Iridium acyl complex

The ability of enzymes to achieve the selective esterification of one enantiomer of an alcohol over the other has been exploited by coupling this process with the in situ metal-catalysed racemisation of the unreactive enantiomer. Marr and co-workers have used the rhodium and iridium NHC complexes 44 and 45 to racemise the unreacted enantiomer of substrate 7 [17]. In combination with a lipase enzyme (Novozyme 435), excellent enantioselectivities were obtained in the acetylation of alcohol 7 to give the ester product 43 (Scheme 11.11). A related dynamic kinetic resolution has been reported by Corberdn and Peris [18]. hi their chemistry, the aldehyde 46 is readily racemised and the iridium NHC catalyst 35 catalyses the reversible reduction of aldehyde 46 to give an alcohol which is acylated by an enzyme to give the ester 47 in reasonable enantiomeric excess. 

Complexes 6 undergo the second migratory insertion in this scheme to form the acyl complexes 7. Complexes 7 can react either with CO to give the saturated acyl intermediates 8, which have been observed spectroscopically, or with H2 to give the aldehyde product and the unsaturated intermediates 3. The reaction with H2 involves presumably oxidative addition and reductive elimination, but for rhodium no trivalent intermediates have been observed. For iridium the trivalent intermediate acyl dihydrides have been observed [29], The Rh-acyl intermediates 8 have also been observed [26] and due to the influence of the more bulky acyl group, as compared to the hydride atom in 2e and 2a, isomer 8ae is the most abundant species. 

CO into (CO) CoMe have computed an Tj -acetyl struchire in the 16-electron intermediate MeC(0)Co(CO)3 containing an agostic interaction to the acetyl methyl group. - Finally, stable, coordinatively unsaturated iri -acyl complexes of rhodium, iridium, and platinum are known. ... 

Whereas the normal oxidative addition reactions of four-co-ordinate iridiumO) complexes produce octahedral iridium(in) complexes, the reaction of rra/w-[IrCl(N2)(PPh3)2] with acyl chlorides is one of oxidative elimination, to produce a five-co-ordinate iridiumfin) compound, e.g. (8),... 

In Albertin s system, the reaction follows different pathways depending on the nature of both the iridium precursor and the alkyne. Thus, the reaction of 347 with HC=CC(CH3)3 in the presence of H2O does not promote C-C bond breakage, but results in the formation of the acyl complex [ItCl2 -C(0)CH2CBu (PPh3)2] 62. Thermolysis of 62 in... 

This type of reaction, which has been the subject of many studies because of its potential utilization in the decarbonylation of acyl halides, has also been investigated with the analogous iridium(I) complex. The reversibility of the carbonylation/decarbonylation process was first described by Heck and Breslow in 1960, 5 and work with a wide range of organic substrates has been... 

Ogo S, Uehara K, Abura T, Watanabe Y, Fukuzumi S (2004) pH-Selective synthesis and structures of alkynyl, acyl, and ketonyl intermediates in anti-Markovnikov and Markovnikov hydrations of a terminal alkyne with a water-soluble iridium aqua complex in water. J Am ChemSoc 126 16520-16527... 

The use of ethylene adduct lb is particularly important when the species added to activate catalyst la is incompatible with one of the reaction components. Iridium-catalyzed monoallylation of ammonia requires high concentrations of ammonia, but these conditions are not compatible with the additive [Ir(COD)Cl]2 because this complex reacts with ammonia [102]. Thus, a reaction between ammonia and ethyl ciimamyl carbonate catalyzed by ethylene adduct lb produces the monoallylation product in higher yield than the same reaction catalyzed by la and [Ir(COD)Cl]2 (Scheme 27). Ammonia reacts with a range of allylic carbonates in the presence of lb to form branched primary allylic amines in good yield and high enantioselectivity (Scheme 28). Quenching these reactions with acyl chlorides or anhydrides leads to a one-pot synthesis of branched allylic amides that are not yet directly accessible by metal-catalyzed allylation of amides. 

When substituted silanes are used instead of hydrogen, the process is referred to as silylformylation or silylcarbonylation. Only rhodium complexes catalyze the transformation of unsaturated compounds to silylaldehydes via the silylformylation reaction. Iridium complexes also are able to catalyze the simultaneous incorporation of substituted silanes and CO into unsaturated compounds, although during the reaction other types of product are formed. In the presence of [ IrCl(C03) ] and [Ir4(CO)i2]) the alkenes react with trisubstituted silanes and CO to give enol silyl ethers of acyl silanes [58] according to Scheme 14.10. 

Neutral formyl complexes which contain ligating CO often decompose by decarbonylation however, several exceptions exist. For instance, the osmium formyl hydride Os(H)(CO)2(PPh3)2(CHO) evolves H2(54). Although the data are preliminary, the cationic iridium formyl hydride 49 [Eq. (14)] may also decompose by H2 evolution (67). These reactions have some precedent in earlier studies by Norton (87), who obtained evidence for rapid alkane elimination from osmium acyl hydride intermediates Os(H)(CO)3(L)(COR) [L = PPh3, P(C2H5)3], Additional neutral formyls which do not give detectable metal hydride decomposition products have been noted (57, 65) however, in certain cases this can be attributed to the instability of the anticipated hydride under the reaction conditions (H2 loss or reaction with halogenated solvents). 

The products of oxidative addition of acyl chlorides and alkyl halides to various tertiary phosphine complexes of rhodium(I) and iridium(I) are discussed. Features of interest include (1) an equilibrium between a five-coordinate acetylrhodium(III) cation and its six-coordinate methyl(carbonyl) isomer which is established at an intermediate rate on the NMR time scale at room temperature, and (2) a solvent-dependent secondary- to normal-alkyl-group isomerization in octahedral al-kyliridium(III) complexes. The chemistry of monomeric, tertiary phosphine-stabilized hydroxoplatinum(II) complexes is reviewed, with emphasis on their conversion into hydrido -alkyl or -aryl complexes. Evidence for an electronic cis-PtP bond-weakening influence is presented. 

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