Steric effects ketones

Protecting groups are generally formed by nucleophilic attack on the carbonyl group and the rate of this process is determined by steric and electronic factors associated with the ketone. In steroid ketones steric effects are usually more important due to the rigid tetracychc skeleton. 

Methyl, ethyl, isopropyl, and r-butyl magnesium bromides were compared in enolization reactions [Eq. (11)]. The relative rates were Et>/-Pr> Me>f-Bu, which reflects a combination of steric and electronic effects. The bulkier Grignard reagents react slower, whereas the more substituted Grignard reagents are stronger bases. With more-hindered ketones, steric effects predominate over electronic. The structures of magnesium enoiates were confirmed by reaction with benzoyl chloride to form enol-benzoates [14,15]. 

Trialky lalanes Stereospecific synthesis of tert. alcohols from ketones Steric effect of solvents... 

Table 17 3 compares the equilibrium constants for hydration of some simple aldehydes and ketones The position of equilibrium depends on what groups are attached to C=0 and how they affect its steric and electronic environment Both effects con tribute but the electronic effect controls A hydr more than the steric effect... 

Electronic and steric effects operate m the same direction Both cause the equilib rium constants for hydration of aldehydes to be greater than those of ketones... 

Substitution reactions by the ionization mechanism proceed very slowly on a-halo derivatives of ketones, aldehydes, acids, esters, nitriles, and related compounds. As discussed on p. 284, such substituents destabilize a carbocation intermediate. Substitution by the direct displacement mechanism, however, proceed especially readily in these systems. Table S.IS indicates some representative relative rate accelerations. Steric effects be responsible for part of the observed acceleration, since an sfp- caibon, such as in a carbonyl group, will provide less steric resistance to tiie incoming nucleophile than an alkyl group. The major effect is believed to be electronic. The adjacent n-LUMO of the carbonyl group can interact with the electnai density that is built up at the pentacoordinate carbon. This can be described in resonance terminology as a contribution flom an enolate-like stmeture to tiie transition state. In MO terminology,.the low-lying LUMO has a... 

Reductions by NaBKt are characterized by low enthalpies of activation (8-13kcal/mol) and large negative entropies of activation (—28 to —40eu). Aldehydes are substantially more reactive than ketones, as can be seen by comparison of the rate data for benzaldehyde and acetophenone. This relative reactivity is characteristic of nearly all carbonyl addition reactions. The reduced reactivity of ketones is attributed primarily to steric effects. Not only does the additional substituent increase the steric restrictions to approach of the nucleophile, but it also causes larger steric interaction in the tetrahedral product as the hybridization changes from trigonal to tetrahedral. 

In the absence of steric factors e.g. 5 ), the attack is antiparallel (A) (to the adjacent axial bond) and gives the axially substituted chair form (12). In the presence of steric hindrance to attack in the preferred fashion, approach is parallel (P), from the opposite side, and the true kinetic product is the axially substituted boat form (13). This normally undergoes an immediate conformational flip to the equatorial chair form (14) which is isolated as the kinetic product. The effect of such factors is exemplified in the behavior of 3-ketones. Thus, kinetically controlled bromination of 5a-cholestan-3-one (enol acetate) yields the 2a-epimer, (15), which is also the stable form. The presence of a 5a-substituent counteracts the steric effect of the 10-methyl group and results in the formation of the unstable 2l5-(axial)halo ketone... 

The direct formation of a dimethyl ketal by reaction of the ketone with methanol is particularly sensitive to steric effects. Only cyclohexanones react under these conditions.In the steroid series only saturated 3-ketones form dimethyl ketals with methanol and acid although partial reaction of a 2-ketone has been observed in the presence of homogenous rhodium catalyst. ... 

