Anti addition reactions ligands

It should be noted that formation of trans-product can be achieved in an anti-addition reaction through the outer-sphere mechanism. Theoretical studies have demonstrated that syn-addition and anti-addition reactions may start from the same 7i-complex, and direction of the multiple bond activation depends on the polarity of solvent [17, 18]. Relative reactivity in the inner-sphere and outer-sphere mechanisms contributes to the overall -/Z- selectivity of the addition reaction to alkynes (stereoselectivity issue). In some cases it is possible to switch the direction of C-Het bond formation by finding a suitable ligand [19]. In case of alkenes syn-addition and a f -addition processes do not necessarily result in different stereochemistry (unrestricted rotation around the single C-C bond in the product). Occurrence of these mechanisms for the N [20, 21], P [22, 23], O [24-26], S, Se [27, 28] heteroatom groups and application of different metal catalysts are discussed in detail in the other chapters of this book. Stereochemical pathways of nucleometallation and development of enantioselective catalytic procedures were reviewed [29]. In this chapter we focus our attention on the mechanism of irmer-sphere insertion reaction involving double and triple carbon-carbon bonds. 

Table 8 Cu-Catalyzed conjugate addition reaction with ligand L6 (6-12mol%) with ZnR2. Products were obtained with good to excellent diastereoselectivity favoring the anti diastereomer...

In the preparation of 7r-allyl complexes from cychc allylic chlorides, the stereochemistry of chloride displacement has been found to depend on the reaction conditions (Scheme 27). When the allylic chloride (17) is reacted with Pd2(dba)3, the product from syn oxidative addition, (18)-trans, predominates in nonpolar solvents, while polar solvents give the product from inversion, (18)-c/i. When the Pd(PPh3)4 complex is used as the source of Pd , the isomer from anti addition is isolated in essentially quantitative yield. Apparently, more powerfrd donor solvents or ligands favor anti attack. 

Evans has recently reported the use of structurally well-defined Sn(II) Lewis acids 119 and 120 (Fig. 9)for the enantioselective aldol addition reactions of a-heterosubstituted substrates [83]. These complexes are easily assembled from Sn(OTf)2 and C2-symmetric bisoxazoline Hgands 124 and 126 (Fig. 10). The facile synthesis of these ligands commences with optically active 1,2-amino alcohols 122, which are themselves readily available from the corresponding a-amino acids 121 [84, 85]. The Sn(II) bis(oxazoHne) complexes were shown to function optimally as catalysts for enantioselective aldol addition reactions with aldehydes and ketone substrates that are suited to putatively chelate the Lewis acid. For example, using 10 mol % of 119, thioacetate and thiopropionate derived silyl ketene acetals add at -78 °C in CH2CI2 to glyoxaldehyde to give hydroxy diesters 130 in superb yields and enantioselectivities as well as diastereo-selectivities (Eq. 12). The process represents an unusual example wherein 2,3-anti-aldol adducts are obtained in a stereoselective manner. 

Use of diisopinocampheyl boron chloride in place of the triflate affords E(0)-enolates, but the isopinocampheyl ligands were ineffective for anti aldol reactions [48]. Encouraged by the molecular mechanics analysis of the ZfOj-enolate additions, Gennari and Paterson used computational methods to design a new boron ligand for use with E(G)-enolates [97]. The design was cued by Still s comment [98] that cis-2-... 

Vinylarenes with electron donating or electron accepting substituents reacted with pinacol-H-phosphonate with excellent anti-Markovnikov selectivity >99% in dioxane at 100 °C using Wilkinson complex as catalyst precursor [78]. Changing the ligand in the RhCILa complex it was possible to find a catalytic system, which selectively reacts with the terminal double bond (L = PCya), while the addition reaction to the internal double bond did not take place [82]. 

Manufacture of rhodium precatalysts for asymmetric hydrogenation. Established literature methods used to make the Rh-DuPhos complexes consisted of converting (1,5-cyclooctadiene) acetylacetonato Rh(l) into the sparingly soluble bis(l,5-cyclooctadiene) Rh(l) tetrafluoroborate complex which then reacts with the diphosphine ligand to provide the precatalyst complex in solution. Addition of an anti-solvent results in precipitation of the desired product. Although this method worked well with a variety of diphosphines, yields were modest and more importantly the product form was variable. The different physical forms performed equally as well in hydrogenation reactions but had different shelf-life and air stability. 

A most significant advance in the alkyne hydration area during the past decade has been the development of Ru(n) catalyst systems that have enabled the anti-Markovnikov hydration of terminal alkynes (entries 6 and 7). These reactions involve the addition of water to the a-carbon of a ruthenium vinylidene complex, followed by reductive elimination of the resulting hydridoruthenium acyl intermediate (path C).392-395 While the use of GpRuGl(dppm) in aqueous dioxane (entry 6)393-396 and an indenylruthenium catalyst in an aqueous medium including surfactants has proved to be effective (entry 7),397 an Ru(n)/P,N-ligand system (entry 8) has recently been reported that displays enzyme-like rate acceleration (>2.4 x 1011) (dppm = bis(diphenylphosphino)methane).398... 

The uncatalyzed hydroboration-oxidation of an alkene usually affords the //-Markovnikov product while the catalyzed version can be induced to produce either Markovnikov or /z/z-Markovnikov products. The regioselectivity obtained with a catalyst has been shown to depend on the ligands attached to the metal and also on the steric and electronic properties of the reacting alkene.69 In the case of monosubstituted alkenes (except for vinylarenes), the anti-Markovnikov alcohol is obtained as the major product in either the presence or absence of a metal catalyst. However, the difference is that the metal-catalyzed reaction with catecholborane proceeds to completion within minutes at room temperature, while extended heating at 90 °C is required for the uncatalyzed transformation.60 It should be noted that there is a reversal of regioselectivity from Markovnikov B-H addition in unfunctionalized terminal olefins to the anti-Markovnikov manner in monosubstituted perfluoroalkenes, both in the achiral and chiral versions.70,71... 

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