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A series of Pd(II) complexes containing ortho-cyano-aminothiophenolate (ocap) ligands have been prepared and their molecular structures elucidated. Hg(II) ocap complexes, [Hg{SC6H3XN(CîN)}]n (X = H, Me) (1), react with Na2S to afford HgS and Na2[ocap] which reacts in situ with K2[PdCl4] to afford palladium ocap complexes [Pd{SC6H3XN(CîN)}]n (2). A second route to these coordination polymers has also been developed from reactions of 2-aminobenzothiazole (abt) complexes, trans-PdCl2(abt)2 (3), with NaOH. We have not been able to crystallographically characterise coordination polymers 2, but addition of PPh3, a range of phosphines and cyclic diamines affords mono and binuclear complexes in which the ocap ligand adopts different coordination geometries. With PPh3, binuclear [Pd(µ-κ2,κ1-ocap)(PPh3)]2 (4) results, in which the ocap bridges the Pd2 centre acting as an S,N-chelate to one metal centre and binding the second via coordination of the cyanide nitrogen. In contrast, with diphosphines, Ph2P(CH2)nPPh2 (n = 1-4), mononuclear species predominate as shown in the molecular structures of Pd(κ2-ocap){κ2-Ph2P(CH2)nPPh2} (5-7; n = 1-3). With 2,2'-bipy and 1,10-phen we propose that related monomeric chelates Pd(κ2-ocap)(κ2-bipy) (9) and Pd(κ2-ocap)(κ2-phen) (10) result but we have been unable to substantiate this crystallographically. Addition of HgCl2(phen) to 9a (generated in situ) affords heterobimetallic Pd(κ2-phen)(µ-κ2,κ1-ocap)HgCl2(κ2-phen) (11), in which Hg(II) is coordinated through the ring sulfur.
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Air and moisture stable diaryl dithiocarbamate salts, Ar2NCS2Li, result from addition of CS2 to Ar2NLi, the latter being formed upon deprotonation of diarylamines by nBuLi. Oxidation with K3[Fe(CN)6] affords the analogous thiuram disulfides, (Ar2NCS2)2, two examples of which (Ar = p-C6H4X; X = Me, OMe) have been crystallographically characterised. The interconversion of dithiocarbamate and thiuram disulfides has also been probed electrochemically and compared with that established for the widely-utilised diethyl system. While oxidation reactions are generally clean and high yielding, for Ph(2-naphthyl)NCS2Li an ortho-cyclisation product, 3-phenylnaphtho[2,1-d]thiazole-2(3H)-thione, is also formed, resulting from a competitive intramolecular free-radical cyclisation. To demonstrate the coordinating ability of diaryl dithiocarbamates, a small series of Co(III) complexes have been prepared, with two examples, [Co{S2CN(p-tolyl)2}3] and [Co{S2CNPh(m-tolyl)}3] being crystallographically characterised. Solvothermal decomposition of [Co{S2CN(p-tolyl)2}3] in oleylamine generates phase pure CoS2 nanospheres in an unexpected phase-selective manner.
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[FeFe]-Ase biomimics containing a redox-active ferrocenyl diphosphine have been prepared and their ability to reduce protons and oxidise H2 studied, including 1,1'-bis(diphenylphosphino)ferrocene (dppf) complexes Fe2(CO)4(µ-dppf)(µ-S(CH2)nS) (n = 2, edt; n = 3, pdt) and Fe2(CO)4(µ-dppf)(µ-SAr)2 (Ar = Ph, p-tolyl, p-C6H4NH2), together with the more electron-rich 1,1'-bis(dicyclohexylphosphino)ferrocene (dcpf) complex Fe2(CO)4(µ-dcpf)(µ-pdt). Crystallographic characterisation of four of these show similar overall structures, the diphosphine spanning an elongated Fe-Fe bond (ca. 2.6 Å), lying trans to one sulfur and cis to the second. In solution the diphosphine is flexible, as shown by VT NMR studies, suggesting that Fe2â¯Fe distances of ca. 4.5-4.7 Å in the solid state vary in solution. Cyclic voltammetry, IR spectroelectrochemistry and DFT calculations have been used to develop a detailed picture of electronic and structural changes occurring upon oxidation. In MeCN, Fe2(CO)4(µ-dppf)(µ-pdt) shows two chemically reversible one-electron oxidations occurring sequentially at Fe2 and Fc sites respectively. For other dppf complexes, reversibility of the first oxidation is poor, consistent with an irreversible structural change upon removal of an electron from the Fe2 centre. In CH2Cl2, Fe2(CO)4(µ-dcpf)(µ-pdt) shows a quasi-reversible first oxidation together with subsequent oxidations suggesting that the generated cation has some stability but slowly rearranges. Both pdt complexes readily protonate upon addition of HBF4·Et2O to afford bridging-hydride cations, [Fe2(CO)4(µ-H)(µ-dcpf)(µ-pdt)]+, species which catalytically reduce protons to generate H2. In the presence of pyridine, [Fe2(CO)4(µ-dppf)(µ-pdt)]2+ catalytically oxidises H2 but none of the other complexes do this, probably resulting from the irreversible nature of their first oxidation. Mechanistic details of both proton reduction and H2 oxidation have been studied by DFT allowing speculative reaction schemes to be developed.
