monodentate nitrate group [39].
The perchlorate complex 4 shows a band at 1089 cm−1 split into three components and a strong band at 628 cm−1. Splitting of this band indicates a bidentate coordination of the perchlorate group [38].
The frequency at 3436 cm−1 in HL, is assigned to the stretching vibration of the OH group of the thiosemicarbazone nucleus. All the complexes (except 7) exhibit υ(OH) and γ(H2O) bands in the 3445–3453 and 1132–1143 cm−1 regions, which are indicative of coordinated water [40].

2.1.3. Electronic Spectra and Magnetic Studies

The electronic spectrum in the polycrystalline state of ligand HL showed the maximum intraligand absorption: 34,820 and 30,900 cm−1, assigned to π→π* and n→π* transitions, corresponding to azomethine and thioamide groups of the ligand [41]. These bands are shifted after complexation and new bands appeared in the 28,250–27,340 cm−1 region and were attributed to S→Cu(II) charge transfer bands.
The electronic spectra for complexes 1, 2, 4 and 5 show d–d bands in the regions 12,550–13,570 and at 20,000 cm−1 (Figure S1) which may be assigned to d x 2 y 2 d x y and d x 2 y 2 d x z , y z transitions, respectively, due to the distorted octahedral geometry (D4h) around Cu(II) [42].
Likewise, the electronic spectra of the Cu(II) complex 3 suggests the typical axial behavior for a square-pyramidal geometry with a d x 2 y 2   ground state [43].
The electronic spectra of the complexes 6 and 7 showed a square-planar geometry for the palladium and platinum ions. The very intense bands at about 22,220 cm−1 and 23,250 cm−1, respectively, are assignable to a combination of metal–ligand charge transfer and d–d bands (Table 1) [44].
The values of µeff, for complexes 15 suggest the presence of an unpaired electron. They also indicate the existence of monomeric species.

2.1.4. Mass Spectra

The FAB mass spectra of the Cu(II) complexes with thiosemicarbazone HL have been recorded (Table S1). The molecular ion [M]+ peaks obtained from complexes are as follow: m/z = 372.5 (1), m/z = 374.2 (2), m/z = 371.5 (3), m/z = 372.5 (4), m/z = 681.3 (5), m/z = 474.5 (6), m/z = 794.1 (7). The data obtained are in good agreement with the proposed molecular formulae for complexes 17. The FAB mass spectra of these complexes show peaks assignable to various fragments arising from the thermal cleavage of the complexes.

2.1.5. Thermal Decomposition

The thermal decompositions of the complexes 17 were studied by thermogravimetry (TG). For complexes 16 the thermogravimetric analysis show a weight loss in the range 138.89–170.03 °C. This mass loss corresponds to the elimination of two water molecules (in 15) and one molecule of water for complex 6, respectively. The second weight loss steps correspond to the release of small coordinated anions: OAc, SO42−, NO3 (complexes 13 and 6). The other weight loss refers to the decomposition of the ligand. The final residue for complexes 13 and 5 was analyzed by IR spectroscopy, which confirmed the formation of CuO (Figure S2).

2.1.6. EPR Spectra

To elucidate the structure of the copper complexes, EPR spectra were recorded in the polycrystalline state and in frozen DMSO solution. The EPR spectral assignments of the copper complexes 15 and orbital reduction parameters in the polycrystalline state at 298 K and in DMSO solution at 298 K and 77 K are presented in Table 2. The EPR spectra of the complexes recorded in the polycrystalline and solution state provide information about the coordination environment around Cu(II). The spectrum of the complex 1 in the polycrystalline state at 298 K shows a signal consisting of a single slightly asymmetrical broad line, with ΔH = 160G (Figure 2).
The EPR spectrum of complex 2 shows a signal with a breadth of approximate 260 G and parameters A// = 135 G, g// = 2.371 and g = 2.103.
The spectra of the complexes 3 and 5 show axial symmetry with well-defined g// and g values, respectively g// = 2.208; g = 2.041 (for 3) and g// = 2.237; g = 2.065 (for 5). In these Cu(II) complexes, tensor values of g// > g > 2.0023 are consistent with a dx2−y2 ground state [45]. The EPR spectrum of complex 4 (Figure 3) both at room temperature (298 K) as well as at 77 K, is typical for an orthorhombic symmetry center, for which the evaluated parameters are: g1 = 2.011; g2 = 2.193; g3 = 2.409.
To assess the exchange interaction between the copper centers in the polycrystalline compound is calculated geometric parameter G using the equation G = (g// − 2.0023)/(g − 2.0023) for axial spectra [46]. If G is higher than 4, then the exchange interaction is negligible (compounds 13, 5), but if G is less than 4, considerable exchange interaction is indicated in the solid complex (for complex 4).
The EPR spectrum of complex 5 recorded in DMSO solution at 298 K and its second derivative, which shows five nitrogen superhyperfine lines in the high field component are given in Figure 4a,b. For complexes 14, three nitrogen superhyperfine lines in the high field component are observed.
The spectra of complexes 1, 2, 4 and 5, in DMSO solution at 77 K, show a typical distorted octahedral geometry and hyperfine splitting into four lines (Figure 5). These show four well defined hyperfine lines in the parallel region corresponding to the electron spin–nuclear spin interaction. In all Cu(II) complexes tensor values of g// > g > 2.0023 are consistent with a dx2−y2 ground state [47].
The EPR parameters g//, g, A// and the energies of the d–d transition were used to evaluate the bonding parameters α2, β2 and δ2, which may be regarded as measures of the covalency of the in-plane σ bonds, in-plane π bonds and out-of-plane π bonds [48]. The orbital reduction factors K// = α2β2 and K = α2δ2, were calculated using expressions reported elsewhere [49]. Hathaway has pointed out that for pure σ bonding, K// ≈ K ≈ 0.77 and for in-plane π-bonding, K// < K, while for out-of-plane π-bonding, K// > K [46].
The empirical factor f = g// /A// cm−1 is an index of tetragonal distortion. The values of this factor may vary from 105 to 135 for small to extreme distortions in square planar complexes and depends on the nature of the coordinated atoms [39,50]. The f values of complexes 15 are higher than 135, indicating significant distortion from planarity.

2.2. Antibacterial and Antifungal Activity

All synthesized complexes and ligand were tested for their in vitro antibacterial activity against Gram-positive bacteria (S. aureus, E. faecalis), Gram-negative bacteria (E. coli, S. enteritidis) and anti-fungal activity (C. albicans) strains using paper disc diffusion technique (for the qualitative determination) and the serial dilutions in liquid broth method (for determination of MIC). Furacillinum and nystatin were used as standard drugs.
The results of the antimicrobial activity study of the synthesized compounds are shown in Table 3. It shows that the ligand HL type thiosemicarbazones show only bacteriostatic activity against the microorganisms named above, concentration limits 0.5–10 mg/mL, and coordination compounds of copper with this ligand have both bacteriostatic and bactericidal activity in the concentration range 0.12–10 mg/mL for the Gram-positive bacteria and 0.25–10 mg/mL against Gram-negative bacteria.
These experimental data shows that copper ion coordination of the thiosemicarbazone favors an increased antimicrobial activity. In many cases, the minimum inhibitory concentrations (MIC) of the synthesized compounds are close to or coincide with the minimum bactericidal concentrations, which confirms the bactericidal antimicrobial activity of these coordination compounds. The experimental data show that the highest sensitivity to the investigated compounds corresponds to Gram-positive (MIC = 0.12–0.5 mg/mL, MBC = 0.12–10 mg/mL) bacteria and Candida albicans (MIC = 0.12–10 mg/mL, CMB = 0.12–10 mg/mL), and the highest resistance is manifest in Gram-negative (MIC = 0.25–10 mg/mL, MBC > 10 mg/mL) strains. It may be observed that the antibacterial and antifungal activity of the coordination compounds is directly increased by the amount of thiosemicarbazone HL, the internal area and the nature of the acid to ligand bond. The detected properties of the synthesized compounds are of interest in terms of extending antibacterial and antifungal arsenal of existing drugs.

