Preparation of mononuclear and dinuclear Rh hydrotris(pyrazolyl)borato complexes containing arenethiolato ligands and conversion of the mononuclear complexes into dinuclear Rh-Rh and Rh-Ir complexes with bridging arenethiolato ligands

Reactions of [Tp*Rh(coe)(MeCN)](; Tp*= HB(3,5-dimethylpyrazol-1-yl)(3); coe = cyclooctene) with one equiv. of the organic disulfides, PhSSPh, TolSSTol (Tol = 4-MeC(6)H(4)), PySSPy (Py = 2-pyridyl), and tetraethylthiuram disulfide in THF at room temperature afforded the mononuclear Rh(III) complexes [Tp*Rh(SPh)(2)(MeCN)](3a), [Tp*Rh(STol)(2)(MeCN)](3b), [Tp*Rh(eta(2)-SPy)(eta(1)-SPy)](6), and [Tp*Rh(eta(2)-S(2)CNEt(2))(eta(1)-S(2)CNEt(2))](7), respectively, via the oxidative addition of the organic disulfides to the Rh(I) center in 1. For the Tp analogue [TpRh(coe)(MeCN)](2, Tp = HB(pyrazol-1-yl)(3)), the reaction with TolSSTol proceeded similarly to give the bis(thiolato) complex [TpRh(STol)(2)(MeCN)](4) as a major product but the dinuclear complex [[TpRh(STol)](2)(micro-STol)(2)](5) was also obtained in low yield. Complex 3 was treated further with the Rh(III) or Ir(III) complexes [(Cp*MCl)(2)(micro-Cl)(2)](Cp*=eta(5)-C(5)Me(5)) in THF at room temperature, yielding the thiolato-bridged dinuclear complexes [Tp*RhCl(micro-SPh)(2)MCp*Cl](8a: M = Rh, 8b: M = Ir). Dirhodium complex [TpRhCl(micro-STol)(2)RhCp*Cl](9) was obtained similarly from 4 and [(Cp*RhCl)(2)(micro-Cl)(2)]. Anion metathesis of 8a proceeds only at the Rh atom with the Cp* ligand to yield [Tp*RhCl(micro-SPh)(2)RhCp*(MeCN)][PF(6)](10), when treated with excess KPF(6) in CH(2)Cl(2)-MeCN. The X-ray analyses have been undertaken to determine the detailed structures of 3b, 4, 5, 6, 7, 8a, 9, and 10.     

Variable coordination of amine functionalised N-heterocyclic carbene ligands to Ru, Rh and Ir: C-H and N-H activation and catalytic transfer hydrogenation

Chelating amine and amido complexes of late transition metals are highly valuable bifunctional catalysts in organic synthesis, but complexes of bidentate amine-NHC and amido-NHC ligands are scarce. Hence, we report the reactions of a secondary-amine functionalised imidazolium salt 2a and a primary-amine functionalised imidazolium salt 2b with [(p-cymene)RuCl(2)](2) and [Cp*MCl(2)](2) (M = Rh, Ir). Treating 2a with [Cp*MCl(2)](2) and NaOAc gave the cyclometallated compounds Cp*M(C,C)I (M = Rh, 3; M = Ir, 4), resulting from aromatic C-H activation. In contrast, treating 2b with [(p-cymene)RuCl(2)](2), Ag(2)O and KI gave the amine-NHC complex [(p-cymene)Ru(C,NH(2))I]I (5). The reaction of 2b with [Cp*MCl(2)](2) (M = Rh, Ir), NaO(t)Bu and KI gave the amine-NHC complex [Cp*Rh(NH(2))I]I (6) or the amido-NHC complex Cp*Ir(C,NH)I (7); both protonation states of the Ir complex could be accessed: treating 7 with trifluoroacetic acid gave the amine-NHC complex [Cp*Ir(C,NH(2))I][CF(3)CO(2)] (8). These are the first primary amine- or amido-NHC complexes of Rh and Ir. Solid-state structures of the complexes 3-8 have been determined by single crystal X-ray diffraction. Complexes 5, 6 and 7 are pre-catalysts for the catalytic transfer hydrogenation of acetophenone to 1-phenylethanol, with ruthenium complex 5 demonstrating especially high reactivity.     

Silylenediamido [(CH3)2Si(NTs)2(2-); Ts = p-CH3C6H4SO2] complexes of iridium: synthesis, structures and facile Si-N bond cleavage

The N,N'-bis(sulfonyl)diaminosilane TsdmsinH(2) (TsdmsinH(2) = (CH(3))(2)Si(NHTs)(2), Ts = p-CH(3)C(6)H(4)SO(2)) reacted with [Cp*IrCl(2)](2) (Cp* = eta(5)-C(5)(CH(3))(5)) in the presence of a base to give the coordinatively unsaturated (silylenediamido)iridium complex [Cp*Ir(Tsdmsin)] (2), which was further converted to the 18e adducts [Cp*Ir(Tsdmsin)L] (L = P(C(6)H(5))(3) (3a), P(OC(2)H(5))(3), CO); the reactions of 2 and 3a with water led to the formation of the imido-bridged dinuclear complex [Cp*Ir(micro(2)-NTs)(2)IrCp*] and the bis(amido) complex [Cp*Ir(NHTs)(2){P(C(6)H(5))(3)}], respectively.     

