Synthesis and coordination chemistry of organotin(IV) complexes of 2,3-methylenedioxyphenylpropenoic acid

The synthesis, spectroscopy, and antitumor behavior of organotin(IV) complexes of 2,3-methylenedioxyphenylpropenoic acid are described. The spectroscopic data indicate 1 : 2 and 1 : 1 metal to ligand stoichiometry in case of di- and trioganotin(IV) compounds and hypervalency of Sn(IV) in trigonal bipyramidal and octahedral modes. Mass spectrometric and elemental analysis data support the solid and solution spectroscopic results. The complexes have been evaluated in vitro against crown gall tumor and bio-activity screenings showed in vitro biological potential. The nature of covalent attachments (methyl, ethyl, n-butyl, phenyl, and n-octyl) of Sn(IV) played a decisive role for bioactivity. All the compounds have been studied in solution by NMR (¹H, ¹³C) and also in solid state using FTIR, mass spectrometry, and by X-ray crystallography. The molecular structure of Et₂Sn(IV) and Me₃Sn(IV) derivatives confirm the behavior of di- and tri-organotin(IV) compounds in solid state. Mono-organotin derivatives are octahedral both in solid and solution.     

Synthesis,characterization, and antibacterial activity of organotin(IV) complexes with 2-hydroxyacetophenone thiocarbohydrazone

Six new organotin(IV) complexes were synthesized by direct reaction of RSnCl₃ (R?=?Me, Bu and Ph) or R₂SnCl₂ (R?=?Me, Bu and Ph) and 2-hydroxyacetophenone thiocarbohydrazone [H₂APTC] under purified nitrogen in the presence of base in 1?:?2?:?1 molar ratio (metal: base: ligand). Complexes 2–7 have been characterized by elemental analyses, molar conductivity, UV-Visible, IR and ¹H NMR spectral studies. Complexes 2–7 are non-electrolytes. The molecular structure of [Me₂Sn(APTC)]?·?(C₂H₅OH) (5) has been determined by X-ray diffraction analysis. The thiocarbohydrazone ligand (1) and 2–7 have been tested for antibacterial activity against Escherichia coli, Staphylococcus aureus, Salmonella typhi and Enterococci aeruginosa.     

Synthesis,structure and biological activity of organotin derivatives with pyridylmethylthiobenzoic acid

Reaction of 2-(2-pyridylmethylthio)benzoic acid (1) with R₂SnO (R = Et or ⁿBu) in a 1:1 molar ratio gives the dimeric compounds {[(2-PyCH₂SC₆H₄CO₂)SnR₂]₂O}₂. A similar reaction of 2-(4-pyridylmethylthio)benzoic acid (2) with Et₂SnO yields an analogous result. However, treatment of 2 with ⁿBu₂SnO in a 1:1 molar ratio only gives the diorganotin dicarboxylate (4-PyCH₂SC₆H₄CO₂)₂Sn(ⁿBu)₂. X-ray crystal structure analyses indicate that the pyridyl nitrogen atoms do not coordinate to the tin atoms in the dimer, whilst in the diorganotin dicarboxylate the tin atom has a seven-coordinate distorted pentagonal-bipyramidal geometry, and this compound forms a linkage coordination polymer through the interactions of the pyridyl nitrogen atoms with the adjacent tin atoms. In addition, treatment of 1 or 2 with (Ph₃Sn)₂O in a 2:1 molar ratio affords triphenyltin carboxylates, in which the tin atoms also show different coordination environments. In the solid state, triphenyltin 2-(2-pyridylmethylthio)benzoate is a monomer and the pyridyl nitrogen atom does not participate in coordination to the tin atom either, while the interactions between the pyridyl nitrogen atoms and the adjacent tin atoms link triphenyltin 2-(4-pyridylmethylthio)benzoate into a coordination polymer. Preliminary in vitro tests for fungicidal activity show that all these compounds display good activity to Physolospora piricola in a low concentration. Moreover, the triphenyltin carboxylates show a higher inhibition percentage than the diorganotin carboxylates.     

Synthesis and cytotoxicity of novel podophyllotoxin derivatives

In order to find novel synthetic antitumor agents with superior cytotoxicity and overcoming multidrug resistance,a novel series of 4β-N-substituted podophyllotoxin derivatives were synthesized and evaluated as potential antitumor agents.Seven novel podophyllotoxin derivatives were synthesized by linking 4β-amino-4-deoxypodophyllotoxin with N-substituted 5-methylindol-3- yl-glyoxyl chlorides and tested against K562 and K562/A02 using SRB methods in vitro,KB and KBV using MTT methods in vitro.     