2.3. Antiproliferative Activity

Using the Alamar blue or MTS antiproliferative assays, the antiproliferative activity of HL and complexes on several primary cancer cell lines (A375, SKBR-3, MCF-7 and NCI-H1573) and on HL-60 leukemia cells was tested. Figure 6 show the percent inhibition of the compounds on the tested cell lines after 48 h of exposure.
In the case of primary cancer cell lines, one can notice (Table S2) that for all the compounds the highest antiproliferative activity was for the NCI-H1573 lung adenocarcinoma cell line, while the SKBR-3 breast cancer cell line seems to be the most resistant to treatment. The ligand HL proved to exert a moderate antiproliferative activity on breast cancer, with an inhibition index of 28.57% and 24.87% for MCF-7 and SKBR-3 cells, respectively.
A lack of HL activity was detected for A375 cells. In the case of NCI-H157 cells, the inhibition was 12.37%. A different behavior was observed after exposure to the complexes 1-7. In term of MCF-7 cells, except for 6, HL complexation increased the antiproliferative activity of the compound, decreasing the proliferation of MCF-7 cells to 89.97%. The highest antiproliferative effect was observed for complexation with CuSO4 (complex 2). In contrast, the HL complexation proved to be ineffective for SKBR-3 cells. Only complexation with CuSO4 (complex 2) and Cu(ClO4)2 (complex 4) produced a poor increase in HL’s antiproliferative activity. In term of A375 cells, HL complexation decreased cell proliferation, the best antiproliferative effect being detected for the complex 2 (64.32%). Regarding the proliferation of NCI-H1573 cells, HL complexation proved to have a beneficial effect, decreasing cell proliferation. Except for complexes 5 and 7, all derivatives decreased the proliferation of NCI-H1573 cells by more than 50%, the best result being obtained for 4, with an inhibition index of 73.58%. Complex 5 decreased cell proliferation with 41.45%, while complex 7 decreased cell proliferation only with 16.46%. In conclusion, the efficiency of complexes depends on the cancer cell line, with NCI-H1573 being the most sensitive.
In case of human leukemia HL-60 cells, the ligand (8-ethyl-2-hydroxytricyclo(7.3.1.02,7) tridecan-13-one-thiosemicarbazone) and its metal complexes (Table 4) were tested as inhibitors of cell proliferation using three concentrations: 0.1, 1.0 and 10 µM.
No effect on HL-60 cell proliferation was noted for the free ligand or salts (data not shown) used in the synthesis of complexes, but as observed, the antiproliferative activity increases by complexation. Compounds 17 proved to have antiproliferative effects for concentrations higher than 1 µM. This fact is confirmed, especially for copper complex 2, palladium complex 6 and platinum complex 7. The antiproliferative activity of the complexes 2, 6 and 7 at 10 µM is of the same significance as that of doxorubicin, which is utilized in medicinal practice as an antileukemia drug. At this concentration the complexes totally inhibited HL-60 cell proliferation.
The copper complexes 2, including the bidentate NS ligand and sulfato group, demonstrate an important antiproliferative activity for HL-60 leukemia cells compared to those containing other inner sphere anions. The antiproliferative activity is the highest and the concentration dependence changes from 5.14% to 100%. A similar effect was observed in the case of complexes 6 and 7. The structures of the tested compounds seemed to be the principal factor influencing the biological activity.

3. Experimental Section

3.1. General Information

All commercially available reagents and chemicals were of analytical- or reagent-grade purity and used as received. The chemical elemental analysis for the determination of C, H, N was done on a LA-118 microdosimeter (Carlo-Erba, Lakewood, CO, USA). The Cu(II) content has been determined by atomic absorption spectroscopy with a AAS 1N spectrometer (Carl Zeiss Jena, Überlingen, Germany); palladium was determined following the method described by Fries and Getrost [51]. IR spectra were recorded on a Specord-M80 spectrophotometer (Leipzig, Germany) in the 4000–400 cm−1 region using KBr pellets. 1H-NMR and 13C-NMR spectra were recorded at room temperature on a DRX 400 spectrometer (Bruker, Billerica, MA, USA) in DMSO-d6, using TMS as the internal standard. The complexes were studied by thermogravimetry (TG) in a static air atmosphere, with a sample heating rate of 10 °C/min using a STA 6000 instrument (Perkin Elmer, Waltham, MD, USA). Electronic spectra were recorded using a V-670 spectrophotometer (Jasco, Tokyo, Japan), in diffuse reflectance mode, using MgO dilution matrices. The FAB mass spectra were recorded on a JMS-AX-500 mass spectrometer (JEOL, Tokyo, Japan). GCMS analysis was performed on a GCMS-QP5050A instrument (Shimadzu, Duisburg, Germany). EPR spectra were recorded on polycrystalline powders and DMSO solutions at room temperature and 77 K with a MiniScope MS200 X-band spectrometer (9.3–9.6 GHz) (Magnetech Ltd., Berlin, Germany), connected to a PC equipped with a 100 KHz field modulation unit. The molar conductance of the complexes in dimethylforamide solutions (10−3 M), at room temperature, were measured using a Consort type C-533 conductivity instrument (Turnhout, Belgium). The magnetic susceptibility measurements were done at room temperature in the polycrystalline state on a homemade Faraday magnetic balance.

3.2. Synthesis

3.2.1. Synthesis of 8-Ethyl-2-hydroxytricyclo[7.3.1.02,7]tridecan-13-one

A flask was flushed with nitrogen and then charged with cyclohexanone (10 mL, 0.947 g, 9.66 mmol). The cyclohexanone was stirred and heated to 70–75 °C under nitrogen. A solution of potassium hydroxide (0.9 g, 16 mmol) in absolute ethanol (15 mL) was added in one portion, and then a solution of propanal (10 mL, 13.6 g, 0.23 mol) in absolute ethanol (14 mL) was added dropwise over a 5 h period while maintaining the reaction mixture at 70–75 °C. The reaction mixture was stirred for an additional 12 h and then cooled to room temperature. The reaction flask was immersed in an ice bath and the mixture was kept at 0 °C for 4 h to complete the crystallization. The colorless crude product was collected by vacuum filtration and washed with cold ether (100 mL). The product was recrystalized from methanol to give 8-ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one (1.82 g, 80%), m.p. 167–169 °C, Rf = 0.3 (DCM-petroleum ether = 1:2, silica gel, visualization with KMnO4). HRMS [ESI, (+), OrbiTrap] m/z Calc. for C15H24O2Na [M + Na]+ 259.18; Found: 259.1686 [M + Na]+.

