New cationic palladium (II) and rhodium (I) complexes of [Ph2PCH2C(Ph)N(2,6-Me2C6H3)]

Treatment of the bulky iminophosphine ligand [Ph₂PCH₂C(Ph)N(2,6-Me₂C₆H₃)] (L) with [M(CH₃CN)₂(ligand)]⁺ⁿ, where for M = Pd(II): ligand = η³-allyl, n = 1, and for M = Rh(I), ligand: 2(C₂H₄), 2(CO) or cod, n = 0, yields the mono-cationic iminophosphine complexes [Pd(η³-C₃H₅)(L)][BF₄] (1), [Rh(cod)(L)][BF₄] (2), [Rh(CO)(CH₃CN)(L)][BF₄] (3), and cis-[Rh(L)₂][BF₄] (4). All the new complexes have been characterised by NMR spectroscopy and X-ray diffraction. Complex 1 shows moderate activity in the copolymerisation of CO and ethene but is inactive towards Heck coupling of 4-bromoacetophenone and n-butyl acrylate.     

Trifluoroacetylacetonate rhodium(III) methyl complexes, cis-[Rh(TFA)(PPh3)2(CH3)(L)][BPh4] and cis-[Rh(TFA)(PPh3)2(CH3)(I)] (L = CH3CN, NH3, pyridine), in comparison with their acetylacetonate analogs

The oxidative addition of CH₃I to planar rhodium(I) complex [Rh(TFA)(PPh₃)₂] in acetonitrile (TFA is trifluoroacetylacetonate) leads to the formation of cationic, cis-[Rh(TFA)(PPh₃)₂(CH₃)(CH₃CN)][BPh₄] (1), or neutral, cis-[Rh(TFA)(PPh₃)₂(CH₃)(I)] (4), rhodium(III) methyl complexes depending on the reaction conditions. 1 reacts readily with NH₃ and pyridine to form cationic complexes, cis-[Rh(TFA)(PPh₃)₂(CH₃)(NH₃)][BPh₄] (2) and cis-[Rh(TFA)(PPh₃)₂(CH₃)(Py)][BPh₄] (3), respectively. Acetylacetonate methyl complex of rhodium(III), cis-[Rh(Acac)(PPh₃)₂(CH₃)(I)] (5), was obtained by the action of NaI on cis-[Rh(Acac)(PPh₃)₂(CH₃)(CH₃CN)][BPh₄] in acetone at −15 °C. Complexes 1-5 were characterized by elemental analysis, ³¹P{¹H}, ¹H and ¹⁹F NMR. For complexes 2, 3, 4 conductivity data in acetone solutions are reported. The crystal structures of 2 and 3 were determined. NMR parameters of 1-5 and related complexes are discussed from the viewpoint of their isomerism.     

Synthesis and properties of new Mo(II) complexes with N-heterocyclic and ferrocenyl ligands

New Mo(II) complexes with 2,2′-dipyridylamine (L1), [Mo(CH₃CN)(η³-C₃H₅)(CO)₂(L1)]OTf (C1a) and [{MoBr(η³-C₃H₅)(CO)₂(L1)}₂(4,4′-bipy)](PF₆)₂ (C1b), with {[bis(2-pyridyl)amino]carbonyl}ferrocene (L2), [MoBr(η³-C₃H₅)(CO)₂(L2)] (C2), and with the new ligand N,N-bis(ferrocenecarbonyl)-2-aminopyridine (L3), [MoBr(η³-C₃H₅)(CO)₂(L3)] (C3), were prepared and characterized by FTIR and ¹H and ¹³C NMR spectroscopy. C1a, C1b, L3, and C2 were also structurally characterized by single crystal X-ray diffraction. The Mo(II) coordination sphere in all complexes features the facial arrangement of allyl and carbonyl ligands, with the axial isomer present in C1a and C2, and the equatorial in the binuclear C1b. In both C1a and C1b complexes, the L1 ligand is bonded to Mo(II) through the nitrogen atoms and the NH group is involved in hydrogen bonds. The X-ray single crystal structure of C2 shows that L2 is coordinated in a κ²-N,N-bidentate chelating fashion. Complex C3 was characterized as [MoBr(η³-C₃H₅)(CO)₂(L3)] with L3 acting as a κ²-N,O-bidentate ligand, based on the spectroscopic data, complemented by DFT calculations.The electrochemical behavior of the monoferrocenyl and diferrocenyl ligands L2 and L3 has been studied together with that of their Mo(II) complexes C2 and C3. As much as possible, the nature of the different redox changes has been confirmed by spectrophotometric measurements. The nature of the frontier orbitals, namely the localization of the HOMO in Mo for both in C2 and C3, was determined by DFT studies.     