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Hidrogenasas , Cristalografía por Rayos X , Hidrogenasas/química , Ligandos , Oxidación-Reducción , ProtonesRESUMEN
Addition of 2-aminobenzothiazole (abt) and substituted derivatives to Hg(OAc)2 leads to the high yield formation of ortho-cyano-aminothiophenolate (ocap) complexes [Hg{SC6H3XN(CîN)}]n (X = H, Me, Cl, Br, NO2) resulting from dehydrogenation and C-S bond cleavage. The reaction appears to be unique to Hg(OAc)2 and with HgCl2 the product [HgCl2(abt)]n contains an intact abt ligand, but reacts with acetate to afford the ocap complex [Hg{SC6H4N(CîN)}]n. Binding of abt to Hg(II) has previously been probed in molecular structures of [Hg(sac)2(abt)L] (L = MeOH, DMSO) and these have been reexamined to understand the perturbation of abt upon coordination. When the reaction of abt and Hg(OAc)2 was carried out at low temperatures the intermediate [Hg(κ2-OAc)(EtOH)(µ-HNCNSC6H4)]2 was isolated resulting from a single ligand deprotonation thus allowing a mechanism for ring-opening to be proposed. Reactions of [Hg{SC6H3XN(CîN)}]n with mono- and bidentate phosphines have been studied, affording a series of complexes in which the ocap ligands adopt four different binding modes in the solid state, as shown by a number of crystallographic studies. In all, the ligand chelates to a single mercury centre but spans to the second via either: (i) a simple S,N-chelate, (ii) coordination through nitrogen of the CîN group, (iii) the sulfur acting as a thiolate-bridge, (iv) both thiolate bridging and cyanide coordination. With PPh3 two different binding modes are seen in complexes [Hg{SC6H3XN(CîN)}(PPh3)]2 being dependant upon the nature of the arene-substituent, while addition of excess PPh3 affords mononuclear [Hg{SC6H3XN(CîN)}(PPh3)2]. With dppm, binuclear [Hg{SC6H3XN(CîN)}(κ1-dppm)]2 result in which the diphosphine binds in a monodentate fashion. With the more flexible diphosphines, dppe and dppb, coordination polymers [Hg{SC6H3XN(CîN)}(κ1,κ1-diphosphine)]n result in which ocap binds in a simple chelate fashion. Somewhat unexpectedly, with dppp, binuclear complexes [Hg2{SC6H3XN(CîN)}2(µ,κ1,κ1-dppp)] result in which two diphosphines bridge the Hg2 centre, while with dppf mononuclear chelates are proposed to result. Thus, the simple and high-yielding ring-opening of 2-aminobenzothiazole and substituted derivatives by mercuric acetate provides ready access to a range of novel ortho-cyano-aminothiophenolate complexes, being shown to be a highly versatile ligand that can adopt a number of different coordination modes.