Cyclodiphosphazanes with hemilabile ponytails: synthesis, transition metal chemistry (Ru(II), Rh(I), Pd(II), Pt(II)), and crystal and molecular structures of mononuclear (Pd(II), Rh(I)) and bi- and tetranuclear rhodium(I) complexes

Cyclodiphosphazanes having hemilabile ponytails such as cis-[(t)()BuNP(OC(6)H(4)OMe-o)](2) (2), cis-[(t)()BuNP(OCH(2)CH(2)OMe)](2) (3), cis-[(t)BuNP(OCH(2)CH(2)SMe)](2) (4), and cis-[(t)BuNP(OCH(2)CH(2)NMe(2))](2) (5) were synthesized by reacting cis-[(t)()BuNPCl](2) (1) with corresponding nucleophiles. The reaction of 2 with [M(COD)Cl(2)] afforded cis-[MCl(2)(2)(2)] derivatives (M = Pd (6), Pt (7)), whereas, with [Pd(NCPh)(2)Cl(2)], trans-[MCl(2)(2)(2)] (8) was obtained. The reaction of 2 with [Pd(PEt(3))Cl(2)](2), [{Ru(eta(6)-p-cymene)Cl(2)](2), and [M(COD)Cl](2) (M = Rh, Ir) afforded mononuclear complexes of Pd(II) (9), Ru(II) (11), Rh(I) (12), and Ir(I) (13) irrespective of the stoichiometry of the reactants and the reaction condition. In the above complexes the cyclodiphosphazane acts as a monodentate ligand. The reaction of 2 with [PdCl(eta(3)-C(3)H(5))](2) afforded binuclear complex [(PdCl(eta(3)-C(3)H(5)))(2){((t)BuNP(OC(6)H(4)OMe-o))(2)-kappaP}] (10). The reaction of ligand 3 with [Rh(CO)(2)Cl](2) in 1:1 ratio in CH(3)CN under reflux condition afforded tetranuclear rhodium(I) metallamacrocycle (14), whereas the ligands 4 and 5 afforded bischelated binuclear complexes 15 and 16, respectively. The crystal structures of 8, 9, 12, 14, and 16 are reported.     

Synthesis, reactivity, spectroscopic characterization, X-ray structures, PGSE, and NOE NMR studies of (eta5-C5Me5)-rhodium and -iridium derivatives containing bis(pyrazolyl)alkane ligands

Rhodium(III) and iridium(III) complexes containing bis(pyrazolyl)methane ligands (pz = pyrazole, L' in general; specifically, L1 = H2C(pz)2, L2 = H2C(pzMe2)2, L3 = H2C(pz4Me)2, L4 = Me2C(pz)2), have been prepared in a study exploring the reactivity of these ligands toward [Cp*MCl(mu-Cl)]2 dimers (M = Rh, Ir; Cp* = pentamethylcyclopentadienyl). When the reaction was carried out in acetone solution, complexes of the type [Cp*M(L')Cl]Cl were obtained. However, when L1 and L2 ligands have been employed with excess [Cp*MCl(mu-Cl)]2, the formation of [Cp*M(L')Cl][Cp*MCl3] species has been observed. PGSE NMR measurements have been carried out for these complexes, in which the counterion is a cyclopentadienyl metal complex, in CD2Cl2 as a function of the concentration. The hydrodynamic radius (rH) and, consequently, the hydrodynamic volume (VH) of all the species have been determined from the measured translational self-diffusion coefficients (Dt), indicating the predominance of ion pairs in solution. NOE measurements and X-ray single-crystal studies suggest that the [Cp*MCl3]- approaches the cation, orienting the three Cl-legs of the "piano-stool" toward the CH2 moieties of the bis(pyrazolyl)methane ligands. The reaction of 1 equiv of [Cp*M(L')Cl]Cl or [Cp*M(L')Cl][Cp*MCl3] with 1 equiv of AgX (X = ClO4 or CF3SO3) in CH2Cl2 allows the generation of [Cp*M(L')Cl]X, whereas the reaction of 1 equiv of [Cp*M(L')Cl] with 2 equiv of AgX yields the dicationic complexes [Cp*M(L')(H2O)][X]2, where single water molecules are directly bonded to the metal atoms. The solid-state structures of a number of complexes were confirmed by X-ray crystallographic studies. The reaction of [Cp*Ir(L')(H2O)][X]2 with ammonium formate in water or acetone solution allows the generation of the hydride species [Cp*Ir(L')H][X].     

