The Silicon-Hydrogen Exchange Reaction: A Catalytic σ-Bond Metathesis Approach to the Enantioselective Synthesis of Enol Silanes.

The use of chiral enol silanes in fundamental transformations such as Mukaiyama aldol, Michael, and Mannich reactions as well as Saegusa-Ito dehydrogenations has enabled the chemical synthesis of enantiopure natural products and valuable pharmaceuticals. However, accessing these intermediates in high enantiopurity has generally required the use of either stoichiometric chiral precursors or stoichiometric chiral reagents. We now describe a catalytic approach in which strongly acidic and confined imidodiphosphorimidates (IDPi) catalyze highly enantioselective interconversions of ketones and enol silanes. These "silicon-hydrogen exchange reactions" enable access to enantiopure enol silanes via tautomerizing σ-bond metatheses, either in a deprotosilylative desymmetrization of ketones with allyl silanes as the silicon source or in a protodesilylative kinetic resolution of racemic enol silanes with a carboxylic acid as the silyl acceptor.

Silicon–hydrogen exchange reactions can be described as formal σ-bond metatheses, interconverting silylated (C–SiR3 or O–SiR3) and hydrogenated (C–H or O–H) compounds (Scheme A). These reactions are used to install protecting groups,[1] synthesize reagents such as trimethylsilyl cyanide[2] or enol silanes,[3−6] and also increase the volatility of compounds for analytical applications.[7] Despite the value of silicon–hydrogen exchange reactions and their potential to generate enantiopure silylated compounds that are otherwise challenging to obtain, their use in asymmetric catalysis has been rare, and applications toward chiral enol silanes are currently unknown.[8−12] Access to enantiopure enol silanes traditionally requires stoichiometric amounts of strong chiral bases such as Simpkins’ lithium amides (Scheme B).[13] Alternatively, silicon–hydrogen exchange reactions have recently been used by Takasu et al.[14] to prepare achiral and racemic enol silanes from ketones with silylated triflimide as a catalyst. Independently, we found that, under certain conditions, enol silanes can also form as side products in Mukaiyama aldol and Hosomi–Sakurai reactions via silylium asymmetric counteranion-directed catalysis (Si-ACDC).[15−17] Inspired by these observations, we became intrigued by the opportunity to develop asymmetric silicon–hydrogen exchange reactions toward enantiopure enol silanes. We envisioned a catalytic cycle in which, upon the formation of a chiral silylium ion-equivalent (R3SiX*) and propene, via protodesilylation of an allylsilane by the strong acid HX*, a siloxocarbenium ion intermediate could be reversibly generated from the starting ketone (Scheme C). Its enantioselective deprotonation by the chiral counteranion X*– would then produce the enantioenriched enol silane and simultaneously regenerate the Brønsted acid precatalyst HX*.

Scheme 1

Design of a Catalytic Asymmetric Silicon–Hydrogen Exchange Reaction

While the overall transformation is generally disfavored thermodynamically, here it would presumably be driven by the release of volatile propene. In contrast, the corresponding reverse reaction, the protodesilylation of an enol silane, is thermodynamically favored and indeed well-known.[18−22] Such reactions are readily catalyzed by acids, and an asymmetric protodesilylation of racemic silyl enol ethers should be attainable by applying the same catalysis concept outlined above. Only now, instead of using an allylsilane as the silylating reagent, the reaction would be mediated by a suitable proton source (Scheme D). We speculated that, if the identical chiral catalyst would be used in the protodesilylation and if the mechanism of the protonation step would be the exact reverse of or very similar to the above oxocarbenium deprotonation, then, in line with the principle of microscopic reversibility,[23] the same enantiomer that is created in the forward reaction should be selectively protodesilylated in the reverse. As a result, the opposite enantiomer would be obtained in a kinetic resolution.[24]

Indeed, when we reacted 4-phenylcyclohexanone (1a) with commercially available allyl silane 2a in the presence of IDPi catalyst 4a, enol silane product 3a was obtained in 95% yield with a promising e.r. of 82:18 (Table , entry 1). Other commonly used Brønsted acid catalysts such as phosphoric acids, imidodiphosphates, and disulfonimides did not catalyze the reaction under these conditions (Supporting Information, Table S1).