Syntheses of new Mo(II) and W(II) mono(hydrosulfido) complexes and their conversion into di- and tetranuclear sulfido-bridged heterobimetallic complexes

Treatment of [Cp′MH(CO)₃] (M = Mo, W; Cp′ = η⁵-C₅H₅ (Cp), η⁵-C₅Me₅ (Cp*)) with 1/8 equiv of S₈ in THF, followed by the reaction with dppe under UV irradiation, gave new mono(hydrosulfido) complexes [Cp′M(SH)(CO)(dppe)] (Cp′ = Cp: M = Mo (5), W (6); Cp′ = Cp*: M = Mo (7), W (8); dppe = Ph₂PCH₂CH₂PPh₂). When 5 and 6 dissolved in THF were allowed to react with [RhCl(PPh₃)₃] in the presence of base, heterodinuclear complexes with bridging S and dppe ligands [CpM(CO)(μ-S)(μ-dppe)Rh(PPh₃)] (M = Mo (9), W(10)) were obtained. Semi-bridging feature of the CO ligands were also demonstrated. Upon standing in CH₂Cl₂ solutions, 9 and 10 were converted further to the dimerization products [(CpM)₂{Rh(dppe)}₂(μ₂-CO)₂(μ₃-S)₂] (M = Mo (13), W). Detailed structures of mononuclear 7 and 8, dinuclear 9 and tetranuclear 13 have been determined by the X-ray diffraction.     

Addition of benzenethiol to terminal alkynes catalyzed by hydrotris(3,5-dimethylpyrazolyl)borate-Rh(III) bis(thiolate) complex: Mechanistic studies with characterization of the key intermediate

The Rh(III)-thiolate complex [Tp^∗Rh(SPh)₂(MeCN)] (2; Tp^∗ = hydrotris(3,5-dimethylpyrazolyl)borate) readily undergoes substitution of MeCN by XyNC (Xy = 2,6-dimethylphenyl) to give the isocyanide complex [Tp^∗Rh(SPh)₂(XyNC)] (3), whereas reaction of 2 with terminal alkynes results in the formation of the rhodathiacyclobutene complex [Tp^∗Rh(SPh){η²-CHCR(SPh)}] (4; R = aryl, alkyl). Molecular structures of 3 and 4 (R = CH₂Ph) have been determined by single crystal X-ray diffraction. Complex 2 as well as [Tp^∗Rh(cyclooctene)(MeCN)] have been found to catalyze regioselective addition of benzenethiol to terminal alkynes RCCH at 50 °C to give R(PhS)CCH₂ in moderate to high yields. The above products are selectively formed when R = CH₂Ph and n-C₆H₁₃, while cis-RCHCHSPh and RC(SPh)₂CH₃ are also obtained as by-products when R = p-MeOC₆H₄. Catalytic cycle involving 2 and 4 is proposed based on the mechanistic studies using NMR measurement.     

Ruthenium(II), rhodium(III) and iridium(III) based effective catalysts for hydrogenation under aerobic conditions

The new cationic mononuclear complexes [(η⁶-arene)Ru(Ph-BIAN)Cl]BF₄ [η⁶-arene = benzene (1), p-cymene (2)], [(η⁵-C₅H₅)Ru(Ph-BIAN)PPh₃]BF₄ (3) and [(η⁵-C₅Me₅)M(Ph-BIAN)Cl]BF₄ [M = Rh (4), Ir (5)] incorporating 1,2-bis(phenylimino)acenaphthene (Ph-BIAN) are reported. The complexes have been fully characterized by analytical and spectral (IR, NMR, FAB-MS, electronic and emission) studies. The molecular structure of the representative iridium complex [(η⁵-C₅Me₅)Ir(Ph-BIAN)Cl]BF₄ has been determined crystallographically. Complexes 1–5 effectively catalyze the reduction of terephthaldehyde in the presence of HCOOH/CH₃COONa in water under aerobic conditions and, among these complexes the rhodium complex [(η⁵-C₅Me₅)Rh(Ph-BIAN)Cl]BF₄ (4) displays the most effective catalytic activity.     

