Dibenzyltin(IV) complexes of the 5-[(E)-2-(aryl)-1-diazenyl]quinolin-8-olates: Synthesis and an investigation of structures by X-ray diffraction, solution and solid-state tin NMR, Sn Mössbauer and electrospray ionization MS

A series of cis-bis{5-[(E)-2-(aryl)-1-diazenyl]quinolinolato}dibenzyltin(IV) complexes have been synthesized by reacting sodium salts of 5-[(E)-2-(aryl)-1-diazenyl]quinolin-8-ol (LH) and dibenzyltin dichloride. These complexes have been characterized by ¹H, ¹³C, ¹¹⁹Sn NMR, ESI-MS in solution and by IR and ^119mSn Mössbauer, ¹¹⁷Sn CP-MAS NMR spectroscopy in solid state. In addition, the structures of three of the dibenzyltin(IV) complexes, viz., Bz₂Sn(L²)₂ (2), Bz₂Sn(L³)₂ (3), and Bz₂Sn(L⁵)₂ (5) (L = 5-[(E)-2-(aryl)-1-diazenyl]quinolin-8-ol: aryl = 4′-methylphenyl- (L²H), 4′-methoxylphenyl- (L³H) and 4′-bromophenyl- (L⁵H)) were determined by single-crystal X-ray diffraction. In general, the complexes were found to adopt a distorted cis-octahedral arrangement around the tin atom in both solution and solid state.     

A cationic mononuclear and a neutral trinuclear boron compound derived from boric acid and N2O2-type ligands of the Salan class

Four different ligands of the Salan class have been prepared and reacted with boric acid. Reaction of saleanH₄ (saleanH₄ = N,N′-bis(o-hydroxybenzyl)-1,2-diaminoethane) with three equivalents of boric acid gave a neutral trinuclear boron complex containing two four-coordinate and one three-coordinate boron atom involved in a system of four heterocyclic rings of the composition {C₃BNO}, {C₂B₂N₂O} and {B₃O₃}. The salceanH₄ ligand (salceanH₄ = N,N′-bis(o-hydroxybenzyl)-trans-1,2-diaminocyclohexane) gave a so far unknown mononuclear boronium complex of the general formula [(RO)₂B(NR′R′′)₂]⁺. Both compounds might have applications, the trinuclear species as Lewis acid catalyst and the borocation as positively charged counterion for voluminous anions. With salpanH₄ (salpanH₄ = N,N′-bis(o-hydroxybenzyl)-1,3-diaminopropane) and salophanH₄ (salophanH₄ = N,N′-bis(o-hydroxybenzyl)-1,2-diaminobenzene) only unseparable product mixtures of oligo- and/or polymeric boron complexes could be obtained.     

Diphenyltin(IV) complexes of the 5-[(E)-2-(aryl)-1-diazenyl]quinolin-8-olates: Synthesis and multinuclear NMR, Sn Mössbauer, electrospray ionization MS, X-ray characterization and assessment of in vitro cytotoxicity

A series of cis-bis{5-[(E)-2-(aryl)-1-diazenyl]quinolinolato}diphenyltin(IV) complexes have been synthesized and characterized by ¹H, ¹³C, ¹¹⁹Sn NMR, ESI-MS, IR and ^119mSn Mössbauer spectroscopic techniques in combination with elemental analysis. The structures of a ligand L⁶H (i.e., 5-[(E)-2-(4-ethoxyphenyl)-1-diazenyl]quinolin-8-ol) and three diphenyltin(IV) complexes, viz., Ph₂Sn(L¹)₂ · (CH₃)₂CO (1), Ph₂Sn(L⁴)₂ (4) and Ph₂Sn(L⁵)₂ (5) (L = 5-[(E)-2-(aryl)-1-diazenyl]quinolin-8-ol: aryl = phenyl - (L¹H); 4′-methylphenyl - (L⁴H) and 4′-bromophenyl - (L⁵H)) were determined by single crystal X-ray diffraction. In general, the complexes were found to adopt a distorted cis-octahedral arrangement around the tin atom. These complexes retain their solid-state structure in non-coordinating solvent as evidenced by ¹¹⁹Sn NMR spectroscopic results. The in vitro cytotoxicity of 1 is reported and compared with Ph₂Sn(Ox)₂ (Ox = deprotonated quinolin-8-ol) against seven well characterized human tumor cell lines.     