Table 1

Optimization of the Catalytic Asymmetric Synthesis of Enol Silanea

entry	catalyst	solvent	T (°C)	yieldb (%)	e.r.c
1	4a	toluene	25	95	82:18
2	4b	toluene	25	99	85.5:14.5
3	4c	toluene	25	99	88:12
4	4d	toluene	25	99	80:20
5	4e	toluene	25	80	80:20
6	4f	toluene	25	99	75:25
7	4c	toluene:dioxane (2:1)	0	99	94:6
8	4c	toluene:dioxane (2:1)	–20	99	97:3

Reactions were performed with 1a (0.025 mmol), 2a (2.0 equiv), and 4a–4f (1 mol %).

1H NMR yield.

e.r. determined by HPLC.

With this encouraging result, we began optimizing the reaction. IDPi catalysts with different steric environments were designed by further modifying the sulfonamide core and the substitution pattern of the 3,3′-arenes of the chiral 1,1′-bi-2-naphthol (BINOL) scaffold. With the newly synthesized catalysts 4b–4f, the e.r. was further improved (entries 2–6). Gratifyingly, using a mixed solvent system at a lower temperature significantly improved the enantioselectivity with catalyst 4c, ultimately giving the product with an e.r. of 97:3 in quantitative yield (entries 7 and 8).

Using the developed conditions, a variety of 4-aryl-substituted enol silanes were prepared and isolated with generally excellent enantioselectivities (up to 98:2 e.r.) and yields (up to 99%) (Table , products 3a–3o). In addition, 4-alkyl substituted cyclohexanones 1p–1r were also tolerated, giving the desired products 3p–3r with enantioselectivities in the range of 92:8 to 97:3. 4,4-Disubstituted cyclohexanone 1s provided product 3s, featuring a quaternary stereogenic carbon center, in 94:6 e.r. Satisfyingly, product 3t bearing an ester group was generated smoothly in 92% yield with an excellent e.r. of 98:2. Additionally, we explored a bicyclic cyclopentanone (1u) and a 3-substituted cyclobutanone (1v) to probe the generality of the methodology. To our delight, the corresponding enol silanes 3u and 3v were obtained with 95:5 e.r. (98% yield) and 89:11 e.r. (96% yield), respectively.

Table 2

Substrate Scope of the Catalytic Asymmetric Deprotosilylation of Ketonesa

Performed with 1 (0.2 mmol), 2a (2.0 equiv), and 4c (1 mol %) in 2.4 mL of toluene/dioxane. Isolated yields. e.r. determined by HPLC.

With 4d.

With 4a.

With 4b;

With 4e.

With triethyl(2-methylallyl)silane (2b).

To illustrate the synthetic utility of the method, the reaction between ketone 1a and allylsilane 2a was conducted on a gram scale and furnished the product without erosion of enantioselectivity (Scheme ). Meanwhile, IDPi catalyst 4c could be recovered (93%) and remained active in further transformations, demonstrating the practicality of the process. The produced enol silane 3a could be readily transformed into different structural motifs via α-bromination,[25] α-fluorination,[26] Saegusa–Ito oxidation,[27] [2 + 2] cycloaddition,[28] and α-benzylation reactions.[29] All of these transformations proceeded smoothly to give products 5–9, with complete conservation of the enantiomeric purity. Importantly, our method could successfully be applied to furnish enol silane 3w, which is a known intermediate toward the synthesis of the prostacyclin analogue iloprost, a commercial drug used for the treatment of pulmonary arterial hypertension.[30]