Palladium(II)-allyl complexes containing chiral N-donor ferrocenyl ligands

A study of the reactivity of enantiopure ferrocenylimine (S_C)-[FcCHN-CH(Me)(Ph)] {Fc =  (η⁵-C₅H₅)Fe{(η⁵-C₅H₄)-} (1a) with palladium(II)-allyl complexes [Pd(η³-1R¹,3R²-C₃H₃)(μ-Cl)]₂ {R¹ = H and R² = H (2), Ph (3) or R¹ = R² = Ph (4)} is reported. Treatment of 1a with 2 or 3 {in a molar ratio Pd(II):1a = 1} in CH₂Cl₂ at 298 K produced [Pd(η³-3R²-C₃H₄){FcCHN-CH(Me)(Ph)}Cl] {R² = H (5a) or Ph (6a)}. When the reaction was carried out under identical experimental conditions using complex 4 as starting material no evidence for the formation of [Pd(η³-1,3-Ph₂-C₃H₃){FcCHN-CH(Me)(Ph)}Cl] (7a) was found. Additional studies on the reactivity of (S_C)-[FcCHN-CH(R³)(CH₂OH)] {R³ = Me (1b) or CHMe₂ (1c)} with complex 4 showed the importance of the bulk of the substituents on the palladium(II) allyl-complex (2-4) or on the ferrocenylimines (1) in this type of reaction. The crystal structure of 5a showed that: (a) the ferrocenylimine adopts an anti-(E) conformation and behaves as an N-donor ligand, (b) the chloride is in acis-arrangement to the nitrogen and (c) the allyl group binds to the palladium(II) in a η³-fashion. Solution NMR studies of 5a and 6a and [Pd(η³-1,3-Ph₂-C₃H₃){FcCHN-CH(Me)(CH₂OH)}Cl] (7b) revealed the coexistence of several isomers in solution. The stoichiometric reaction between 6a and sodium diethyl 2-methylmalonate reveals that the formation of the achiral linear trans-(E) isomer of Ph-CHCH-CH₂Nu (8) was preferred over the branched derivative (9). A comparative study of the potential utility of ligand 1a, complex 5a and the amine (S_C)-H₂N-CH(Me)(Ph) (11) as catalysts in the allylic alkylation of (E)-3-phenyl-2-propenyl (cinnamyl) acetate with the nucleophile diethyl 2-methylmalonate (Nu⁻) is reported.     

Rhodium(I) complexes with 1′-(diphenylphosphino)ferrocenecarboxylic acid as active and recyclable catalysts for 1-hexene hydroformylation

The rhodium complex trans-[Rh(CO)(Hdpf-κP)(dpf-κ²O,P)] (1), (Hdpf = 1′-(diphenylphosphino)ferrocenecarboxylic acid) was used as an efficient and recyclable catalyst for 1-hexene hydroformylation producing ca. 80% of aldehydes at 10 atm CO/H₂ and 80 °C. After the reaction, unchanged complex 1 was separated from the reaction mixture and used again three times with the same catalytic activity. The effect of modifying ligands, phosphines and phosphites, on the reactivity of 1 was investigated. The active catalytic systems containing 1 or trans-[Rh(CO)(L)(dpf-κ²O,P)] (2) were formed in situ from acetylacetonato rhodium(I) precursors [Rh(CO)₂(acac)] (3) or [RhL(CO)(acac)] (4) and Hdpf or Medpf (L = phosphine, Medpf = methyl ester of Hdpf).     

Synthesis and characterization of the cluster complexes containing tetrahedral FeCrCo(μ3-S) cluster cores generated by isolobal displacement reactions. Crystal structures of (η-RC5H4)FeCrCo(μ3-S)(CO)8 (R=H, CO2Et) and FeCo2(μ3-S)2(CO)9

