Tin-119 NMR Studies on adduct formation and stereochemistry of organoyltin(IV)trihalides

qazTin-119 and phosphorus-31 NMR spectra have been recorded for a series of adducts of RSnX₃ (R  Me, Ph; X  Cl, Br) with halide, tributylphosphine (P) and tributylphosphine oxide (L). The adducts were either 1:1 five coordinate or 1:2 six coordinate complexes. The tin-ll9 NMR spectra of mixtures of corresponding chloro and bromo complexes reveal, in most cases, all possible mixed halide species but much additional structural information is obtained from these spectra which could not be extracted from the spectra of individual compounds themselves. Thus in some cases, in the five coordinate species the Berry pseudorotation between isomers within a particular stoichiometry could be slowed on the NMR timescale which allowed a determination of the molecular structure. An equimolar mixture of [PhSnCl₅]²⁻ and [PhSnBr₅]²⁻ shows eleven of the twelve geometries possible for [PhSnCl_xBr_5−x]²⁻. In the six coordinate series [RSnX₄P]⁻ the tin-119 NMR spectra of the mixtures of [RSnCl₄P]⁻ and [RSnBr₄P]⁻ allow the geometry to be determined as trans. Application of the pairwise additivity model for calculation of the tin-119 chemical shift positions for the mixed halide systems are discussed.     

31P and 119Sn NMR Spectra of Complexes of Diphenyltin(IV)dichloride with Tri(n-octyl)phosphine Oxide

The ³¹P and ¹¹⁹Sn NMR spectra of the system diphenyltin(IV)-dichloride-tri(n-octyl)phosphine oxide, deuteriochloroform, were studied. The existence of the compound Ph₂SnCl₂·L (L=(n-C₈H₁₇)₃PO) and five isomers of the compound Ph₂SnCl₂·2L was revealed.     

Synthesis and structural studies by infrared and Mössbauer spectroscopy of adducts of tin(IV) and organotin(IV) derivatives with 2,2′-azopyridine

A number of complexes have been prepared by the reaction between 2,2′-azopyridine(AZP) and tin(IV) halides and organotin(IV) halides, and characterized by elemental analysis and infrared and variable temperature ¹¹⁹Sn Mössbauer spectroscopies. All of the new compounds have 1:1 stoichiometry, with the AZP ligand occupying two coordination sites by bonding through one of the ring and one of the azo group nitrogen atoms, to give rise to distorted octahedral structures. In the diorganotin complexes the two organic groups occupy trans positions. The infrared and Mössbauer spectroscopic data suggest that these compounds are monomeric in the solid state.     

Tellurium-125 NMR of Te(II) and Te(IV) dithiocarbamates

¹²⁵Te chemical shifts for Te(R₂NCS₂)₂ and Te(R₂NCS₂)₄ compounds were found to be separated by ca. 1400 ppm. When R is an alkyl group, the electronic contributions to the chemical shifts appear to be very small for both oxidation states of tellurium. The chemical shifts of these compounds display a positive temperature dependence consistent with the major contributions arising from paramagnetic shielding.     

cis-1,4-diaminocyclohexane-Pt(II) and -(IV) adducts with DNA bases and nucleosides

A series of new platinum(II) and platinum(IV) adducts of type [P(II)(cis-1,4-DACH)LCl]NO(3,) where cis-1,4-DACH=cis-1,4-diaminocyclohexane, and L=9-ethylguanine, 1-methylcytosine, adenine, adenosine, cytosine, cytidine, guanine, and [Pt(IV)(cis-1,4-DACH)Ltrans-(X)(2)Cl]NO(3), (where Y=hydroxo or acetato), were synthesized and characterized by elemental analysis, infrared spectroscopy, and 1H and 195Pt nuclear magnetic resonance spectroscopy.     

31P NMR and computational studies on stereochemistry of conversion of phosphoramidate diesters into the corresponding phosphotriesters

31P NMR spectroscopy was used to investigate a stereochemical course of a nitrite-promoted conversion of phosphoramidate diesters into the corresponding phosphotriesters. It was found that this reaction occurred with almost complete epimerization at the phosphorus center and at the C1 atom in the amine moiety. On the basis of the 31P NMR data, a plausible mechanism for the reaction was proposed. The density functional theory calculation of the key step of the reaction, i.e., breaking of the P-N bond and formation of the P-O bond, suggested a one-step S(N)2(P) process with retention of configuration at the phosphorus center.     