One-step synthesis of alkenyl ketone complexes from Cp*RhCl2(PPh3), alkyne and H2O in the presence of KPF6

The reaction of Cp*RhCl2(PPh3) 1 with 1-alkyne and H2O in the presence of KPF6 afforded the alkenyl ketone complex [Cp*Rh(PPh3)(CPh=CHCOCH2R)](PF6) [R = p-tolyl (3a), R = Ph (3b)], whereas Cp*IrCl2(PPh3) 2 or [(eta 6-C6Me6)RuCl2(PPh3) gave the corresponding [Cp*IrCl(CO)(PPh3)](PF6) 5a and [(eta 6-C6Me6)RuCl(CO)(PPh3)](PF6).     

Mechanism of the mild functionalization of arenes by diboron reagents catalyzed by iridium complexes. Intermediacy and chemistry of bipyridine-ligated iridium trisboryl complexes

This paper describes mechanistic studies on the functionalization of arenes with the diboron reagent B(2)pin(2) (bis-pinacolato diborane(4)) catalyzed by the combination of 4,4'-di-tert-butylbipyridine (dtbpy) and olefin-ligated iridium halide or olefin-ligated iridium alkoxide complexes. This work identifies the catalyst resting state as [Ir(dtbpy)(COE)(Bpin)(3)] (COE = cyclooctene, Bpin = 4,4,5,5-tetramethyl-1,3,2-dioxaborolanyl). [Ir(dtbpy)(COE)(Bpin)(3)] was prepared by independent synthesis in high yield from [Ir(COD)(OMe)](2), dtbpy, COE, and HBpin. This complex is formed in low yield from [Ir(COD)(OMe)](2), dtbpy, COE, and B(2)pin(2). Kinetic studies show that this complex reacts with arenes after reversible dissociation of COE. An alternative mechanism in which the arene reacts with the Ir(I) complex [Ir(dtbpy)Bpin] after dissociation of COE and reductive elimination of B(2)pin(2) does not occur to a measurable extent. The reaction of [Ir(dtbpy)(COE)(Bpin)(3)] with arenes and the catalytic reaction of B(2)pin(2) with arenes catalyzed by [Ir(COD)(OMe)](2) and dtbpy occur faster with electron-poor arenes than with electron-rich arenes. However, both the stoichiometric and catalytic reactions also occur faster with the electron-rich heteroarenes thiophene and furan than with arenes, perhaps because eta(2)-heteroarene complexes are more stable than the eta(2)-arene complexes and the eta(2)-heteroarene or arene complexes are intermediates that precede oxidative addition. Kinetic studies on the catalytic reaction show that [Ir(dtbpy)(COE)(Bpin)(3)] enters the catalytic cycle by dissociation of COE, and a comparison of the kinetic isotope effects of the catalytic and stoichiometric reactions shows that the reactive intermediate [Ir(dtbpy)(Bpin)(3)] cleaves the arene C-H bond. The barriers for ligand exchange and C-H activation allow an experimental assessment of several conclusions drawn from computational work. Most generally, our results corroborate the conclusion that C-H bond cleavage is turnover-limiting, but the experimental barrier for this bond cleavage is much lower than the calculated barrier.     

Synthesis and characterization of the hexagonal prismatic cage [THF[subset or is implied by][PhB(CN)(3)](6)[Cp*Rh](6)](6+)

Condensation of [Cp*Rh(CH(3)NO(2))(n)](2+) and the tricyanoborate [PhB(CN)(3)](-) affords the hexagonal bipyramidal cage [[PhB(CN)(3)](6)[Cp*Rh](6)](6+), demonstrating that tetrahedral tricyanide building blocks can lead to novel cage structures.     

Iridium(III) molecular catalysts for water oxidation: the simpler the faster

We report on three Ir(iii) molecular catalysts for water oxidation: 1, [Cp*Ir(ppy)Cl]; 2, [Cp*Ir(bzpy)NO(3)]; 3, [Cp*Ir(H(2)O)(3)](NO(3))(2). 2 and 3 are water-soluble and show a long-term activity ca. 2 and 3 times higher than 1. It is remarkable that 3, having the simplest structure, is the catalyst with the highest activity.     

On the reactivity toward ketones of new methyl amino complexes of Rh(III) and Ag(I). Synthesis of ortho-rhodiated acetophenone methyl imine complexes