3.2.2. Synthesis of the 8-Ethyl-2-hydroxytricyclo[7.3.1.02,7]tridecane-13-one-thiosemicarbazone (HL)

The ketone 8-ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one (0.5 g, 2.12 mmol) was dissolved in ethanol (10 mL). A solution of thiosemicarbazide (0.285 g, 3.13 mmol) in ethanol (7 mL) and water (2.5 mL) was then added. The reaction mixture was refluxed for 24 h and left to cool to room temperature. The resulting precipitate was collected by vacuum filtration. The crude product was recrystallized from a mixture alcohol–water 1:1, to give 0.55 g of the title compound as white crystals, m.p. 201–203 °C, Rf = 0.5 (EtOAc-petroleum ether = 1:2, silica gel). Yield 85%; Anal. Calc. for C16H27N3OS: C, 62.13; H, 8.73; N, 13.59%. Found: C, 62.37; H, 8.52; N, 13.33%. IR (KBr, cm−1): υ(N4′-H) 3361; υ(N2′-H) 3214; υ(C=N1’) 1588; υ(C=S + C=N, C=S) 1276, 815; υ(N1′–N2′) 920. HRMS [ESI, (+)] m/z Calcd. for C16H27N3OS: 310.1948 [M + H]+, 322.1767 [M + Na]+, 348.1506 [M + K]+; Found: 310.1968 [M + H]+, 322.1788 [M + Na]+, 348.1529 [M + K]+ (Figure S3). 1H-NMR (DMSO-d6, δ, ppm, J, Hz): 0.80 (t, 6.9, 3H, H-β); 1.00–2.90 (m, 20H, aliphatic hydrogen); 7.50 (s, 1H, OH,); 9.80 (s, 2H, NH2); 10.41 (s, NH); 13C-NMR (DMSO-d6, δ, ppm): 11.89 (C-β); 20.19 (C-6); 20.88(C-11); 20.06 (C-b); 21.42 (C-12); 24.58 (C-4); 26.88 (C-5); 28.35(C-10); 32.67 (C-α); 35.85(C-9); 36.02 (C-3); 42.04 (C-8); 45.07 (C-1); 51.93 (C-7); 75.19 (C-2); 163.88 (C-13); 178.27(C-3′) (Figure S4).

3.2.3. General Procedure for the Preparation of the Metal Complexes

To a solution of 8-ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone (HL, 0.620 g, 1 mmol) in methanol (20 mL) was added a solution of the corresponding metal salt in methanol (10 mL). The molar ratio used was 1:2 (M:L) for the copper(II) complexes and 1:1(M:L) for the palladium(II) and platinum(II) complexes. The following metal salts were used: Cu(OAc)2·(H2O) for complex 1, CuSO4·5H2O for complex 2, Cu(NO3)2·3H2O for complex 3, Cu(ClO4)2·6H2O for complex 4, CuCl2·2H2O for complex 5, Pd(OAc)2 for complex 6, K2(PtCl4) for complex 7. The mixture was stirred for 7 h at 50 °C. The precipitate obtained was filtered, washed with methanol followed by ether and dried in vacuo.
(Cu(L)(H2O)2(OAc)) (1). Green solid. Yield: 90%; m.p. 230–233 °C; M. wt.: 466.5; Anal. Calc. for C18H33CuN3O5S: C, 46.30; H, 7.07; Cu, 13.61; N, 9.00%. Found: C, 46.53; H, 6.93; Cu, 13.42; N, 8.81%. IR (KBr, cm−1): υ(N4’-H) 3358; υ(N2’-H) 3176; υ(C=N1’) 1533; υ(C=S+C=N, C=S) 1267, 802; υ(N1’–N2’) 934; υ(N2’=C) 1617; υ(C-S)600.
(Cu(HL)(H2O)2(SO4)) (2). Green solid. Yield: 81%; m.p. 219-221 °C; M. wt.: 505.5; Anal. Calc. for C16H31CuN3O7S2: C, 38.05; H, 6.14; Cu, 12.58; N, 8.32%. Found: C, 38.27; H, 5.93; Cu, 12.36; N, 8.18%. IR (KBr, cm−1): υ(N4′-H) 3360; υ(N2′-H) 3212; υ(C=N1′) 1570; υ(C=S+C=N, C=S) 1265, 803; υ(N1′–N2′) 927.
(Cu(L)(H2O)2(NO3)) (3). Brown solid. Yield: 78%; m.p. 240 °C; M. wt.: 469.5; Anal. Calc. for C16H30CuN4O6S: C, 40.89; H, 6.38; Cu, 13.52; N, 11.92%. Found: C, 41.13; H, 6.12; Cu, 13.32; N, 11.72%. IR (KBr, cm’1): υ(N4’-H) 3362; υ(N2’-H) 3184; υ(C=N1’) 1543; υ(C=S+C=N, C=S)1251, -; υ (N1’–N2’) 933; υ(N2’=C) 1631; υ(C-S)616.
(Cu(L)(H2O)2(ClO4)) (4). Green solid. Yield: 84%; m.p. = 220-222 °C; M. wt.: 507; Anal. Calc. for C16H30CuN3O7SCl: C, 37.86; H, 5.91; Cu, 12.52; N, 8.28%. Found: C, 38.21; H, 5.63; Cu, 12. 32; N, 8.18%. IR (KBr, cm−1): υ(N4′-H) 3357; υ(N2′-H) 3198; υ(C=N1′) 1570; υ(C=S+C=N, C=S) 1252, 802; υ(N1′–N2′) 928; υ(N2′=C) 1625; υ(C-S) 600.
(Cu(L)2(H2O)2) (5). Green solid. Yield: 75%; m.p. 235-237 °C; M. wt.: 715.5; Anal. Calc. for C32H56CuN6O4S2: C, 53.66; H, 7.82; Cu, 8.87; N, 11.74%. Found: C, 54.03; H, 7.63; Cu, 8.62; N, 11.58%. IR (KBr, cm−1): υ(N4′-H) 3359; υ(N2′-H) 3185; υ(C=N1′) 1570; υ(C=S+C=N, C=S) 1256, 804; υ(N1′–N2′) 931; υ(N2′=C) 1626; υ(C-S) 581.
(Pd(L) (OAc)).H2O (6). Brown solid. Yield: 76 %; m.p. = 264 °C; M. wt.: 491.4; Anal. Calc. for C18H31PdN3O4S: C, 43.95; H, 6.30; Pd, 21.65; N, 8.54%. Found: C, 44.13; H, 6.18; Pd, 21.51; N, 8.38%. IR (KBr, cm−1): υ(N4′-H) 3362; υ(N2′-H) 3192; υ(C=N1′) 1575; υ(C=S+C=N, C=S) 1247, 804; υ(N1′–N2′) 929; υ(N2′=C) 1613; υ(C-S) 618.
(Pt(L)2) (7). Yellow solid. Yield: 84 %; m.p. > 300 °C; M. wt.: 811; Anal. Calc. for C32H52PtN6O2S2: C, 47.34; H, 6.41; N, 10.35%. Found: C, 47.52; H, 6.23; N, 10.20%. IR (KBr, cm−1): υ(N4′-H) 3358; υ(N2′-H) 3190; υ(C=N1′) 1578; υ(C=S+C=N, C=S) 1254, 804; υ(N1′–N2′) 928; υ(N2′=C) 1618; υ(C-S) 624.