The monoanions (η⁵-RC₅H₄)(CO)₃Cr⁻ (1, R=H; 2, R=Me; 3, R=CO₂Et) reacted with tetrahedral cluster FeCo₂(μ₃-S)(CO)₉ to give single isolobal displacement products (η⁵-RC₅H₄)FeCrCo(μ₃-S)(CO)₈ (4, R=H; 5, R=Me; 6, R=CO₂Et) in 86-89% yields, whereas monoanion (η⁵-RC₅H₄)(CO)₃Cr⁻ (7, R=C(O)Me) reacted with FeCo₂(μ₃-S)(CO)₉ to afford the expected single isolobal displacement product (η⁵-RC₅H₄)FeCrCo(μ₃-S)(CO)₈ (8, R=C(O)Me) in 5% yield and an unexpected square pyramidal cluster FeCo₂(μ₃-S)₂(CO)₉ (9) in 45% yield. Similarly, the dianions [η⁵-C₅H₄CH₂(CH₂OCH₂)_nCH₂C₅H₄-η⁵][(CO)₃Cr⁻]₂ (10, n=1; 11, n=2; 12, n=3) reacted with two molecules of FeCo₂(μ₃-S)(CO)₉ to produce double isolobal displacement products [η⁵-C₅H₄CH₂(CH₂OCH₂)_nCH₂C₅H₄-η⁵][FeCrCo(μ₃-S)(CO)₈]₂ (13, n=1; 14, n=2; 15, n=3) in 32-36% yields, while treatment of dianion [η⁵-C₅H₄C(O)CH₂]₂[(CO)₃Cr⁻]₂ (16) with two molecules of FeCo₂(μ₃-S)(CO)₉ gave the unexpected square pyramidal cluster FeCo₂(μ₃-S)₂(CO)₉ (9) in 42% yield and the corresponding double isolobal displacement product [η⁵-C₅H₄C(O)CH₂]₂[FeCrCo(μ₃-S)(CO)₈]₂ (17) in 8% yield. Products 4-6, 8, 9, 13-15 and 17 were characterized by elemental analyses, IR and ¹H NMR spectroscopy, as well as for 4, 6 and 9 by X-ray diffraction techniques.     

Conformational behaviour of dinuclear Rh(I) complexes of the open-chain tetrapyrrolic ligand 2,2′-bidipyrrin (H2BDP)

The reaction of 2,2′-bidipyrrins H₂BDP with the Rh^I complexes [Rh(COD)(μ-OMe)]₂ and [Rh(CO)₂(μ-Cl)]₂ yields the neutral species [{Rh(COD)}₂BDP] (7, 8) and [{Rh(CO)₂}₂BDP] (2, 9), respectively. Treatment of the COD complexes with carbon monoxide results in the exchange of all COD ligands against CO. Ligand exchange studies on the carbonyl complexes 2 and 9 with different phosphane donors reveal the regioselective exchange of one CO per metal ion. In most cases, the reaction is accompanied by a large conformational change of the tetrapyrrole from a syn to an anti conformation. This conformational change was resolved by a combination of NMR spectroscopy and X-ray diffraction studies.     

Synthesis, characterization and reactivity of the molybdenum(VI) complex [MoCl(NAr)2(CH2CMe2Ph)] (Ar=2,6-Pr2C6H3)

The compounds [MoCl(NAr)₂R] (R=CH₂CMe₂Ph (1) or CH₂CMe₃(2); Ar=2,6-Prⁱ₂C₆H₃) have been prepared from [MoCl₂(NAr)₂(dme)] (dme=1,2-dimethoxyethane) and one equivalent of the respective Grignard reagent RMgCl in diethyl ether. Similarly, the mixed-imido complex [MoCl₂(NAr)(NBu^t)(dme)] affords [MoCl(NAr)(NBu^t)(CH₂CMe₂Ph)] (3). Chloride substitution reactions of 1 with the appropriate lithium reagents afford the compounds [MoCp(NAr)₂(CH₂CMe₂Ph)] (4) (Cp=cyclopentadienyl), [MoInd(NAr)₂(CH₂CMe₂Ph)] (5) (Ind=Indenyl), [Mo(OBu^t)(NAr)₂(CH₂CMe ₂Ph)] (6), [MoMe(NAr)₂(CH₂CMe₂Ph)] (7), [MoMe(PMe₃)(NAr)₂(CH₂CMe ₂Ph)] (8) (formed in the presence of PMe₃) and [Mo(NHAr)(NAr)₂(CH₂CMe₂P h)](9). In the latter case, a by-product {[Mo(NAr)₂(CH₂CMe₂Ph) ]₂(μ-O)}(10) has also been isolated. The crystal structures of 1, 4, 5 and 10 have been determined. All possess distorted tetrahedral metal centres with cis near-linear arylimido ligands; in each case (except 5, for which the evidence is unclear) there are α-agostic interactions present.     