MeNH(2) reacts with silver salts AgX (2:1) to give [Ag(NH(2)Me)(2)]X [X = TfO = CF(3)SO(3) (1.TfO) and ClO(4) (1.ClO(4))]. Neutral mono(amino) Rh(III) complexes [Rh(Cp*)Cl(2)(NH(2)R)] [R = Me (2a), To = C(6)H(4)Me-4 (2b)] have been prepared by reacting [Rh(Cp*)Cl(mu-Cl)](2) with RNH(2) (1:2). The following cationic methyl amino complexes have also been prepared: [Rh(Cp*)Cl(NH(2)Me)(PPh(3))]TfO (3.TfO), from [Rh(Cp*)Cl(2)(PPh(3))] and 1.TfO (1:1); [Rh(Cp*)Cl(NH(2)R)2]X, where R = Me, X = Cl, (4a.Cl), from [Rh(Cp*)Cl(mu-Cl)]2 and MeNH2 (1:4), or R = Me, X = ClO4 (4a.ClO4), from 4a.Cl and NaClO4 (1:4.8), or R = To, X = TfO (4b.TfO), from [Rh(Cp*)Cl(mu-Cl)](2), ToNH(2) and TlTfO (1:4:2); [Rh(Cp*)(NH(2)Me)(tBubpy)](TfO)(2) (tBubpy = 4,4'-di-tert-butyl-2,2'-bipyridine, 5.TfO), from 2a, TlTfO and tBubpy (1:2:1); [Rh(Cp*)(NH(2)Me)(3)](TfO)2 (6.TfO) from [Rh(Cp*)Cl(mu-Cl)](2) and 1.TfO (1:4). 2-6 constitute the first family of methyl amino complexes of rhodium. 1 and 4a.ClO(4) react with acetone to give, respectively, the methyl imino complexes [Ag{N(Me)=CMe(2)}()]X [X = TfO (7.TfO), ClO(4) (7.ClO(4))], and [Rh(Cp*)Cl(Me-imam)]ClO(4) [8.ClO(4), Me-imam = N,N'-N(Me)=C(Me)CH(2)C(Me)(2)NHMe]. 7.X (X = TfO, ClO(4)) are new members of the small family of methyl acetimino complexes of any metal whereas 8.ClO4 results after a double acetone condensation to give the corresponding bis(methyl acetimino) complex and an aldol-like condensation of the two imino ligands. The acetimino complex [Ag(NH=CMe(2))(2)]ClO(4) reacts with [Rh(Cp*)Cl(imam)]ClO(4) [1:1, imam = N,N'-NH=C(Me)CH(2)C(Me)(2)NH(2)] to give [Rh(Cp*)(imam)(NH=CMe(2))](ClO(4))(2) (9a.ClO(4)). 8.ClO(4) reacts with AgClO(4) (1:1) in MeCN to give [Rh(Cp*)(Me-imam)(NCMe)](ClO(4))2 (9b.ClO(4)), which in turn reacts with XyNC (Xy = C(6)H(3)Me(2)-2,6) or with MeNH(2) (1:1) to give [Rh(Cp*)(Me-imam)L](ClO(4))(2) [L = XyNC (9c.ClO(4)), MeNH(2) (9d.ClO(4))]. 6.TfO reacts with acetophenone to give [Rh(Cp*){C,N-C(6)H(4)C(Me)=N(Me)-2}(NH(2)Me)]TfO (10a.TfO), the first complex resulting from such a condensation and cyclometalation reaction. In turn, 10a.TfO reacts with isocyanides RNC (1:1) at room temperature to give [Rh(Cp*){C,N-C(6)H(4)C(Me)=NMe-2}(CNR)]TfO [R = tBu (10b.TfO), Xy (10c.TfO)], or 1:12 at 60 degrees C to give [Rh(Cp*){C,N-C(=NXy)C(6)H(4)C(Me)=N(Me)-2}(CNXy)]TfO (11.TfO). The crystal structures of 9a.ClO(4).acetone-d6, 9c.ClO(4), and 10a.TfO have been determined.     

Synthesis and reactivity of fluoro complexes: Part 2. Rhodium(I) fluoro complexes with alkene and phosphine ligands. Synthesis of the first isolated rhodium(I) bifluoride complexes. Structure of [Rh3(mu3-OH)2(COD)(3)](HF2) by X-ray powder diffraction

The reaction between [Rh(mu-OH)(COD)](2) (COD = 1,5-cyclooctadiene) and 73% HF in THF gives [Rh(3)(mu(3)-OH)(2)(COD)(3)](HF(2)) (1). Its crystal structure, determined by ab initio X-ray powder diffraction methods (from conventional laboratory data), contains complex trimetallic cations linked together in 1D chains by a mu(3)-OH...F-H-F...HO-mu(3) sequence of strong hydrogen bonds. The complex [Rh(mu-F)(COE)(2)](2) (COE = cyclooctene; 2), prepared by reacting [Rh(mu-OH)(COE)(2)](2) with NEt(3).3HF (3:2), has been characterized. Complex 1 reacts with PR(3) (1:3) to give [RhF(COD)(PR(3))] [R = Ph (3), C(6)H(4)OMe-4 (4), (i)Pr (5), Cy (6)] that can be prepared directly by reacting [Rh(mu-OH)(COD)](2) with 73% HF and PR(3) (1:2:2). The reactions of 1 with PPh(3) or Et(3)P have been studied by NMR spectroscopy at different molar ratios. Complexes [RhF(PEt(3))(3)] (7), [RhF(COD)(PEt(3))] (8), and [RhF(PPh(3))(3)] (9) have been detected. The complex [Rh(F)(NBD)(iPr(3)P)] (NBD = norbornadiene; 10) was prepared by the sequential treatment of [Rh(mu-OMe)(NBD)](2) with 1 equiv of NEt(3).3HF and (i)Pr(3)P. The first isolated bifluoride rhodium(I) complexes [Rh(FHF)(COD)(PR(3))] [R = Ph (11), (i)Pr (12), Cy (13)], obtained by reacting fluoro complexes 3, 5, and 6 with NEt(3).3HF (3:1), have been characterized. The crystal structures of 3 and 11 have been determined.     

