Rhodium synthesis activity

In the absence of a detailed characterization of the supported rhodium, it is premature but nevertheless interesting to speculate about which property of the oxide support induces methanol synthesis activity in small rhodium particles. The effects that might be involved here are acid-base or electron transfer interactions between the support and the rhodium particles, including the change of the effective valence state of rhodium. Basic oxides such as ZnO or MgO will tend to donate electron pairs to the rhodium... 

Efficient enantioselective asymmetric hydrogenation of prochiral ketones and olefins has been accompHshed under mild reaction conditions at low (0.01— 0.001 mol %) catalyst concentrations using rhodium catalysts containing chiral ligands (140,141). Practical synthesis of several optically active natural... 

A synthesis of optically active citroneUal uses myrcene (7), which is produced from P-piaene. Reaction of diethylamine with myrcene gives A/,A/-diethylgeranyl- and nerylamines. Treatment of the aHyUc amines with a homogeneous chiral rhodium catalyst causes isomerization and also induces asymmetry to give the chiral enamines, which can be readily hydrolyzed to (+)-citroneUal (151). 

Asymmetric hydrosilylation can be extended to 1,3-diynes for the synthesis of optically active allenes, which are of great importance in organic synthesis, and few synthetic methods are known for their asymmetric synthesis with chiral catalysts. Catalytic asymmetric hydrosilylation of butadiynes provides a possible way to optically allenes, though the selectivity and scope of this reaction are relatively low. A chiral rhodium complex coordinated with (2S,4S)-PPM turned out to be the best catalyst for the asymmetric hydrosilylation of butadiyne to give an allene of 22% ee (Scheme 3-20) [59]. 

The use of rhodium catalysts for the synthesis of a-amino acids by asymmetric hydrogenation of V-acyl dehydro amino acids, frequently in combination with the use of a biocatalyst to upgrade the enantioselectivity and cleave the acyl group which acts as a secondary binding site for the catalyst, has been well-documented. While DuPhos and BPE derived catalysts are suitable for a broad array of dehydroamino acid substrates, a particular challenge posed by a hydrogenation approach to 3,3-diphenylalanine is that the olefin substrate is tetra-substituted and therefore would be expected to have a much lower activity compared to substrates which have been previously examined. 

When irradiated in the presence of norbornadiene and high-pressure synthesis gas, rhodium chloride is converted to a catalyst which is active for a variety of reactions. /2A/. The salt is probably converted photochemically to the rhodium norbornadiene complex 9. This dimer may undergo a consecutive photoreaction to give the monomeric hydrido complex 10, which is the actual catalyst for polymerisation, hydrogenation, and hydroformylation reactions. 

Rhodium and cobalt carbonyls have long been known as thermally active hydroformylation catalysts. With thermal activation alone, however, they require higher temperatures and pressures than in the photocatalytic reaction. Iron carbonyl, on the other hand, is a poor hydroformylation catalyst at all temperatures under thermal activation. When irradiated under synthesis gas at 100 atm, the iron carbonyl catalyzes the hydroformylation of terminal olefins even at room temperatures, as was first discovered by P. Krusic. ESR studies suggested the formation of HFe9(C0) radicals as the active catalyst, /25, 26/. Our own results support this idea, 111,28/. Light is necessary to start the hydroformylation of 1-octene with the iron carbonyl catalyst. Once initiated, the reaction proceeds even in the... 

Platinum complexes with chiral phosphorus ligands have been extensively used in asymmetric hydroformylation. In most cases, styrene has been used as the substrate to evaluate the efficiency of the catalyst systems. In addition, styrere was of interest as a model intermediate in the synthesis of arylpropionic acids, a family of anti-inflammatory drugs.308,309 Until 1993 the best enantio-selectivities in asymmetric hydroformylation were provided by platinum complexes, although the activities and regioselectivities were, in many cases, far from the obtained for rhodium catalysts. A report on asymmetric carbonylation was published in 1993.310 Two reviews dedicated to asymmetric hydroformylation, which appeared in 1995, include the most important studies and results on platinum-catalogued asymmetric hydroformylation.80,81 A report appeared in 1999 about hydrocarbonylation of carbon-carbon double bonds catalyzed by Ptn complexes, including a proposal for a mechanism for this process.311... 

