Alkenes catalysts, rhodium complexes

Steric effects in the alkene structure also affect linearity. As a result, quaternary carbon atoms are rarely formed in hydroformylation45 In contrast, electronic effects in hydroformylation of arylalkenes often result in the predominant formation of the branched aldehyde.6 40 43 46- 8 Styrene has a marked tendency to form 2-phenylpropanal when hydroformylated in the presence of rhodium catalysts. Rhodium complexes modified by biphosphine49 or mixed amino phosphine oxide ligands50 were shown to give the branched aldehyde with high reactivity and selectivity (iso normal ratios <61.5). 

Secondary amines can be added to certain nonactivated alkenes if palladium(II) complexes are used as catalysts The complexation lowers the electron density of the double bond, facilitating nucleophilic attack. Markovnikov orientation is observed and the addition is anti An intramolecular addition to an alkyne unit in the presence of a palladium compound, generated a tetrahydropyridine, and a related addition to an allene is known.Amines add to allenes in the presence of a catalytic amount of CuBr " or palladium compounds.Molybdenum complexes have also been used in the addition of aniline to alkenes. Reduction of nitro compounds in the presence of rhodium catalysts, in the presence of alkenes, CO and H2, leads to an amine unit adding to the alkene moiety. An intramolecular addition of an amine unit to an alkene to form a pyrrolidine was reported using a lanthanide reagent. 

The addition of allcenes to alkenes can also be accomplished by bases as well as by the use of catalyst systems consisting of nickel complexes and alkylaluminum compounds (known as Ziegler catalysts), rhodium catalysts, and other transition metal catalysts, including iron. These and similar catalysts also catalyze the 1,4 addition of alkenes to conjugated dienes, for example. 

Similar reactions have been carried out on acetylene. Aldehydes add to alkynes in the presence of a rhodium catalyst to give conjugated ketones. In a cyclic version of the addition of aldehydes, 4-pentenal was converted to cyclopen-tanone with a rhodium-complex catalyst. In the presence of a palladium catalyst, a tosylamide group added to an alkene unit to generate A-tosylpyrrolidine derivatives. ... 

In the hydroformylation of lower alkenes using a modified cobalt catalyst complex separation is achieved by distillation. The ligands are high-boiling so that they remain with the heavy ends when these are removed from the alcohol product. Distillation is not possible when higher alcohols or aldehydes are produced, because of decomposition of the catalyst ligands at the higher temperatures required. Rhodium complexes can usually also be removed by distillation, since these complexes are relatively stable. 

The mechanism of alkene hydrogenation catalyzed by the neutral rhodium complex RhCl(PPh3)3 (Wilkinson s catalyst) has been characterized in detail by Halpern [36-38]. The hydrogen oxidative addition step involves initial dissociation of PPI13, which enhances the rate of hydrogen activation by a factor... 

The monosulfonated PPh derivative, Ph2P(m-C6H4S03K) (DPM) and its rhodium complex, HRh(CO)(DPM)3 have been synthesized and characterized by IR and NMR spectroscopic techniques. The data showed that the structure was similar to [HRh(CO)(PPh3)3]. The catalytic activity and selectivity of [HRh(CO)(DPM)3] in styrene hydroformylation were studied in biphasic catalytic systems.420 421 Rh1 complexes [Rh(acac)(CO)(PR3)] with tpa (131), cyep (132), (126), ompp (133), pmpp (134), tmpp (135), PPh2(pyl), PPh(pyl)2, and P(pyl)3 were characterized with NMR and IR spectra. Complexes with (131), (132), and (126) were catalysts for hydrogenation of C—C and C—O bonds, isomerization of alkenes, and hydroformylation of alkenes.422 Asymmetric hydroformylation of styrene was performed using as catalyst precursor [Rh(//-0 Me)(COD)]2 associated with sodium salts of m-sulfonated diarylphosphines.423... 

It was recognized during the development of propene hydroformylation that propene provided some stabilization for the catalyst. In the absence of the alkene, but in the presence of carbon monoxide and hydrogen, the catalyst can undergo what has been termed intrinsic deactivation. [3 3] Apparently after oxidative addition of triphenyl-phosphine to rhodium, diphenylphosphido bridged rhodium complexes are formed. 

The first example of an enantioselective [5 + 2]-cycloaddition was reported for the tethered alkene-VCP 7a, which upon treatment with a chiral rhodium complex afforded the m-fused bicyclo[5.3.0]decene 8a in 80% yield and 63% enantiomeric excess (ee) (Equation (6)).39 A later study found that when a 2,2-bis(diphenyl-phosphanyl)-l,l-binaphthyl (BINAP)-modified rhodium(l) catalyst is used, good to excellent ee s and yields are achieved with a variety of substrates (Equation (7)).40... 