3.3. Antibacterial Activity

The antibacterial activity of complexes and also of their prototype furaciline has been determined in liquid nutritive medium (2% of peptonate broth, pH 7.0), using the successive dilutions method. Escherichia coli, Salmonella enteritidis, Staphylococcus aureus, Enterococcus faecalis stems were used as reference culture for in vitro experiment. The dissolution of the studied substances in dimethylformamide, microorganisms cultivation, suspension obtaining, determination of minimal inhibition concentration (MIC) and minimal bactericide concentration (MBC) have been carried out according to the method previously reported.

3.4. Antifungal Bioassay

Antimycotic properties of the complexes were investigated in vitro on laboratory stem Candida albicans. The activity has been determined in liquid Sabouroud nutritive environment (pH 6.8). The innoculates were prepared from fungi stems which were harvested during 3–7 days. Their concentration in suspension is (2–4) × 106 colonies forming unities in milliliter. Sowings for yeasts and micelles were incubated at 37 °C during 7 and 14 days, respectively.

3.5. Antiproliferative Activity

3.5.1. Preparation of Tested Substances Solutions

Compounds 17 were dissolved in dimethyl sulfoxide (DMSO; Sigma-Aldrich, Ayrshire, UK) and stored at 2–8 °C. For all experiments, final concentrations of the tested compounds were prepared by diluting the stock solution (10 mM) with culture medium. The final concentration for in vitro analysis was 10 µM in case of primary cancer cell lines, while in case of human leukemia HL-60 cells three concentrations (0.1, 1.0 and 10 µM) were used.

3.5.2. Cell Culture

SKBR-3 human breast cancer cell line was cultured in McCoy’s 5a Medium Modified (Sigma Aldrich, Darmstadt, Germany) supplemented with 10% FCS (fetal bovine serum, PromoCell, Heidelberg, Germany), 1% penicillin-streptomycin (Pen/Strep, 10,000 IU/mL; PromoCell). MCF-7 human breast cancer cell line (ATCC, Rockville, MD, USA) was cultured in EMEM (Sigma Aldrich) supplemented with 10% FCS (fetal bovine serum, PromoCell), 1% penicillin-streptomycin (Pen/Strep, 10,000 IU/mL; PromoCell), 1% non-essential amino acids and 1% glutamine (PromoCell). A375 human melanoma cell line was cultured in DMEM containing 15% FCS (fetal bovine serum, PromoCell) and 1% penicillin-streptomycin (Pen/Strep, 10,000 IU/mL; PromoCell). Cells were maintained at an atmosphere of 5% CO2 at 37 °C. NCI-H1573 lung adenocarcinoma cell line was cultured in RPMI-1640 Medium (ATCC) supplemented with 10% FCS (fetal bovine serum, PromoCell), 1% penicillin-streptomycin (Pen/Strep, 10,000 IU/mL; PromoCell).
Human promyelocytic leukemia cells HL-60 (ATCC) were routinely grown in suspension in 90% RPMI-1640 (Sigma, St. Louis, MD, USA) containing l-glutamine (2 nM), antibiotics (100 IU penicillin/mL, 100 µg streptomycin/mL) and supplemented with 10% (v/v) foetal bovine serum (FBS), in a 5% CO2 humidified atmosphere at 37 °C. Cells were currently maintained twice a week by diluting the cells in RPMI 1640 medium containing 10% FBS.

3.5.3. Cell Proliferation Assays

Alamar Blue in Vitro Analysis

Human breast cancer cell lines (SKBR-3 and MCF-7), lung adenocarcinoma cell line (NCI-H1573) and human melanoma cell line (A375) were seeded onto a 96-well microplate (5000 cells/plate) and let overnight to attach to the bottom of the well. Next day, a volume of 150 μL of the tested substances dissolved into the culture medium were added. After an incubation of 48 h, 15 μL of the Alamar blue (BioSource, Camarillo, CA, USA) solution was added and the cells were incubated at 37 °C. After another 10 h, a microplate reader was used to spectrophotometrically analyze the samples. The wave lengths used were 570 nm, 600 nm respectively. Wells with untreated cells were used as controls. The highest concentration of DMSO (0.1%) used to prepare stock solutions of the tested substances did not have any significant effect on cell proliferation.
Cells viability was calculated using the formula:
100 − {((εOX21 − (εOX12 of test agent dilution)/((εOX2 A°λ1 − (εOX1 A°λ2 of untreated positive growth control)} × 100
where εOX = molar extinction coefficient of Alamar blue oxidized form (BLUE); A = absorbance of test wells; A° = absorbance of positive growth control well ( cells without tested compounds); λ1 = 570 nm, λ2 = 600 nm. All measurements were performed in triplicate and data were presented as mean ± standard deviation.

MTS Cell Proliferation Assay

The cell proliferation assay was performed using 3-(4,5-dimethylthiazol-2-yl)-5-(3-carboxymethoxyphenyl)2-(4-sulfophenyl)-2H-tetrazolium (MTS) (Cell Titer 96 Aqueous, Promega, Madison, WI, USA), which allowed us to measure the number of viable cells. In brief, triplicate cultures of 1 × 104 cells in a total of 100 µL medium in 96-well microtiter plates (Becton Dickinson and Company, Lincoln Park, NJ, USA) were incubated at 37 °C, 5% CO2. Final concentrations of the tested compounds and doxorubicin (Novapharm, Toronto, ON, Canada) were added to each well and incubated for 3 days. Following each treatment, 12 µL MTS was added to each well and incubated for 4 h. MTS is converted to water-soluble colored formazan by a dehydrogenase enzyme present in metabolically active cells. Subsequently, the plates were read at 490 nm using a microplate reader (Molecular Devices, Sunnyvale, CA, Canada).

4. Conclusions

The coordination ability of the thiosemicarbazone 8-ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone (HL) has been proved in complexation reactions with Cu(II), Pd(II) and Pt(II) ions. The physico-chemical analyses confirmed the composition and the structures of the newly obtained complexes. Independent of the metal salt anion used, the ligand acts as a mononegative bidentate species through the thioenolic sulphur and the azomethinic nitrogen, except for in complex 2, in which the ligand acts as neutral bidentate.
The EPR spectra of the copper (II) complexes 15 in DMSO solution confirmed the new structures. The EPR parameters g//, g, A// and the energies of d–d transitions were used to evaluate the bonding parameters. The orbital reduction factors indicate the presence of out-of-plane π-bonding for complexes 2, 4, 5 and of some in-plane π-bonding for the complexes 1 and 3.
The ligand and the metal complexes 17 have been screened for their in vitro antiproliferative activity against NCI-H1573 lung adenocarcinoma, SKBR-3 human breast, MCF-7 human breast, A375 human melanoma cancer cells and HL-60 human promyelocytic leukemia cells and for their in vitro antimicrobial activity against Escherichia coli, Salmonella enteritidis, Staphylococcus aureus, Enterococcus faecalis and Candida albicans.
The highest antiproliferative activity of all compounds was for the NCI-H1573 lung adenocarcinoma and MCF-7 breast cancer cell lines, while SKBR-3 breast cancer cells seems to be more resistant to treatment. Results of antiproliferative activity towards HL-60 cells indicated that the ligand alone has no cytotoxic effects at the three tested concentrations. The complexes 2, 6 and 7 significantly reduced the malignant HL-60 cell growth.
The quantitative antimicrobial activity test results proved that both the ligand and complex combinations have specific antimicrobial activity, depending on the microbial species tested.
We believe that the antiproliferative activity is influenced by the type of chemical bond existing in-plane and out-of-plane of the molecule. Good results were recorded for compounds showing K// > K⊥. These promising results are encouraging for further research in this field. Our continued, detailed studies of the toxicity of these compounds, as well as mechanism of action are in process, which could be helpful in designing more potent antitumor agents for therapeutic use.

