Stereochemical outcomes

Stereochemictry of the product is related to the reactant in a mechanistically defined manner no other stereochemical outcome is mechanistically possible, i.e. SN2 reaction- inversion of configuration is required... 

When more than one stereochemical outcome is possible, but one is formed in excess (even if that excess is 100 0). 

In summary, when using a ligand catalyst ratio of 1.75 1 at pH 5-6 the enantioselectivity of the Diels-Alder reaction between 3.8c and 3.9 is dictated by the activated complexes involving ligand, copper(ir) ion, dienophile and diene. Considering that four different products are formed in this reaction (see Scheme 3.5), at least four different activated complexes are involved However, each of these complexes hus two degrees of freedom that determine the stereochemical outcome of the... 

The stereochemical outcome of these reactions can be explained by considering the transition-state geometry. For example, applying the Houk model (495) to akyhc alcohols and their derivatives, the smallest substituent at the preexisting chiral center is oriented "inside" over the face of the transition-state ring and the oxygen atom "outside" (483). 

The study of the stereochemical course of organic reactions often leads to detailed insight into reaction mechanisms. Mechanistic postulates ftequently make distinctive predictions about the stereochemical outcome of the reaction. Throughout the chapters dealing with specific types of reactions, consideration will be given to the stereochemistry of a reaction and its relationship to the reaction mechanism. As an example, the bromination of alkenes can be cited. A very simple mechanism for bromination is given below ... 

Studies of the stereochemical course of rmcleophilic substitution reactions are a powerful tool for investigation of the mechanisms of these reactions. Bimolecular direct displacement reactions by the limSj.j2 meohanism are expected to result in 100% inversion of configuration. The stereochemical outcome of the lirnSj l ionization mechanism is less predictable because it depends on whether reaction occurs via one of the ion-pair intermediates or through a completely dissociated ion. Borderline mechanisms may also show variable stereochemistry, depending upon the lifetime of the intermediates and the extent of internal return. It is important to dissect the overall stereochemical outcome into the various steps of such reactions. 

Epoxides are regio- and stereoselectively transformed into fluorohydrins by silicon tetrafluoride m the presence of a Lewis base, such as diisopropyleth-ylamme and, m certain instances, water or tetrabutylammonium fluoride The reactions proceed under very mild conditions (0 to 20 C in 1,2-diohloroethane or diethyl ether) and are highly chemoselective alkenes, ethers, long-chain internal oxiranes, and carbon-silicon bonds remain intact The stereochemical outcome of the epoxide ring opening with silicon tetrafluoride depends on an additive used, without addition of water or a quaternary ammonium fluoride, as fluorohydrins are formed, whereas m the presence of these additives, only anti opening leading to trans isomers is observed [17, 18] (Table 2)... 

The reaction of diethyl tartrate with sulfur tetrafluonde at 25 °C results in replacement of one hydroxyl group, whereas at 100 °C, both hydroxyl groups are replaced by fluonne to form a,a -difluorosuccinate [762] The stereochemical outcome of the fluonnation of tartrate esters is retention of configuration at one of the chiral carbon atoms and inversion of configuration at the second chiral center [163,164, 165] Thus, treatment ofdimethyl(+)-L-tartrate with sulfur tetrafluonde gives dimethyl meso-a,a difluorosuccinate as the final product [163, 164], whereas dimethyl meso tartrate is converted into a racemic mixture of D- and L-a,a -difluorosuccmates [765] (equation 80)... 

The Woodward-Hoffifumn (WH) rules are qualitative statements regarding relative activation energies for two possible modes of reaction, which may have different stereochemical outcomes. For simple systems the rules may be derived from a... 

An important aspect is the control of the stereochemical outcome.During the course of the reaction two new chiral centers can be created and thus two diastereomeric pairs of enantiomers (syn/anti resp. erythro/threo pairs) may be obtained. 

The enantiomers are obtained as a racemic mixture if no asymmetric induction becomes effective. The ratio of diastereomers depends on structural features of the reactants as well as the reaction conditions as outlined in the following. By using properly substituted preformed enolates, the diastereoselectivity of the aldol reaction can be controlled. Such enolates can show E-ot Z-configuration at the carbon-carbon double bond. With Z-enolates 9, the syn products are formed preferentially, while fi-enolates 12 lead mainly to anti products. This stereochemical outcome can be rationalized to arise from the more favored transition state 10 and 13 respectively ... 