Preparation and structural characterization of [Ph3Sn(IV)] complexes with pyridine-carboxylic acids or hydroxypyridine, -pyrimidine and -quinoline

A number of [Ph₃Sn(IV)]⁺ complexes formed with ligands containing -OH (-CO), or -COOH group(s) and aromatic {N} donor atom have been prepared. The binding sites of the ligands were identified by FT-IR spectroscopic measurements. In the complexes containing hydroxy and carboxylate functions, the carboxylato group is coordinated to the organotin(IV) centres in monodentate or bridging bidentate manner. It was also found that in the hydroxypyridine and -pyrimidine complexes the [Ph₃Sn(IV)]⁺ moiety in most cases reacts with the phenolic form of the ligands. The rationalisation of the experimental ¹¹⁹Sn Mössbauer nuclear quadrupole splittings, |Δ_exp| - according to the point charge model formalism - together with the FT-IR data support the formation of trigonal bipyramidal (Tbp) or octahedral (O_h) molecular structures. Furthermore, X-ray diffraction analysis has been performed on the triphenyltin(IV)-3-phenolato-2(1H)-pyridinone-O,O′ single crystals. The penta-coordinated tin center exhibits a Tbp geometry. In case of 2-picolinic acid, a trans-phenylation was observed during the complexation, resulting [Ph₂Sn(IV)]²⁺ complex and Ph₄Sn(IV).     

Dendritic BINOL ligands for asymmetric catalysis: effect of the linking positions and generations of the dendritic wedges on catalyst properties

Three types of new chiral BINOL ligands (2, 3 and 4) bearing dendritic wedges have been synthesized through coupling reaction between 3-hydroxymethyl-2,2′-bis(methoxymethyl)-1,1′-binaphthol (7), 6,6′-dihydroxymethyl-2,2′-bis(methoxymethyl)-1,1′-binaphthol (12), 6-hydroxymethyl-2,2′-bis(methoxymethyl)-1,1′-binaphthol (15) and Fréchet-type polyether dendritic benzyl bromide, followed by deprotection of methoxymethyl groups by ⁱPrOH/HCl, respectively. These new ligands obtained were assessed in enantioselective Lewis acid-catalyzed addition of diethylzinc to benzaldehyde. Compared to the enantioselectivity observed with dendrimer 1 bearing the dendritic wedges at 3,3′-positions of the binaphthyl backbone, higher enantioselectivity for all these ligands was observed. Difference in the effect of linking positions and generations on enantioselectivity and/or activity for all three kinds of dendritic ligand-derived catalysts was observed. Among these dendritic ligands, (R)-3/Ti(IV) catalyst with the dendritic wedges at 6,6′-positions of BINOL gave the highest enantioselectivity (up to 87% ee).     

Structure and conformational motion of seven-coordinate diorganotin(IV) complexes derived from salen and salan type ligands

Reaction of R₂SnCl₂ (R = Me, nBu, Ph) and the potassium salts of salenN₃H₃ (N,N′-bis(salicylidene)diethylenetriamine) and saleanN₃H₅ (N,N′-bis(o-hydroxybenzyl)diethylenetriamine) provided diorganotin(IV) complexes of the composition [Me₂Sn(salenN₃H)]·solvate (solvate = 2.5H₂O, MeOH or DMSO), [nBu₂Sn(salenN₃H)]·H₂O, [Ph₂Sn(salenN₃H)]·2EtOH and [Me₂Sn(saleanN₃H₃)]·2.5H₂O. In all compounds the tin atoms are seven-coordinate and have pentagonal-bipyramidal coordination environments, in which the organic substituents attached to the tin atoms occupy the axial positions. This occurs both in solution and the solid state; however, in solution the molecules are involved in conformational equilibria that require the presence of intermediates, in which the N → Sn bonds are dissociated. Although the [saleanN₃H₃]²⁻ ligand is more flexible and basic, a very similar complexing behavior to that of [salenN₃H]²⁻ has been found, and there is evidence that it is even a weaker ligand. Both ligands show the tendency to adopt a curved conformation within the complex, thus indicating that the dynamic process resembles the flapping of butterfly wings. However, the folding is reduced with increasing steric bulk of the organic substitutents attached to the tin atoms. The six-membered heterocyclic rings in the [R₂Sn(salenN₃H)] derivatives have envelope conformation, while those in [Me₂Sn(saleanN₃H₃)] have distorted boat-conformation. Thus, small changes in the hybridization and basicity of the nitrogen atoms cause significant differences of the stability and the dynamic behavior of the resulting molecules.     