Synthesis and characterization of new organotin(IV) complexes with polyfunctional ligands

New mono-, di- and tri-organotin(IV) derivatives containing the neutral bis(2-pyridylthio)methane ligand, [(pyS)₂CH₂] and tris(2-pyridylthio)methane ligand, [(pyS)₃CH] have been synthesized from reaction with SnR_nCl_4−n (R = Me, ⁿBu, Ph and Cy, n = 1-3) acceptors. Mono-nuclear adducts of the type {[(pyS)₂CH₂]R_nSnCl_4−n} and {[(pyS)₃CH]R_nSnCl_4−n} have been obtained and characterized by elemental analyses, FT-IR, ESI-MS, multinuclear (¹H and ¹¹⁹Sn) NMR spectral data. The ¹H and ¹¹⁹Sn NMR and ESI-MS data suggest for the triorganotin(IV) derivatives a complete dissociation of the compounds in solution. The mono- and di-organotin(IV) derivatives show a greater stability in solution, and their spectroscopic data are in accordance with the existence of six-coordinated RSnCl₃N₂ or R₂SnCl₂N₂ species.     

Synthesis, crystal structures, electrochemical studies and anti-tumor activities of three polynuclear organotin(IV) carboxylates containing ferrocenyl moiety

A novel ferrocene-containing ligand 3-trifluoromethyl-5-ferrocenyl -pyrazol-1-yl-acetic acid (LCOOH) and three organotin(IV) carboxylate derivatives [Ph₄Sn₂O(OCH₃)(OOCL)]₂(1), [BuSnO(OOCL)]₆(2) and [Bu₄Sn₂O(OOCL₂)₂] (3) have been synthesized and structurally characterized by means of FT-IR, elemental analysis, ¹H NMR, ¹¹⁹Sn NMR, X-ray crystallography and cyclic voltammetry. Both complexes 1 and 3 are centrosymmetric with ladder framework. Complex 2 is a hexanuclear one with drum structure. Furthermore, their anti-tumor activities were also evaluated, using HepG2 human hepatocellular liver carcinoma cells, A549 human lung carcinoma cells and B16-F10 melanoma cells. Complex 1 displayed the best cytotoxicity and can be pointed out as a promising substrate to be subject of further investigations.     

Synthesis,characterization, semi-empirical study and biological activities of homobimetallic complexes of tranexamic acid with organotin(IV)

The Schiff base has been synthesized by reacting tranexamic acid with indol-3-carboxyaldehyde in the first step and then with carbon disulfide at room temperature in the second step. The homobimetallic complexes have been synthesized by reaction of Schiff base with R₂SnCl₂ and R₃SnCl in 1?:?2?M ratio under stirring, where R?=?methyl, n-butyl and phenyl. The ligand and complexes have been characterized by elemental analysis, FT-IR, multinuclear NMR (¹H, ¹³C and ¹¹⁹Sn) and semi-empirical study. IR data reveal the bidentate nature of the ligand. Five- or six-coordinate geometry was confirmed in solution by NMR spectroscopy. The homobimetallic complexes and ligand were tested in vitro against some pathogenic bacteria and fungi to assess their antimicrobial properties. The complexes show biological activities with few exceptions.     

Synthesis, characterization, and molecular structures of di- and triorganotin(IV) complexes with 9-anthracenecarboxylic acid: The structural diversity in organotin 9-anthracenecarboxylates

The di- and triorganotin(IV) derivatives of anthracenecarboxylic acid, Ph₂MeSnOC(O)C₁₄H₉ (2), Me₃SnOC(O)C₁₄H₉ (3), Me₂Sn[OC(O)C₁₄H₉]₂ · CH₃OH (4) Ph₃SnOC(O)C₁₄H₉ · CH₃OH (5), Ph₂EtSnOC(O)C₁₄H₉ (6), Ph₂Sn[OC(O)(C₁₄H₉)]₂ (7) and PhMe₂SnOC(O)C₁₄H₉ (8) were synthesized by the reaction of Ph₂MeSnI, Me₃SnCl, Me₂SnCl₂, Ph₃SnCl, Ph₂EtSnI, Ph₂SnCl₂, and PhMe₂SnI with 9-anthracenecarboxylic acid, respectively, with the aid of potassium iso-propoxide. All complexes were characterized by elemental analysis, mass spectrometry, IR, ¹H, ¹³C and ¹¹⁹Sn NMR spectroscopes. The molecular structures of complexes 2, 3 and 4 were determined by single crystal X-ray analysis. The X-ray structures reveal that complex 2 and 3 adopt a polymeric trans-C₃SnO₂ trigonal bipyamidal configuration with the oxygen atoms occupying axial positions. Complex 4 adopts a monomeric structure with two carboxylates coordinated to tin in a monodentate form from axial and equatorial positions, and with the coordination number raised to five as the methanol occupies the apical position of the trigonal bipyramid.     