The synthesis, aggregation behavior, and catalytic activity of Rh complexes of Xantphos derivatives (129) with surface-active pendant groups have been described.416 The complex [HRh(CO)(TPPTS)3] was used as a catalyst precursor in the hydroformylation of 1-butene, 1-octene, and styrene under biphasic reaction conditions 417 The two-phase hydroformylation of buta-1,3-diene with [HRh(CO)(TPPTS)3], with excess TPPPS, gives high yields of C5-monoaldehydes.418 The coordination behavior of the catalytic species HRh(130)(CO)2] was studied by HP NMR spectroscopy which showed the desired bis-equatorial coordination of the ligand to the rhodium center.419... 

Nielson125 reports the synthesis of 7-((V-aIkylamino)- and T-(N,N-di-alkylamino)-l,3,5-triazaadamantanes by reductive alkylation of 94, which is obtained from 91 by an improved hydrogenation procedure (rhodium-charcoal catalyst, 25.5 psi). Paper chromatography54 and the Kovats indices and relative elution volumes of 1,3,5-triazaadamantane derivatives are measured.55 7-Amino-l,3,5-triazaadamantane is used as a vulcanization accelerator.127 7-(N,N-Dialkylamino)-l,3,5-triazaadamantanes are utilized as a new class of high-density fuel (DIADAM).128 Some 7-substituted 1,3,5-triazaadamantanes have bacteriostatic and fungistatic activity.129 7-Bromo-,... 

Another important reaction principle in modem organic synthesis is carbon-hydrogen bond activation [159]. Bergman, Ellman, and coworkers have introduced a protocol that allows otherwise extremely sluggish inter- and intramolecular rhodium-catalyzed C-H bond activation to occur efficiently under microwave heating conditions. In their investigations, these authors found that heating of alkene-tethered benzimidazoles in a mixture of 1,2-dichlorobenzene and acetone in the presence of di-//-... 

Arya et al. used solid phase synthesis to prepare immobilised dendritic catalysts with the rhodium centre in a shielded environment to mimic nature s approach of protecting active sites in a macromolecular environment (e.g. catalytic sites inside enzymes) [51], Two generations PS immobilised rhodium-complexed dendrimers, 6 and the more shielded 7, were synthesised.The PS resin immobilised rhodium-complexed dendrimers were used in the hydroformylation of styrene, p-methoxystyrene, vinyl acetate and vinyl benzoate using a total pressure of 70 bar 1 1 CO/H2 at 45 °C in CH2C12. 

The system is not limited to the use of synthesis gas as feed. Mixtures of carbon dioxide and hydrogen also give rise to the formation of polyhydric alcohols, and it is also claimed that the reaction mixture can consist of steam and carbon monoxide (62). This latter claim is consistent with the presence of C02 in the reaction mixture when CO/H2 is used as feed [infrared data (62)], and suggests that these ionic rhodium systems are also active catalysts for the water gas-shift reaction (vide infra). 

With reference to the homogeneous catalyst systems thus far reported for the synthesis of hydrocarbons/chemicals from carbon monoxide and hydrogen, only the anionic rhodium systems of Union Carbide show any appreciable shift activity. With neutral species of the type M3(CO)12 (M = Ru or Os), only small quantities of carbon dioxide are produced under the synthesis conditions (57). 

The signature application for the G-H insertion in synthesis is probably the total synthesis of (—)-tetrodotoxin 126 by Du Bois and Hinman.233 Two stereospecific G-H activation steps, rhodium-catalyzed carbene G-H insertion and carbamate-based nitrene C-H insertion, have been used to install the two tetrasubstituted centers C6 and C8a (Scheme 12). Diazoketone 122 was treated with 1.5mol% Rh2(HNCOCPh3)4, and cyclic ketone 123 was selectively formed in high yield without purification. The reaction of carbamate 124 with 10mol% Rh2(HNCOCF3)4, PhI(OAc)4, and MgO in C6H6 solvent furnished the insertion product 125 in 77% yield. 

The hydrogenation of ketones with O or N functions in the a- or / -position is accomplished by several rhodium compounds [46 a, b, e, g, i, j, m, 56], Many of these examples have been applied in the synthesis of biologically active chiral products [59]. One of the first examples was the asymmetric synthesis of pantothenic acid, a member of the B complex vitamins and an important constituent of coenzyme A. Ojima et al. first described this synthesis in 1978, the most significant step being the enantioselective reduction of a cyclic a-keto ester, dihydro-4,4-dimethyl-2,3-furandione, to D-(-)-pantoyl lactone. A rhodium complex derived from [RhCl(COD)]2 and the chiral pyrrolidino diphosphine, (2S,4S)-N-tert-butoxy-carbonyl-4-diphenylphosphino-2-diphenylphosphinomethyl-pyrrolidine ((S, S) -... 

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