The saturated 3-ketone can also be protected as the ethylene ketal, which is prepared directly by reaction with ethylene glycol or by exchange dioxo-lanation. Selective formation of 3-ethylenedioxy compounds is also possible, but the former method is not particularly effective in the presence of 6-, 17- or 20-ketones. However, the exchange dioxolanation technique is more sensitive to steric effects and good selectivity at C-3 can be achieved in the presence of a 17-ketone, provided the reagent does not contain glycol. ... 

Virtually any aldehyde or ketone and any CH-acidic methylene compound can be employed in the Knoevenagel reaction however the reactivity may be limited due to steric effects. Some reactions may lead to unexpected products from side-reactions or from consecutive reactions of the initially formed Knoevenagel product. 

Since equatorial attack is roughly antiperiplanar to two C-C bonds of the cyclic ketone, an extended hypothesis of antiperiplanar attack was proposed39. Since the incipient bond is intrinsically electron deficient, the attack of a nucleophile occurs anti to the best electron-donor bond, with the electron-donor order C—S > C —H > C —C > C—N > C—O. The transition state-stabilizing donor- acceptor interactions are assumed to be more important for the stereochemical outcome of nucleophilic addition reactions than the torsional and steric effects suggested by Felkin. 

With reactive aldehydes an early transition state is probably involved and therefore the steric demands of the aldehyde substituents are not highly influential. On the other hand, with less reactive ketones, the carbon-carbon bond formation is established further along the reaction coordinate, permitting the steric effects to play a greater role in the determination of the transition stale structure. 

The relative reactivities of alkyltin compounds towards tert-butoxyl radicals, ketone triplets, and succinimidyl radicals are dominated by the steric effect of the alkyl ligands (R" > R"), but that towards bromine atoms follows the reverse sequence (R" < R ). 

Ordinary ketones are generally much more difficult to cleave than trihalo ketones or p-diketones, because the carbanion intermediates in these cases are more stable than simple carbanions. However, nonenolizable ketones can be cleaved by treatment with a 10 3 mixture of t-BuOK—H2O in an aprotic solvent such as ether, dimethyl sulfoxide, 1,2-dimethoxyethane (glyme), and so on, or with sohd t-BuOK in the absence of a solvent. When the reaction is applied to monosubstituted diaryl ketones, that aryl group preferentially cleaves that comes off as the more stable carbanion, except that aryl groups substituted in the ortho position are more readily cleaved than otherwise because of the steric effect (relief of stain). In certain cases, cyclic ketones can be cleaved by base treatment, even if they are enolizable. " OS VI, 625. See also OS VH, 297. 

In this chapter, the definitions used by Perrin in his book on pA a prediction (which also includes a very convenient compilation of o values) will be used. One must be alert to the importance of the number of hydrogens directly attached to the carbonyl carbon several groups have pointed out that aldehydes and ketones give separate but parallel lines, with formaldehyde displaced by the same amount again. What this means is that given one equilibrium constant for an aldehyde (or ketone) one may estimate the equilibrium constant for other aldehydes (or ketones) from this value and p for the addition using a value from experiment, if available, or estimated if necessary. This assumes that there is no large difference in steric effects between the reference compound and the unknown of interest. 

The BS2 catalyst was more selective toward the formation of the dialkylated product than the Pd catalysts tested. The activity of BS2 for DAE-MIBK reaction was slower than that with acetone due to steric effects posed by the larger ketone. Here again, the imine tends to rapidly cychze to form imidazolidines or pyrimidines. Figure 17.2 shows the stepwise formation of various side products observed during the reductive alkylation of DAE with acetone. 

Grignard additions are sensitive to steric effects and with hindered ketones a competing process leading to reduction of the carbonyl group can occur. A cyclic TS is involved. 

