Subtle reactivity patterns of non-heteroatom-substituted manganese alkynyl carbene complexes in the presence of phosphorus probes

The non-heteroatom-substituted manganese alkynyl carbene complexes (eta5-MeC5H4)(CO)2Mn=C(R)C[triple bond]CR'(3; 3a: R = R'= Ph, 3b: R = Ph, R'= Tol, 3c: R = Tol, R'= Ph) have been synthesised in high yields upon treatment of the corresponding carbyne complexes [eta5-MeC5H4)(CO)2Mn[triple bond]CR][BPh4]([2][BPh4]) with the appropriate alkynyllithium reagents LiC[triple bond]CR' (R'= Ph, Tol). The use of tetraphenylborate as counter anion associated with the cationic carbyne complexes has been decisive. The X-ray structures of (eta5-MeC5H4)(CO)2Mn=C(Tol)C[triple bond]CPh (3c), and its precursor [(eta5-MeC5H4)(CO)2Mn=CTol][BPh4]([2b](BPh4]) are reported. The reactivity of complexes toward phosphines has been investigated. In the presence of PPh3, complexes act as a Michael acceptor to afford the zwitterionic sigma-allenylphosphonium complexes (eta5-MeC5H4)(CO)2MnC(R)=C=C(PPh3)R' (5) resulting from nucleophilic attack by the phosphine on the remote alkynyl carbon atom. Complexes 5 exhibit a dynamic process in solution, which has been rationalized in terms of a fast [NMR time-scale] rotation of the allene substituents around the allene axis; metrical features within the X-ray structure of (eta5-MeC5H4)(CO)2MnC(Ph)=C=C(PPh3)Tol (5b) support the proposal. In the presence of PMe3, complexes undergo a nucleophilic attack on the carbene carbon atom to give zwitterionic sigma-propargylphosphonium complexes (eta5-MeC5H4)(CO)2MnC(R)(PMe3)C[triple bond]CR' (6). Complexes 6 readily isomerise in solution to give the sigma-allenylphosphonium complexes (eta5-MeC5H4)(CO)2MnC(R')=C=C(PMe3)R (7) through a 1,3 shift of the [(eta5-MeC5H4)(CO)2Mn] fragment. The nucleophilic attack of PPh2Me on 3 is not selective and leads to a mixture of the sigma-propargylphosphonium complexes (eta5-MeC5H4)(CO)2MnC(R)(PPh(2)Me)C[triple bond]CR' (9) and the sigma-allenylphosphonium complexes (eta5-MeC5H4)(CO)2MnC(R)=C=C(PPh(2)Me)R' (10). Like complexes 6, complexes 9 readily isomerize to give the sigma-allenylphosphonium complexes (eta5-MeC5H4)(CO)2MnC(R')=C=C(PPh2Me)R'). Upon gentle heating, complexes 7, and mixtures of 10 and 10' cyclise to give the sigma-dihydrophospholium complexes (eta5-MeC5H4)(CO)2MnC=C(R')PMe2CH2CH(R)(8), and mixtures of complexes (eta5-MeC5H4)(CO)2MnC=C(Ph)PPh2CH2CH(Tol)(11) and (eta5-MeC5H4)(CO)2MnC=C(Tol)PMe2CH2CH(Ph)(11'), respectively. The reactions of complexes 3 with secondary phosphines HPR(1)(2)(R1= Ph, Cy) give a mixture of the eta2-allene complexes (eta5-MeC5H4)(CO)2Mn[eta2-{R(1)(2)PC(R)=C=C(R')H}](12), and the regioisomeric eta4-vinylketene complexes [eta5-MeC5H4)(CO)Mn[eta4-{R(1)(2)PC(R)=CHC(R')=C=O}](13) and (eta5-MeC5H4)(CO)Mn[eta4-{R(1)(2)PC(R')=CHC(R)=C=O}](13'). The solid-state structure of (eta5-MeC5H4)(CO)2Mn[eta2-{Ph2PC(Ph)=C=C(Tol)H}](12b) and (eta5-MeC5H4)(CO)Mn[eta4-{Cy2PC(Ph)=CHC(Ph)=C=O}](13d) are reported. Finally, a mechanism that may account for the formation of the species 12, 13, and 13' is proposed.     

The first acetimine gold(I) and gold(III) complexes and the first acetonine complexes

Ketimino(phosphino)gold(I) complexes of the type [Au[NR=C(Me)R']L]X (X = ClO4, R = H, L = PPh3, R'=Me (la), Et (2a); L=PAr3 (Ar=C6H4OMe-4), R'=Me (1b), Et (2b); L=PPh3, R=R'=Me (3); X= CF3SO3 (OTf), L=PPh3, R=R'=Me (3'); R=Ar, R'=Me (4)) have been prepared from [Au(acac)L] (acac = acetyl acetonate) and ammonium salts [RNH3]X dissolved in the appropriate ketone MeC(O)R'. Complexes [Au(NH=CMe2)2]X (X = C1O4 (6), OTf (6')) were obtained from solutions of [Au(NH3)2]X in acetone. The reaction of 6 with PPN[AuCl2] or with PhICl2 gave [AuCl(NH=CMe2)] (7) or [AuCI2(NH=CMe2)2]ClO4 (8), respectively. Complex 7 was oxidized with PhICl2 to give [AuCl3(NH=CMe2)] (9). The reaction of [AuCl(tht)] (tht = tetrahydrothiophene), NaClO4, and ammonia in acetone gave [Au(acetonine)2]ClO4 (10) (acetonine = 2,2,4,4,6-pentamethyl-2,3,4,5-tetrahydropyrimidine) which reacted with PPh3 or with PPN[AuCl2] to give [Au(PPh3)(acetonine)]ClO4 (11) or [AuCl(acetonine)] (12), respectively. Complex 11 reacts with [Au(PPh3)(Me2CO)]ClO4 to give [(AuPPh3)2(mu-acetonine)](ClO4)2 (13). The reaction of AgClO4 with acetonine gave [Ag(acetonine)(OClO3)] (14). The crystal structures of [Au(NH2Ar)(PPh3)]OTf (5), 6' and 10 have been determined.     