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Nanodimensional metal sulfides are a developing class of low-cost materials with potential applications in areas as wide-ranging as energy storage, electrocatalysis, and imaging. An attractive synthetic strategy, which allows careful control over stoichiometry, is the single source precursor (SSP) approach in which well-defined molecular species containing preformed metal-sulfur bonds are heated to decomposition, either in the vapor or solution phase, resulting in facile loss of organics and formation of nanodimensional metal sulfides. By careful control of the precursor, the decomposition environment and addition of surfactants, this approach affords a range of nanocrystalline materials from a library of precursors. Dithiocarbamates (DTCs) are monoanionic chelating ligands that have been known for over a century and find applications in agriculture, medicine, and materials science. They are easily prepared from nontoxic secondary and primary amines and form stable complexes with all elements. Since pioneering work in the late 1980s, the use of DTC complexes as SSPs to a wide range of binary, ternary, and multinary sulfides has been extensively documented. This review maps these developments, from the formation of thin films, often comprised of embedded nanocrystals, to quantum dots coated with organic ligands or shelled by other metal sulfides that show high photoluminescence quantum yields, and a range of other nanomaterials in which both the phase and morphology of the nanocrystals can be engineered, allowing fine-tuning of technologically important physical properties, thus opening up a myriad of potential applications.
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The syntheses of two platinum(ii) dithiocarbamate complexes (1 and 2) that show quinoplatin- and phenanthriplatin-type axial protection of the Pt-plane are described. The Pt-plane of complex 2 is axially more protected than that of complex 1. Furthermore, both complexes adopt two different stereochemical conformations in the solid state (based on single-crystal X-ray structures) owing to the structurally flexible piperazine backbone; i.e., C-e,e-Anti (1) and C-e,a-Syn (2), where "C" stands for the chair configuration, "e" and "a" stand for the equatorial and axial positions and "Anti" (opposite side) and "Syn" (same side) represent the relative orientations in space of the terminal substituents on the piperazine ring. In complex 2, the C-e,a-Syn conformation may provide additional steric hindrance to the Pt-plane. Despite the lower lipophilicity of 2 as compared to that of 1, the in vitro anticancer action against selected cancer cell lines is better for the former revealing the superior role of the axial protection over lipophilicity in modulating anticancer activity. The activity against the cancer promoting protein NF-κB signifies that the mode of cancer cell death may be the result of hindering the activity of NF-κB in the initiation of apoptosis. The apoptotic mode of cell death has been established earlier in a study using Annexin V-FITC. Finally, DNA binding studies revealed that the complex-DNA adduct formation is spontaneous and the mode of interaction is non-intercalative (electrostatic/covalent).
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Complejos de Coordinación/química , Complejos de Coordinación/farmacología , ADN/metabolismo , Compuestos Organoplatinos/química , Compuestos Organoplatinos/farmacología , Fenantridinas/química , Fenantridinas/farmacología , Tiocarbamatos/química , Antineoplásicos/química , Antineoplásicos/metabolismo , Antineoplásicos/farmacología , Línea Celular Tumoral , Complejos de Coordinación/metabolismo , Humanos , Interacciones Hidrofóbicas e Hidrofílicas , Isomerismo , Conformación Molecular , FN-kappa B/metabolismo , Compuestos Organoplatinos/metabolismo , Fenantridinas/metabolismo , Piperazina/química , Electricidad EstáticaRESUMEN
Reaction of [Fe3(CO)9(µ3-Te)2] (1) with the corresponding phosphine has been used to prepare the phosphine-substituted tellurium-capped triiron clusters [Fe3(CO)9(µ3-Te)2(PPh3)] (2), [Fe3(CO)8(µ3-Te)2(PPh3)] (3) and [Fe3(CO)7(µ3-Te)2(µ-R2PXPR2)] (X = CH2, R = Ph (4), Cy (5); X = NPri, R = Ph (6)). The directly related cluster [Fe3(CO)7(µ3-CO)(µ3-Te)(µ-dppm)] (7) was isolated from the reaction of [Fe3(CO)10(µ-Ph2PCH2PPh2)] with elemental tellurium. The electrochemistry of these new clusters has been probed by cyclic voltammetry, and selected complexes have been tested as proton reduction catalysts. Each 50-electron dicapped cluster exhibits two reductive processes; the first has good chemical reversibility in all cases but the reversibility of the second is dependent upon the nature of the supporting ligands. For the parent cluster 1 and the diphosphine derivatives 4-5 this second reduction is reversible, but for the PPh3 complex 3 it is irreversible, possibly as a result of CO or phosphine loss. The nature of the reduced products of 1 has been probed by DFT calculations. Upon addition of one electron, an elongation of one of the Fe-Te bonding interactions is found, while the addition of the second electron affords an open-shell triplet which is more stable by 8.8 kcal mol-1 than the closed-shell singlet dianion and has two elongated Fe-Te bonds. The phosphine-substituted clusters also exhibit oxidation chemistry but with poor reversibility in all cases. Since the reduction potentials for the tellurium-capped clusters occur at more positive potentials than for the sulfur and selenium analogues, and the redox processes also show better reversibility than for the S/Se analogues, the tellurium-capped clusters 1 and 3-5 have been examined as proton reduction catalysts. In the presence of p-toluenesulfonic acid (TsOH) or trifluoroacetic acid (TFA), these clusters reduce protons to H2 at both their first and second reduction potentials. Electron uptake at the second reduction potential is far greater than the first, suggesting that the open-shell triplet dianions are efficient catalysts. As expected, the catalytic overpotential increases upon successive phosphine substitution but so does the current response. A mechanistic scheme that takes the roles of the supporting ligands on the preferred route(s) to H2 production and release into account is presented.