New di- and triorganotin(IV) complexes of tripodal Schiff base ligand containing three imidazole arms: Synthesis, structural characterization, anti-inflammatory activity and thermal studies

Some new tri- and diorganotin(IV) complexes of the general formula, R₃Sn(H₂L) and R′₂Sn(HL) [where R = Me, n-Pr, n-Bu and Ph; R′ = Me, n-Bu, Ph and n-Oct; H₃L = Schiff base (abbreviated as tren(4-Me-5-ImH)₃) derived from condensation of tris(2-aminoethyl)amine (tren) and 4-methyl-5-imidazolecarboxaldehyde (4-Me-5-ImH)] have been synthesized. The coordination behaviour of Schiff base towards organotin(IV) moieties is discussed on the basis of infrared and far-infrared, ¹¹⁹Sn Mössbauer and multinuclear (¹H, ¹³C and ¹¹⁹Sn) magnetic resonance (NMR) spectroscopic studies. Thermal studies of all of the synthesized organotin(IV) complexes have been carried out using TG, DTG and DTA techniques. The residues thus obtained from pyrolysis of the studied complexes have been characterized by X-ray powder diffraction analysis and IR. The newly synthesized complexes have been tested for their anti-inflammatory activity and toxicity (LD₅₀).     

Scalable synthesis of substituted 2,7-dimethyl-9-phenylxanthen-9-ol (DMPx-OH): useful for the preparation of crystalline 5′-O-DMPx-protected nucleosides

A convenient single-step synthesis of several 2,7-dimethyl-9-phenylxanthen-9-ol (DMPx-OH) analogs has been accomplished using a Friedel-Crafts reaction. Treatment of various DMPx-OH with unprotected 2′-O-methoxyethyl-ribonucleosides (MOE) in the presence of B(C₆F₅)_3, as a Lewis Acid catalyst, furnished 5′-O-protected derivatives of 2′-MOE-ribonucleosides in good yields. The deprotection of the DMPx groups was accomplished by acid hydrolysis under very mild conditions. Among the five DMPx analogs synthesized, the 2,7-dimethyl-9-(4-nitrophenyl)xanthene-9-yl group furnished crystalline products enabling non-chromatographic isolation of 5′-O-protetced nucleosides.     

Regioselective synthesis of optically active (pyrazolyl)pyridines with adjacent quaternary carbon stereocenter: chiral N,N-donating ligands

Novel optically active 2-(pyrazol-1-yl)pyridines have been prepared using resolved the O-methyl ether of atrolactic acid as a source of the adjacent quaternary carbon stereocenter. Different regioisomers were formed selectively in the reaction of 2-hydrazinopyridines with the chiral 1,3-diketone and in the nucleophilic substitution of 2-chloropyridines with the potassium salt of the chiral pyrazole. The second route gave 2-(pyrazol-1-yl)pyridines with the stereogenic center neighboring the coordinating nitrogen in the pyrazole ring. Also, new C₂-symmetric chiral ligands based on 2,6-bis(pyrazolyl)pyridine and 6,6′-bis(pirazolyl)-2,2′-bipyridine structures were obtained.     

C-O and C-C bond formation in the cyclisation of gem-(dialkoxymethyl)-1,6-dienes catalysed by tin(IV) triflimidate at room temperature

We described herein a Sn(NTf₂)₄-catalysed cyclisation of gem-(dialkoxymethyl)-1,6-dienes and derivatives where cyclohexane or tetrahydrofuran rings are formed following either a 6-enexo-endo-trig process or a 5-exo-trig process, respectively, depending on substitution patterns. The latter process features an unusual dealkylative ether cyclisation, triggered by the strong Lewis acid character of the tin(IV) triflimidate catalyst.     