Bis-imine-cyclometalated macrocycles: synthesis, characterization and observation of solution behaviour

A novel class of cyclometalated macrocycles [(Cp*Ir)(2)(R-N=C-C(6)H(2)-C=N-R)(2)](2)(pyrazine)(2)·(OTf)(4) [R = Ph (4a), p-MeOC(6)H(4) (4b), p-MeC(6)H(4) (4c), p-ClC(6)H(4) (4d), Me (4e)]; [(Cp*Rh)(2)(R-N=C-C(6)H(2)-C=N-R)(2)](2)(pyrazine)(2)·(OTf)(4) [R = Ph (4a'), p-MeOC(6)H(4) (4b'), p-MeC(6)H(4) (4c')] and [(Cp*Ir)(2)(R-C=N-C(6)H(4)-N=C-R)(2)](2)(pyrazine)(2)·(OTf)(4) [R = Ph (5a), p-MeOC(6)H(4) (5b)] was stepwise constructed through the double-site C-H activation of aromatic bis-imine substrates. The structures of binuclear complexes and tetranuclear macrocycles were confirmed by single-crystal X-ray diffraction. Isomers were found both in binuclear species and macrocyclic complexes. Flexible substrates led to the existence of isomers for binuclear species, yet gave no isomers after macrocyclic constructions; rigid ones, in contrast, led to isomers only for macrocyclic species. The isomers of tetranuclear macrocycles were thermodynamically stable to reversible transformation on a scale of days. Robust bonding and a certain degree of rigidity were invoked to explain the existence of isomers. This is the first example, to our knowledge, in which coordinated macrocycles containing half-sandwich Cp*M (M = Ir, Rh) fragments have been constructed, without a dynamic reversible process.     

The chemoselective reactions of tyrosine-containing G-protein-coupled receptor peptides with [Cp*Rh(H2O)3](OTf)2, including 2D NMR structures and the biological consequences

The bioconjugation of organometallic complexes with peptides has proven to be a novel approach for drug discovery. We report the facile and chemoselective reaction of tyrosine-containing G-protein-coupled receptor (GPCR) peptides with [Cp*Rh(H(2)O)(3)](OTf)(2), in water, at room temperature, and at pH 5-6. We have focused on three important GPCR peptides; namely, [Tyr(1)]-leu-enkephalin, [Tyr(4)]-neurotensin(8-13), and [Tyr(3)]-octreotide, each of which has a different position for the tyrosine residue, together with competing functionalities. Importantly, all other functional groups present, i.e., amino, carboxyl, disulfide, phenyl, and indole, were not prominent sites of reactivity by the Cp*Rh tris aqua complex. Furthermore, the influence of the Cp*Rh moiety on the structure of [Tyr(3)]-octreotide was characterized by 2D NMR, resulting in the first representative structure of an organometallic-peptide complex. The biological consequences of these Cp*Rh-peptide complexes, with respect to GPCR binding and growth inhibition of MCF7 and HT29 cancer cells, will be presented for [(η(6)-Cp*Rh-Tyr(1))-leu-enkephalin](OTf)(2) and [(η(6)-Cp*Rh-Tyr(3))-octreotide](OTf)(2).     

Coordination solids derived from Cp*M(CN)3- (M = Rh,Ir)

Solutions of Rh2(OAc)4 and Et4N[Cp*Ir(CN)3] react to afford crystals of the one-dimensional coordination solid [Et4N[Cp*Ir(CN)3][Rh2(OAc)4]]. This reaction is reversed by coordinating solvents such as MeCN. The structure of the polymer consists of helical anionic chains containing Rh2(OAc)4 units linked via two of the three CN ligands of Cp*Ir(CN)3-. Use of the more Lewis acidic Rh2(O2CCF3)4 in place of Rh2(OAc)4 gave purple [(Et4N)2[Cp*Ir(CN)3]2[Rh2(O2CCF3)4]3], whose insolubility is attributed to stronger Rh-NC bonds as well as the presence of cross-linking. The species [[Cp*Rh(CN)3][Ni(en)n](PF6)] (n = 2, 3) crystallized from an aqueous solution of Et4N[Cp*Rh(CN)3] and [Ni(en)3](PF6)2; [[Cp*Rh(CN)3][Ni(en)2](PF6)] consists of helical chains based on cis-Ni(en)(2)2+ units. Aqueous solutions of Et4N[Cp*Ir(CN)3] and AgNO3 afforded the colorless solid Ag-[Cp*Ir(CN)3]. Recrystallization of this polymer from pyridine gave the hemipyridine adduct [Ag[Ag(py)][Cp*Ir(CN)3]2]. The 13C cross-polarization magic-angle spinning NMR spectrum of the pyridine derivative reveals two distinct Cp* groups, while in the pyridine-free precursor, the Cp*'s appear equivalent. The solid-state structure of [Ag[Ag(py)][Cp*Ir(CN)3]2] reveals a three-dimensional coordination polymer consisting of chains of Cp*Ir(CN)3- units linked to alternating Ag+ and Ag(py)+ units. The network structure arises by the linking of these helices through the third cyanide group on each Ir center.     