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BACKGROUND AND PURPOSE: A clinical need exists for targeted, safe, and effective sulfide donors. We recently reported that ammonium tetrathiomolybdate (ATTM) belongs to a new class of sulfide-releasing drugs. Here, we investigated the cellular uptake mechanisms of this drug class compared to sodium hydrosulfide (NaHS) and the effects of a thiometallate tungsten congener of ATTM, ammonium tetrathiotungstate (ATTT). EXPERIMENTAL APPROACH: In vitro H2 S release was determined by headspace gas sampling of vials containing dissolved thiometallates. Thiometallate and NaHS bioactivity was assessed by spectrophotometry-derived sulfhaemoglobin formation. Cellular uptake dependence on the anion exchange protein (AE)-1 was investigated in human red blood cells. ATTM/glutathione interactions were assessed by LC-MS/MS. Rodent pharmacokinetic and pharmacodynamic studies focused on haemodynamics and inhibition of aerobic respiration. KEY RESULTS: ATTM and ATTT both exhibit temperature-, pH-, and thiol-dependence of sulfide release. ATTM/glutathione interactions revealed the generation of inorganic and organic persulfides and polysulfides. ATTM showed greater ex vivo and in vivo bioactivity over ATTT, notwithstanding similar pharmacokinetic profiles. Cellular uptake mechanisms of the two drug classes are distinct; thiometallates show dependence on AE-1, while hydrosulfide itself was unaffected by inhibition of this pathway. CONCLUSIONS AND IMPLICATIONS: The cellular uptake of thiometallates relies upon a plasma membrane ion channel. This advances our pharmacological knowledge of this drug class, and further supports their utility as cell-targeted sulfide donor therapies. Our results indicate that, as a more stable form, ATTT is better suited as a copper chelator. ATTM, a superior sulfide donor, may additionally participate in intracellular redox recycling. LINKED ARTICLES: This article is part of a themed section on Hydrogen Sulfide in Biology & Medicine. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v177.4/issuetoc.
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Sulfuro de Hidrógeno , Espectrometría de Masas en Tándem , Cromatografía Liquida , Glutatión , SulfurosRESUMEN
Zinc sulfide is an important wide-band gap semi-conductor and dithiocarbamate complexes [Zn(S2CNR2)2] find widespread use as single-source precursors for the controlled synthesis of ZnS nanoparticulate modifications. Decomposition of [Zn(S2CNiBu2)2] in oleylamine gives high aspect ratio wurtzite nanowires, the average length of which was increased upon addition of thiuram disulfide to the decomposition mixture. To provide further insight into the decomposition process, X-ray absorption spectroscopy (XAS) of [Zn(S2CNMe2)2] was performed in the solid-state, in non-coordinating xylene and in oleylamine. In the solid-state, dimeric [Zn(S2CNMe2)2]2 was characterised in accord with the single crystal X-ray structure, while in xylene this breaks down into tetrahedral monomers. In situ XAS in oleylamine (RNH2) shows that the coordination sphere is further modified, amine binding to give five-coordinate [Zn(S2CNMe2)2(RNH2)]. This species is stable to ca. 70 °C, above which amine dissociates and at ca. 90 °C decomposition occurs to generate ZnS. The relatively low temperature onset of nanoparticle formation is associated with amine-exchange leading to the in situ formation of [Zn(S2CNMe2)(S2CNHR)] which has a low temperature decomposition pathway. Combining these observations with the previous work of others allows us to propose a detailed mechanistic scheme for the overall process.