New optically active organoantimony (BINASb) and bismuth (BINABi) compounds comprising a 1,1′-binaphthyl core: synthesis and their use in transition metal-catalyzed asymmetric hydrosilylation of ketones

Racemic 2,2′-bis[diarylstibano]-1,1′-binaphthyls [(±)-BINASbs] and 2,2′-bis[di(p-tolyl)bismuthano]-1,1′-binaphthyl [(±)-BINABi], which are the antimony and bismuth congeners of BINAP, have been prepared from 2,2′-dibromo-1,1′-binaphthyl (DBBN) via 2,2′-dilithio-1,1′-binaphthyl intermediate by treatment with the appropriate metal halides [(p-Tol)₂SbBr, Ph₂SbBr and (p-Tol)₂BiCl]. The optical resolution of the (±)-BINASbs could be achieved via the separation of a mixture of the diastereomeric Pd-complexes derived from the reaction of (±)-BINASbs with di-μ-chlorobis{(S)-2-[1-(dimethylamino)-ethyl]phenyl-C¹,N}dipalladium(II). Optically active (R)-BINASb and (R)-BINABi could be also obtained from optically active (R)-DBBN by the same procedure. The enantiopure BINASbs have been shown to be effective chiral ligands for the rhodium-catalyzed asymmetric hydrosilylation of ketones.     

From oxides of internal perfluoroolefins to fluorocontaining camphor thiazolinylhydrazones

The reaction of oxides of internal trans- and cis-perfluoroolefins with (1S, 4S)- or racemic camphor thiosemicarbazone leads to the formation of trans- and cis-isomers of (1S, 4S)- or racemic camphor 5′-fluoro-4′-hydroxy-4′,5′-di(perfluoroalkyl)-1′,3′-thiazolinyl-2′-hydrazones, respectively. Unsymmetrical dodecafluoro-2,3-epoxyhexane yields a mixture of regioisomeric hydrazones. The molecular structure of the trans-isomer of (1S, 4S)-camphor 5′-fluoro-4′-hydroxy-4′,5′-bis(trifluoromethyl)-1′,3′-thiazolinyl-2′-hydrazone has been established by X-ray crystallography. The quite rare example of cocrystallization of two diastereomers of the latter in homochiral crystal (sp. group P2₁) has been revealed.     

Synthesis of 2,5-bis{(diethyl-3′-indolyl)methyl}furan and its N,N′-dimetallated complexes (lithium, sodium and potassium): X-ray crystal structures of 2,5-bis{(diethyl-3′-indolyl)methyl}furan and the polymeric tetrahydrofuran adduct of the dilithiated complex

The synthesis of 2,5-bis{(diethyl-3′-indolyl)methyl}furan by the acid catalysed condensation of 2,5-bis(diethylhydroxymethyl)furan with indole is presented. Dilithium, disodium and dipotassium derivatives are prepared by the reaction of the bis(indole) with n-BuLi, NaH and K, respectively, in the presence of various Lewis bases. The X-ray structures of 2,5-bis{(diethyl-3′-indolyl)methyl}furan and the dilithiated derivative (as a polymeric tetrahydrofuran adduct) are reported.     

Synthesis and characterization of the first diorganotin(IV) complexes containing mixed arylazobenzoic acids and having skew trapezoidal bipyramidal geometry

Three diorganotin(IV) complexes of the type, [R₂Sn(L^aH)(L^bH)] (R = ⁿBu or Me and, L^aH and L^bH are two different 5-[(E)-2-(aryl)-1-diazenyl]-2-hydroxybenzoate residues; a: aryl = 4′-Cl-(held constant) and b: aryl = 4′-Me or 4′-Br) have been prepared either by reacting ⁿBu₂SnO, L^aHH′ and L^bHH′ (1:1:1) in anhydrous toluene or by reacting Me₂SnCl₂, L^aHNa and L^bHNa (1:1:1) in anhydrous methanol. The products were characterized by microanalysis, IR, NMR (¹H, ¹³C, ¹¹⁹Sn) and ^119mSn Mössbauer spectroscopy. A full characterization of the structures of the complexes [ⁿBu₂Sn(L^aH)(L^bH)] (1 and 2) and [Me₂Sn(L^aH)(L^bH)] (3) in the solid state were accomplished by single crystal X-ray crystallography. These complexes were found to adopt the usual dicarboxylato structural type with a skew-trapezoidal bipyramidal arrangement around the tin atom.     