Cationic methyl complexes of rhodium(III): synthesis, structure, and some reactions

Cationic methyl complex of rhodium(III), trans-[Rh(Acac)(PPh₃)₂(CH₃)(CH₃CN)][BPh₄] (1) is prepared by interaction of trans-[Rh(Acac)(PPh₃)₂(CH₃)I] with AgBPh₄ in acetonitrile. Cationic methyl complexes of rhodium(III), cis-[Rh(Acac)(PPh₃)₂ (CH₃)(CH₃CN)][BPh₄] (2) and cis-[Rh(BA)(PPh₃)₂(CH₃)(CH₃CN)][BPh₄] (3) (Acac, BA are acetylacetonate and benzoylacetonate, respectively), are obtained by CH₃I oxidative addition to rhodium(I) complexes [Rh(Acac)(PPh₃)₂] and [Rh(BA)(PPh₃)₂] in acetonitrile in the presence of NaBPh₄. Complexes 2 and 3 react readily with NH₃ at room temperature to form cis-[Rh(Acac)(PPh₃)₂(CH₃)(NH₃)][BPh₄] (4) and cis-[Rh(BA)(PPh₃)₂(CH₃)(NH₃)][BPh₄] (5), respectively. Complexes 1-5 were characterized by elemental analysis, ¹H and ³¹P{¹H} NMR spectra. Complexes 1, 2, 3 and 4 were characterized by X-ray diffraction analysis. Complexes 2 and 3 in solutions (CH₂Cl₂, CHCl₃) are presented as mixtures of cis-(PPh₃)₂ isomers involved into a fluxional process. Complex 2 on heating in acetonitrile is converted into trans-isomer 1. In parallel with that isomerization, reductive elimination of methyl group with formation of [CH₃PPh₃][BPh₄] takes place. Replacement of CH₃CN in complexes 1 and 2 by anion I⁻ yields in both cases the neutral complex trans-[Rh(Acac)(PPh₃)₂(CH₃)I]. Strong trans influence of CH₃ ligand manifests itself in the elongation (in solid) and labilization (in solution) of rhodium-acetonitrile nitrogen bond.     

Syntheses and structures of iron carbonyl complexes derived from N-(5-methyl-2-thienylmethylidene)-2-thiolethylamine and N-(6-methyl-2-pyridylmethylidene)-2-thiolethylamine

The reaction of N-(5-methyl-2-thienylmethylidene)-2-thiolethylamine (1) with Fe₂(CO)₉ in refluxing acetonitrile yielded di-(μ₃-thia)nonacarbonyltriiron (2), μ-[N-(5-methyl-2-thienylmethyl)-η¹:η¹(N);η¹:η¹(S)-2-thiolatoethylamido]hexacarbonyldiiron (3), and N-(5-methyl-2-thienylmethylidene)amine (4). If the reaction was carried out at 45 °C, di-μ-[N-(5-methyl-2-thienylmethylidene)-η¹(N);η¹(S)-2-thiolethylamino]-μ-carbonyl-tetracarbonyldiiron (5) and trace amount of 4 were obtained. Stirring 5 in refluxing acetonitrile led to the thermal decomposition of 5, and ligand 1 was recovered quantitatively. However, in the presence of excess amount of Fe₂(CO)₉ in refluxing acetonitrile, complex 5 was converted into 2-4. On the other hand, the reaction of N-(6-methyl-2-pyridylmethylidene)-2-thiolethylamine (6) with Fe₂(CO)₉ in refluxing acetonitrile produced 2, μ-[N-(6-methyl-2-pyridylmethyl)-η¹ (N_py);η¹:η¹(N); η¹:η¹(S)-2-thiolatoethylamido]pentacarbonyldiiron (7), and μ-[N-(6-methyl-2-pyridylmethylidene)-η²(C,N);η¹:η¹(S)-2- thiolethylamino]hexacarbonyldiiron (8). Reactions of both complex 7 and 8 with NOBF₄ gave μ-[(6-methyl-2-pyridylmethyl)-η¹(N_py);η¹:η¹(N);η¹:η¹(S)-2-thiolatoethylamido](acetonitrile)tricarbonylnitrosyldiiron (9). These reaction products were well characterized spectrally. The molecular structures of complexes 3, 7-9 have been determined by means of X-ray diffraction. Intramolecular 1,5-hydrogen shift from the thiol to the methine carbon was observed in complexes 3, 7, and 9.     