Synthesis, structure, and reactivity of ruthenium carboxylato and 2-oxocarboxylato complexes bearing the bis(3,5-dimethylpyrazol-1-yl)acetato ligand

A series of ruthenium(II) acetonitrile, pyridine (py), carbonyl, SO2, and nitrosyl complexes [Ru(bdmpza)(O2CR)(L)(PPh3)] (L = NCMe, py, CO, SO2) and [Ru(bdmpza)(O2CR)(L)(PPh3)]BF4 (L = NO) containing the bis(3,5-dimethylpyrazol-1-yl)acetato (bdmpza) ligand, a N,N,O heteroscorpionate ligand, have been prepared. Starting from ruthenium chlorido, carboxylato, or 2-oxocarboxylato complexes, a variety of acetonitrile complexes [Ru(bdmpza)Cl(NCMe)(PPh3)] (4) and [Ru(bdmpza)(O2CR)(NCMe)(PPh3)] (R = Me (5a), R = Ph (5b)), as well as the pyridine complexes [Ru(bdmpza)Cl(PPh3)(py)] (6) and [Ru(bdmpza)(O2CR)(PPh3)(py)] (R = Me (7a), R = Ph (7b), R = (CO)Me (8a), R = (CO)Et (8b), R = (CO)Ph) (8c)), have been synthesized. Treatment of various carboxylato complexes [Ru(bdmpza)(O2CR)(PPh3)2] (R = Me (2a), Ph (2b)) with CO afforded carbonyl complexes [Ru(bdmpza)(O2CR)(CO)(PPh3)] (9a, 9b). In the same way, the corresponding sulfur dioxide complexes [Ru(bdmpza)(O2CMe)(PPh3)(SO2)] (10a) and [Ru(bdmpza)(O2CPh)(PPh3)(SO2)] (10b) were formed in a reaction of the carboxylato complexes with gaseous SO2. None of the 2-oxocarboxylato complexes [Ru(bdmpza)(O2C(CO)R)(PPh3)2] (R = Me (3a), Et (3b), Ph (3c)) showed any reactivity toward CO or SO2, whereas the nitrosyl complex cations [Ru(bdmpza)(O2CMe)(NO)(PPh3)](+) (11) and [Ru(bdmpza)(O2C(CO)Ph)(NO)(PPh3)](+) (12) were formed in a reaction of the acetato 2a or the benzoylformato complex 3c with an excess of nitric oxide. Similar cationic carboxylato nitrosyl complexes [Ru(bdmpza)(O2CR)(NO)(PPh3)]BF4 (R = Me (13a), R = Ph (13b)) and 2-oxocarboxylato nitrosyl complexes [Ru(bdmpza)(O2C(CO)R)(NO)(PPh3)]BF4 (R = Me (14a), R = Et (14b), R = Ph (14c)) are also accessible via a reaction with NO[BF4]. X-ray crystal structures of the chlorido acetonitrile complex [Ru(bdmpza)Cl(NCMe)(PPh3)] (4), the pyridine complexes [Ru(bdmpza)(O2CMe)(PPh3)(py)] (7a) and [Ru(bdmpza)(O2CC(O)Et)(PPh3)(py)] (8b), the carbonyl complex [Ru(bdmpza)(O2CPh)(CO)(PPh3)] (9b), the sulfur dioxide complex [Ru(bdmpza)(O2CPh)(PPh3)(SO2)] (10b), as well as the nitrosyl complex [Ru(bdmpza)(O2C(CO)Me)(NO)(PPh3)]BF4 (14a), are reported. The molecular structure of the sulfur dioxide complex [Ru(bdmpza)(O2CPh)(PPh3)(SO2)] (10b) revealed a rather unusual intramolecular SO2-O2CPh Lewis acid-base adduct.     

Amidoximes provide facile platinum(II)-mediated oxime-nitrile coupling

The nucleophilic addition of amidoximes R'C(NH(2))═NOH [R' = Me (2.Me), Ph (2.Ph)] to coordinated nitriles in the platinum(II) complexes trans-[PtCl(2)(RCN)(2)] [R = Et (1t.Et), Ph (1t.Ph), NMe(2) (1t.NMe(2))] and cis-[PtCl(2)(RCN)(2)] [R = Et (1c.Et), Ph (1c.Ph), NMe(2) (1c.NMe(2))] proceeds in a 1:1 molar ratio and leads to the monoaddition products trans-[PtCl(RCN){HN═C(R)ONC(R')NH(2)}]Cl [R = NMe(2); R' = Me ([3a]Cl), Ph ([3b]Cl)], cis-[PtCl(2){HN═C(R)ONC(R')NH(2)}] [R = NMe(2); R' = Me (4a), Ph (4b)], and trans/cis-[PtCl(2)(RCN){HN═C(R)ONC(R')NH(2)}] [R = Et; R' = Me (5a, 6a), Ph (5b, 6b); R = Ph; R' = Me (5c, 6c), Ph (5d, 6d), correspondingly]. If the nucleophilic addition proceeds in a 2:1 molar ratio, the reaction gives the bisaddition species trans/cis-[Pt{HN═C(R)ONC(R')NH(2)}(2)]Cl(2) [R = NMe(2); R' = Me ([7a]Cl(2), [8a]Cl(2)), Ph ([7b]Cl(2), [8b]Cl(2))] and trans/cis-[PtCl(2){HN═C(R)ONC(R')NH(2)}(2)] [R = Et; R' = Me (10a), Ph (9b, 10b); R = Ph; R' = Me (9c, 10c), Ph (9d, 10d), respectively]. The reaction of 1 equiv of the corresponding amidoxime and each of [3a]Cl, [3b]Cl, 5b-5d, and 6a-6d leads to [7a]Cl(2), [7b]Cl(2), 9b-9d, and 10a-10d. Open-chain bisaddition species 9b-9d and 10a-10d were transformed to corresponding chelated bisaddition complexes [7d](2+)-[7f](2+) and [8c](2+)-[8f](2+) by the addition of 2 equiv AgNO(3). All of the complexes synthesized bear nitrogen-bound O-iminoacylated amidoxime groups. The obtained complexes were characterized by elemental analyses, high-resolution ESI-MS, IR, and (1)H NMR techniques, while 4a, 4b, 5b, 6d, [7b](Cl)(2), [7d](SO(3)CF(3))(2), [8b](Cl)(2), [8f](NO(3))(2), 9b, and 10b were also characterized by single-crystal X-ray diffraction.     

