Silyl protection

Silylation of alcohols, amines and carboxylic acids with hydrosilanes is catalyzed by Pd catalysts[l 19], Based on this reaction, silyl protection of alcohols, amines, and carboxylic acids can be carried out with /-butyldimethylsilane using Pd on carbon as a catalyst. This method is simpler and more convenient than the silylation with /-butyldimethylsilyl chloride, which is used commonly for the protection. Protection of P-hydroxymethyl-(3-lactam (125) is an example 120]. 

The ability to convert a protective group to another functional group directly without first performing a deprotection is a potentially valuable transformation. Silyl-protected alcohols have been converted directly to aldehydes, ketones, bro-mides, acetates, and ethers without first liberating the alcohol in a prior deprotection step. 

Pyrroles and indoles can be protected with the r-butyldimethylsilyl group by treatment with TBDMSCl and n-BuLi or NaH. Triisopropylsilyl chloride (NaH, DMF, 0°-rt, 73% yield) has been used to protect the pyrrole nitrogen in order to direct electrophilic attack to the 3-position.It has also been used to protect an indole.This derivative can be prepared from the silyl chloride and The silyl protective group is cleaved with Bu4N F , THF, rt or with CF3COOH. 

Synthesis of multisubstituted furan rings using silyl protection 99CSR209. Synthetic applications of furan Diels-Alder chemistry 97T14179. Transformation of furans to N-heterocycles by aza-Achmatovicz reaction 98SL105. 

Carboximide 160, the C35-C42 fragment, can be traced retro-synthetically to phosphonate 169 and aldehyde 170. In the synthetic direction, the C35-C36 bond in 160 could be constructed by an intermolecular Horner-Wadsworth-Emmons (HWE)70 coupling of intermediates 169 and 170. Reduction of the unsaturated coupling product and exchange of silyl protecting groups would then furnish compound 160. 

Similarly, in another example, alkylation of 111 with diepoxide (—)-115 (1 equiv.) in the presence of HMPA (1.3 equiv.) furnished diol (+)-117. Protection of (+)-117 to form the acetonide, removal of the silyl protecting groups (TBAF), and hydrolysis of the dithiane with Hg(Cl04)2 provided the diketone (+)-118. Hydroxy-directed syn-reduction of both carbonyl groups with NaBI U in the presence of Et2BOMe, and triacetonide formation, followed by hydrogenolysis and monosilylation, afforded the desired Schreiber subtarget (+)-119, which was employed in the synthesis of (+)-mycoticins A and B (Scheme 8.31) [56b]. 

The enantiomerically pure (/ )- and (iS )-ketones are prepared from the corresponding enantiomer of mandelic acid by catalytic hydrogenation, treatment of the resulting hexahydroman-delic acid with ethyllithium, and subsequent introduction of the silyl protecting group33. 

Surprisingly, the size of the silyl protecting group significantly influences the stereochemical outcome of aldol additions performed with the lithium enolates of (S )-l-trimethylsiloxy-and (S)-l-f< rt-butyldimethylsiloxy-l-cyclohexyl-2-butanone. Thus, the former reagent attacks benzaldehyde preferably from the Si-face (9 1), which is the opposite topicity to that found in the addition of the corresponding titanium enolates of either ketone ... 

R)- and (,S )-1.1,2-Triphenyl-l,2-ethancdiol which are reliable and useful chiral auxiliary groups (see Section 1.3.4.2.2.3.) also perform ami-sclcctive aldol additions with remarkable induced stereoselectivity72. The (/7)-diastercomer, readily available from (7 )-methyl mandelate (2-hy-droxy-2-phcnylaeetate) and phenylmagnesium bromide in a 71 % yield, is esterified to give the chiral propanoate which is converted into the O-silyl protected ester by deprotonation, silylation, and subsequent hydrolysis. When the protected ester is deprotonated with lithium cyclohexyliso-propylamide, transmetalated by the addition of dichloro(dicyclopentadienyl)zirconium, and finally reacted with aldehydes, predominantly twm -diastereomers 15 result. For different aldehydes, the ratio of 15 to the total amount of the syn-diastereomers is between 88 12 and 98 2 while the chemical yields are 71 -90%. Furthermore, high induced stereoselectivity is obtained the diastereomeric ratios of ami-15/anti-16 arc between 95 5 and >98 2. 