Oxalate-bridged dirhenium(I) hexacarbonyl complexes: synthesis, reactions, and crystal structures

The complex [{Re(CO)₅}₂(μ,η¹:η¹-C₂O₄)] 1 undergoes thermal decarbonylation to give [Re₂(CO)₆(C₂O₄)]_n, which reacts with triphenylphosphine and trans-1,2-bis(diphenylphosphino)ethylene (dppene) to give anti-[Re₂(PPh₃)₂(CO)₆(μ,η²:η²-C₂O₄)] 2 and [Re₂(μ-dppene)(CO)₆(μ,η²:η²-C₂O₄)] 4, respectively. Complex 2 is oxidized on prolonged exposure to air (1 week) to form anti-[Re₂(OPPh₃)₂(CO)₆(μ,η²:η²-C₂O₄)] 3. In the presence of excess dppene, the complex [Re₂(μ-dppene)₂(CO)₆(μ,η¹:η¹-C₂O₄)] 5 is also formed alongside 4. With the chelating diphosphine 1,3-bis(diphenylphosphino)propane (dppp), the complex [(η²-dppp)Re(CO)₃(μ,η¹:η¹-C₂O₄)Re(CO)₃(η²-dppp)] 6 is formed. The structures of 3 and 4 have been determined by X-ray crystallography. The dppene ligand in complex 4 adopts an unusual “syn” conformation wherein the two phosphorus lone pairs of electrons are eclipsed, thus forming an “A-frame” type of bridge.     

Comparative reactivity studies of dppf-containing CpRu and (C6Me6)Ru complexes towards different donor ligands (dppf=1,1-bis(diphenylphosphino)ferrocene)

[CpRu(dppf)Cl] (Cp=η⁵-C₅H₅) (1) and [(HMB)Ru(dppf)Cl]PF₆ ((HMB)=η⁶-C₆Me₆) (3) react with different donor ligands to give rise to N-, P- and S-bonded complexes. The stoichiometric reactions of 1 and 3 with NaNCS give the mononuclear complexes [CpRu(dppf)(NCS)] (2) and [(HMB)Ru(dppf)(NCS)]PF₆ (4), respectively, in yields above 80%, while 3 also gives a dppf-bridged diruthenium complex [(HMB)Ru(NCS)₂]₂(μ-dppf) (5) in 67% yield from reaction with four molar equivalents of NaNCS. Compound 5 is also obtained in 70% yield from the reaction of 4 with excess NaNCS. With CH₃CN in the presence of salts, both 1 and 3 give their analogous solvento derivatives [CpRu(dppf)(CH₃CN)]BPh₄ (6) and [(HMB)Ru(dppf)(CH₃CN)] (PF₆)₂ (7). With phosphines, the reaction of 1 gives chloro-displaced complexes [(CpRu(dppf)L]PF₆ (L =PMe₃ (8), PMe₂Ph(9)), whereas the reaction of 3 with PMe₂Ph leads to substitution of dppf, giving [(HMB)Ru(PMe₂Ph)₂Cl] PF₆ (10). The reaction of 1 with NaS₂CNEt₂ gives a dinuclear dppf-bridged complex [{CpRu(S₂CNEt₂)}₂(μ-dppf)] (11), whereas that of 3 results in loss of the HMB ligand giving a mononuclear complex [Ru(dppf)(S₂CNEt₂)₂] (12). With elemental sulfur S₈, 1 is oxidized to give a dinuclear CpRu^III dppf-chelated complex [{CpRu(dppf)}₂(μ-S₂)](BPh₄)Cl (13), whereas 3 undergoes oxidation at the ligand, giving a dppf-displaced complex [(HMB)Ru(CH₃CN)₂Cl]PF₆ (14) and free dppfS₂. The structures of 1, 2, 5-9, 11, 13 and 14 were established by X-ray single crystal diffraction analyses. Of these, 5 and 11 both contain a dppf-bridge between Ru^II centers, while 13 is a dinuclear CpRu^III disulfide-bridged complex; all the others are mononuclear. All complexes obtained were also spectroscopically characterized.     

Synthesis of the water-soluble [Rh(Tpms)(CO)(PTA)] compound, the first transition metal complex bearing the 1,3,5-triaza-7-phosphaadamantane (PTA) and the tris(1-pyrazolyl)methanesulfonate (Tpms) ligands