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A series of diiron bis(2-diphenylphosphinoethyl)phenylphosphine (triphos) complexes Fe2(CO)3(µ-dithiolate)(µ,κ1,κ2-triphos) (1-4) [dithiolate = 1 pdt; 2 edt; 3 adt (R = Bz), 4 (SMe)2] have been prepared and investigated as biomimics of the diiron site of [FeFe]-hydrogenases. The triphos ligand bridges the diiron vector whilst also chelating to one iron and 1-3 exist as a mixture of basal-basal-apical (bba) and basal-basal-basal (bbb) isomers which differ in the mode of chelation. In solution the bba and bbb forms do not interconvert on the NMR time scale, but the bba isomers are fluxional, and at low temperature four forms of 1bba are seen as the conformations for the pdt ring and triphos methylene groups are frozen. Crystallographic studies have established bba (pdt) and bbb (adt) ground state conformations and in both there is a significant deviation away from the expected eclipsed conformation (Lap-Fe-Fe-Lap torsion angle 0°) by 49.4 and 24.9° respectively, suggesting that introduction of triphos leads to significant strain and DFT calculations have been used to understand the relative energies of isomers. The electron rich nature of the diiron centre in 1-4 would suggest rapid protonation, but while bridging hydride complexes such as [Fe2(CO)3(µ-pdt)(µ,κ1,κ2-triphos)(µ-H)][BF4] (1H+) can be formed the process is slow. This behavior is likely a result of the high energy barrier in forming the initial (not observed) terminal hydride which requires a significant conformational change in triphos coordination. CV studies show that all starting compounds oxidize at low potentials and the addition of [Cp2Fe][PF6] to 1 affords [Fe2(CO)3(µ-pdt)(µ,κ1,κ2-triphos)][PF6] (1+) which has been characterised by IR spectroscopy. DFT studies suggest a ground state for 1+ with a partially rotated Fe(CO)2P moiety that yields a weak semi-bridging carbonyl with the adjacent Fe(CO)P2 group. No reduction peaks are seen for 1-4 within the solvent window but 1H+ undergoes reduction at -1.7 V. All complexes act as proton-reduction catalysts in the presence of HBF4·Et2O. For 1, three separate processes are observed and their dependence on acid concentration has been probed, and a mechanistic scheme is proposed based on formation via a CECE process of 1(µ-H)H which can either slowly release H2 or undergo further reduction. Relative contributions of the three processes to the total current were found to be highly dependent upon the background electrolyte, being attributed to their relative abilities to facilitate proton transfer processes. While 2 and 4 show similar proton reduction behaviour, the adt complex 3 is quite different being attributed to facile protonation of nitrogen which is followed by addition of a second proton at the diiron centre.
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Phosphines react with the benzisothiazolinate (bit) paddlewheel dimer, [Ni2(µ-bit)4·2H2O], resulting in sulfur-nitrogen bond scission and a series of unexpected transformations leading to novel Ni(ii) complexes containing 2-cyanophenylthiolate and related thiolate ligands.
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[FeFe]-hydrogenases contain strongly electronically coupled diiron [2Fe]H and tetrairon [Fe4-S4]H clusters, and thus much recent effort has focused on the chemistry of diiron-dithiolate biomimics with appended redox-active ligands. Here we report on the synthesis and electrocatalytic activity of Fe2(CO)4(µ-edt)(κ2-bpcd) (2) in which the electron-acceptor 4,5-bis(diphenylphosphino)-4-cyclopenten-1,3-dione (bpcd) acts as a surrogate of the [Fe4-S4]H sub-cluster. The complex is prepared in low yield but has been fully characterised, including a crystallographic study which shows that the diphosphine adopts a basal-apical coordination geometry in the solid state. Cyclic voltammetry shows that 2 undergoes four reduction events with DFT studies confirming that the first reduction is localised on the low-lying π* system of the diphosphine ligand. The addition of the second electron furnishes a triplet dianion that exhibits spin density distributed over the diphosphine and diiron subunits. Protonation at the Fe-Fe bond of the triplet dianion furnishes the corresponding bridging hydride as the thermodynamically favoured species that contains a reduced bpcd ligand. Complex 2 functions as a catalyst for proton-reduction at its second reduction potential, in contrast to the related 2,3-bis(diphenylphosphino)maleic anhydride (bma) complex, Fe2(CO)4(µ-pdt)(κ2-bma) (1), which shows similar electrochemical behaviour but is not catalytically active. The difference in chemical behaviour is attributed to greater stability of the 4-cyclopenten-1,3-dione platform in 2 as compared to the maleic anhydride ring of the bma ligand in 1 following the uptake of the second electron. Thus protonation of the Fe-Fe bond in the 22- affords a species which is stable enough to undergo a further reduction-protonation event, unlike the bma ligand whose maleic anhydride ring undergoes deleterious C-O bond scission upon protonation or reaction with adventitious moisture. DFT studies, however, suggest that electron-transfer from the diphosphine to the diiron centre is not significant, probably due to their poor redox levelling. Thus, while the diphosphine is readily reduced, the added electron is apparently not utilised in proton-reduction and hence cannot truly be considered as an [Fe4-S4]H surrogate.