Supplementary Materials

Supplementary materials can be accessed at: https://0-www-mdpi-com.brum.beds.ac.uk/1420-3049/21/5/674/s1.

Acknowledgments

The authors thank the Organic Chemistry Department, ICECHIM Bucharest (Romania) for microanalysis, “Horia Hulubei” National Institute of Physics and Nuclear Engineering Bucharest for help with EPR spectroscopy. The authors wish to thank the Research Center and Universite Laval, CHUQ-CHUL, Canada. Supported by National Authority for Scientific Research of Ministry of Education and Research, Bucharest, Romania (Bilateral Grant Romania-Moldova No. 680/2013).

Author Contributions

Elena Pahontu designed the research, performed the synthesis of the compounds, contributed to the analysis of the data and wrote the paper. Codruța Paraschivescu performed FAB mass spectroscopy and wrote the paper; Diana-Carolina Ilieș performed IR, UV-Vis spectroscopy and thermal analysis; Tudor Roșu performed EPR spectroscopy and contributed to the interpretation of the data; Donald Poirier, Camelia Oprean, Virgil Păunescu and Ovidiu Bratu performed antiproliferative activity and contributed to the interpretation of the data; Aurelian Gulea performed antimicrobial activity. All authors read and approved the final manuscript.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. Padhye, S.; Kauffman, G.B. Transition metal complexes of semicarbazones and thiosemicarbazones. Coord. Chem. Rev. 1985, 63, 127–160. [Google Scholar] [CrossRef]
  2. West, D.X.; Liberta, A.E.; Padhye, S.; Chilkate, R.C.; Sonawane, P.B.; Kumbhar, A.S.; Yerande, R.G. Thiosemicarbazone complexes of copper(II): Structural and biological studies. Coord. Chem. Rev. 1993, 123, 49–71. [Google Scholar] [CrossRef]
  3. Berkessel, A.; Hermann, G.; Rauch, O.-T.; Büchner, M.; Jacobi, A.; Huttner, G. Preparation and X-ray Crystal Structure of the First Trimeric Nickel Thiosemicarbazone Complex: The First Example of Oligomerization by Both Ni-O-Ni and Ni-S-Ni Bridging. Chem. Ber. 1996, 129, 1421–1423. [Google Scholar] [CrossRef]
  4. Casas, J.S.; Garcia-Tasende, M.S.; Sordo, J. Corrigendum to Main group metal Complexes of semicarbazones and thiosemicarbazones. A structural review. Coord. Chem. Rev. 2000, 209, 197–261. [Google Scholar] [CrossRef]
  5. Lobana, T.S.; Kumari, P.; Butcher, R.J.; Akitsu, T.; Aritake, Y.; Perles, J.; Fernandez, F.J.; Vega, M.C. Thiosemicarbazonates of palladium(II): The presence of methyl/phenyl substituents (R2) at C2 carbon atom induces C–H activation of R1 rings of thiosemicarbazones {R1R2C2=N3–N2H–C1(=S)–N1HR3}. J. Organometal. Chem. 2012, 701, 17–26. [Google Scholar] [CrossRef]
  6. Chunfang, G.; Jianguo, C.; Shaoyang, S.; Qifu, L.; Linyi, J.; Lianghua, F.; Yanmin, H. Synthesis and antiproliferative activity of some steroidal thiosemicarbazones, semicarbazones and hydrozones. Steroids 2014, 87, 99–107. [Google Scholar]
  7. Liberta, A.E.; West, D.X. Antifungal and antitumor activity of Heterocyclic thiosemicarbazones and their metal complexes: current status. Biometals 1992, 5, 121–126. [Google Scholar] [CrossRef] [PubMed]
  8. Liu, M.-C.; Lin, T.-S.; Sartorelli, A.C. Chemical and biological properties of cytotoxic alpha-(N)-heterocyclic carboxaldehyde thiosemicarbazones. Prog. Med. Chem. 1995, 32, 1–35. [Google Scholar] [PubMed]
  9. Rajasekaran, A.; Murugesan, S. Synthesis and antimicrobial evaluation of Thiosemicarbazones. J. Indian Chem. Soc. 2002, 79, 544–545. [Google Scholar] [CrossRef]
  10. Rodriguez-Arguelles, M.C.; Lopez-Silva, E.C.; Sanmartin, J.; Pelagatti, P.; Zani, F. Copper complexes of imidazole-2-, pyrrole-2- and indol-3 carbaldehyde thiosemicarbazones: Inhibitory activity against fungi and bacteria. J. Inorg. Biochem. 2005, 99, 2231–2239. [Google Scholar] [CrossRef] [PubMed]
  11. Huang, H.; Chen, Q.; Ku, X.; Meng, L.; Lin, L.; Wang, X.; Zhu, C.; Wang, Y.; Chen, Z.; Li, M.; Jiang, H.; Chen, K.; Ding, J.; Liu, H. A series of α-heterocyclic carboxaldehyde thiosemicarbazones inhibit topoisomerase IIα catalytic activity. J. Med. Chem. 2010, 53, 3048–3064. [Google Scholar] [CrossRef] [PubMed]
  12. Ferrari, M.B.; Fava, G.G.; Tarasconi, P.; Albertini, R.; Pinelli, S.; Satarcich, R. Synthesis, spectroscopic and structural characterization and biological activity of aquachloro(pyridoxal thiosemicarbazone) copper(II) chloride. J. Inorg. Biochem. 1994, 53, 13–25. [Google Scholar] [CrossRef]
  13. Kowol, C.R.; Trondl, R.; Heffeter, P.; Arion, V.B.; Jakupec, M.A.; Roller, A.; Galanski, M.; Berger, W.; Keppler, B.K. Impact of metal coordination on cytotoxicity of 3-aminopyridine-2-carboxaldehyde thiosemicarbazone (triapine) and novel into terminal dimethylation. J. Med. Chem. 2009, 52, 5032–5043. [Google Scholar] [CrossRef] [PubMed]
  14. Easmon, J.; Purstinger, G.; Heinisch, G.; Roth, T.; Fiebig, H.H.; Holzer, W.; Jager, W.; Jenny, M.; Hofmann, J. Synthesis, Cytotoxicity, and Antitumor Activity of Copper(II) and Iron(II) Complexes of 4N-Azabicyclo(3.2.2)nonane Thiosemicarbazones Derived from Acyl Diazines. J. Med. Chem. 2001, 44, 2164–2171. [Google Scholar] [CrossRef] [PubMed]
  15. Moorthy, N.S.; Cerqueira, N.M.; Ramos, M.J.; Fernandes, P.A. Aryl- and heteroaryl-thiosemicarbazone derivatives and their metal complexes: A pharmacological template. Recent Pat Anticancer Drug Discov. 2013, 8, 168–182. [Google Scholar] [CrossRef] [PubMed]
  16. Gokhale, N.; Jain, S.; Yadav, M. Design and virtual screening towards synthesis of novel substituted thiosemicarbozones as ribonuleotide reductase (RNR) inhibitors with improved cellular trafficking and anticancer activity. Curr. Top. Med. Chem. 2015, 15, 37–42. [Google Scholar] [CrossRef] [PubMed]
  17. Ebrahimi, H.P.; Hadi, J.S.; Alsalim, T.A.; Ghali, T.S.; Bolandnazar, Z. A novel series of thiosemicarbazone drugs: from synthesis to structure. Spectrochim. Acta. A Mol. Biomol. Spectrosc. 2015, 137, 1067–1077. [Google Scholar] [CrossRef] [PubMed]
  18. Khan, S.A.; Yusuf, M. Synthesis, spectral studies and in vitro antibacterial activity of steroidal thiosemicarbazone and their palladium (Pd (II)) complexes. Eur. J. Med. Chem. 2009, 44, 2270–2274. [Google Scholar] [CrossRef] [PubMed]
  19. Festa, R.A.; Thiele, D.J. Copper: an essential metal in biology. Curr. Biol. 2011, 21, R877–R883. [Google Scholar] [CrossRef] [PubMed]
  20. Paterson, B.M.; Donnelly, P.S. Copper complexes of bis(thiosemicarbazones): From chemotherapeutics to diagnostic and therapeutic radiopharmaceuticals. Chem. Soc. Rev. 2011, 40, 3005–3018. [Google Scholar] [CrossRef] [PubMed]
  21. Wong, E.; Giandomenico, C.M. Current status of platinum-based antitumor drugs. Chem. Rev. 1999, 99, 2451–2466. [Google Scholar] [CrossRef] [PubMed]