The water-soluble Rh^I compound [Rh(Tpms)(CO)(PTA)] (1) (Tpms = O₃SC(pz)₃⁻, PTA = 1,3,5-triaza-7-phosphaadamantane) has been easily prepared in high yield by a single-pot reaction of [{Rh(CO)₂(μ-Cl)}₂] with PTA and the tris(1-pyrazolyl)methanesulfonate lithium salt Li(Tpms), in a CH₂Cl₂/MeOH solution at room temperature. This synthetic strategy can be easily applied to the preparation of general [Rh(Tpms)(CO)(L)] (L = phosphine) complexes and constitutes a substantial improvement over the previously described procedures. Compound 1 is air stable in the solid state and water-soluble, affording stable solutions under an inert atmosphere. It has been characterized by IR, ¹H, ³¹P{¹H} and ¹³C{¹H} NMR spectroscopies, elemental and single crystal X-ray diffraction structural analyses. The solid state structure of 1 has a square-planar geometry with the Tpms ligand coordinating the metal centre in a (κ²: N,N) bipodal mode. The title compound has also been investigated by cyclic voltammetry in CH₃CN, and values of the E_L Lever and P_L Pickett electrochemical parameters (which measure the ligand net electron-donor character) are proposed for the PTA ligand. Complex 1 represents the first example of a transition metal complex bearing both PTA and Tpms (or any other tris(1-pyrazolyl)methane or derivative) ligands.     

Functionalized cyclodiphosphazanes cis-[BuNP(OR)]2 (R=C6H4OMe-o, CH2CH2OMe, CH2CH2SMe, CH2CH2NMe2) as neutral 2e, 4e or 8e donor ligands

Cyclodiphosphazanes having donor functionalities such as cis-[^tBuNP(OR)]₂ (R = C₆H₄OMe-o (2); R = CH₂CH₂OMe (3); R = CH₂CH₂SMe (4); R = CH₂CH₂NMe₂ (5)) were obtained in good yield by reacting cis-[^tBuNPCl]₂ (1) with corresponding nucleophiles. The reactions of 2-5 with [RuCl₂(η⁶-cymene)]₂, [MCl(COD)]₂ (M = Rh, Ir), [PdCl₂(PEt₃)]₂ and [MCl₂(COD)] (M=Pd, Pt) result in the formation of exclusively monocoordinated mononuclear complexes of the type cis-[{^tBuNP(OR)}₂ML_n-κP] irrespective of the reaction stoichiometry and the reaction conditions. In contrast, 2-5 react with [RhCl(CO)₂]₂, [PdCl(η³-C₃H₅)]₂, CuX (X=Cl, Br, I) to give homobinuclear complexes. Interestingly, CuX produces both mono and binuclear complexes depending on the stoichiometry of the reactants and the reaction conditions. The mononuclear complexes on treatment with appropriate metal reagents furnish heterometallic complexes.     

Chemistry of Fischer-type rhenacyclobutadiene complexes. II. Reactions with alkynes and sulfonium ylides, and rearrangements induced by nitriles and pyridine

Further investigations into the chemistry of the rhenacyclobutadiene complexes (CO)₄Re(η²-C(R)C(CO₂Me)C(X)) (1: R=Me, X=OEt (1a), O(CH₂)₃CCH (1b), NEt₂ (1c); R=CHEt₂, X=OEt (1d); R=Ph, X=OEt (1e)) are reported. Reactions of 1 with alkynes at reflux temperature of toluene and at ambient temperature either under photochemical conditions or in the presence of PdO yield ring-substituted η⁵-cyclopentadienylrhenium tricarbonyl complexes, 2. The symmetrical alkynes R^′CCR^′ (R^′=Ph, Me, CO₂Me) afford the pentasubstituted complexes (η⁵-C₅(Me)(CO₂Me)(OEt)(Ph)(Ph))Re(CO)₃ (2d), (η⁵-C₅(Me)(CO₂Me)(OEt)(Me)(Me))Re(CO)₃ (2e), (η⁵-C₅(Me)(CO₂Me)(OEt)(CO₂Me)(CO₂Me))Re(CO)₃ (2f), and (η⁵-C₅(Me)(CO₂Me)(NEt₂)(CO₂Me)(CO₂Me))Re(CO)₃ (2i) on reaction with the appropriate 1, whereas the unsymmetrical alkynes R^′CCR″ (R^′=Ph; R″=H, Me) give either only one, (η⁵-C₅(Me)(CO₂Me)(OEt)(Ph)H)Re(CO)₃ (2a)), or both, (η⁵-C₅(Me)(CO₂Me) (OEt)(Ph)(Me))Re(CO)₃ (2b) and (η⁵-C₅(Me)(CO₂Me)(OEt)(Me)(Ph))Re(CO)₃ (2c), (η⁵-C₅(Ph)(CO₂Me)(OEt)(Ph)H)Re(CO)₃ (2g) and (η⁵-C₅(Ph)(CO₂Me)(OEt)(H)(Ph))Re(CO)₃ (2h), of the possible products of [3 + 2] cycloaddition of alkyne to η²-C(R)C(CO₂Me)C(X). Thermolysis of (CO)₄Re(η²-C(Me)C(CO₂Me)C(O(CH₂)₃CCH)) (1b) containing a pendant alkynyl group proceeds to (η⁵-C₅(Me)(CO₂Me)(O(CH₂)₃)H)Re(CO)₃ (2j), a η⁵-cyclopentadienyl-dihydropyran fused-ring product. Competition experiments showed that each of PhCCH and MeO₂CCCCO₂Me reacts faster than PhCCPh with 1a. The results with unsymmetrical alkynes are rationalized by steric properties of substituents at the CC and ReC bonds and by a preference of ReC(Me) over ReC(OEt) to undergo alkyne insertion. A mechanism is proposed that involves substitution of a trans CO by alkyne in 1, insertion of alkyne into ReC bond to give a rhenabenzene intermediate, and collapse of the latter to 2. Complexes 1a and 1d undergo rearrangement in MeCN at reflux temperature to give rhenafuran-like products, (CO)₄Re(κ²-OC(OMe)C(CHCR₂)C(OEt)) (R=H (3a) or Et (3b)). The reaction of 1d also proceeds in EtCN, PhCN, and t-BuCN at comparable temperature, but is slower (especially in t-BuCN) than in MeCN. In pyridine at reflux temperature, 1a undergoes a similar rearrangement, with CO substitution, to give (CO)₃(py)Re(κ²-OC(OMe)C(CHCEt₂)C(OEt)) (4). A mechanism is proposed for these reactions. The sulfonium ylides Me₂SCHC(O)Ph and Me₂SC(CN)₂ (Me₂SCRR^′) react with 1a in acetonitrile at reflux temperature by nucleophilic addition of the ylide to the ReC(Me) carbon, loss of Me₂S, and rearrangement to a rhenafuran-type structure to yield (CO)₄Re(κ²-OC(OMe)C(C(Me)CRR^′)C(OEt)) (R=H, R^′=C(O)Ph (5a); R=R^′CN (5b)). All new compounds were characterized by a combination of elemental analysis, mass spectrometry, and IR and NMR spectroscopy.     