The synthesis, characterisation and reactivity of 2-phosphanylethylcyclopentadienyl complexes of cobalt, rhodium and iridium

2-Phosphanylethylcyclopentadienyl lithium compounds, Li[C(5)R'(4)(CH(2))(2)PR(2)] (R = Et, R' = H or Me, R = Ph, R' = Me), have been prepared from the reaction of spirohydrocarbons C(5)R'(4)(C(2)H(4)) with LiPR(2). C(5)Et(4)HSiMe(2)CH(2)PMe(2), was prepared from reaction of Li[C(5)Et(4)] with Me(2)SiCl(2) followed by Me(2)PCH(2)Li. The lithium salts were reacted with [RhCl(CO)(2)](2), [IrCl(CO)(3)] or [Co(2)(CO)(8)] to give [M(C(5)R'(4)(CH(2))(2)PR(2))(CO)] (M = Rh, R = Et, R' = H or Me, R = Ph, R' = Me; M = Ir or Co, R = Et, R' = Me), which have been fully characterised, in many cases crystallographically as monomers with coordination of the phosphorus atom and the cyclopentadienyl ring. The values of nu(CO) for these complexes are usually lower than those for the analogous complexes without the bridge between the cyclopentadienyl ring and the phosphine, the exception being [Rh(Cp'(CH(2))(2)PEt(2))(CO)] (Cp' = C(5)Me(4)), the most electron rich of the complexes. [Rh(C(5)Et(4)SiMe(2)CH(2)PMe(2))(CO)] may be a dimer. [Co(2)(CO)(8)] reacts with C(5)H(5)(CH(2))(2)PEt(2) or C(5)Et(4)HSiMe(2)CH(2)PMe(2) (L) to give binuclear complexes of the form [Co(2)(CO)(6)L(2)] with almost linear PCoCoP skeletons. [Rh(Cp'(CH(2))(2)PEt(2))(CO)] and [Rh(Cp'(CH(2))(2)PPh(2))(CO)] are active for methanol carbonylation at 150 degrees C and 27 bar CO, with the rate using [Rh(Cp'(CH(2))(2)PPh(2))(CO)] (0.81 mol dm(-3) h(-1)) being higher than that for [RhI(2)(CO)(2)](-) (0.64 mol dm(-3) h(-1)). The most electron rich complex, [Rh(Cp'(CH(2))(2)PEt(2))(CO)] (0.38 mol dm(-3) h(-1)) gave a comparable rate to [Cp*Rh(PEt(3))(CO)] (0.30 mol dm(-3) h(-1)), which was unstable towards oxidation of the phosphine. [Rh(Cp'(CH(2))(2)PEt(2))I(2)], which is inactive for methanol carbonylation, was isolated after the methanol carbonylation reaction using [Rh(Cp'(CH(2))(2)PEt(2))(CO)]. Neither of [M(Cp'(CH(2))(2)PEt(2))(CO)] (M = Co or Ir) was active for methanol carbonylation under these conditions, nor under many other conditions investigated, except that [Ir(Cp'(CH(2))(2)PEt(2))(CO)] showed some activity at higher temperature (190 degrees C), probably as a result of degradation to [IrI(2)(CO)(2)](-). [M(Cp'(CH(2))(2)PEt(2))(CO)] react with MeI to give [M(Cp'(CH(2))(2)PEt(2))(C(O)Me)I] (M = Co or Rh) or [Ir(Cp'(CH(2))(2)PEt(2))Me(CO)]I. The rates of oxidative addition of MeI to [Rh(C(5)H(4)(CH(2))(2)PEt(2))(CO)] and [Rh(Cp'(CH(2))(2)PPh(2))(CO)] are 62 and 1770 times faster than to [Cp*Rh(CO)(2)]. Methyl migration is slower, however. High pressure NMR studies show that [Co(Cp'(CH(2))(2)PEt(2))(CO)] and [Cp*Rh(PEt(3))(CO)] are unstable towards phosphine oxidation and/or quaternisation under methanol carbonylation conditions, but that [Rh(Cp'(CH(2))(2)PEt(2))(CO)] does not exhibit phosphine degradation, eventually producing inactive [Rh(Cp'(CH(2))(2)PEt(2))I(2)] at least under conditions of poor gas mixing. The observation of [Rh(Cp'(CH(2))(2)PEt(2))(C(O)Me)I] under methanol carbonylation conditions suggests that the rhodium centre has become so electron rich that reductive elimination of ethanoyl iodide has become rate determining for methanol carbonylation. In addition to the high electron density at rhodium.     

P-C versus C-H bond cleavage in coordinated bis(dimethylphosphino)methane: controlled access to either phosphinite or functionalized diphosphine complexes

Treatment of fac-[Mn(CNPh)(CO)3(dmpm)]ClO4 (1) with KOH affords neutral phosphinite complex fac-[Mn(PMe2O)(CNPh)(CO)3(PMe3)] (2) as a result of P-C bond cleavage on the dmpm ligand, whereas when carrying out the reaction in the presence of iodine the diphosphinoketenimine derivative fac-[MnI(CO)3[(PMe2)2C=C=NPh]] (4) is obtained after deprotonation and further functionalization of the central carbon atom of the diphosphine.     

High structural control in metal-mediated synthesis of new functionalized diphosphines using diphosphinoketenimines as precursors

The diphosphinoketenimine ligand in the neutral complexes fac-[MnI(CO)(3){(PPh(2))(2)C=C=NR}] (1 a: R = Ph; 1 b: R = p-tolyl) undergoes nucleophilic attack by MeLi and nBuMgCl yielding, after hydrolysis, the diphosphinoenamine-containing complexes fac-[MnI(CO)(3){(PPh(2))(2)C=C(R')NHR}] (3 a,b: R' = Me; 4 a,b: R' = nBu). Complex 1 a reacts under the same conditions with H(2)C=C=CHMgBr to afford fac-[MnI(CO)(3){(PPh(2))(2)C=C(CH(2)CC[triple chemical bond]CH)NHR}] (5 a), which contains a terminal alkyne group on the alpha-carbon atom of the diphosphinoenamine ligand. The cationic complexes fac-[Mn(CO)(4){(PPh(2))(2)C=C=NR}](+) (6) react with H(2)C=C=CHMgBr to afford diphosphinomethanide derivatives bearing three different types of functional groups, depending upon the substituent on the nitrogen atom of the ketenimine: cumulene in fac-[Mn(CO)(4){(PPh(2))(2)C--C(CH=C=CH(2))=N-xylyl}] (7 d), internal alkyne in fac-[Mn(CO)(4){(PPh(2))(2)C--C(C[triple chemical bond]CCH(3))=NtBu}] (8), and quinoline in 9 (R = Ph), whose formation implies an unusual cyclization process. Protonation of 7 d, 8, and 9 with HBF(4) occurs at the nitrogen atom to give the cationic derivatives 10 d, 11, and 12, respectively, which contain the corresponding functionalized diphosphine ligands. Irradiation of 3 a,b and 4 a,b with Vis/UV light makes it possible to isolate the free ligands (PPh(2))(2)C=C(R')NHR (13 a,b and 14 a,b), completing the metal-assisted synthesis of these novel functionalized diphosphines. Irradiation of 12 with Vis/UV light generates free phosphinoquinoline ligand 15, which readily affords a complex 16 containing 15 as a P,N-chelating ligand when treated with [PdCl(2)(NCMe)(2)], thus demonstrating its coordination capability.     