  22. Casas, J.C.; Castellano, E.E.; Ellena, J.; García-Tasende, M.S.; Pérez-Parallé, M.L.; Sánches, A.; Sánches-González, A.; Sordo, J.; Touceda, A. New Pd(II) and Pt(II) complexes with N,S-chelated pyrazolonate ligands: Molecular and supramolecular structure and preliminary study of their in vitro antitumoral activity. J. Inorg. Biochem. 2008, 102, 33–45. [Google Scholar] [CrossRef] [PubMed]
  23. Jansson, P.J.; Sharpe, P.C.; Bernhardt, P.V.; Richardson, D.R. Novel Thiosemicarbazones of the ApT and DpT series and their copper complexes: Identification of pronounced redox activity and characterization of their antitumor activity. J. Med. Chem. 2010, 53, 5759–5769. [Google Scholar] [CrossRef] [PubMed]
  24. Ramachandran, E.; Kalaivani, P.; Prabhakaran, R.; Rath, N.P.; Brinda, S.; Poornima, P.; Vijaya Padma, V.; Natarajan, K. Synthesis, X-ray crystal structure, DNA binding, antioxidant and cytotoxicity studies of Ni(II) and Pd(II) thiosemicarbazone complexes. Metallomics. 2012, 4, 218–227. [Google Scholar] [CrossRef] [PubMed]
  25. Munira Haidad Ali, S.; Yan, Y.K.; Lee, P.P.F.; Khong, K.Z.X.; Alam Sk, M.; Lim, K.H.; Klejevskaja, B.; Vilar, R. Copper(II) complexes of substituted salicylaldehyde dibenzyl semicarbazones: Synthesis, cytotoxicity and interaction with quadruplex DNA. Dalton Trans. 2014, 43, 1449–1459. [Google Scholar] [CrossRef] [PubMed]
  26. Santini, C.; Pellei, M.; Gandin, V.; Porchia, M.; Tisato, F.; Marzano, C. Advances in copper complexes as anticancer agents. Chem. Rev. 2014, 114, 815–862. [Google Scholar] [CrossRef] [PubMed]
  27. Belicchi-Ferrari, M.; Bisceglie, F.; Pelosi, G.; Tarasconi, P. Heterocyclic substituted thiosemicarbazones and their Cu(II) complexes: Synthesis, characterization and studies of substituent effects on coordination and DNA binding. Polyhedron 2008, 27, 1361–1367. [Google Scholar] [CrossRef]
  28. Roşu, T.; Pahonţu, E.; Păsculescu, S.; Georgescu, R.; Stănică, N.; Curaj, A.; Popescu, A.; Leabu, M. Synthesis and characterization of novel Cu(II) and Pd(II) complexes with 2-hydroxy-8-R-tricyclo(7.3.1.0.2,7)tridecane-13-one thiosemicarbazone. Study on biological activity. Eur. J. Med. Chem. 2010, 45, 1627–1634. [Google Scholar]
  29. Barry, A. Procedures and theoretical considerations for testing antimicrobial agents in agar media. In Antibiotics in Laboratory Medicine, 5th ed.; Williams and Wilkins: Baltimore, MD, USA, 1991; pp. 1–16. [Google Scholar]
  30. National Committee for Clinical Laboratory Standard. NCCLS: Methods for Anti-microbial Dilution and Disk Susceptibility Testing of Infrequently Isolated or Fastidious Bacteria, Approved Guideline; Document M45-A 26(19); NCCLS: Willanova, PA, USA, 1999. [Google Scholar]
  31. Geary, W.J. The use of conductivity measurements in organic solvents for the characterization of coordination compounds. Coord. Chem. Rev. 1971, 7, 81–115. [Google Scholar] [CrossRef]
  32. Ali, A.Q.; Teoh, S.G.; Salhin, A.; Eltayeb, N.E.; Ahamed, M.B.K.; Majid, A.M.S.A. Synthesis of platinum(II) complexes of isatin thiosemicarbazones derivatives: In vitro anti-cancer and deoxyribose nucleic acid binding activities. Inorg. Chim. Acta. 2014, 416, 235–244. [Google Scholar] [CrossRef]
  33. Joseph, M.; Suni, V.; Prathapachandra Kurup, M.R.; Nethaji, M.; Kishore, A.; Bhat, S.G. Structural, spectral and antimicrobial studies of copper(II) complexes of 2-benzoylpyridine N(4)-cyclohexyl thiosemicarbazone. Polyhedron 2004, 23, 3069–3080. [Google Scholar] [CrossRef]
  34. Youssef, N.S.; Hegab, K.H. Synthesis and Characterization of some Transition Metal Complexes of Thiosemicarbazones Derived from 2-acetylpyrrole and 2-acetylfuran. Synth. React. Inorg. Met-Org. Nano-Met. Chem. 2005, 35, 391–398. [Google Scholar] [CrossRef]
  35. Dilovic, I.; Rubcic, M.; Vrdoljak, V. Novel thiosemicarbazone derivatives as potential antitumor agents: Synthesis, physicochemical and structural properties, DNA interactions and antiproliferative activity. Bioorg. Med. Chem. 2008, 16, 5189–5198. [Google Scholar] [CrossRef] [PubMed]
  36. Latheef, L.; Prathapachandra Kurup, M.R. Spectral and structural studies of copper(II) complexes of thiosemicarbazones derived from salicylaldehyde and containing ring incorporated at N(4)-position. Spectrochim. Acta Part A 2008, 70, 86–93. [Google Scholar] [CrossRef] [PubMed]
  37. Ibrahim, K.M.; Bekheit, M.M. Synthesis and characterization of new metal complexes of thiosemicarbazone derived from 4-phenyl-3-thiosemicarbazide and chromone-3-carboxaldehyde. Trans. Met. Chem. 1988, 13, 230–232. [Google Scholar] [CrossRef]
  38. Nakamoto, K. Infrared and Raman Spectra of Inorganic and Coordination Compounds, 5th ed.; Wiley-Interscience: New York, NY, USA, 1997; p. 86. [Google Scholar]
  39. Jayakumar, K.; Sithambaresan, M.; Ambili Aravindakshan, A.; Prathapachandra Kurup, M.R. Synthesis and spectral characterization of copper(II) complexes derived from 2-benzoylpyridine-N4,N4-dimethyl-3-thiosemicarbazone: Crystal structure of a binuclear complex. Polyhedron 2014, 75, 50–56. [Google Scholar] [CrossRef]
  40. Chandra, S.; Vandana. Synthesis, spectroscopic, anticancer and antibacterial studies of Ni(II) and Cu(II) complexes with 2-carboxybenzaldehyde thiosemicarbazone. Spectrochim. Acta Part A Mol. Biomol. Spectrosc. 2014, 129, 333–338. [Google Scholar] [CrossRef] [PubMed]
  41. Sreekanth, A.; Sivakumar, S.; Prathapachandra Kurup, M.R. Structural studies of six and four coordinate zinc(II), nickel(II) and dioxovanadium(V) complexes with thiosemicarbazones. J. Mol. Struct. 2003, 655, 47–58. [Google Scholar] [CrossRef]
  42. Chandra, S.; Bargujar, S.; Nirwal, R.; Yadav, N. Synthesis, spectral characterization and biological evaluation of copper(II) and nickel(II) complexes with thiosemicarbazones derived from a bidentate Schiff base. Spectrochimica Acta Part A: Mol. Biomol. Spectrosc. 2013, 106, 91–98. [Google Scholar] [CrossRef] [PubMed]
  43. Lever, A.P.B. Inorganic Electronic Spectroscopy, 2th ed.; Elsevier Science: New York, NY, USA, 1984. [Google Scholar]
  44. Kovala-Demertzi, D.; Alexandratos, A.; Papageorgiou, A.; Yadav, P.N.; Dalezis, P.; Demertzis, M.A. Synthesis, characterization, crystal structures, in vitro and in vivo antitumor activity of palladium(II) and zinc(II) complexes with 2-formyl and 2-acetyl pyridine N(4)-1-(2-pyridyl)-piperazinyl thiosemicarbazone. Polyhedron 2008, 27, 2731–2738. [Google Scholar] [CrossRef]
  45. Sreekanth, A.; Prathapachandra Kurup, M.R. Structural and spectral studies on four coordinate copper (II) complexes of 2-benzoylpyridine N(4),N(4)-(butane-1,4-diyl)thiosemicarbazone. Polyhedron 2003, 22, 3321–3332. [Google Scholar] [CrossRef]
  46. Hathaway, B.J.; Billing, D.E. The electronic properties and stereochemistry of mononuclear complexes of the copper(II) ion. Coord. Chem. Rev. 1970, 5, 143–207. [Google Scholar] [CrossRef]
  47. El-Metwally, N.M.; Al-Hazmi, G.A.A. Spectroscopic evaluation for VO(II), Ni(II), Pd(II) and Cu(II) complexes derived from thiosemicarbazide: A special emphasis on EPR study and DNA cleavage. Spectrochim. Acta Part A Mol. Biomol. Spectrosc. 2013, 107, 289–295. [Google Scholar] [CrossRef] [PubMed]