The synthesis of cationic rhodium complexes constitutes another important contribution of the late 1960s. The preparation of cationic complexes of formula [Rh(diene)(PR3)2]+ was reported by several laboratories in the period 1968-1970 [17, 18]. Osborn and coworkers made the important discovery that these complexes, when treated with molecular hydrogen, yield [RhH2(PR3)2(S)2]+ (S = sol-vent). These rhodium(III) complexes function as homogeneous hydrogenation catalysts under mild conditions for the reduction of alkenes, dienes, alkynes, and ketones [17, 19]. Related complexes with chiral diphosphines have been very important in modern enantioselective catalytic hydrogenations (see Section 1.1.6). 

In less-coordinating solvents such as dichloromethane or benzene, most of the cationic rhodium catalysts [Rh(nbd)(PR3)n]+A (19) are less effective as alkyne hydrogenation catalysts [21, 27]. However, in such solvents, a few related cationic and neutral rhodium complexes can efficiently hydrogenate 1-alkynes to the corresponding alkene [27-29]. A kinetic study revealed that a different mechanism operates in dichloromethane, since the rate law for the hydrogenation of phenyl acetylene by [Rh(nbd)(PPh3)2]+BF4 is given by r=k[catalyst][alkyne][pH2]2 [29]. 

The first step consists of the substitution of one of the ligands (L) of 18 by dioxane (39) in an oxidative addition (a) (Scheme 20.16). / -Elimination of 40 releases 2,3-dihydro-dioxine (41) and the 16-electron dihydrogen rhodium complex (42) (b). Alkene 43 coordinates to the vacant site of 42 (c) to give complex 44. A hydride insertion then takes place (d), affording complex 45. After a reductive elimination (e) of the product 46, the coordination of a ligand reconstitutes the Wilkinson-type catalyst (18). 

Brunner, Leitner and others have reported the enantioselective transfer hydrogenation of alpha-, beta-unsaturated alkenes of the acrylate type [50]. The catalysts are usually rhodium phosphine-based and the reductant is formic acid or salts. The rates of reduction of alkenes using rhodium and iridium diamine complexes is modest [87]. An example of this reaction is shown in Figure 35.8. Williams has shown the transfer hydrogenation of alkenes such as indene and styrene using IPA [88]. 

Rhodium (I) complexes of chiral phosphines have been the archetypical catalysts for the hydrocarbonylation of 1-alkenes, with platinum complexes such as (61) making an impact also in the early 1990s[1461. More recently, rhodium(I)-chiral bisphosphites and phosphine phosphinites have been investigated. Quite remarkable results have been obtained with Rh(I)-BINAPHOS (62), with excellent ee s being obtained for aldehydes derived for a wide variety of substrates1 471. For example, hydroformylation of styrene gave a high yield of (R)-2-phenylpropanal (94% ee). The same catalyst system promoted the conversion of Z-but-2-ene into (5)-2-methylbutanal (82% ee). 

Alkynes react with the bulky germanium hydride (MejSdjGeH to selectively yield (Z)-alkenes (Equation (105)).67 The hydrogermylation of alkynols or alkynes can be catalyzed by a rhodium complex (Equation (106), Table 18) and some of the intermediates were identified (Scheme 16).132 Similar rhodium species react with alkynes to yield alkenyl complexes,133 and other transition metal complexes have been employed as hydrogermylation catalysts including those containing palladium.134,135... 

The synthesis of aldehydes via hydroformylation of alkenes is an important industrial process used to produce in the region of 6 million tonnes a year of aldehydes. These compounds are used as intermediates in the manufacture of plasticizers, soaps, detergents and pharmaceutical products [7], While the majority of aldehydes prepared from alkene hydroformylation are done so in organic solvents, some research in 1975 showed that rhodium complexes with sulfonated phosphine ligands immobilized in water were able to hydroformylate propene with virtually complete retention of rhodium in the aqueous phase [8], Since catalyst loss is a major problem in the production of bulk chemicals of this nature, the process was scaled up, culminating in the Ruhrchemie-Rhone-Poulenc process for hydroformylation of propene, initially on a 120000 tonne per year scale [9], The development of this biphasic process represents one of the major transitions since the discovery of the hydroformylation reaction. The key transitions in this field include [10] ... 

This complex easily looses CO, which enables co-ordination of a molecule of alkene. As a result the complexes with bulky phosphite ligands are very reactive towards otherwise unreactive substrates such as internal or 2,2-dialkyl 1-alkenes. The rate of reaction reaches the same values as those found with the triphenylphosphine catalysts for monosubstituted 1-alkenes, i.e. up to 15,000 mol of product per mol of rhodium complex per hour at 90 °C and 10-30 bar. When 1-alkenes are subjected to hydroformylation with these monodentate bulky phosphite catalysts an extremely rapid hydroformylation takes place with turnover frequencies up to 170,000 mole of product per mol of rhodium per hour [65], A moderate linearity of 65% can be achieved. Due to the very fast consumption of CO the mass transport of CO can become rate determining and thus hydroformylation slows down or stops. The low CO concentration also results in highly unsaturated rhodium complexes giving a rapid isomerisation of terminal to internal alkenes. In the extreme situation this means that it makes no difference whether we start from terminal or internal alkenes. 

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