Mixed dinitrogen-organocyanamide complexes of molybdenum(0) and their protic conversion into hydrazide and amidoazavinylidene derivatives

Organocyanamides, Ntbd1;CNR(2) (R = Me or Et), react with trans-[Mo(N(2))(2)(dppe)(2)] (1, dppe = Ph(2)PCH(2)CH(2)PPh(2)), in THF, to give the first mixed molybdenum dinitrogen-cyanamide complexes trans-[Mo(N(2))(NCNR(2))(dppe)(2)] (R = Me 2a or Et 2b) which are selectively protonated at N(2) by HBF(4) to yield the hydrazide(2-) complexes trans-[Mo(NNH(2))(NCNR(2))(dppe)(2)][BF(4)](2) (R = Me, 3a, or Et, 3b). On treatment with Ag[BF(4)], oxidation and metal fluorination occur, and the ligating cyanamide undergoes an unprecedented beta-protonation at the unsaturated C atom to form trans-[MoF(NCHNR(2))(dppe)(2)][BF(4)](2) (R = Me, 4a, or Et, 4b) compounds which present the novel amidoazavinylidene (or amidomethyleneamide) ligands. Complexes 4 are also formed from the corresponding compounds 3, with liberation of ammonia and hydrazine. The crystal structure of 2b was determined by single-crystal X-ray diffraction analysis which indicates that the N atom of the amide group has a trigonal planar geometry.     

Lithium aluminates on a molecular titanium oxide

Lithium aluminates Li[Al(O-2,6-Me(2)C(6)H(3))R'(3)] (R' = Et, Ph) react with the μ(3)-alkylidyne oxoderivative ligands [{Ti(η(5)-C(5)Me(5))(μ-O)}(3)(μ(3)-CR)] [R = H (1), Me (2)] to afford the aluminum-lithium-titanium cubane complexes [{R'(3)Al(μ-O-2,6-Me(2)C(6)H(3))Li}(μ(3)-O)(3){Ti(η(5)-C(5)Me(5))}(3)(μ(3)-CR)] [R = H, R' = Et (5), Ph (7); R = Me, R' = Et (6), Ph (8)]. Complex 7 evolves with the formation of a lithium dicubane species and a Li{Al(μ-O-2,6-Me(2)C(6)H(3))Ph(3)}(2)] unit.     

Synthesis and reactivity of Ir(I) and Ir(III) complexes with MeNH2, Me2C=NR (R = H, Me), C,N-C6H4{C(Me)=N(Me)}-2, and N,N'-RN=C(Me)CH2C(Me2)NHR (R = H, Me) ligands

Complexes [Ir(Cp*)Cl(n)(NH2Me)(3-n)]X(m) (n = 2, m = 0 (1), n = 1, m = 1, X = Cl (2a), n = 0, m = 2, X = OTf (3)) are obtained by reacting [Ir(Cp*)Cl(mu-Cl)]2 with MeNH2 (1:2 or 1:8) or with [Ag(NH2Me)2]OTf (1:4), respectively. Complex 2b (n = 1, m = 1, X = ClO 4) is obtained from 2a and NaClO4 x H2O. The reaction of 3 with MeC(O)Ph at 80 degrees C gives [Ir(Cp*){C,N-C6H4{C(Me)=N(Me)}-2}(NH2Me)]OTf (4), which in turn reacts with RNC to give [Ir(Cp*){C,N-C6H4{C(Me)=N(Me)}-2}(CNR)]OTf (R = (t)Bu (5), Xy (6)). [Ir(mu-Cl)(COD)]2 reacts with [Ag{N(R)=CMe2}2]X (1:2) to give [Ir{N(R)=CMe2}2(COD)]X (R = H, X = ClO4 (7); R = Me, X = OTf (8)). Complexes [Ir(CO)2(NH=CMe2)2]ClO4 (9) and [IrCl{N(R)=CMe2}(COD)] (R = H (10), Me (11)) are obtained from the appropriate [Ir{N(R)=CMe2}2(COD)]X and CO or Me4NCl, respectively. [Ir(Cp*)Cl(mu-Cl)]2 reacts with [Au(NH=CMe2)(PPh3)]ClO4 (1:2) to give [Ir(Cp*)(mu-Cl)(NH=CMe2)]2(ClO4)2 (12) which in turn reacts with PPh 3 or Me4NCl (1:2) to give [Ir(Cp*)Cl(NH=CMe2)(PPh3)]ClO4 (13) or [Ir(Cp*)Cl2(NH=CMe2)] (14), respectively. Complex 14 hydrolyzes in a CH2Cl2/Et2O solution to give [Ir(Cp*)Cl2(NH3)] (15). The reaction of [Ir(Cp*)Cl(mu-Cl)]2 with [Ag(NH=CMe2)2]ClO4 (1:4) gives [Ir(Cp*)(NH=CMe2)3](ClO4)2 (16a), which reacts with PPNCl (PPN = Ph3=P=N=PPh3) under different reaction conditions to give [Ir(Cp*)(NH=CMe2)3]XY (X = Cl, Y = ClO4 (16b); X = Y = Cl (16c)). Equimolar amounts of 14 and 16a react to give [Ir(Cp*)Cl(NH=CMe2)2]ClO4 (17), which in turn reacts with PPNCl to give [Ir(Cp*)Cl(H-imam)]Cl (R-imam = N,N'-N(R)=C(Me)CH2C(Me)2NHR (18a)]. Complexes [Ir(Cp*)Cl(R-imam)]ClO4 (R = H (18b), Me (19)) are obtained from 18a and AgClO4 or by refluxing 2b in acetone for 7 h, respectively. They react with AgClO4 and the appropriate neutral ligand or with [Ag(NH=CMe2)2]ClO4 to give [Ir(Cp*)(R-imam)L](ClO4)2 (R = H, L = (t)BuNC (20), XyNC (21); R = Me, L = MeCN (22)) or [Ir(Cp*)(H-imam)(NH=CMe2)](ClO4)2 (23a), respectively. The later reacts with PPNCl to give [Ir(Cp*)(H-imam)(NH=CMe2)]Cl(ClO4) (23b). The reaction of 22 with XyNC gives [Ir(Cp*)(Me-imam)(CNXy)](ClO4)2 (24). The structures of complexes 15, 16c and 18b have been solved by X-ray diffraction methods.     