  48. Joseph, M.; Kuriakose, M.; Prathapachandra Kurup, M.R.; Suresh, E.; Kishore, A.; Bhat, S.G. Structural, antimicrobial and spectral studies of copper(II) complexes of 2-benzoylpyridine N(4)-phenyl thiosemicarbazone. Polyhedron 2006, 25, 61–70. [Google Scholar] [CrossRef]
  49. Hathaway, B.J. Structure and Bonding; Springer Verlag: Heidelberg, Germany, 1973; p. 60. [Google Scholar]
  50. Pogni, R.; Bartoo, M.C.; Diaz, A.; Basosi, R. EPR characterization of mono(thiosemicarbazones) copper(II) complexes. J. Inorg. Biochem. 2000, 79, 333–337. [Google Scholar] [CrossRef]
  51. Fries, J.; Getrost, H. Organic Reagents for Trace Analysis; E. Merck: Darmstadt, Germany, 1977; pp. 291–298. [Google Scholar]
  • Sample Availability: Samples of the compounds are not available from the authors.
Scheme 1. Synthesis of the ligand 8-ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thio-semicarbazone (HL).
Scheme 1. Synthesis of the ligand 8-ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thio-semicarbazone (HL).
Molecules 21 00674 sch001
Figure 1. Proposed structures of the newly obtained metal complexes 17.
Figure 1. Proposed structures of the newly obtained metal complexes 17.
Molecules 21 00674 g001
Figure 2. EPR spectra of complexes 15 in the polycrystalline state at 298 K.
Figure 2. EPR spectra of complexes 15 in the polycrystalline state at 298 K.
Molecules 21 00674 g002
Figure 3. EPR spectrum of complex 5 in the state at 298 K and 77 K.
Figure 3. EPR spectrum of complex 5 in the state at 298 K and 77 K.
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Figure 4. EPR spectra of complexes 15 in DMSO solution (a) at 298 K; (b) second derivative spectra.
Figure 4. EPR spectra of complexes 15 in DMSO solution (a) at 298 K; (b) second derivative spectra.
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Figure 5. EPR spectra of complexes 15 in DMSO solution at 77 K.
Figure 5. EPR spectra of complexes 15 in DMSO solution at 77 K.
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Figure 6. The effects of ligand HL and complexes 17 on SKBR-3, MCF-7, A375, NCI-H1573 and HL-60 cell proliferation. (a) Inhibition of cell proliferation on SKBR-3 human breast cancer cell line; (b) Inhibition of cell proliferation on MCF-7 human breast cancer cell line; (c) Inhibition of cell proliferation on A375 melanoma cell line; (d) Inhibition of cell proliferation on NCI-H1573 lung adenocarcinoma cell line; (e) Inhibition of cell proliferation on human leukemia HL-60 cells after exposure to 10 µM of tested compounds.
Figure 6. The effects of ligand HL and complexes 17 on SKBR-3, MCF-7, A375, NCI-H1573 and HL-60 cell proliferation. (a) Inhibition of cell proliferation on SKBR-3 human breast cancer cell line; (b) Inhibition of cell proliferation on MCF-7 human breast cancer cell line; (c) Inhibition of cell proliferation on A375 melanoma cell line; (d) Inhibition of cell proliferation on NCI-H1573 lung adenocarcinoma cell line; (e) Inhibition of cell proliferation on human leukemia HL-60 cells after exposure to 10 µM of tested compounds.
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Table 1. Electronic spectra (cm−1) and magnetic moment (BM) of the complexes 17.
Table 1. Electronic spectra (cm−1) and magnetic moment (BM) of the complexes 17.
Metal Complex Molecular Formula Transitions d–d (cm−1) µeff (BM)Geometry
(Cu(L)(H2O)2(OAc)) (1)2B1g2A1g -2B1g2B2g 13,5702B1g2Eg 20,0001.99Octahedral distorted
(Cu(HL)(H2O)2(SO4)) (2)2B1g2A1g -2B1g2B2g 13,5702B1g2Eg 20,0001.83Octahedral distorted
(Cu(L)(H2O)2(NO3)) (3)2B1g2A1g -2B1g2B2g 12,6902B1g2Eg 20,0001.69Square-pyramidal
(Cu(L)(H2O)2(ClO4)) (4)2B1g2A1g -2B1g2B2g 13,5702B1g2Eg 20,1001.88Octahedral distorted
(Cu(L)2(H2O)2) (5)2B1g2A1g -2B1g2B2g 12,5502B1g2Eg 20,0001.97Octahedral distorted
(Pd(L)(OAc))(H2O) (6)1A1g1B1g -1A1g1A2g 22,2201A1g1Eg -*Square-planar
(Pt(L)2) (7)1A1g1B1g -1A1g1A2g 23,2501A1g1Eg -*Square-planar
* diamagnetic.
Table 2. EPR spectral parameters of the Cu(II) complexes 15.
Table 2. EPR spectral parameters of the Cu(II) complexes 15.
12345
Polycrystalline (298 K)
g//2.4042.3712.2082.409 (g3)2.237
g2.0872.1032.0412.193 (g2)2.065
2.011 (g1)
DMSO (77K)
g//2.3942.4002.3992.3992.400
g2.0822.0882.0762.0782.098
A//117.4118.0119.2118.0119.0
α20.7890.8380.8020.7920.831
β20.9890.9980.8900.9960.978
δ20.9920.8790.9730.9690.952
K//0.7800.8410.7170.7690.787
K0.7910.5690.7850.7580.753
Table 3. Antibacterial and antifungal activities of ligand (HL) and complexes 17 as MIC a/MBC b values (mg/mL).
Table 3. Antibacterial and antifungal activities of ligand (HL) and complexes 17 as MIC a/MBC b values (mg/mL).
CompoundsE. coli (G−)S. enteritidis (G−)S. aureus (G+)E. faecalis (G+)C. albicans
MICMBCMICMBCMICMBCMICMBCMICMBC
C16H27N3OS (HL)0.5>10.0>10.0>10.00.5>10.0>10.0>10.00.5>10.0
(Cu(L)(H2O)2(OAc)) (1)>10.0>10.00.5>10.0>10.0>10.0>10.0>10.0>10.0>10.0
(Cu(HL)(H2O)2(SO4)) (2)0.25>10.00.250.120.120.120.120.120.120.12
(Cu(L)(H2O)2(NO3)) (3)>10.0>10.0>10.0>10.00.120.250.120.120.50.5
(Cu(L)(H2O)2(ClO4)) (4)0.5>10.00.5>10.00.12>10.00.12>10.00.120.12
(Cu(L)2(H2O)2) (5)>10.0>10.00.5>10.00.12>10.00.12>10.00.120.12
(Pd(L)(OAc))(H2O) (6)>10.0>10.00.5>10.00.5>10.0>10.0>10.0>0.5>0.5
(Pt(L)2) (7)>10.0>10.00.5>10.0>10.0>10.00.12>10.0>10.0>10.0
Cu(OAc)2·H2O0.5-1.024-1.024-0.5---
CuSO4·5H2O0.5-1.024-0.5-0.5-1.024-
Cu(NO3)2·3 H2O1.024-1.024-1.024-1.024---
Cu(ClO4)2·6 H2O1.024-1.024-1.024-0.5- -
CuCl2·2H2O1.024-0.5-0.5-0.5---
Pd(OAc)21.024-1.024-1.024-0.5- -
K2(PtCl4)1.024-1.024-1.024-0.5- -
Furacillinum0.0180.0370.0090.0090.0090.0090.0370.037--
Nystatine--------0.080.08
E. coli (Escherichia coli, ATCC 25922); S. enteritidis (Salmonella enteritidis); S. aureus (Staphylococcus aureus, ATCC 25923); E. faecalis (Enterococcus faecalis); C. albicans (Candida albicans). a MIC–minimum inhibitory concentration. b MBC—minimum bactericide concentration. G(−): Gram-negative bacteria; G(+): Gram-positive bacteria.
Table 4. Antiproliferative activity of ligand and metal complexes on human leukemia HL-60 cells at three concentrations a.
Table 4. Antiproliferative activity of ligand and metal complexes on human leukemia HL-60 cells at three concentrations a.
CompoundInhibition of Cell Proliferation %IC50 (µM) b
10 µM1 µM0.1 µM
C16H27N3OS (HL)−2.90−5.720.31-
(Cu(L)(H2O)2(OAc)) (1)21.97−2.11−2.58≥10
(Cu(HL)(H2O)2(SO4)) (2)100.005.14-5.251.6 ± 3
(Cu(L)(H2O)2(NO3)) (3)63.918.121.356.4 ± 5
(Cu(L)(H2O)2(ClO4)) (4)48.946.481.136.5 ± 4
(Cu(L)2(H2O)2) (5)43.438.737.2014.2 ± 3
(Pd(L)(OAc))(H2O) (6)100.00−22.99−3.856.5 ± 4
(Pt(L)2) (7)100.00−10.32−8.136.4 ± 2
DOXO c91.9494.5577.00≤0.1
a SEM < ± 4% of a single experiment in triplicate. b The IC50 value was defined as the concentration at which 50% survival of cells was observed. c DOXO (doxorubicin) used as a positive control.