Synthesis and characterization of heterometallic clusters (Ir2Rh, Ir2W, Rh3) Containing 1,2-dicarba-closo-dodecaborane(12)-1,2-dithiolate chelate ligands, [(B10H10)C2S2]2-

The 16-electron half-sandwich complex [Cp*Ir[S2C2(B10H10)]] (Cp* = eta5-C5Me5) (1a) reacts with [[Rh(cod)(mu-Cl)]2] (cod = cycloocta-1,5-diene, C8H12) in different molar ratios to give three products, [[Cp*Ir[S2C2(B10H9)]]Rh(cod)] (2), trans-[[Cp*Ir[S2C2(B10H9)]]Rh[[S2C2(B10H10)]IrCp*]] (3), and [Rh2(cod)2[(mu-SH)(mu-SC)(CH)(B10H10)]] (4). Complex 3 contains an Ir2Rh backbone with two different Ir-Rh bonds (3.003(3) and 2.685(3) angstroms). The dinuclear complex 2 reacts with the mononuclear 16-electron complex 1a to give 3 in refluxing toluene. Reaction of 1a with [W(CO)3(py)3] (py = C5H5N) in the presence of BF3.EtO2 leads to the trinuclear cluster [[Cp*Ir[S2C2(B10H10)]]2W(CO)2] (5) together with [[Cp*Ir(CO)[S2C2(B10H10)]]W(CO)5] (6), and [Cp*Ir(CO)[S2C2(B10H10)]] (7). Analogous reactions of [Cp*Rh[S2C2(B10H10)]] (1 b) with [[Rh(cod)(mu-Cl)]2] were investigated and two complexes cis-[[Cp*Rh[S2C2(B10H10)]]2Rh] (8) and trans-[[Cp*Rh[S2C2(B10H10)]]2Rh] (9) were obtained. In refluxing THF solution, the cisoid 8 is converted in more than 95 % yield to the transoid 9. All new complexes 2-9 were characterized by NMR spectroscopy (1H, 11B NMR) and X-ray diffraction structural analyses are reported for complexes 2-5, 8, and 9.     

Discrete half-sandwich Ir, Rh-based organometallic molecular boxes: synthesis, characterization, and their properties

The treatment of binuclear complexes [Cp*(2)M(2)(μ-QA)Cl(2)] (M = Ir, 2a; M = Rh, 2b) (H(2)QA = 1,4-dihydroxyanthraquinone) with pyrazine or bifuncational pyridyl-based ligands (4,4'-dipyridine (bpy), E-1,2-bis(4-pyridyl)ethene (bpe), 2,5-bis(4-pyridyl)-1,3,4-oxadiazole (bpo), and 2,5-bis(4-pyridyl)-1,3,4-thiadiazol (bpt)) in the presence of AgOTf (OTf = CF(3)SO(3)) in CH(3)OH, gave the corresponding tetra-nuclear complexes, with a general formula of [Cp*(4)M(4)(μ-QA)(2)(μ-L)(2)](OTf)(4) (M = Ir, 3a-7a; M = Rh, 3b-7b), respectively. The molecular structure of [Cp*(4)Ir(4)(μ-QA)(2)(μ-pyrazine)(2)](OTf)(4) (3a) has been determined by single-crystal X-ray analysis, revealing that the metal centers were connected by pyrazine and bis-bidentate QA(2-) ligands to construct a rectangular cavity with the dimension of 7.30 × 8.41 × 6.92 ?. Complexes 3a and 3b were found to exhibit selective trapping of halocarbons properties.     

