Benzyl alcohol/ether groups

Loss of catalytic activity resulting from internal displacements is not usually a serious problem below temperatures of about 100 C. However, highly active R-groups, such as benzyl, methyl and allyl, undergo internal displacement more readily, particularly in the presence of strong nucleopfiles. For instance, the presence phenolates and thiolates may lead to the formation of benzyl alcohol, ethers, or sulphides from benzyl-substituted quaternary ammonium salts. 

Substitution Reactions on Side Chains. Because the benzyl carbon is the most reactive site on the propanoid side chain, many substitution reactions occur at this position. Typically, substitution reactions occur by attack of a nucleophilic reagent on a benzyl carbon present in the form of a carbonium ion or a methine group in a quinonemethide stmeture. In a reversal of the ether cleavage reactions described, benzyl alcohols and ethers may be transformed to alkyl or aryl ethers by acid-catalyzed etherifications or transetherifications with alcohol or phenol. The conversion of a benzyl alcohol or ether to a sulfonic acid group is among the most important side chain modification reactions because it is essential to the solubilization of lignin in the sulfite pulping process (17). 

A one-pot conversion of benzyl alcohols to benzyl fluorides by treatment of the alcohols with a combination of methanesulfonyl fluoride, cesium fluoride and 18-crown 6 ether in tetrahydrofuran has been repotted The reaction involves mesylation of the alcohols followed by cleavage of the resultant mesyl esters with a fluoride ion The reaction has been extended also to certain heterocycles bearing the N hydroxymethyl group [43] (equation 31)... 

PdO, cyclohexene, methanol, 30 min for a primary ROH, 90-95% yield. Secondary alcohols require longer times. The primary TBDPS and TIPS groups are cleaved much more slowly (18-21 h). Benzylic TBDMS ethers are cleaved without hydrogenolysis. ... 

DMSO or other sulfoxides react with trimethylchlorosilanes (TCS) 14 or trimefhylsilyl bromide 16, via 789, to give the Sila-Pummerer product 1275. Rearrangement of 789 and further reaction with TCS 14 affords, with elimination of HMDSO 7 and via 1276 and 1277, methanesulfenyl chloride 1278, which is also accessible by chlorination of dimethyldisulfide, by treatment of DMSO with Me2SiCl2 48, with formation of silicon oil 56, or by reaction of DMSO with oxalyl chloride, whereupon CO and CO2 is evolved (cf also Section 8.2.2). On heating equimolar amounts of primary or secondary alcohols with DMSO and TCS 14 in benzene, formaldehyde acetals are formed in 76-96% yield [67]. Thus reaction of -butanol with DMSO and TCS 14 gives, via intermediate 1275 and the mixed acetal 1279, formaldehyde di-n-butyl acetal 1280 in 81% yield and methyl mercaptan (Scheme 8.26). Most importantly, use of DMSO-Dg furnishes acetals in which the 0,0 -methylene group is deuter-ated. Benzyl alcohol, however, affords, under these reaction conditions, 93% diben-zyl ether 1817 and no acetal [67]. 

As seen in the retro-synthetic Scheme 5.3, intermediate 15 is useful for both routes. The choice of benzyl protection group was made based on the robust stability of benzyl phenol ethers toward most reactions and several possible avenues to remove it, although it was reported from Medicinal Chemistry that benzyl group removal via hydrogenolysis posed challenges in this compound. The choice of iodide substitution was born out of the known high reactivity of iodides in the Ullmann-type coupling reaction with alcohols and the robust stability of aryl iodides in many other common reactions. 

Ono and Kamimura have found a very simple method for the stereo-control of the Michael addition of thiols, selenols, or alcohols. The Michael addition of thiolate anions to nitroalkenes followed by protonation at -78 °C gives anti-(J-nitro sulfides (Eq. 4.8).11 This procedure can be extended to the preparation of a/jti-(3-nitro selenides (Eq. 4.9)12 and a/jti-(3-nitro ethers (Eq. 4.10).13 The addition products of benzyl alcohol are converted into P-amino alcohols with the retention of the configuration, which is a useful method for anri-P-amino alcohols. This is an alternative method of stereoselective nitro-aldol reactions (Section 3.3). The anti selectivity of these reactions is explained on the basis of stereoselective protonation to nitronate anion intermediates. The high stereoselectivity requires heteroatom substituents on the P-position of the nitro group. The computational calculation exhibits that the heteroatom covers one site of the plane of the nitronate anion.14... 

The combination Et3SiH/(C6F5)3B reduces acid chlorides to methyl groups (Eq. 138).281,282 If a smaller amount of triethylsilane is used, the same combination reduces aryl acid chlorides to the trimethylsilyl ethers of the benzyl alcohols.281,282... 

Since lignin is not a uniform entity, chemical criteria for its characterization have centred around analytical detenninations of its functional groups, e.g. total hydroxyl content, phenolic hydroxyls (56), methoxyl and other ether groups, benzyl alcohol groups (7a), carbonyl groups (6), etc., and estimations of its content of special structural features, e.g. phenylcoumaran units (5), biphenylyl linkages (123), etc. 

The concept of a diastereoselective Friedel-Crafts alkylation of a-chiral benzyl alcohols was first examined by Bach and coworkers [62, 63]. The initial protocol required stoichiometric amounts of strong Brpnsted acids like HBF4 and was followed by a more valuable methodology in which catalytic amounts of AuC L were employed for the diastereoselective functionalization of chiral benzyl alcohols [64], Beside arenes, allyl silanes, 2,4-pentanediones and silyl enol ethers have been used as nucleophiles. Depending on the diastereodiscriminating group and on the catalyst (Brpnsted or Lewis acid), the authors observed either the syn or the anti diastereoisomer as the major product. 

In addition to the alkylation of benzyl alcohols with silyl enol ethers, the hydroxyl group could be removed in a reduction employing triethylsilane Et3SiH as the reductant. With 1 mol% of Bi(OTf)3 as the catalyst, the desired (5-arylester 34 could be isolated in 75% yield (Scheme 26). 

---