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Pahonțu, E.; Paraschivescu, C.; Ilieș, D.-C.; Poirier, D.; Oprean, C.; Păunescu, V.; Gulea, A.; Roșu, T.; Bratu, O. Synthesis and Characterization of Novel Cu(II), Pd(II) and Pt(II) Complexes with 8-Ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone: Antimicrobial and in Vitro Antiproliferative Activity. Molecules 2016, 21, 674. https://0-doi-org.brum.beds.ac.uk/10.3390/molecules21050674

AMA Style

Pahonțu E, Paraschivescu C, Ilieș D-C, Poirier D, Oprean C, Păunescu V, Gulea A, Roșu T, Bratu O. Synthesis and Characterization of Novel Cu(II), Pd(II) and Pt(II) Complexes with 8-Ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone: Antimicrobial and in Vitro Antiproliferative Activity. Molecules. 2016; 21(5):674. https://0-doi-org.brum.beds.ac.uk/10.3390/molecules21050674

Chicago/Turabian Style

Pahonțu, Elena, Codruța Paraschivescu, Diana-Carolina Ilieș, Donald Poirier, Camelia Oprean, Virgil Păunescu, Aurelian Gulea, Tudor Roșu, and Ovidiu Bratu. 2016. "Synthesis and Characterization of Novel Cu(II), Pd(II) and Pt(II) Complexes with 8-Ethyl-2-hydroxytricyclo(7.3.1.02,7)tridecan-13-one-thiosemicarbazone: Antimicrobial and in Vitro Antiproliferative Activity" Molecules 21, no. 5: 674. https://0-doi-org.brum.beds.ac.uk/10.3390/molecules21050674

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