Scheme 2

Synthetic Applications

As proposed above, our catalytic asymmetric ketone silylation reaction is likely driven by the irreversible protodesilylation of the allylsilane. We therefore hypothesized that, if a suitable proton source could be identified, a kinetic resolution of racemic enolsilanes may also be achievable with IDPi catalysts, in what is effectively the reverse of our enol silane synthesis. Importantly, such a kinetic resolution would not only be expected to be applicable to racemic enol silanes derived from symmetric ketones, such as 4-substituted cyclohexanones, but possibly also to enol silanes derived from unsymmetrical ketones. To explore this possibility, we investigated the protodesilylation of racemic enol silane 3x as a model substrate and isopropanol as the initial proton source. Indeed, the reaction proceeded smoothly and provided moderate enantioselectivity at 68% conversion when we used catalyst 4c (Table , entry 1). Interestingly, sulfonamide-modified catalyst 4d gave significantly higher selectivity and was therefore further investigated (entry 2). Lowering the temperature to −30 °C increased the s factor to a promising 12 (entry 3).[31,32] We also explored different proton sources using IDPi catalyst 4d at lower temperatures (entries 4–6). While water and TMP proved to be unsuitable (entry 4), 2-biphenyl carboxylic acid (BCA) 10 turned out to be an optimal reagent (entry 6). Finally, recovered silyl enol ether 3x was obtained in 97:3 e.r. at 51% conversion, corresponding to a selectivity of 70, when the reaction was conducted at −60 °C for 24 h (entry 7). As expected, even though this protonation presumably occurs via a slightly different mechanism than the enol silane synthesis described above, the opposite enantiomer of product 3x was indeed obtained, confirming the possibility to produce both enantiomers of the enol silane using the same catalyst enantiomer.

Table 3

Optimization of the Protodesilylative Kinetic Resolution of rac-3xa

entry	catalyst	proton source	conversionb (%)	e.r.c	sd
1	4c	i-PrOH	68	64:36	2
2	4d	i-PrOH	66	87:13	5
3e	4d	i-PrOH	55	91:9	12
4e	4d	H2O	49	66:34	3
5e	4d	TMP	62	85:15	5
6e	4d	BCA	52	91:9	18
7f	4d	BCA	51	97:3	70

Performed with 3x (0.1 mmol), proton sources (0.25–0.5 equiv), and catalyst (1 mol %) in 0.2 mL of toluene.

Conversion determined by GC analysis.

e.r. determined by HPLC.

s = ln[(1 – C)(1 – ee)]/ln[(1 – C)(1 + ee)].

–30 °C.

–60 °C.

Under the optimized reaction conditions, the kinetic resolution of a broad range of enol silanes was realized (Table ). For example, enol silane 3a was recovered in 50% yield after 11 h with an e.r. of 94:6 corresponding to an s-factor of 122. Similarly, the enantioenriched 4-alkyl enol silanes 3x–3z and 4-ester group substituted (S)-3t were recovered in high yields and enantioselectivities. Moreover, 2-substituted enol silanes 3aa and 3ab also underwent an efficient kinetic resolution and were recovered in remarkably high selectivities, with both an aryl and an alkyl substituent. However, the ketone byproducts 1aa and 1ab did undergo partial racemization (see the Supporting Information, Figures S7 and S8). Importantly, 3-phenyl cyclopentanone derived enol silane 3ac was also recovered with synthetically useful selectivity.

Table 4

Kinetic Resolution of the Racemic Silyl Enol Ethersa

Performed with 3 (0.2 mmol), 10 (0.5 equiv), and 4d (1 mol %) in 0.4 mL of toluene.

Conversions and yields determined by GC analysis or isolation.

e.r. determined by HPLC.

s = ln[(1 – C)(1 – ee)]/ln[(1 – C)(1 + ee)].

–60 °C.

