Bases 4-Dimethylaminopyridine

Having proved the synthetic utility of their system, the authors subsequently evaluated a second supported base, 4-dimethylaminopyridine (AO-DMAP) 118, toward the acylation of 2° alcohols (Scheme 30). Employing a premixed solution of phenyl-l-ethanol 119, Et3N 14 and acetic anhydride 37 (0.33, 0.50, and 0.50 M) in hexane, reactions were conducted at room temperature and the effect of residence time evaluated (10-50 s). Using a 60 cm packed bed, the authors were able to obtain near quantitative conversions to 120 employing residence times <20 s, with flow reactions providing superior results to those obtained in analogous batch reactions. 

Vinylpyridine (23) came into prominence around 1950 as a component of latex. Butadiene and styrene monomers were used with (23) to make a terpolymer that bonded fabric cords to the mbber matrix of automobile tires (25). More recendy, the abiUty of (23) to act as a Michael acceptor has been exploited in a synthesis of 4-dimethylaminopyridine (DMAP) (24) (26). The sequence consists of a Michael addition of (23) to 4-cyanopyridine (15), replacement of the 4-cyano substituent by dimethylamine (taking advantage of the activation of the cyano group by quatemization of the pyridine ring), and base-cataly2ed dequatemization (retro Michael addition). 4-r)imethyl aminopyri dine is one of the most effective acylation catalysts known (27). 

These rate constants are for the hydrolysis of cinnamic anhydride in carbonate buffer, pH 8.45, total buffer concentration 0.024 M, in the presence of the catalysts pyridine, A -methylimidazole (NMIM), or 4-dimethylaminopyridine (DMAP). In the absence of added catalyst, but the presence of buffer, the rate constant was 0.005 24 s . You may assume that only the conjugate base form of each catalyst is catalytically effective. Calculate the catalytic rate constant for the three catalysts. What is the catalytic power of NMIM and of DMAP relative to pyridine ... 

The second step, nucleophilic attack of an alcohol or phenol on the activated carboxylic acid RCOIm (carboxylic acid imidazolide), is usually slow (several hours), but it can be accelerated by heating[7] or by adding a base[8] [9] such as NaH, NaNH2, imidazole sodium (ImNa), NaOR, triethylamine, diazabicyclononene (DBN), diazabicycloimdecene (DBU), or /7-dimethylaminopyridine to the reaction mixture (see Tables 3—1 and 3—2). This causes the alcohol to become more nucleophilic. Sodium alcoholate applied in catalytic amounts accelerates the ester synthesis to such an extent that even at room temperature esterification is complete after a short time, usually within a few minutes.[7H9] This catalysis is a result of the fact that alcoholate reacts with the imidazolide very rapidly, forming the ester and imidazole sodium. 

The alternative method for making activated esters is base-catalyzed transesterification. Fmoc-amino acids are esterified in excellent yields by reaction with pentafluorophenyl trifluoroacetate at 40°C in the presence of pyridine (Figure 7.13). A mixed anhydride is formed initially, and the anhydride is then attacked by the pentafluorophenoxy anion that is generated by the pyridine. Succinimido, chlorophe-nyl, and nitrophenyl esters were made by this method when it was introduced decades ago. A unique variant of this approach is the use of mixed carbonates that contain an isopropenyl group [Cf C CfyO-COjR]. These react with hydroxy compounds in the presence of triethylamine or 4-dimethylaminopyridine (see Section 4.19) to give the esters and acetone.30 35... 

Dimethylaminopyridine (4) is a moderately strong base, and as a nucleophile, is a good catalyst for esterifying. V-proiecled residues activated as... 

It seems reasonable that polyester cyclics could be prepared by an extension of the /wendo-high-dilution [17] chemistry used for the preparation of cyclic carbonate oligomers [18, 19] however, such proved not to be the case. Brunelle et al. showed that the reaction of terephthaloyl chloride (TPC) with diols such as 1,4-butanediol did not occur quickly enough to prevent concentration of acid chlorides from building up during condensation [14]. Even slow addition of equimolar amounts of TPC and butanediol to an amine base (triethylamine, pyridine or dimethylaminopyridine) under anhydrous conditions did not form cyclic oligomers. (The products were identified by comparison to authentic materials isolated from commercial PBT by the method of Wick and Zeitler [9].)... 

The application of ionic liquids as a reaction medium for the copper-catalyzed aerobic oxidation of primary alcohols was reported recently by various groups, in attempts to recycle the relatively expensive oxidant TEMPO [150,151]. A TEMPO/CuCl-based system was employed using [bmim]PF6 (bmim = l-butyl-3-methylimodazolium) as the ionic liquid. At 65 °C a variety of allylic, benzylic, aliphatic primary and secondary alcohols were converted to the respective aldehydes or ketones, with good selectiv-ities [150]. A three-component catalytic system comprised of Cu(C104)2, dimethylaminopyridine (DMAP) and acetamido-TEMPO in the ionic liquid [bmpy]Pp6 (bmpy = l-butyl-4-methylpyridinium) was also applied for the oxidation of benzylic and allylic alcohols as well as selected primary alcohols. Possible recycling of the catalyst system for up to five runs was demonstrated, albeit with significant loss of activity and yields. No reactivity was observed with 1-phenylethanol and cyclohexanol [151]. 

The second protonation of dimethylaminopyridines and their N-oxides, all weak bases whose pK determination involves acidity function theory, yield o values in good agreement with previous values, affording thereby a check on the validity of the acidity function procedure. 

A BINOL-dimethylaminopyridine hybrid was seen to be efficient in mediating the MBH reaction (Table 5.14) [96], with optimal reaction conditions being found as —15 °C with a mixed solvent system consisting of toluene and cyclopentyl methyl ether (CPME) in a 1 9 ratio. The reaction was sensitive to the structure of the catalyst 112, the position of the Lewis base attached to BINOL, the substitution pattern of the amino group, and the length of the spacer. It should be noted that the bulky i-Pr substituent on the amino group showed the best selectivity and kinetic profile (Table 5.14, entry 5) [98]. (For experimental details see Chapter 14.10.4). 

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