Triflates alcoholic groups

Tin(II) triflate has been used to catalyse the condensation between tetra-O-acetyl-a-D-glucopyranosyl bromide and primary and secondary alcohol groups on other monosaccharide derivatives. The products had the 3-configuration exclusively but the yields were modest (30-65%). In a related study the influences of catalyst, solvent, and temperature on the reaction of 0-(tetra-O-benzyl-a-D-glucopyranosyDtrichloroacetimidate with primary and secondary sugar alcohols were examined. With boron trifluoride in dichloro-methane at -I8—good yields (e.g. 80 for a secondary alcohol) and anomeric ratios (a,3, ca. 1 4) were obtained. 

Tosylates, Mesylates, and Triflates Leaving Group Derivatives of Alcohols 514... 

TOSYLATES, MESYLATES, AND TRIFLATES LEAVING GROUP DERIVATIVES OF ALCOHOLS... 

Alkyl esters of trifluoromethanesulfonic acid, commonly called triflates, have been prepared from the silver salt and an alkyl iodide, or by reaction of the anhydride with an alcohol (18,20,21). Triflates of the 1,1-dihydroperfluoroalkanols, CF2S020CH2R can be prepared by the reaction of perfluoromethanesulfonyl fluoride with the dihydroalcohol in the presence of triethylamine (22,23). Triflates are important intermediates in synthetic chemistry. They are among the best leaving groups known, so they are commonly employed in anionic displacement reactions. 

The second element of general importance in the synthesis of a task-specific ionic liquid is the source of the functional group that is to be incorporated. Key to success here is the identification of a substrate containing two functional groups with different reactivities, one of which allows the attachment of the substrate to the core, and the other of which either is the functional group of interest or is modifiable to the group of interest. Functionalized alkyl halides are commonly used in this capacity, although the triflate esters of functionalized alcohols work as well. 

To obtain this compound the key step consisted in the epimerization of the C-5 in compound 6. This was acomplished by triflation of the alcohol 6 and nucleophilic substitution of the triflate by a large excess of tetrabutylammonium acetate in dichloromethane. A controlled (4 °C, 3 h) basic methanolysis of the enol benzoate led to the keto-ester 11" whose hydroxyl functions at C-4 and C-6 were simultaneously deprotected under acidic conditions to furnish 12. Finally a Zemplen deprotection of the 5-acetoxy group led to 13 obtained in five steps and 11% overall yield from 6 (figure 4). 

Bismuth(III) triflate is also a powerful acylation catalyst that catalyzes reactions with acetic anhydride and other less reactive anhydrides such as benzoic and pivalic anhydrides.113 Good results are achieved with tertiary and hindered secondary alcohols, as well as with alcohols containing acid- and base-sensitive functional groups. 

Polymers with triflate groups react with alcohols to form alkoxysubstituted polysilanes. This reaction occurs readily in the presence of bases. The best results were obtained using triethylamine and hindered pyridine. In Fig. 3c the NMR spectrum of the reaction mixture containing the excess of triethylamine is shown, the methyl groups from the polymer chains absorb in the range typical for alkoxysilanes. Reaction in the presence of unsubstituted pyridine leads to the formation of insoluble polymer probably by attack at the p-C atom in the silylated pyridine. 

The palladium-catalyzed cross-coupling reaction featured in this procedure occurs under neutral conditions in the presence of many synthetically useful functional groups (e.g. alcohol, ester, nitro, acetal, ketone, and aldehyde). The reaction works best in N,N-dimethylformamide with bis(triphenylphosphine)palladium(ll) chloride, PdCI2(PPh3)2, as the catalyst. Lithium chloride is added to prevent decomposition of the catalyst.143 13 It is presumed that conversion of the intermediate aryl palladium triflate to an aryl palladium chloride is required for the transmetallation step to proceed.9... 

An intramolecular acetal has also been introduced by the treatment of a mixture of a 1-thio-mannoside, having a methoxybenzyl protecting group at C-2 and an alcohol with DDQ [71] (Scheme 4.4c). Activation of the thioglycoside with methyl triflate gave a P-mannoside as the only anomer. This approach was employed for the synthesis of the core pentasaccharide of N-linked glycoproteins. 

The introduction of the allylic silane moiety required for the intermolec-ular Hosomi-Sakurai reaction is depicted in Scheme 16. Following the formation of the enol triflate 97, a Stille coupling provided excess to the allylic alcohol 98 [51]. The allylic alcohol (98) was endowed with a phosphate leaving group for the subsequent allylic substitution. Utilizing a trimethylsilyl cuprate as nucleophile for the 5 2 reaction, the allylic phosphate was converted into the allylic silane 89. A useful substrate-induced diastereoselectivity in favour of (14i )-89 was encountered at small scale but decreased significantly upon up-scaling. 

Treatment of the alcohol ( ) with trifluoromethylsulfonic anhydride (triflic anhydride) at -78 C afforded the ester (1 ) which could be isolated and characterized. We knew from previous experience (2J that sulfonyl esters vicinal to an isopropylidene acetal are relatively stable. The triflate T,) reacted cleanly with potassium azide and 18-crown-6 in dichloromethane at room temperature. The crystalline product [68% overall from (1 )] was not the azide ( ) but the isomeric A -triazoline ( )- Clearly the initially formed azide (18) had undergone intramolecular 1,3-cyclo-addition to the double bond of the unsaturated ester (21- ). The stereochemistry of the triazoline (1 ), determined by proton nmr spectroscopy, showed that the reaction was stereospecific. There are several known examples of this reaction ( ), including one in the carbohydrate series ( ). When the triazoline was treated with sodium ethoxide ( ) the diazoester ( ) was rapidly formed by ring-opening and was isolated in 85% yield, Hydrogenolysis of the diazo group of (M) gave the required pyrrolidine ester ( ) (90%). 

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