Construction of optically active multimetallic systems of rhodium(I), palladium(II), and ruthenium(II) with a P-chiral tetraphosphine ligand

The treatment of optically P-chiral tetraphosphine, (3S,6R,9R,12S)-6,9-di-tert-butyl-2,2,3,12,13,13-hexamethyl-3,6,9,12-tetraphosphatetradecane (1), with rhodium(I), palladium(II), and ruthenium(II) complex precursors led to the selective formation of mono-, di-, or trinuclear homo- or heterometallic complexes, [Rh(1)]SbF₆ (4), [{Rh(nbd)}₂(1)](SbF₆)₂ (3), [{Pd(η³-allyl)}₂(1)](SbF₆)₂ (5), [{RuCl(η⁵-C₅(CH₃)₅)}₂(1)] (6), and [{RuCl₂(η⁶-benzene)}₂(PdCl₂)(1)] (8). These complexes were characterized by NMR and X-ray crystallographic analysis.     

Mono- and bis-(2-dimethylaminoethyl)tetramethylcyclopentadienyl zirconium(IV) complexes: synthesis and structural studies in crystalline state and in solutions

A novel half-sandwich Zr(IV) complex [η⁵:η¹-N-C₅(CH₃)₄CH₂CH₂N(CH₃)₂]ZrCl₃ (6) together with zirconocene dichlorides [η⁵-C₅(CH₃)₄CH₂CH₂N(CH₃)₂][η⁵-C₅(CH₃)₅]ZrCl₂ (4) and [η⁵-C₅(CH₃)₄CH₂CH₂N(CH₃)₂]₂ZrCl₂ (5) have been prepared. Complex 6 has been isolated and characterized in three different forms, namely, as an adduct with THF 6a, an adduct with tetrahydrothiophene 6b, and a solvent-free form 6c. Molecular structures of complexes 4, 6b, and 6c have been established by X-ray diffraction analysis. Complex 6c has been shown to be a monomeric solvent-free half sandwich Zr(IV) complex. The dynamic behavior of complex 6a in a non-solvating medium (an equilibrium between 6a and 6c along with a degenerate interconversion of the Zr-C_cp-CH₂-CH₂-N(CH₃)₂-(Zr) pseudo-five-member metallacycle) have been studied by the variable-temperature ¹H and ¹³C{¹H} NMR spectroscopy. The activation parameters for the degenerate five-member cycle interconversion have been elucidated.