M-P versus M=M bonds as protonation sites in the organophosphide-bridged complexes [M2Cp2(mu-PR2)(mu-PR'2)(CO)2], (M = Mo, W; R, R' = Ph, Et, Cy)

The unsaturated complexes [W2Cp2(mu-PR2)(mu-PR'2)(CO)2] (Cp = eta5-C5H5; R = R' = Ph, Et; R = Et, R' = Ph) react with HBF4.OEt2 at 243 K in dichloromethane solution to give the corresponding complexes [W2Cp2(H)(mu-PR2)(mu-PR'2)(CO)2]BF4, which contain a terminal hydride ligand. The latter rearrange at room temperature to give [W2Cp2(mu-H)(mu-PR2)(mu-PR'2)(CO)2]BF4, which display a bridging hydride and carbonyl ligands arranged parallel to each other (W-W = 2.7589(8) A when R = R' = Ph). This explains why the removal of a proton from the latter gives first the unstable isomer cis-[W2Cp2(mu-PPh2)2(CO)2]. The molybdenum complex [Mo2Cp2(mu-PPh2)2(CO)2] behaves similarly, and thus the thermally unstable new complexes [Mo2Cp2(H)(mu-PPh2)2(CO)2]BF4 and cis-[Mo2Cp2(mu-PPh2)2(CO)2] could be characterized. In contrast, related dimolybdenum complexes having electron-rich phosphide ligands behave differently. Thus, the complexes [Mo2Cp2(mu-PR2)2(CO)2] (R = Cy, Et) react with HBF4.OEt2 to give first the agostic type phosphine-bridged complexes [Mo2Cp2(mu-PR2)(mu-kappa2-HPR2)(CO)2]BF4 (Mo-Mo = 2.748(4) A for R = Cy). These complexes experience intramolecular exchange of the agostic H atom between the two inequivalent P positions and at room-temperature reach a proton-catalyzed equilibrium with their hydride-bridged tautomers [ratio agostic/hydride = 10 (R = Cy), 30 (R = Et)]. The mixed-phosphide complex [Mo2Cp2(mu-PCy2)(mu-PPh2)(CO)2] behaves similarly, except that protonation now occurs specifically at the dicyclohexylphosphide ligand [ratio agostic/hydride = 0.5]. The reaction of the agostic complex [Mo2Cp2(mu-PCy2)(mu-kappa2-HPCy2)(CO)2]BF4 with CN(t)Bu gave mono- or disubstituted hydride derivatives [Mo2Cp2(mu-H)(mu-PCy2)2(CO)2-x(CNtBu)x]BF4 (Mo-Mo = 2.7901(7) A for x = 1). The photochemical removal of a CO ligand from the agostic complex also gives a hydride derivative, the triply bonded complex [Mo2Cp2(H)(mu-PCy2)2(CO)]BF4 (Mo-Mo = 2.537(2) A). Protonation of [Mo2Cp2(mu-PCy2)2(mu-CO)] gives the hydroxycarbyne derivative [Mo2Cp2(mu-COH)(mu-PCy2)2]BF4, which does not transform into its hydride isomer.     

Direct addition of alcohols to organonitriles activated by ligation to a platinum(IV) center

Treatment of trans-[PtCl(4)(RCN)(2)] (R = Me, Et) with R'OH (R' = Me, Et, n-Pr, i-Pr, n-Bu) at 45 degrees C in all cases allowed the isolation of the trans-[PtCl(4)[(E)-NH=C(R)OR'](2)] imino ester complexes, while the reaction between cis-[PtCl(4)(RCN)(2)] and the least sterically hindered alcohols (methanol and ethanol) results in the formation of cis-[PtCl(4)[(E)-NH=C(R)OR'](2)] (R/R' = Me/Me) or trans-[PtCl(4)[(E)-NH=C(Et)OR'](2)] (R' = Me, Et), the latter being formed via thermal isomerization (ROH, reflux, 3 h) of the initially formed corresponding cis isomers. The reaction between alcohols R'OH and cis-[PtCl(4)(RCN)(2)] (R = Me, R' = Et, n-Pr, i-Pr, n-Bu; R = Et; R' = n-Pr, i-Pr, n-Bu), exhibiting greater R/R' steric congestion, allowed the isolation of cis-[PtCl(4)[(E)-NH=C(R)OR'][(Z)-NH=C(R)OR']] as the major products. The alcoholysis reactions of poorly soluble [PtCl(4)(RCN)(2)] (R = CH(2)Ph, Ph) performed under heterogeneous conditions, directly in the appropriate alcohol and for a prolonged time and, for R = Ph, with heating led to trans-[PtCl(4)[(E)-NH=C(R)OR'](2)] (R = CH(2)Ph, R' = Me, Et, n-Pr, i-Pr; R = Ph, R' = Me) isolated in moderate yields. In all of the cases, in contrast to platinum(II) systems, addition of R'OH to the organonitrile platinum(IV) complexes occurs under mild conditions and does not require a base as a catalyst. The formed isomerically pure (imino ester)Pt(IV) complexes can be reduced selectively, by Ph(3)P=CHCO(2)Me, to the corresponding isomers of (imino ester)Pt(II) species, exhibiting antitumor activity, without change in configuration of the imino ester ligands. Furthemore, the imino esters NH=C(R)OR' can be liberated from both platinum(IV) and platinum(II) complexes [PtCl(n)[H=C(R)OR'](2)] (n = 2, 4) by reaction with 1,2-bis(diphenylphosphino)ethane and pyridine, respectively. All of the prepared compounds were characterized by elemental analyses (C, H, N), FAB mass spectrometry, IR, and (1)H, (13)C[(1)H], and (195)Pt (metal complexes) NMR spectroscopies; the E and Z configurations of the imino ester ligands in solution were determined by observation of the nuclear Overhauser effect. X-ray structure determinations were performed for trans-[PtCl(4)[(E)-NH=C(Me)OEt](2)] (2), trans-[PtCl(4)[(E)-NH=C(Et)OEt](2)] (10), trans-[PtCl(4)[(E)-NH=C(Et)OPr-i](2)] (11), trans-[PtCl(4)[(E)-NH=C(Et)OPr-n](2)] (12), and cis-[PtCl(4)[(E)-NH=C(Et)OMe](2)] (14). Ab initio calculations have shown that the EE isomers are the most stable ones for both platinum(II) and platinum(IV) complexes, whereas the most stable configurations for the ZZ isomers are less stable than the respective EZ isomers, indicating an increase of the stability on moving from the ZZ to the EE configurations which is more pronounced for the Pt(IV) complexes than for the Pt(II) species.     