Organotin flufenamates: Synthesis, characterization and antiproliferative activity of organotin flufenamates

The organotin flufenamates [Me₂(flu)SnOSn(flu)Me₂]₂ (1), [Bu₂(flu)SnOSn(flu)Bu₂]₂ (2) and [Bu₂Sn(flu)₂] (3) have been prepared and structurally characterized by means of vibrational and NMR (¹H, ¹³C and ¹¹⁹Sn) spectroscopy. The crystal structure of [Me₂(flu)SnOSn(flu)Me₂]₂ (1) has been determined by X-ray crystallography. Three distannoxane rings are present to the dimeric tetraorganodistannoxane of planar ladder arrangement. The structure is centro-symmetric and features a central rhombus Sn₂O₂ unit with two additional tin atoms linked at the O atoms. Six-coordinated tin centers are present in the dimer distannoxane. This structure is self-assembled via π → π and C-H → π stacking interactions. Flufenamic acid and flufenamates were evaluated for antiproliferative activity in vitro. Among the compounds tested [Bu₂(flu)SnOSn(flu)Bu₂]₂ (2) and [Bu₂Sn(flu)₂] (3) exhibited high cytotoxic activity against the cancer cell line A549 (non-small cell lung carcinoma).     

Synthesis,characterization, and biological activity of some lanthanide ternary complexes

Five complexes have been synthesized by the reaction of lanthanide(III) nitrate with 2-thenoyltrifluoroacetone (HTTA) and p-hydroxybenzoic acid (L). The complexes have been characterized by elemental analysis, molar conductivity, FT-IR, UV-Vis, ¹H NMR, TG-DTA, XPS, and transmission electron microscope. The general formula of the complexes is Na[Ln(TTA)₃L] (Ln?=?La³⁺,?Ce³⁺,?Nd³⁺,?Eu³⁺,?Er³⁺). The antibacterial activities indicate that all five complexes exhibit antibacterial ability against Escherichia coli and Staphylococcus aureus with broad antimicrobial spectrums. The antitumor activity of the five complexes against K562 tumor cell in vitro is measured using methyl thiazolyl tetrazolium (MTT) colorimetry. The results show that the complexes induce K562 tumor cell apoptosis, and the complexes exhibit inhibitory effect on leukemia K562 cells.     

Synthesis,characterization, semi-empirical study,and biological activities of organotin(IV) complexes with cyclohexylcarbamodithioic acid as biological active ligand

Cyclohexylcarbamodithioic acid has been synthesized by the reaction of cyclohexylamine with carbon disulfide at room temperature. Its complexes have been synthesized by the reaction of cyclohexylcarbamodithioic acid with organotin(IV) chlorides in 1?:?1/1?:?2 molar ratio. The ligand and complexes have been characterized by elemental analysis, infrared (IR), and multinuclear (¹H, ¹³C, and ¹¹⁹Sn) NMR spectroscopy. Elemental data show good agreement between calculated and found values of carbon, hydrogen, nitrogen, and sulfur. IR data show that the ligand is bidentate and complexes exhibit a five-coordinate geometry in the solid state, which is also confirmed by semi-empirical studies. NMR data show that the complexes exhibit tetrahedral geometry in solution state. The ligand and its complexes were screened for their in vitro mutagenic, antimicrobial, MIC, antioxidant activities, and cytotoxicity. Biological screening data demonstrate that complexes show significant activity against various bacterial and fungal strains and are good antioxidants. The cytotoxicity data show positive lethality for complexes as compared to ligand and can play a very significant role in drug development.     

Synthesis, characterization and hydrolytic behavior of new bis(2-pyridylthio)acetate ligand and related organotin(IV) complexes

The new sodium bis(2-pyridylthio)acetate ligand, Na[(pyS)₂CHCO₂], has been prepared in ethanol solution using 2-mercaptopyridine, dibromoacetic acid and NaOH. New mono- and di-organotin(IV) derivatives containing the anionic bis(2-pyridylthio)acetate have been synthesized from reaction between SnR_nCl_4−n (R = Me, Ph and ⁿBu, n = 1-2) acceptors and Na[(pyS)₂CHCO₂]. Mono-nuclear complexes of the type {[(pyS)₂CHCO₂]R_nSnCl_4−n−1} have been obtained and characterized by elemental analyses, FT-IR, ESI-MS, multinuclear (¹H and ¹¹⁹Sn) NMR spectral data and X-ray crystallography. ESI-MS spectra of methanol solution of the complexes show the existence of hydrolysed species. Attempts to crystallize the dimethyltin(IV) derivative (3), from acetonitrile solution yield the dimeric dicarboxylatotetramethyldistannoxane (8), which was characterized by single crystal diffraction analysis.     