Synthesis, structure, and reactivity of rhodium and iridium complexes of the chelating bis-sulfoxide tBuSOC2H4SOtBu. Selective O-H activation of 2-hydroxy-isopropyl-pyridine

The chloro-bridged rhodium and iridium complexes [M2(BTSE)2Cl2] (M = Rh 1, Ir 2) bearing the chelating bis-sulfoxide tBuSOC2H4SOtBu (BTSE) were prepared by the reaction of [M2(COE)4Cl2] (M = Rh, Ir; COE = cyclooctene) with an excess of a racemic mixture of the ligand. The cationic compounds [M(BTSE)2][PF6] (M = Rh 3, Ir 4), bearing one S- and one O-bonded sulfoxide, were also obtained in good yields. The chloro-bridges in 2 can be cleaved with 2-methyl-6-pyridinemethanol and 2-aminomethyl pyridine, resulting in the iridium(I) complexes [Ir(BTSE)(Py)(Cl)] (Py = 2-methyl-6-pyridinemethanol 5, 2-aminomethyl-pyridine 6). In case of the bulky 2-hydroxy- isopropyl-pyridine, selective OH oxidative addition took place, forming the Ir(III)-hydride [Ir(BTSE)(2-isopropoxy-pyridine)(H)(Cl)] 7, with no competition from the six properly oriented C-H bonds. The cationic rhodium(I) and iridium(I) compounds [M(BTSE)(2-aminomethyl-pyridine)][X] (M = Rh 8, Ir 10), [Rh(BTSE)(2-hydroxy- isopropyl-pyridine)][X] 9(stabilized by intramolecular hydrogen bonding), [Ir(BTSE)(pyridine)2][PF6] 12, [Ir(BTSE)(alpha-picoline)2][PF6] 13, and [Rh(BTSE)(1,10-phenanthroline)][PF6] 14 were prepared either by chloride abstraction from the dimeric precursors or by replacement of the labile oxygen bonded sulfoxide in 3 or 4. Complex 14 exhibits a dimeric structure in the solid state by pi-pi stacking of the phenanthroline ligands.     

Dimethylsulfoxide as a ligand for RhI and IrI complexes--isolation, structure, and reactivity towards X-H bonds (X=H, OH, OCH3)

Novel neutral and cationic Rh(I) and Ir(I) complexes that contain only DMSO molecules as dative ligands with S-, O-, and bridging S,O-binding modes were isolated and characterized. The neutral derivatives [RhCl(DMSO)(3)] (1) and [IrCl(DMSO)(3)] (2) were synthesized from the dimeric precursors [M(2)Cl(2)(coe)(4)] (M=Rh, Ir; COE=cyclooctene). The dimeric Ir(I) compound [Ir(2)Cl(2)(DMSO)(4)] (3) was obtained from 2. The first example of a square-planar complex with a bidentate S,O-bridging DMSO ligand, [(coe)(DMSO)Rh(micro-Cl)(micro-DMSO)RhCl(DMSO)] (4), was obtained by treating [Rh(2)Cl(2)(coe)(4)] with three equivalents of DMSO. The mixed DMSO-olefin complex [IrCl(cod)(DMSO)] (5, COD=cyclooctadiene) was generated from [Ir(2)Cl(2)(cod)(2)]. Substitution reactions of these neutral systems afforded the complexes [RhCl(py)(DMSO)(2)] (6), [IrCl(py)(DMSO)(2)] (7), [IrCl(iPr(3)P)(DMSO)(2)] (8), [RhCl(dmbpy)(DMSO)] (9, dmbpy=4,4'-dimethyl-2,2'-bipyridine), and [IrCl(dmbpy)(DMSO)] (10). The cationic O-bound complex [Rh(cod)(DMSO)(2)]BF(4) (11) was synthesized from [Rh(cod)(2)]BF(4). Treatment of the cationic complexes [M(coe)(2)(O=CMe(2))(2)]PF(6) (M=Rh, Ir) with DMSO gave the mixed S- and O-bound DMSO complexes [M(DMSO)(2)(DMSO)(2)]PF(6) (Rh=12; Ir=in situ characterization). Substitution of the O-bound DMSO ligands with dmbpy or pyridine resulted in the isolation of [Rh(dmbpy)(DMSO)(2)]PF(6) (13) and [Ir(py)(2)(DMSO)(2)]PF(6) (14). Oxidative addition of hydrogen to [IrCl(DMSO)(3)] (2) gave the kinetic product fac-[Ir(H)(2)Cl(DMSO)(3)] (15) which was then easily converted to the more thermodynamically stable product mer-[Ir(H)(2)Cl(DMSO)(3)] (16). Oxidative addition of water to both neutral and cationic Ir(I) DMSO complexes gave the corresponding hydrido-hydroxo addition products syn-[(DMSO)(2)HIr(micro-OH)(2)(micro-Cl)IrH(DMSO)(2)][IrCl(2)(DMSO)(2)] (17) and anti-[(DMSO)(2)(DMSO)HIr(micro-OH)(2)IrH(DMSO)(2)(DMSO)][PF(6)](2) (18). The cationic [Ir(DMSO)(2)(DMSO)(2)]PF(6) complex (formed in situ from [Ir(coe)(2)(O=CMe(2))(2)]PF(6)) also reacts with methanol to give the hydrido-alkoxo complex syn-[(DMSO)(2)HIr(micro-OCH(3))(3)IrH(DMSO)(2)]PF(6) (19). Complexes 1, 2, 4, 5, 11, 12, 14, 17, 18, and 19 were characterized by crystallography.     