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The synthesis of colloidal semiconductor nanocrystals (NCs) from single-source precursors offers simplified manufacturing processes at the cost of reduced atom efficiency. Self-capping routes have the potential to maximise this efficiency although investigation has so far been limited to organic solvents. Here we present the synthesis of copper sulfide NCs via the decomposition of a copper dithiocarbamate complex in water. Nanocrystalline covellite particles were prepared without the need for additional capping ligand and exhibited a hollow nanosphere morphology. Mass spectrometry of the water-stable NCs indicated the presence of a number of surface ligands, including a small amine fragment of the single-source precursor (SSP) complex. A broad plasmon resonance in the near-infrared (NIR) at 990 nm was also observed and the photothermal effect of this demonstrated. Cytotoxicity experiments indicated cell viability remained above 95% for NC concentrations up to 1 mg mL-1, indicating high biocompatibility.
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We report the use of cheap, readily accessible and easy to handle di-isobutyl-dithiocarbamate complexes, [M(S2CNiBu2) n ], as single source precursors (SSPs) to ternary sulfides of iron-nickel, iron-copper and nickel-cobalt. Varying decomposition temperature and precursor concentrations has a significant effect on both the phase and size of the nanomaterials, and in some instances meta-stable phases are accessible. Decomposition of [Fe(S2CNiBu2)3]/[Ni(S2CNiBu2)2] at ca. 210-230 °C affords metastable FeNi2S4 (violarite) nanoparticles, while at higher temperatures the thermodynamic product (Fe,Ni)9S8 (pentlandite) results. Addition of tetra-isobutyl-thiuram disulfide to the decomposition mixture can significantly affect the nature of the product at any particular temperature-concentration, being attributed to suppression of the intramolecular Fe(iii) to Fe(ii) reduction. Attempts to replicate this simple approach to ternary metal sulfides of iron-indium and iron-zinc were unsuccessful, mixtures of binary metal sulfides resulting. Oleylamine is non-innocent in these transformations, and we propose that SSP decomposition occurs via primary-secondary backbone amide-exchange with primary dithiocarbamate complexes, [M(S2CNHoleyl) n ], being the active decomposition precursors.