To gain insight into the reaction mechanism, we first compared the reactions using either triflimide (Tf2NH) or IDPi catalyst 4c in the reaction of 4-phenylcyclohexanone 1a with allyl silane 2a. Remarkably, when we used triflimide as the catalyst, only homoaldol product 11 was obtained in quantitative yield as a mixture of diastereomers.[33] Even when we lowered the temperature to −20 °C, only ∼5% of the enol silane was observed and the homoaldol adducts remained the major products. In contrast, IDPi 4c exclusively led to the formation of product 3a in 99% isolated yield and 88:12 e.r. (Scheme A). In light of our recent studies,[34] we explain this remarkable chemoselectivity by invoking confinement effects: the competing self-aldolization is sterically challenged, as its relatively larger cationic transition state cannot be accommodated by the confined active site of our IDPi catalyst anion. The acidity difference may also play a role.[35]

Scheme 3

Mechanistic Studies

We furthermore investigated the reaction progression of cyclohexanone 1a with 2a by 1H NMR and 31P NMR spectroscopy. When following the reaction under standard conditions in toluene-d8:dioxane-d8 mixture, a significant dormant period, in which adventitious water and TBSOH were first converted to TBS2O, was observed before the enol silane formation began (Scheme B). Such dormant periods are quite characteristic for silylium–ACDC reactions and have been described before in detail.[36] A shorter dormant period was observed with only toluene as solvent; hence, toluene-d8 was used for all further NMR experiments.

Toward a deeper understanding of the mechanism, we analyzed the reaction by variable time normalization analysis with kinetic data obtained from 1H NMR (Scheme C–E). When following the procedures described by the Burés group,[37] we found that the overall reaction is first order in catalyst and allyl silane but zeroth order in ketone.[38] Alternatively, 31P NMR data acquired at the beginning of the reaction shows the presence of catalyst 4c as a sharp singlet at −16.9 ppm. After approximately 12 h, small amounts of silylated catalyst 4c can be detected. The two doublets at −11.3 and −20.8 ppm with J = 132 Hz indicate that the TBS group is bound preferentially to one site of the activated catalyst. After 24 h, the reaction is complete and the catalyst is almost exclusively present in its silylated form (see the Supporting Information, Figure S9). On the basis of the data obtained, we propose that the initial silylation of the catalyst with silane is the turnover-limiting step of the reaction (Scheme F, right). Only if all easily exchangeable protons are consumed, the silylated IDPi catalyst can engage in the reversible activation of the ketone. Interestingly, it is possible that the ketone silylation could already initiate the desymmetrization, by furnishing two different diastereomeric silyloxocarbenium–IDPi ion pairs. Ultimately, it is the final deprotonation step at the α-position of the silyloxocarbenium ion which establishes the enantiopurity of the produced enol silane, while regenerating the free catalyst 4c.

Based on previously reported asymmetric protonations of enol silanes with phenols,[22] we speculate that the protodesilylative kinetic resolution is initiated via protonation of the achiral BCA reagent by the IDPi catalyst 4d to form an ion pair [BCAH]+ X*–. In fact, the formation of this species was supported by ESI-MS (see the Supporting Information, Figure S10). As the enantioselectivity depends on the proton source, we propose that it is this complex and not the free IDPi catalyst that engages in the enantioselective protonation of the (R)-enol silane, leaving the corresponding (S)-enantiomer untouched. This step furnishes the same silyloxocarbenium–IDPi ion pair intermediate that is also generated in the corresponding forward reaction. Finally, the catalytic cycle is completed upon desilylation of the oxocarbenium ion by the carboxylic acid BCA, liberating ketone 1 and ester BCA–TBS, while regenerating the IDPi catalyst (Scheme F, left).

We report a general asymmetric catalytic methodology for tautomeric σ-bond metathesis reactions between ketones and enol silanes. Our reactions are catalyzed by strong and confined acids and enable both desymmetrizations of achiral cyclic ketones and kinetic resolutions of racemic cyclic enol silanes. Our findings suggest further utility in selective reactions of carbonyl compounds and enol silanes.