Protonation reactions of dinuclear pyrazolato iridium(I) complexes

The complex [[Ir(mu-Pz)(CNBu(t))(2)](2)] (1) undergoes double protonation reactions with HCl and with HO(2)CCF(3) to give the neutral dihydride complexes [[Ir(mu-Pz)(H)(X)(CNBu(t))(2)](2)] (X = Cl, eta(1)-O(2)CCF(3)), in which the hydride ligands were located trans to the X groups and in the boat of the complexes, both in the solid state and in solution. The complex [[Ir(mu-Pz)(H)(Cl)(CNBu(t))(2)](2)] evolves in solution to the cationic complex [[Ir(mu-Pz)(H)(CNBu(t))(2)](2)(mu-Cl)]Cl. Removal of the anionic chloride by reaction with methyltriflate allows the isolation of the triflate salt [[Ir(mu-Pz)(H)(CNBu(t))(2)](2)(mu-Cl)]OTf. This complex undergoes a metathesis reaction of hydride by chloride in CDCl(3) under exposure to the direct sunlight to give the complex [[Ir(mu-Pz)(Cl)(CNBu(t))(2)](2)(mu-Cl)]OTf. Protonation of both metal centers in [[Ir(mu-Pz)(CO)(2)](2)] with HCl occurs at low temperature, but eventually the mononuclear compound [IrCl(HPz)(CO)(2)] is isolated. The related complex [[Ir(mu-Pz)(CO)(P[OPh](3))](2)] reacts with HCl and with HO(2)CCF(3) to give the neutral Ir(III)/Ir(III) complexes [[Ir(mu-Pz)(H)(X)(CO)(P[OPh](3))](2)], respectively. Both reactions were found to take place stepwise, allowing the isolation of the intermediate monohydrides. They are of different natures, i.e., the metal-metal-bonded Ir(II)/Ir(II) compound [(P[OPh](3))(CO)(Cl)Ir(mu-Pz)(2)Ir(H)(CO)(P[OPh](3))] and the mixed-valence Ir(I)/Ir(III) complex [(P[OPh](3))(CO)Ir(mu-Pz)(2)Ir(H)(eta(1)-O(2)CCF(3))(CO)(P[OPh](3))].     

Group 9 Chalcogenometalates

The compounds [K(18-crown-6)](3)[Ir(Se(4))(3)] (1), [K(2.2.2-cryptand)](3)[Ir(Se(4))(3)].C(6)H(5)CH(3) (2), and [K(18-crown-6)(DMF)(2)][Ir(NCCH(3))(2)(Se(4))(2)] (3) (DMF = dimethylformamide) have been prepared from the reaction of [Ir(NCCH(3))(2)(COE)(2)][BF(4)] (COE = cyclooctene) with polyselenide anions in acetonitrile/DMF. Analogous reactions utilizing [Rh(NCCH(3))(2)(COE)(2)][BF(4)] as a Rh source produce homologues of the Ir complexes; these have been characterized by (77)Se NMR spectroscopy. [NH(4)](3)[Ir(S(6))(3)].H(2)O.0.5CH(3)CH(2)OH (4) has been synthesized from the reaction of IrCl(3).nH(2)O with aqueous (NH(4))(2)S(m)(). In the structure of [K(18-crown-6)](3)[Ir(Se(4))(3)] (1) the Ir(III) center is chelated by three Se(4)(2)(-) ligands to form a distorted octahedral anion. The structure contains a disordered racemate of the Deltalambdalambdalambda and Lambdadeltadeltadelta conformers. The K(+) cations are pulled out of the planes of the crowns and interact with Se atoms of the [Ir(Se(4))(3)](3)(-) anion. [K(2.2.2-cryptand)](3)[Ir(Se(4))(3)].C(6)H(5)CH(3) (2) possesses no short K.Se interactions; here the [Ir(Se(4))(3)](3)(-) anion crystallizes as the Deltalambdalambdadelta/Lambdadeltadeltalambda racemate. In the crystal structure of [K(18-crown-6)(DMF)(2)][Ir(NCCH(3))(2)(Se(4))(2)] (3), the K(+) cation is coordinated by an 18-crown-6 ligand and two DMF molecules and the anion comprises an octahedral Ir(III) center bound by two chelating Se(4)(2)(-) chains and two trans acetonitrile groups. The [Ir(Se(4))(3)](3)(-) and [Rh(Se(4))(3)](3)(-) anions undergo conformational transformations as a function of temperature, as observed by (77)Se NMR spectroscopy. The thermodynamics of these transformations are: [Ir(Se(4))(3)](3)(-), DeltaH = 2.5(5) kcal mol(-)(1), DeltaS = 11.5(2.2) eu; [Rh(Se(4))(3)](3)(-), DeltaH = 5.2(7) kcal mol(-)(1), DeltaS = 24.7(3.0) eu.