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Nanoparticulate iron sulfides have many potential applications and are also proposed to be prebiotic catalysts for the reduction of CO2 to biologically important molecules, thus the development of reliable routes to specific phases with controlled sizes and morphologies is important. Here we focus on the use of iron dithiocarbamate complexes as single source precursors (SSPs) to generate greigite and pyrrhotite nanoparticles. Since these minerals contain both iron(iii) and iron(ii) centres, SSPs in both oxidation states, [Fe(S2CNR2)3] and cis-[Fe(CO)2(S2CNR2)2] respectively, have been utilised. Use of this Fe(ii) precursor is novel and it readily loses both carbonyls in a single step (as shown by TGA measurements) providing an in situ source of the extremely air-sensitive Fe(ii) dithiocarbamate complexes [Fe(S2CNR2)2]. Decomposition of [Fe(S2CNR2)3] alone in oleylamine affords primarily pyrrhotite, although by careful control of reaction conditions (ca. 230 °C, 40-50 nM SSP) a window exists in which pure greigite nanoparticles can be isolated. With cis-[Fe(CO)2(S2CNR2)2] we were unable to produce pure greigite, with pyrrhotite formation dominating, a similar situation being found with mixtures of Fe(ii) and Fe(iii) precursors. In situ X-ray absorption spectroscopy (XAS) studies showed that heating [Fe(S2CNiBu2)3] in oleylamine resulted in amine coordination and, at ca. 60 °C, reduction of Fe(iii) to Fe(ii) with (proposed) elimination of thiuram disulfide (S2CNR2)2. We thus carried out a series of decomposition studies with added thiuram disulfide (R = iBu) and found that addition of 1-2 equivalents led to the formation of pure greigite nanoparticles between 230 and 280 °C with low SSP concentrations. Average particle size does not vary significantly with increasing concentration, thus providing a convenient route to ca. 40 nm greigite nanoparticles. In situ XAS studies have been carried out and allow a decomposition pathway for [Fe(S2CNiBu2)3] in oleylamine to be established; reduction of Fe(iii) to Fe(ii) reduction triggers substitution of the secondary amide backbone by oleylamine (RNH2) resulting in the in situ formation of a primary dithiocarbamate derivative [Fe(RNH2)2(S2CNHR)2]. This in turn extrudes RNCS to afford molecular precursors of the observed FeS nanomaterials. The precise role of thiuram disulfide in the decomposition process is unknown, but it likely plays a part in controlling the Fe(iii)-Fe(ii) equilibrium and may also act as a source of sulfur allowing control over the Fe : S ratio in the mineral products.
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Reaction of 2-vinylpyrazine with Ru3(CO)12 results in multiple C-H bond activations to afford penta- and octa-ruthenium clusters, Ru5(CO)15(µ5-C4H2N2CH[double bond, length as m-dash]CH)(µ-H)2 (2) and Ru8(CO)24(µ7-C4H2N2CH[double bond, length as m-dash]C)(µ-H)3 (3), in which a Ru3 sub-unit is linked to Ru2 and Ru5 centres via di- and tri-metalated 2-vinylpyrazine ligands, exhibiting novel coordination modes including the loss of ring aromaticity in 2. The bonding of 2 and the mechanism for the fluxional behaviour of the hydrides have been examined by electronic structure calculations.
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Mixed-valence dimolybdenum complexes Mo2(O)(CO)2{µ-κ2-S(CH2)nS}2(κ2-Ph2P(CH2)mPPh2) (n = 2, 3; m = 1, 2) (1-4) have been synthesized from one-pot reactions of fac-Mo(CO)3(NCMe)3 and dithiols, HS(CH2)nSH, in the presence of diphosphines. The dimolybdenum framework is supported by two thiolate bridges, with one molybdenum carrying a terminal oxo ligand and the second two carbonyls. The dppm (m = 1) products exist as a pair of diastereomers differing in the relative orientation of the two carbonyls (cis and trans) at the Mo(CO)2(dppm) center, while dppe (m = 2) complexes are found solely as the trans isomers. Small amounts of Mo(CO){κ3-S(CH2CH2S)2}(κ2-dppe) (5) also result from the reaction using HS(CH2)2SH and dppe. The bonding in isomers of 1-4 has been computationally explored by DFT calculations, trans diastereomers being computed to be more stable than the corresponding pair of cis diastereomers for all. The calculations confirm the existence of Mo[triple bond, length as m-dash]O and Mo-Mo bond orders and suggest that the new dimeric compounds are best viewed as Mo(v)-Mo(i) mixed-valence systems. The electrochemical properties of 1 have been investigated by CV and show a reversible one-electron reduction associated with the Mo(v) centre, while two closely spaced irreversible oxidation waves are tentatively assigned to oxidation of the Mo(i) centre of the two isomers as supported by DFT calculations.