Chiral phospholene and phospholane chalcogenides: stereochemistry and chiral recognition by multinuclear NMR spectroscopy of their Rh2[(R)-MTPA]4 adducts

Full NMR spectral assignments of the phospholene chalcogenides 1-12 are presented and their stereochemistry proven. The enantiomeric ratio of any of these compounds can be monitored easily by adding one mole equivalent of the chiral auxiliary Rh(2)[(R)-MTPA](4) (MTPA-H identical with Mosher's acid) and subsequent NMR inspection. Some surprisingly large diastereomeric signal dispersion is observed in the (1)H NMR spectra of the adducts, leading to the conclusion that intramolecular anisotropy interaction between groups inside the ligand molecules exists. The dependence of dispersion effects on the nature of the chalcogenide atom is investigated.     

Reactions of platinum(IV) amine compounds with 9-methylhypoxanthine at high temperature result in both platinum(II) and platinum(IV) amine adducts

The products obtained from the reaction of Pt(IV)Cl₄(LL) compounds (LL denotes the chelating ligands ethylenediamine (en) and 2,2-dimethyl-1,3-diaminopropane (dmdap), or two cis- or trans-coordinated ammines) with 9-methylhypoxanthine (mHyp) at high temperature (80°C) have been characterized by proton NMR spectroscopy. It appeared that both platinum(II) and platinum(IV) adducts were present in the reaction mixtures. After cation-exchange chromatography, the Pt(II) compound could be characterized as Pt(II)(LL)(mHyp)₂, whereas the Pt(TV) fractions appeared to contain mainly one or two adducts for the chelating diamine compound but more adducts for the ammine compounds. A ³J(¹⁹⁵Pt-¹H) coupling was observed for the Pt(IV), but not for the Pt(II) compounds at the used spectrometer frequency. This supplies a useful tool to discriminate between these two types of platinum adducts.     

Cobalt(III) affinity-labeled aspartokinase. Formation of substrate and inhibitor adducts.

The kinase active site of the aspartokinase-homoserine dehydrogenase enzyme complex of Excherichia coli has been affinity labeled both with substrates aspartate and adenosine triphosphate and feedback inhibitor threonine. Co(III) exchange-inert adducts of aspartokinase and inhibitor or substrates were produced in situ by oxidation of Co(II) with H2O2. Emzyme-Co(III)-adenosine 5'-triphosphate (ATP), enzyme-Co(III)-aspartate, and enzyme-Co(III)-threonine ternary adducts were produced in this manner. The formation of the enzyme-Co(III)-threonine adduct leads us to conclude that threonine inhibits the kinase activity of this enzyme complex by binding in the first coordination sphere of the catalytic metal ion cofactor, a conclusion which is consistent with evidence derived from previous nuclear magnetic resonance data obtained in this laboratory. The quaternary adducts formed by H2O2 oxidation in the presence of aspartokinase, Co(II), ATP, aspartate, and threonine comprised a mixture of both ezyme-Co(III)-ATP-aspartate and enzyme-Co(III)-ATP-threonine adducts. The formation of the quaternary aspartate-containing adduct was unexpected, since the presence of threonine was expected to prevent access of the aspartate to the active site; most significantly however, the the sum of the numbers of aspartate plus threonine molecules incorporated per active site is one. We believe that this shows direct steric overlap between the metal-adjacent binding sites for aspartate and threonine. Aspartate or threonine can not occupy the kinase active site simultaneously; this conclusion is consistent with the direct competitive inhibition of aspartate by threonine observed in steady-state kinetic studies.     