In the presence of a catalytic amount of tetrabutylammonium fluoride, either freshly dried over molecular sieves22 or as the trihydrate16, silylnitronates 2 derived from primary nitroalkanes react readily at — 78 C or below, via their in situ generated nitronates. with aromatic and aliphatic aldehydes to give the silyl-protected (/J, S )-nitroaldol adducts 3 in excellent yield4,22-24-26,27. Silylnitronates, derived from secondary nitroalkanes. afford the adducts in 30 40% overall yield24. In contrast to the classical Henry reaction (vide supra), the addition of silylnitronates to aldehydes is irreversible. Ketones are unreaetive under such conditions. 

The synthesis of 5-phosphono-l,2,4-triazolin-3-one 137 began with the low-temperature metalation and phosphorylation (77) of the f-butyldimethylsilyl (TBDMS)-protectedlV-benzyl-tiiazolinone 134. The phosphonate diester 135 was obtained ter the silyl protecting group... 

At this point, completion of the total synthesis required removal of the three acetonides and the two silyl protecting groups (Scheme 18). Removal of the silyl groups with TBAF and subsequent treatment to acidic deprotection conditions led to complete deprotection of 110, but failed to provide filipin III. It was sus-... 

Fig. 3. Known and hitherto elusive perethynylated building blocks for two- and three-dimensional acetylenic scaffolding. The only compounds shown are those with either free or silyl-protected ethynyl groups...

The hydrosilylation of carbonyl compounds by EtjSiH catalysed by the copper NHC complexes 65 and 66-67 constitutes a convenient method for the direct synthesis of silyl-protected alcohols (silyl ethers). The catalysts can be generated in situ from the corresponding imidazolium salts, base and CuCl or [Cu(MeCN) ]X", respectively. The catalytic reactions usually occur at room tanperature in THE with very good conversions and exhibit good functional group tolerance. Complex 66, which is more active than 65, allows the reactions to be run under lower silane loadings and is preferred for the hydrosilylation of hindered ketones. The wide scope of application of the copper catalyst [dialkyl-, arylalkyl-ketones, aldehydes (even enoUsable) and esters] is evident from some examples compiled in Table 2.3 [51-53],... 

Oxidative addition of a silyl-protected 4-(bromomethyl)phenol precursor to (tme-da)Pd(II)Me2 (tmeda = tetramethylethylenediamine), followed by ethane reductive elimination, resulted in formation of the benzylic complex 16 (Scheme 3.10). Exchange of tmeda for a diphosphine ligand (which is better suited for stabilizing the ultimate Pd(0) QM complex), followed by removal of the protecting silyl group with fluoride anion, resulted in the expected p-QM Pd(0) complex, 17, via intermediacy of the zwitterionic Pd(II) benzyl complex. In this way a stable complex of p-BHT-QM, 17b, the very important metabolite of the widely used food antioxidant BHT20 (BHT = butylated hydroxytoluene) was prepared. Similarly, a Pd(0) complex of the elusive, simplest /)-QM, 17a, was obtained (Scheme 3.10). 

A silyl-protected alcohol can be converted into the corresponding sulfonate by treating with p-toluenesulfonylimidazole and tetrabutylammonium fluoride 165... 

Scheme 3.34. Intermolecular domino radical addition procedure for the synthesis of silyl-protected allylic alcohols.

The first asymmetric synthesis of (-l-)-abresoline was achieved from the chiral piperidine derivative 153, which upon treatment of its hydroxy side-chain substituent with carbon tetrabromide, triphenylphosphine, and triethyl-amine cyclized to the frarcr-quinazolidine 154. Deketalization and silyl protection of the phenolic group, followed by stereoselective reduction with lithium tri-t -butylborohydride (L-Selectride ), gave an alcohol, which after acylation and deprotection furnished (-l-)-abresoline 155 (Scheme 25) <2005TL2669>. 

The tricyclic core of spirotryprostatin B can be formed via formation of the dihydropyrrole 325 <2000AGE4596>. Removal of the silyl protecting group of 322, followed by Dess-Martin oxidation, and reaction of the resultant aldehyde with the potassium salt of the diketopiperazine phosphonate 323 led to formation of the enamide 324. 

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