An instructive example on how stereochemical features influence the stereochemical outcome of the elimination is the pyrolysis of xanthates from erythro-and t/zrco-l,2-diphenyl-l-propanol. The erythro-dlcohoX 8 is converted into fi-methylstilbene 9 only, and the threo-dlcohoX 10 is converted into the corresponding Z-isomer 11 only. These results support the assumption of a syn-elimination process through a cyclic transition state ... 

The stereochemical outcome of the reaction is determined by the geometry of the transition state for the Claisen rearrangement a chairlike conformation is preferred,and it proceeds strictly by an intramolecular pathway. It is therefore possible to predict the stereochemical course of the reaction, and thus the configuration of the stereogenic centers to be generated. This potential can be used for the planning of stereoselective syntheses e.g the synthesis of natural products. 

The stereochemical outcome of the Michael addition reaction with substituted starting materials depends on the geometry of the a ,/3-unsaturated carbonyl compound as well as the enolate geometry a stereoselective synthesis is possible. " Diastereoselectivity can be achieved if both reactants contain a stereogenic center. The relations are similar to the aldol reaction, and for... 

As Lewis acid, titanium tetrachloride, boron trifluoride or ethylaluminum dichloride is often used. The stereochemical outcome of the reaction strongly depends on the Lewis acid used. The Sakurai reaction is a relatively new carbon-carbon forming reaction, that has been developed into a useful tool for organic synthesis. ... 

A recently discovered reduction procedure provides a convenient route to axial alcohols in cyclohexyl derivatives (5). The detailed mechanism of the reaction remains to be elucidated, but undoubtedly the reducing agent is an iridium species containing one or more phosphate groups as ligands. In any case, it is clear that the steric demands of the reducing agent must be extraordinary since the stereochemical outcome of the reaction is so specific. The procedure below is for the preparation of a pure axial alcohol from the ketone. 

The anion associated with quarternary ammonium compounds can influence markedly the stereochemical outcome of hydrogenolysis (43bJ67a). 

Because an S jl reaction occurs through a carbocation intermediate, its stereochemical outcome is different from that of an S 2 reaction. Carbocations, as we ve seen, are planar, sp2-hybndized, and achiral. Thus, if we carry out an S jl reaction on one enantiomer of a chiral reactant and go through an achiral carbocation intermediate, the product must be optically inactive (Section 9.10). The symmetrical intermediate carbocation can react with a nucleophile equally well from either side, leading to a racemic, 50 50 mixture of enantiomers (Figure 11.10). 

How can you keep straight all the rules about pericyclic reactions The summary information in Tables 30.1 to 30.3 can be distilled into one mnemonic phrase that provides an easy way to predict the stereochemical outcome of any pericyclic reaction ... 

Because the olefin geometry in compound 9 will most certainly have a bearing on the stereochemical outcome of the hydroboration step, a reliable process for the construction of the trans trisubsti-tuted olefin in 9 must be identified. A priori, the powerful and predictable Wittig reaction28 could be used to construct E u, [3-unsaturated ester 10 from aldehyde 11. Reduction of the ethoxycarbonyl grouping in 10, followed by benzylation of the resulting primary alcohol, would then complete the synthesis of 9. Aldehyde 11 is a known substance that can be prepared from 2-furylacetonitrile (12). 

Scheme 7. Stereochemical outcome of BINAP-Rh(i)-catalyzed asymmetric isomerization of allylic amines.

Additions of oxygen and nitrogen nucleophiles to vinyloxiranes can be achieved with Pd(0) catalysis [103, 104]. Acetate, silanols, amines, sulfonamides, and azide have been used as nucleophiles, and the stereochemical outcome of these additions, where applicable, is normally the result of two consecutive SN2 reactions. This is demonstrated by the additions of NaNHTs to vinylepoxides 29 and 30, affording syn- and anti-amino alcohols 31 and 32, respectively, in good yields and with high diastereoselectivities (Scheme 9.22) [105]. 

In the case of substituted cyclic ketones, particularly cyclohexanones, the stereochemical outcome of an addition reaction is determined by the predominance of either equatorial or axial attack of the nucleophile, leading to axial or equatorial alcohols, respectively 25 -27 (Figure 8). 

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