Hydride transfer reactivity of tetrakis(trimethylphosphine)(hydrido)(nitrosyl)molybdenum(0)

The tetrakis(trimethylphosphine) molybdenum nitrosyl hydrido complex trans-Mo(PMe(3))(4)(H)(NO) (2) and the related deuteride complex trans-Mo(PMe(3))(4)(D)(NO) (2a) were prepared from trans-Mo(PMe(3))(4)(Cl)(NO) (1). From (2)H T(1 min) measurements and solid-state (2)H NMR the bond ionicities of 2a could be determined and were found to be 80.0% and 75.3%, respectively, indicating a very polar Mo--D bond. The enhanced hydridicity of 2 is reflected in its very high propensity to undergo hydride transfer reactions. 2 was thus reacted with acetone, acetophenone, and benzophenone to afford the corresponding alkoxide complexes trans-Mo(NO)(PMe(3))(4)(OCHR'R') (R' = R' = Me (3); R' = Me, R' = Ph (4); R' = R' = Ph (5)). The reaction of 2 with CO(2) led to the formation of the formato-O-complex Mo(NO)(OCHO)(PMe(3))(4) (6). The reaction of with HOSO(2)CF(3) produced the anion coordinated complex Mo(NO)(PMe(3))(4)(OSO(2)CF(3)) (7), and the reaction with [H(Et(2)O)(2)][BAr(F)(4)] with an excess of PMe(3) produced the pentakis(trimethylphosphine) coordinated compound [Mo(NO)(PMe(3))(5)][BAr(F)(4)] (8). Imine insertions into the Mo-H bond of 2 were also accomplished. PhCH[double bond, length as m-dash]NPh (N-benzylideneaniline) and C(10)H(7)CH=NPh (N-1-naphthylideneaniline) afforded the amido compounds Mo(NO)(PMe(3))(4)[NR'(CH(2)R')] (R' = R' = Ph (9), R' = Ph, R' = naphthyl (11)). 9 could not be obtained in pure form, however, its structure was assigned by spectroscopic means. At room temperature 11 reacted further to lose one PMe(3) forming 12 (Mo(NO)PMe(3))(3)[N(Ph)CH(2)C(10)H(6))]) with agostic stabilization. In a subsequent step oxidative addition of the agostic naphthyl C-H bond to the molybdenum centre occurred. Then hydrogen migration took place giving the chelate amine complex Mo(NO)(PMe(3))(3)[NH(Ph)(CH(2)C(10)H(6))] (15). The insertion reaction of 2 with C(10)H(7)N=CHPh led to formation of the agostic compound Mo(NO)(PMe(3))(3)[N(CH(2)Ph)(C(10)H(7))] (10). Based on the knowledge of facile formation of agostic compounds the catalytic hydrogenation of C(10)H(7)N=CHPh and PhN=CHC(10)H(7) with 2 (5 mol%) was tested. The best conversion rates were obtained in the presence of an excess of PMe(3), which were 18.4% and 100% for C(10)H(7)N=CHPh and PhN=CHC(10)H(7), respectively.     

Cationic Rh complexes with novel spiro tetraarylpentaborate anions prepared from arylboronic acids and aryloxorhodium complexes

Ar-B(OH)2 (1a: Ar = C6H4OMe-4, 1b: Ar = C6H3Me2-2,6) react immediately with Rh(OC6H4Me-4)(PMe3)3 (2) in 5 : 1 molar ratio at room temperature to generate [Rh(PMe3)4]+[B5O6Ar4]- (3a: Ar = C6H4OMe-4, 3b: Ar = C6H3Me2-2,6). p-Cresol (92%/Rh), anisole (80%/Rh) and H2O (364%/Rh) are formed from 1a and 2. The reaction of 1a with 2 for 24 h produces [Rh(PMe3)4]+[B5O6(OH)4]- (4) as a yellow solid. This is attributed to hydrolytic dearylation of once formed 3a because the direct reaction of 3a with excess H2O forms 4. An equimolar reaction of 2 with phenylboroxine (PhBO)3 causes transfer of the 4-methylphenoxo ligand from rhodium to boron to produce [Rh(PMe3)4]+[B3O3Ph3(OC6H4Me-4)]- (5). Arylboronic acids 1a and 1b react with Rh(OC6H4Me-4)(PR3)3 (6: R = Et, 8: R = Ph) and with Rh(OC6H4Me-4)(cod)(PR3) (11: R = iPr, 12: R = Ph) to form [Rh(PR3)4]+[B5O6Ar4]- (7a: R = Et, Ar = C6H4OMe-4, 7b: R = Et, Ar = C6H3Me2-2,6, 9a: R = Ph, Ar = C6H3Me2-2,6) and [Rh(cod)(PR3)(L)]+[B5O6Ar4]- (13b: R = iPr, L = acetone, Ar = C6H3Me2-2,6, 14a: R = Ph, L = PPh3, Ar = C6H4OMe-4, 14b: R = Ph, L = PPh3, Ar = C6H3Me2-2,6), respectively. Hydrolysis of 14a yields [Rh(cod)(PPh3)2]+[B5O6(OH)4]- (15) quantitatively.     

Reactions of phosphine oxides with bromophosphoranimines; synthesis and unusual rearrangements of O-donor stabilized phosphoranimine cations

Reaction of phosphine oxides R(3)P═O [R = Me (1a), Et (1c), (i)Pr (1d) and Ph (1e)], with the bromophosphoranimines BrPR'R'P═NSiMe(3) [R' = R' = Me (2a); R' = Me, R' = Ph (2b); R' = R' = OCH(2)CF(3) (2c)] in the presence or absence of AgOTf (OTf = CF(3)SO(3)) resulted in a rearrangement reaction to give the salts [R(3)P═N═PR'R'O-SiMe(3)]X (X = Br or OTf) ([4]X). Reaction of phosphine oxide 1a with the phosphoranimine BrPMe(2)═NSiPh(3) (5) with a sterically encumbered silyl group also resulted in the analogous rearranged product [Me(3)P═N═PMe(2)O-SiPh(3)]X ([8]X) but at a significantly slower rate. In contrast, the direct reaction of the bulky tert-butyl substituted phosphine oxide, (t)Bu(3)P═O (1b) with 2a or 2c in the presence of AgOTf yielded the phosphine oxide-stabilized phosphoranimine cations [(t)Bu(3)P═O·PR'(2)═NSiMe(3)](+) ([3](+), R' = Me (d), OCH(2)CF(3) (e)). A mechanism is proposed for the unexpected formation of [4](+) in which the formation of the donor-stabilized adduct [3](+) occurs as the first step.     