Metalloporphyrins as chemical shift reagents: the unambiguous NMR characterization of the cis- and trans-isomers of meso-(bis)-4′-pyridyl-(bis)-4′-carboxymethylphenylporphyrins

The condensation of pyrrole with 4-pyridylcarboxyaldehyde and methyl 4-formyl benzoate under Adler-Longo conditions yielded the series of meso-(4′-pyridyl)/(4′-carboxymethylphenyl)porphyrins as a mixture. Careful column chromatography afforded each isomer in pure form. In this paper we focus on the two bis-substituted isomeric meso-porphyrins, 5,10-bis(4′-pyridyl)-15,20-bis(4′-carboxymethylphenyl)porphyrin and 5,15-bis(4′-pyridyl)-10,20-bis(4′-carboxymethylphenyl)porphyrin, respectively, 4′-cis and 4′-transDPyDMeP. The assignment of the geometry of the two isomers was performed by ¹H NMR spectroscopy on the trinuclear adducts [(4′-cisDPyDMeP){Ru(TPP)(CO)}₂] and [(4′-transDPyDMeP){Ru(TPP)(CO)}₂], obtained by selective coordination of [Ru(TPP)(CO)(EtOH)] (TPP=tetraphenylporphyrin) to the peripheral nitrogen atoms. The axially bound ruthenium porphyrins act as chemical shift reagents on the central porphyrin, allowing a clear distinction of the pyrrole proton resonances and consequent unambiguous assignment of the geometry of each isomer based upon symmetry considerations.     

Selective synthesis of Neu5Ac2en and its oxazoline derivative using BF3·Et2O

Application of the Lewis acid BF₃·Et₂O to the selective synthesis of 5-acetamido-2,6-anhydro-3,5-dideoxy-d-glycero-d-galacto-non-2-enonic acid (Neu5Ac2en) and the related oxazoline, methyl 7,8,9-tri-O-acetyl-2,3,4,5-tetradeoxy-2,3-didehydro-2,3-trideoxy-4′,5′-dihydro-2′-methyloxazolo[5,4-d]- d-glycero-d-talo-non-2-enonate is described.     

New di- and triorganotin(IV) derivatives of tyrosinylphenylalanine as models for metal-protein interactions: Synthesis and structural characterization. Crystal structure of Me2Sn(Tyr-Phe) · MeOH

New di- and triorganotin(IV) derivatives of tyrosinylphenylalanine (H₂Tyr-Phe) with general formulae R₂Sn(Tyr-Phe) where R = Me,n-Bu, n-Oct and Ph, and R₃^′Sn(HTyr-Phe) where R^′ = Me and Ph have been synthesized. The bonding and coordination behaviour in these derivatives are discussed on the basis of FT-IR, multinuclear ¹H, ¹³C and ¹¹⁹Sn NMR and ¹¹⁹Sn Mössbauer spectroscopic studies. These investigations suggest that dipeptide in R₂Sn(Tyr-Phe) acts as dianionic tridentate coordinating through −C(O)O⁻, -NH₂ and (-CO)N⁻_peptide groups while in case of R^′₃Sn(HTyr-Phe) the ligand acts as monoanionic bidentate coordinating through -C(O)O⁻ and -NH₂, and the polyhedron around tin in R₂Sn(Tyr-Phe) and R^′₃Sn(HTyr-Phe) is a distorted trigonal-bipyramidal. It is further confirmed by the single crystal X-ray structure of Me₂Sn(Tyr-Phe) · MeOH which shows two methyl groups and peptide nitrogen (N⁻_peptide) in the equatorial positions, while the two axial positions are occupied by the carboxylic oxygen (O⁻_carboxyl) and the amino nitrogen (N_amino) atom from the same ligand molecule. One methanol molecule is also present in the asymmetric unit.     