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Greigite and other iron sulfides are potential, cheap, earth-abundant electrocatalysts for the hydrogen evolution reaction (HER), yet little is known about the underlying surface chemistry. Structural and chemical changes to a greigite (Fe3S4)-modified electrode were determined at -0.6 V versus standard hydrogen electrode (SHE) at pH 7, under conditions of the HER. In situ X-ray absorption spectroscopy was employed at the Fe K-edge to show that iron-sulfur linkages were replaced by iron-oxygen units under these conditions. The resulting material was determined as 60% greigite and 40% iron hydroxide (goethite) with a proposed core-shell structure. A large increase in pH at the electrode surface (to pH 12) is caused by the generation of OH- as a product of the HER. Under these conditions, iron sulfide materials are thermodynamically unstable with respect to the hydroxide. In situ infrared spectroscopy of the solution near the electrode interface confirmed changes in the phosphate ion speciation consistent with a change in pH from 7 to 12 when -0.6 V versus SHE is applied. Saturation of the solution with CO2 resulted in the inhibition of the hydroxide formation, potentially due to surface adsorption of HCO3-. This study shows that the true nature of the greigite electrode under conditions of the HER is a core-shell greigite-hydroxide material and emphasizes the importance of in situ investigation of the catalyst under operation to develop true and accurate mechanistic models.
RESUMEN
The cytotoxic properties of a series of nickel(II)-dithiocarbamate phenanthroline complexes is reported. The complexes 1-6 kill bulk cancer cells and cancer stem cells (CSCs) with micromolar potency. Two of the complexes, 2 and 6, kill twice as many breast cancer stem cell (CSC)-enriched HMLER-shEcad cells as compared to breast CSC-depleted HMLER cells. Complex 2 inhibits mammosphere formation to a similar extent as salinomycin (a CSC-specific toxin). Detailed mechanistic studies suggest that 2 induces CSC death by necroptosis, a programmed form of necrosis. Specifically, 2 triggers MLKL phosphorylation, oligomerization, and translocation to the cell membrane. Additionally, 2 induces necrosome-mediated propidium iodide (PI) uptake and mitochondrial membrane depolarisation, as well as morphological changes consistent with necroptotosis. Strikingly, 2 does not evoke necroptosis by intracellular reactive oxygen species (ROS) production or poly(ADP) ribose polymerase (PARP-1) activation.
Asunto(s)
Antineoplásicos/síntesis química , Apoptosis/efectos de los fármacos , Complejos de Coordinación/síntesis química , Células Madre Neoplásicas/efectos de los fármacos , Níquel/química , Fenantrolinas/síntesis química , Tiocarbamatos/síntesis química , Antineoplásicos/farmacología , Línea Celular Tumoral , Supervivencia Celular , Complejos de Coordinación/farmacología , Humanos , Necrosis , Células Madre Neoplásicas/patología , Fenantrolinas/farmacología , Poli(ADP-Ribosa) Polimerasa-1/metabolismo , Especies Reactivas de Oxígeno/metabolismo , Tiocarbamatos/farmacología , Ubiquitina-Proteína Ligasas/antagonistas & inhibidoresRESUMEN
Square-planar nickel bis(dithiocarbamate) complexes, [Ni(S2CNR2)2], have been prepared and utilised as single source precursors to nanoparticulate nickel sulfides. While they are stable in the solid-state to around 300 °C, heating in oleylamine at 230 °C, 5 mM solutions afford pure α-NiS, where the outcome is independent of the substituents. DFT calculations show an electronic effect rather than steric hindrance influences the resulting particle size. Decomposition of the iso-butyl derivative, [Ni(S2CN(i)Bu2)2], has been studied in detail. There is a temperature-dependence of the phase of the nickel sulfide formed. At low temperatures (150 °C), pure α-NiS is formed. Upon raising the temperature, increasing amounts of ß-NiS are produced and at 280 °C this is formed in pure form. A range of concentrations (from 5-50 mM) was also investigated at 180 °C and while in all cases pure α-NiS was formed, particle sizes varied significantly. Thus at low concentrations average particle sizes were ca. 100 nm, but at higher concentrations they increased to ca. 150 nm. The addition of two equivalents of tetra-iso-butyl thiuram disulfide, ((i)Bu2NCS2)2, to the decomposition mixture was found to influence the material formed. At 230 °C and above, α-NiS was generated, in contrast to the results found without added thiuram disulfide, suggesting that addition of ((i)Bu2NCS2)2 stabilises the metastable α-NiS phase. At low temperatures (150-180 °C) and concentrations (5 mM), mixtures of α-NiS and Ni3S4, result. A growing proportion of Ni3S4 is noted upon increasing precursor concentration to 10 mM. At 20 mM a metastable phase of nickel sulfide, NiS2 is formed and as the concentration is increased, α-NiS appears alongside NiS2. Reasons for these variations are discussed.