Construction of titanasiloxanes by incorporation of silanols to the metal oxide model [(Ti(eta 5-C5Me5)(mu-O))3(mu3-CR)]: DFT elucidation of the reaction mechanism

A family of novel titanasiloxanes containing the structural unit {[Ti(eta(5)-C(5)Me(5))O](3)} were synthesized by hydron-transfer processes involving reactions with equimolecular amounts of mu(3)-alkylidyne derivatives [{Ti(eta(5)-C(5)Me(5))(mu-O)}(3)(mu(3)-CR)] (R=H (1), Me (2)) and monosilanols, R(3)'Si(OH), silanediols, R(2)'Si(OH)(2), and the silanetriol tBuSi(OH)(3). Treatment of 1 and 2 with triorganosilanols (R'=Ph, iPr) in hexane affords the new metallasiloxane derivatives [{Ti(eta(5)-C(5)Me(5))(mu-O)}(3)(mu-CHR)(OSiR(3)')] (R=H, R'=Ph (3), iPr (4); R=Me, R'=Ph (5), iPr (6)). Analogous reactions with silanediols, (R'=Ph, iPr), give the cyclic titanasiloxanes [{Ti(eta(5)-C(5)Me(5))(mu-O)}(3)(mu-O(2)SiR'(2))(R)] (R=Me, R'=Ph (7), iPr (8); R=Et, R'=Ph (9), iPr (10)). Utilization of tBuSi(OH)(3) with 1 or 2 at room temperature produces the intermediate complexes [{Ti(eta(5)-C(5)Me(5)) (mu-O)}(3)(mu-O(2)Si(OH)tBu)(R)] (R=Me (11), Et(12)). Further heating of solutions of 11 or 12 affords the same compound with an adamantanoid structure, [{Ti(eta(5)-C(5)Me(5))(mu-O)}(3)(mu-O(3)SitBu)] (13) and methane or ethane elimination, respectively. The X-ray crystal structures of 3, 4, 6, 8, 10, 12, and 13 have been determined. To gain an insight into the mechanism of these reactions, DFT calculations have been performed on the incorporation of monosilanols to the model complex [{Ti(eta(5)-C(5)H(5))(mu-O)}(3)(mu(3)-CMe)] (2 H). The proposed mechanism consists of three steps: 1) hydron transfer from the silanol to one of the oxygen atoms of the Ti(3)O(3) ring, forming a titanasiloxane; 2) intramolecular hydron migration to the alkylidyne moiety; and 3) a mu-alkylidene ligand rotation to give the final product.     

Insertion reactions of hydridonitrosyltetrakis(trimethylphosphine) tungsten(0)

[W(H)(NO)(PMe3)4] (1) was prepared by the reaction of [W(Cl)(NO)(PMe3)4] with NaBH4 in the presence of PMe3. The insertion of acetophenone, benzophenone and acetone into the W-H bond of 1 afforded the corresponding alkoxide complexes [W(NO)(PMe3)4(OCHR1R2)](R1 = R2 = Me (2); R1 = Me, R2 = Ph (3); R1 = R2 = Ph (4)), which were however thermally unstable. Insertion of CO2 into the W-H bond of yields the formato-O complex trans-W(NO)(OCHO)(PMe3)4 (5). Reaction of trans-W(NO)(H)(PMe3)4 with CO led to the formation of mer-W(CO)(NO)(H)(PMe3)3 (6) and not the formyl complex W(NO)(CHO)(PMe3)4. Insertion of Fe(CO)(5), Re2(CO)10 and Mn2(CO)10 into trans-W(NO)(H)(PMe3)4 resulted in the formation of trans-W(NO)(PMe3)4(mu-OCH)Fe(CO)4 (7), trans-W(NO)(PMe3)4(mu-OCH)Re2(CO)9 (8) and trans-W(NO)(PMe3)4(mu-OCH)Mn2(CO)9 (9). For Re2(CO)10, an equilibrium was established and the thermodynamic data of the equilibrium reaction have been determined by a variable-temperature NMR experiments (K(298K)= 104 L mol(-1), DeltaH=-37 kJ mol(-1), DeltaS =-86 J K(-1) mol(-1)). Both compounds 7 and 8 were separated in analytically pure form. Complex 9 decomposed slowly into some yet unidentified compounds at room temperature. Insertion of imines into the W-H bond of 1 was also additionally studied. For the reactions of the imines PhCH=NPh, Ph(Me)C=NPh, C6H5CH=NCH2C6H5, and (C6H5)2C=NH with only decomposition products were observed. However, the insertion of C10H7N=CHC6H5 into the W-H bond of led to loss of one PMe3 ligand and at the same time a strong agostic interaction (C17-H...W), which was followed by an oxidative addition of the C-H bond to the tungsten center giving the complex [W(NO)(H)(PMe3)3(C10H6NCH2Ph)] (10). The structures of compounds 1, 4, 7, 8 and 10 were studied by single-crystal X-ray diffraction.     