A general synthetic route to chiral dihydroxy-9,9′-spirobifluorenes

C₂-Symmetric 9,9′-spirobifluorenes with 2,2′-, 3,3′-, and 4,4′-dihydroxyls were conveniently prepared from 1,2-dibromobenzene. The palladium-catalyzed coupling reaction of 1,2-dibromobenzene with methoxyphenylmagnesium bromide or methoxyphenylboronic acid provided methoxy substituted 2-bromobiphenyls. Lithium-bromine exchange with n-butyllithium, followed by reaction with dimethyl carbonate afforded di[2-(methoxyphenyl)phenyl]ketones as the key intermediates. A continuous ring-closure induced by a strong Lewis acid and demethylation gave dihydroxy-9,9′-spirobifluorenes. The racemic dihydroxy products were resolved by inclusion crystallization using chiral resolving reagents or separated by chiral HPLC.     

Synthesis and characterization of a tetraruthenium butterfly cluster containing a quadruply-bridging ligand derived from an N,N′-dipyrid-2-ylurea

The tetraruthenium cluster complex [Ru₄(μ₄-κ⁴-dmpu)(CO)₁₀], H₂dmpu = N,N′-bis(6-methylpyrid-2-yl)urea, has been prepared by treating [Ru₃(CO)₁₂] with H₂dmpu in toluene at reflux temperature. An X-ray diffraction study has determined that this cluster has a butterfly metallic skeleton hold up by a doubly-deprotonated N,N′-bis(6-methylpyrid-2-yl)urea ligand (dmpu). This ligand has the pyridine N atoms attached to the wing-tip Ru atoms and the amido N atoms spanning Ru-Ru wing-edges, in such a way that the cluster has C₂ symmetry. The donor atoms of doubly-deprotonated N,N′-dipyrid-2-ylureas seem to be appropriately arranged to hold butterfly tetranuclear clusters.     

New organotin(IV) complexes with l-Arginine, Nα-t-Boc-l-Arginine and l-Alanyl-l-Arginine: Synthesis, structural investigations and cytotoxic activity

Novel diorganotin(IV) derivatives of l-Arginine (HArg), N_α-(tert-Butoxycarbonyl)-l-Arginine (Boc-Arg-OH) and l-Ala-l-Arg (H₂Ala-Arg), H₂NC(NH)NH(CH₂)₃CH(NHR′)CO₂H, where R′ = H in HArg, R′ = C(O)OC(CH₃)₃ in Boc-Arg-OH, R′ = H₂NCH(CH₃)CO in H₂Ala-Arg and triorganotin(IV) derivatives of Boc-Arg-OH have been synthesized and structurally characterized. The complexes were investigated by FT-IR and ¹¹⁹Sn Mössbauer in the solid state and by ¹H, ¹³C, ¹¹⁹Sn and ¹H-¹H COSY NMR spectroscopy, in solution. The spectroscopic characterization leading to the proposed molecular structures was accomplished on the basis of these experiments. l-Arginine appears to behave as a chelating ligand through carboxylate and -NH₂ groups in Me₂Sn(Arg)₂, while in N_α-t-Boc-l-Arginine complex, the N_α-protected amino group being exempted from coordination, only the carboxylate groups are effectors of bonding to the organometallic moieties. FT-IR spectra give a clear indication that guanidino groups in all the complexes are not involved in coordination, since ν(CN-H) frequency of the terminal guanidino group is fairly constant and unshifted relative to the free ligand. The biological activity of organotin(IV)-complexes was also investigated by use of human HT29 colorectal carcinoma cells. The cytotoxic activity of the compounds was determined by the MTT quantitative colorimetric assay, capable of detecting viable cells in comparison with that exerted by cisplatin. A marked cytotoxic activity for nearly all complexes, is evident being higher than that exerted by cisplatin, while no significant improvement of activity was observed for Me₂Sn(Arg)₂ and Me₂Sn(Ala-Arg), which was confirmed by IC₅₀ values. Then, we assessed whether the cytotoxicity induced by organotin(IV) complexes was associated with the induction of apoptosis. Light microscopy analysis, performed to study the morphological changes induced in HT29 cells, confirmed the results obtained with MTT test. No significant morphological alterations were observed in HT29 cells after treatment with Me₂Sn(Ala-Arg) and Me₂Sn(l-Arg)₂. Cells treated with ⁿBu₂Sn(Boc-Arg)₂, ⁿBu₂Sn(Ala-Arg), ⁿBu₃Sn(Boc-Arg) and Me₃Sn(Boc-Arg), appeared rounded, isolated and detached from culture substrate, indicating the commitment to apoptotic cell death.