Synthesis, spectral characterization and biological studies of some organotin(IV) complexes of L-proline, trans-hydroxy-L-proline and L-glutamine

New organotin(IV) complexes of the general formula R3Sn(L) (where R=Me, n-Bu and HL=L-proline; R=Me, Ph and HL=trans-hydroxy-L-proline and L-glutamine) and R2Sn(L)2 (where R=n-Bu, Ph and HL=L-proline; R=Ph, HL=trans-hydroxy-L-proline) have been synthesized by the reaction of RnSnCl(4-n) (where n=2 or 3) with sodium salt of the amino acid (HL). n-Bu2Sn(Pro)2 was synthesized by the reaction of n-Bu2SnO with L-proline under azeotropic removal of water. The bonding and coordination behavior in these complexes have been discussed on the basis of IR and 119Sn M?ssbauer spectroscopic studies in the solid-state. Their coordination behavior in solution has been discussed with the help of multinuclear (1H, 13C and 119Sn) NMR spectral studies. The 119Sn M?ssbauer and IR studies indicate that L-proline and trans-hydroxy-L-proline show similar coordination behavior towards organotin(IV) compounds. Pentacoordinate trigonal-bipyramidal and hexacoordinate octahedral structures, respectively, have been proposed for the tri- and diorganotin(IV) complexes of L-proline and trans-hydroxy-L-proline, in which the carboxylate group acts as bidentate group. L-glutamine shows different coordination behavior towards organotin(IV) compounds, it acts as monoanionic bidentate ligand coordinating through carboxylate and amino group. The triorganotin(IV) complexes of L-glutamine have been proposed to have trigonal-bipyramidal environment around tin. The newly synthesized complexes have been tested for their antiinflammatory and cardiovascular activities. Their LD50 values are >1000 mg kg-1.     

Macrocyclic organotin(IV) carboxylates based on benzenedicarboxylic acid derivatives: Syntheses, crystal structures and antitumor activities

Six new organotin carboxylates based on 1,3-benzenedicarboxylic acid and 1,4-benzenedicarboxylic acid derivatives, namely (Ph₃Sn)₂(2,5-L¹)(C₂H₅OH)₂ (1) (2,5-H₂L¹ = 2,5-dibenzoylterephthalic acid), (Ph₃Sn)₂(2,5-L²)(C₂H₅OH)₂ (2) (2,5-H₂L² = 2,5-bis(4-methylbenzoyl)terephthalic acid), (Ph₃Sn)₂(2,5-L³)(C₂H₅OH)₂ (3) (2,5-H₂L³ = 2,5-bis(4-ethylbenzoyl)terephthalic acid), [(n-Bu₂Sn)₄(4,6-L¹)O₂(OH)(OC₂H₅)]₂·2(C₂H₅OH) (4) (4,6- H₂L¹ = 4,6-dibenzoylisophthalic acid), [(n-Bu₂Sn)₄(4,6-L¹)O₂(OH)(OC₄H₉)]₂·2(C₄H₉OH) (5) and [(n-Bu₂Sn)₄(4,6-L²)O₂(OH)(OC₂H₅)]₂·2(C₂H₅OH) (6) (4,6-H₂L² = 4,6-bis(4-methylbenzoyl)isophthalic acid), have been synthesized. All the organotin carboxylates have been characterized by elemental analysis, IR, ¹H and ¹³C NMR spectroscopy and X-ray crystallography diffraction analyses. The structural analysis reveals that complexes 1-3 show similar structures, containing binuclear triorganotin skeletons. The significant intermolecular O-H?O hydrogen bonds linked the complexes 1-3 to form a novel 2D network polymer with 38-member macrocycles. In complexes 4-6, two Sn₄O₄ ladders are connected by two 1,3-benzenedicarboxylic acid derivatives to yield ladder-like octanuclear architectures and form macrocycle with 24 atoms. In addition, the antitumor activities of complexes 1-6 have been studied.     

Synthesis,characterization, semi-empirical study,and biological activities of organotin(IV) and transition metal complexes with o-methyl carbonodithioate

Three transition metal and six organotin(IV) complexes have been synthesized by treating potassium o-methyl carbonodithioate with ZnCl₂/CdCl₂/HgCl₂ and R₂SnCl₂/R₃SnCl under stirring. The complexes were characterized by IR, ¹H, and ¹³C NMR spectroscopies. IR results show that the ligand is bidentate in 1–3 while monodentate in 4–9, which is also confirmed by semi-empirical study. NMR data reveal four-coordinate geometry in solution. HOMO–LUMO study shows that 7 and 9 are thermodynamically unstable. The enzyme inhibition study shows that 1 is a potent inhibitor of ALP, EC 3.1.3.1, resulting in very slow rate of formation and breakdown of enzyme–substrate complex. UV/visible spectroscopy was used to assess the mode of interaction and binding of the complexes with DNA which shows that 9 exhibits higher binding constant when compared to 6. In protein kinase inhibition assay, 1 was active, while antifungal activity shows that organotin(IV) complexes are more active than transition metal complexes.