The catalyzed hydrogenation of an aldehyde- vs. a ketone-carbonyl is invariably faster because of steric effects (23), and the data for 6 vs. 10 are in line with this (eqs. 4 and 5). Thus, conversions of 6a-c after 0.5 h at standard conditions are 86, 47, and 97%, respectively, while corresponding values for lOa-c after 4 h are 78, 36 and 49%, respectively. Indeed, the aldehydes can be reduced at 25 °C under otherwise identical conditions (6b gives 38% conversion after 4 h, and 6c gives 99% after 15 h). The above reactivity trend for the ketones lOa-c shows that the hydrogenation rates depend on the substituent para to the carbonyl functionality and increase in the order H > OMe > OH. For the aldehyde susbtrates, the more limited data (substrate 6 with R = H and R = OMe was not available) suggest a similar para-substitucnt effect (at least OMe > OH). Note that this is the reverse trend to that observed for reduction of the activated C=C systems described above. 

Electron spin resonance (ESR) signals, detected from phosphinated polystyrene-supported cationic rhodium catalysts both before and after use (for olefinic and ketonic substrates), have been attributed to the presence of rhodium(II) species (348). The extent of catalysis by such species generally is uncertain, although the activity of one system involving RhCls /phosphinated polystyrene has been attributed to rho-dium(II) (349). Rhodium(II) phosphine complexes have been stabilized by steric effects (350), which could pertain to the polymer alternatively (351), disproportionation of rhodium(I) could lead to rhodium(II) [Eq. (61)]. The accompanying isolated metal atoms in this case offer a potential source of ESR signals as well as the catalysis. 

Steric effects on both the amide and the acyloxyl side chain are similar. Tert-butyl and adamantyl groups on the amide side chain in 29v, 29x, 29c, and 29e (Table 2 entries 53 and 54, 63 and 65) result in lower stretch frequencies that, on average, are only 40 cm-1 higher than their precurser hydroxamic esters. Streck and coworkers have suggested that such changes in dialkyl ketones can be ascribed to destabilisation of resonance form II through steric hindrance to solvation which, in the case of tert-butyl counteracts the inductive stabilisation.127... 

Streck and coworkers showed that in a range of solvents, the 13C carbonyl shifts in dialkyl ketones were affected similarly by branching at the a-position.127 In chloroform, the carbonyls of di-tert-butylketone and diisopropylketone were 11-12 ppm downfield of that of acetone, which they attributed to a mixture of inductive and steric effects. With tertiary systems, particularly in dipolar solvents, hindrance to solvent stabilisation of the polar, basic form of the carbonyl offsets the inductive stabilisation of the branched alkyl. 13C NMR data presented here support this. 

Subsequently, high chemoselectivity and enantioselectivity have been observed in the asymmetric epoxidation of a variety of conjugated enynes using fructose-derived chiral ketone as the catalyst and Oxone as the oxidant. Reported enantioselectivities range from 89% to 97%, and epoxidation occurs chemoselectively at the olefins. In contrast to certain isolated trisubstituted olefins, high enantioselectivity for trisubstituted enynes is noticeable. This may indicate that the alkyne group is beneficial for these substrates due to both electronic and steric effects. 

In one case, the intermolecular Heck reaction of 3-pyridyltriflate with ethyl acrylate was accelerated by LiCl to give 159 [127,128], Here, both electronic and steric effects all favored p-substitution. In another case, however, electronic effects prevailed and complete a-substitution was observed. In the presence of an electron-donating substituent (i.e., a protected amine), 3-bromopyridine 160 was coupled with f-butoxyethylene to give 3-pyridyl methyl ketone 162 [126]. The regiochemistry of the Heck reaction was governed by inductive effects, leading to intermediate 161. 

In summary, a number of effective chiral reducing agents have been developed based on the modification of LAH. Excellent results have been obtained with aryl alkyl ketones and a,p-acetylenic ketones. However, dialkyl ketones are reduced in much lower enantiomeric excess. This clearly indicates that steric effects alone do not control stereoselectivity in these reductions. Systematic studies have been carried out with the objective of designing improved reagents. A better understanding of the mechanisms and knowledge of the active species is required in order to provide more accurate models of the transition states of the key reduction steps. 

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