Bis-phosphites and bis-phosphinites based on distally-functionalised calix[4]arenes: coordination chemistry and use in rhodium-catalysed, low-pressure olefin hydroformylation

Six calix[4]arenes each bearing two non-cyclic PR2 units attached at distal phenolic oxygen atoms, p-Bu t-calix[4]arene-25,27-(OPR2)2-26,28-(OR')2(R = OPh; R'= Prn, L1; R = OPh; R'= CH2CO2Et, L2; R= OPh; R'= CO2 cholesteryl, L3; R = Ph; R'= Prn, 4; R = Ph; R'= CH2CO2Et, L5; R = Ph; R'= CO2cholesteryl, L6) have been synthesized and their coordinative properties investigated. The diphosphites L1-L3, where the P centres are separated by 12 bonds, readily form chelate complexes provided the complexation reaction is achieved either by using a starting complex that possesses good leaving groups or by operating under high dilution in order to avoid oligomer formation. Thus, the cationic complexes [Rh(COD)L1]BF4 and [Rh(COD)L3]BF4 were both formed in high yield by reacting the appropriate diphosphite with either [Rh(COD)(THF)2]BF4 or [Rh(COD)2]BF4. At high dilution, reaction of L3 with the neutral complex [PdCl2(COD)] afforded the chelate complex [PdCl2L3] in 90% yield. The reaction of one equiv. of L1 with [Rh(acac)(CO)2] resulted in the formation of [Rh(acac)L1] without requiring high dilution conditions. When the latter reaction was carried out with 0.5 equiv. of L1, the bimetallic complex [{Rh(acac)(CO)}2(eta]1-P,eta1-P'-L1)] was formed instead. Reaction at high dilution of with the cyclometallated complex [Pd(o-C6H4CH2NMe2)(THF)2]BF4 gave the expected chelate complex [Pd(o-C6H4CH2NMe2)]BF4. The latter slowly converts in solution to an oligomer in which the ligand behaves as a (eta1-P,eta1-P') bridging ligand, thus leading to a less strained structure. All six ligands, when mixed with [Rh(acac)CO2], effectively catalyse the hydroformylation of octene and styrene. In the hydroformylation of octene, the linear aldehyde selectivities observed with L2 and L3 are significantly higher (linear : branched =ca. 10) than those obtained with the other 4 ligands of this study and also with respect to PPh3. Molecular modelling shows that the lower rim substituents of and form tighter pockets about the metal centre than do the other ligands and so sterically favour the formation of Rh(n-alkyl) intermediates over that of Rh(i-alkyl) ones. In styrene hydroformylation, all ligands result in the formation of unusually high amounts of the linear aldehyde, the b : l ratios being all close to 65 : 35. The highest activities were found when using an L/Rh ratio of 1/1.     

Vinylgallium and alkyllithium compounds: transmetalation and generation of oligolithium cages

Vinylgallium compounds [C(6)H(6-n){(H)C=C(SiR(2) R')-GaR'(2)}(n ] (3, R=Ph, Me; R'=Ph, Me; R'=tBu, Et; n=1, 2) are easily accessible by hydrogallation of the corresponding alkynylbenzene derivatives with H-GaCl(2) and subsequent reaction with alkyllithium derivatives. Treatment of 3 with an excess amount of tert-butyl- or ethyllithium yielded by transmetalation and ortho-deprotonation of the aromatic rings the unprecedented solvent-free oligolithium cluster compounds [{(C(6)H(4)Li)HC=C(SiPh(3))Li}(2)(tBuLi)(2)] (4), [{(C(6)H(4)Li)HC=C(SiPh(2)Me)Li}(4)] (5) and [{(C(6)H(3)Li){HC=C(SiMe(3))Li}(2)}(3)] (6) in moderate yields. Their solid-state structures revealed the presence of unique molecular lithium clusters with 6, 8, or 9 lithium atoms that may be derived from two edge-sharing Li(4) tetrahedra (4), three Li(4) tetrahedra in a chain joined by two common edges (5) or a tricapped trigonal prism of lithium atoms (6).     

Primary and secondary phosphine complexes of iron porphyrins and ruthenium phthalocyanine: synthesis, structure, and P-H bond functionalization

Reduction of [Fe(III)(Por)Cl] (Por = porphyrinato dianion) with Na2S2O4 followed by reaction with excess PH2Ph, PH2Ad, or PHPh2 afforded [Fe(II)(F20-TPP)(PH2Ph)2] (1a), [Fe(II)(F20-TPP)(PH2Ad)2] (1b), [Fe(II)(F20-TPP)(PHPh2)2] (2a), and [Fe(II)(2,6-Cl2TPP)(PHPh2)2] (2b). Reaction of [Ru(II)(Pc)(DMSO)2] (Pc = phthalocyaninato dianion) with PH2Ph or PHPh2 gave [Ru(II)(Pc)(PH2Ph)2] (3a) and [Ru(II)(Pc)(PHPh2)2] (4). [Ru(II)(Pc)(PH2Ad)2] (3b) and [Ru(II)(Pc)(PH2Bu(t))2] (3c) were isolated by treating a mixture of [Ru(II)(Pc)(DMSO)2] and O=PCl2Ad or PCl2Bu(t) with LiAlH4. Hydrophosphination of CH2=CHR (R = CO2Et, CN) with [Ru(II)(F20-TPP)(PH2Ph)2] or [Ru(II)(F20-TPP)(PHPh2)2] in the presence of (t)BuOK led to the isolation of [Ru(II)(F20-TPP)(P(CH2CH2R)2Ph)2] (R = CO2Et, 5a; CN, 5b) and [Ru(II)(F20-TPP)(P(CH2CH2R)Ph2)2] (R = CO2Et, 6a; CN, 6b). Similar reaction of 3a with CH2=CHCN or MeI gave [Ru(II)(Pc)(P(CH2CH2CN)2Ph)2] (7) or [Ru(II)(Pc)(PMe2Ph)2] (8). The reactions of 4 with CH2=CHR (R = CO2Et, CN, C(O)Me, P(O)(OEt)2, S(O)2Ph), CH2=C(Me)CO2Me, CH(CO2Me)=CHCO2Me, MeI, BnCl, and RBr (R = (n)Bu, CH2=CHCH2, MeC[triple bond]CCH2, HC[triple bond]CCH2) in the presence of (t)BuOK afforded [Ru(II)(Pc)(P(CH2CH2R)Ph2)2] (R = CO2Et, 9a; CN, 9b; C(O)Me, 9c; P(O)(OEt)2, 9d; S(O)2Ph, 9e), [Ru(II)(Pc)(P(CH2CH(Me)CO2Me)Ph2)2] (9f), [Ru(II)(Pc)(P(CH(CO2Me)CH2CO2Me)Ph2)2] (9g), and [Ru(II)(Pc)(PRPh2)2] (R = Me, 10a; Bu(n), 10b; Bn, 10c; CH2CH=CH2, 10d; CH2C[triple bond]CMe, 10e; CH=C=CH2, 10f). X-ray crystal structure determinations revealed Fe-P distances of 2.2597(9) (1a) and 2.309(2) A (2bx 2 CH2Cl2) and Ru-P distances of 2.3707(13) (3b), 2.373(2) (3c), 2.3478(11) (4), and 2.3754(10) A (5b x 2 CH2Cl2). Both the crystal structures of 3b and 4 feature intermolecular C-H...pi interactions, which link the molecules into 3D and 2D networks, respectively.