Two-dimensional NMR studies on the anthramycin-d(ATGCAT)2 adduct

Two-dimensional NMR experiments were performed on the adduct of anthramycin with d(ATGCAT)2 to obtain the assignments of the nucleotide base and sugar protons as well as the anthramycin protons. Anthramycin is covalently attached to a guanine 2-amino group, forming the d(ATamGCAT).d(ATGCAT) modified duplex. The anthramycin protons in the minor groove exhibit NOEs to several nucleotide protons. The network of anthramycin-nucleotide NOEs and the measurement of the 10-Hz coupling constant between the anthramycin H11 and H11a protons shows that anthramycin is covalently attached as the S stereoisomer at the anthramycin C11 position with the side chain of anthramycin oriented toward the 5' end of the modified strand. The NOE data show that the anthramycin-modified duplex is in a right-handed conformation with all bases in an anti conformation. Analysis of the J1'-2' coupling constants for the resolved H1' resonances shows that the S-type conformation of the sugars is highly preferred.     

Comparative studies on the biospeciation of antidiabetic VO(IV) and Zn(II) complexes

The speciation of several insulin-mimetic/enhancing VO(IV) and Zn(II) complexes in human blood serum was studied and a comparison was made concerning the ability of the serum components to interact with the original metal complexes and the distribution of the metal ions between the low and the high molecular fractions of the serum. It was found that the low molecular mass components may play a larger role in transporting Zn(II) than in the case with VO(IV). Among the high molecular mass serum proteins, transferrin is the primary binder of VO(IV), and albumin is that of Zn(II). The results revealed that protein-ligand interactions may influence the metal ion distribution in the serum.     

119Sn Mössbauer spectroscopic studies of the products of the reaction of triorganotin(IV) derivatives with 6-thiopurine

A structural study of the products of the reaction of R₃Sn^IV derivatives (R = Me, Buⁿ, Ph) with 6-thiopurine, 6-TPH₂, and its sodium salt, 6-TPHNa, has been undertaken using Mössbauer spectroscopy and the point-charge model rationalization of the Mössbauer parameter nuclear quadrupole splitting. The synthetic reactions have been carried out at ca. 0 °C, 20 °C and 50 °C. The Mössbauer spectra of the complexes AlK₃Sn(6-TPH) are consistent with the occurrence of two distinct tin(IV) sites in samples prepared at the lower temperature, while one only site appears by increasing the temperature of the reaction. Two tin sites constantly occur in the products of the reactions involving the Ph₃Sn^IV moiety; the stoichiometry is assumed to be (Ph₃Sn)₃(6-TPH)(6-TP) for the uniquely-formed complex. Solid state polymeric structures with trigonal bipyramidal environments of the tin atoms and planar SnC₃ skeletons have been proposed. The apical ligand atoms have been assumed to be N, S and N, N in the samples showing two individual tin(IV) sites, and N, N when a single site was present.     

Cleavage and synthesis of sialic acids with aldolase. NMR studies of stereochemistry, kinetics, and mechanisms

1H-NMR spectroscopy was used to study cleavage and synthesis of N-acetyl- and N-glycoloyl-D-neuraminic acid by Clostridium perfringens aldolase. Whereas the alpha-anomers of Neu5Ac and Neu5Gc serve as substrate in the cleavage reaction, alpha-ManNAc and alpha-ManNGc are its primary products. The same alpha-anomers are needed by the aldolase for the synthesis of Neu5Ac and Neu5Gc. During the enzyme reaction in D2O both H-atoms at C-3 of Neu5Ac are exchanged by deuterium, H-3e reacting faster than H-3a. Rate constants and concentrations at equilibrium of reactants are temperature- and pH-dependent: The amount of Neu5Ac in equilibrium increases with decreasing temperature and increasing pH-value. Based on these results a mechanism of aldolase action is discussed.     

Kinetic studies on Ce(IV)-induced hydrolysis of single-stranded and double-stranded oligonucleotides

The Ce(IV)-induced hydrolyses of DNA are kinetically investigated. The formation constants of the Ce(IV)-DNA complexes are in the following order: the single-stranded DNA > the double-stranded DNA > the dinucleotide. On the other hand, the catalytic rate constants for the single-stranded DNA and the double-stranded DNA are comparable with each other, but both of them are much smaller than the value for the dinucleotide hydrolysis.     

Amine adducts of porphinato carbonylruthenium(II): studies of conformational effects and dynamics

The ¹H chemical shifts for 4-methylpyridine, imidazole, 2,5-dimethylimidazole, 2-undecylimidazole, pyrazole, 3,5-dimethylpyrazole, benzylamine, and α-methylbenzylamine bound to carbonylruthenium mesoporphyrin-IX-dimethyl ester or carbonylruthenium tetra-p-isopropylphenylporphyrin have been determined. The upfield shifts induced in the bound-nitrogen base resonances have been shown to arise principally from the magnetic anisotropy of the porphinato ligand. On this basis, models for calculating magnetic anisotropy in porphyrin systems have been tested and then applied to the determination of adduct geometry. These studies show that steric bulk of substituents ortho to the nitrogen binding determine the stability of various modes and control conformation in ligands. Furthermore, the results suggest adduct geometry and ligand-to-ring plane distances are relatively independent of porphyrin. Correlations between base structure and adduct stability were developed by measuring relative dissociation constants and first-order rate constants for dissociation. These measurements show a direct correlation between thermodynamic and kinetic stability and an inverse correlation between stability and increased steric bulk ortho to the donor atom.     

Sn and C NMR study of some trivinyltin(IV) compounds and their complexes

The¹¹⁹Sn and ¹³C NMR spectra of ten trivinyltin(IV) compounds in solutions of non-coordinating (deuteriochloroform, trideuterionitromethane) and coordinating (hexadeuteriodimethyl sulphoxide) solvents have been studied. From δ(¹¹⁹Sn) chemical shifts and ¹J(¹¹⁹Sn,¹³C) coupling constants an evaluation of the coordination number of the central tin atom and the shape of coordination polyhedra around the tin atom has been carried out. Various effects on the δ(¹³C) chemical shifts of both carbon atoms of the vinyl group are also discussed.     

H NMR and X-ray studies on hydrogen bonding in alkyloxy ethanols and their MgCl2 adducts

Adducts of alkyloxy ethanols (2-isobutoxy ethanol, 2-isopropoxy ethanol, 2-ethoxy ethanol, and 2-methoxy ethanol) with MgCl₂ were prepared in the presence of excess alkyloxy ethanol in molar ratios 5:1-15:1. MgCl₂/2-isopropoxy ethanol and MgCl₂/2-isobutoxy ethanol adducts were successfully crystallized and their structures determined by single-crystal X-ray diffraction. Alkyloxy ethanol molecules bind to magnesium in 2:1 mol ratio through oxygens of the alcohol and ether groups forming a chelated structure. In the binuclear complexes [(ipe)₂MgCl₂Mg(ipe)₂][Cl]₂ and [(ibe)₂MgCl₂Mg(ibe)₂][Cl]₂ (structures 1 and 2), where ipe stands for 2-isopropoxy ethanol and ibe for 2-isobutoxy ethanol, the two magnesium centers are connected by two chlorine bridges. The mononuclear structure cis-[Mg(ibe)₂(H₂O)₂][Cl]₂ (structure 3) contains, besides two alkyloxy molecules, two water molecules bound to magnesium. Hydrogen bonding in the adducts, in liquid and solid states, was studied by ¹H NMR spectroscopy and X-ray diffraction, respectively. In liquid state, the sample concentration and temperature used in the measurements were observed to influence hydrogen bonding. All crystal structures show extensive hydrogen bonding from anionic chlorines to the OH hydrogen of alcohols or the water hydrogens.     

NMR and FT-IR conformational studies of 8-substituted guanine nucleosides and nucleotides and their metal adducts and cancer

NMR and FT-IR Studies of the conformational changes of guanosine and guanosine-5′-monophosphate upon substitution of the H8 of guanine by a heavy, large atom, such as bromine, are presented. The conformational forms, syn, anti, C2′-endo and C3′-endo and gg, gt and tg rotamers of the above molecules are compared to those of their metal (Mg²⁺ and P^t2+) adducts, where the metal is fixed to the N7 nitrogen atom of guanine. The antitumor activity of cisplatin is discussed with relation to the conformational form and the effect of cisplatin is compared to the effects of the Mg²⁺ ion and carcinogens.