Acyl halides ester formation

Alkyl- and arylmercury(II) halides are used for the ketone formation[402]. When active methylene compounds. such as /f-keto esters or malonates are used instead of alcohols, acylated / -keto esters and malonates 546 are produced, For this reaction, dppf is a good ligand[403]. The intramolecular version of the reaction proceeds by trapping the acylpalladium intermediate with eno-late to give five- and six-membered rings smoothly. Formation of 547 by intramolecular trapping with malonate is an example[404]. 

The Pd-catalyzed hydrogenoiysis of acyl chlorides with hydrogen to give aldehydes is called the Rosenmund reduction. Rosenmund reduction catalyzed by supported Pd is explained by the formation of an acylpalladium complex and its hydrogenolysis[744]. Aldehydes can be obtained using other hydrides. For example, the Pd-catalyzed reaction of acyl halides with tin hydride gives aldehydes[745]. This is the tin Form of Rosenmund reduction. Aldehydes are i ormed by the reaction of the thio esters 873 with hydrosilanes[746,747]. 

In the course of this study, the authors determined /Lvalues for dibenzyl, methyl phenyl, methyl p-nitrophenyl, di-p-tolyl, di-isopropyl and tetramethylene sulphoxides and for diethyl, dipropyl and dibutyl sulphites. The /Lscales are applied to the various reactions or the spectral measurements. The /Lscales have been divided into either family-dependent (FD) types, which means two or more compounds can share the same /Lscale, family-independent (FI) types. Consequently, a variety of /Lscales are now available for various families of the bases, including 29 aldehydes and ketones, 17 carboxylic amides and ureas, 14 carboxylic acids esters, 4 acyl halides, 5 nitriles, 10 ethers, 16 phosphine oxides, 12 sulphinyl compounds, 15 pyridines and pyrimidines, 16 sp3 hybridized amines and 10 alcohols. The enthalpies of formation of the hydrogen bond of 4-fluorophenol with both sulphoxides and phosphine oxides and related derivatives fit the empirical equation 18, where the standard deviation is y = 0.983. Several averaged scales are shown in Table 1588. 

Acyl imidazolides are more reactive than esters but not as reactive as acyl halides. Entry 7 is an example of formation of a (3-ketoesters by reaction of magnesium enolate monoalkyl malonate ester by an imidazolide. Acyl imidazolides also are used for acylation of ester enolates and nitromethane anion, as illustrated by Entries 8, 9, and 10. (V-Methoxy-lV-methylamides are also useful for acylation of ester enolates. 

Scheme 7 comprises the following patterns First, a metallacycle gives rise to ketones by CO insertion and reductive elimination. Next, a nickel hydride inserts an unsaturated substrate L, followed by CO. The acyl intermediate can give rise to reductive elimination with formation of acyl halides or acids and esters by hydrolysis, or it can insert a new ligand with subsequent reductive elimination as before. Alternatively, there may be a new insertion of carbon monoxide with final hydrolysis. Third, an intermediate R—Ni—X is formed by oxidative addition. It can react in several ways It can insert a new ligand L, followed by CO to give an... 

Peptide bond formation involves activation of the carboxyl group of an amino acid residue, followed by aminolysis of the activated residue by the amino group of a second amino acid residue. Two types of activated molecules are recognized those that are not detectable but are postulated and those that are detectable and can be isolated. Postulated intermediates are necessary to account for the formation of the detectable intermediates. The postulated intermediates are consumed as fast as they are formed, either by aminolysis by an amino group or by nucleophilic attack by an oxygen nucleophile, which produces activated molecules that are also immediate precursors of the peptide. More than one activated compound may be generated by a postulated intermediate. Activated esters, acyl halides and azides, and mixed and symmetrical anhydrides are isolatable activated compounds that are generated from postulated intermediates. Peptides are produced by one of three ways ... 

Carboxylic Acid Group. Reactions of the carboxyl group include decarboxylation, reduction to alcohols, and the formation of salts, acyl halides, amides, and esters. 

Salicylic acid can be converted to salicyloyl chloride [1441-87-8] by reaction with thionyl chloride in boiling benzene. The formation of acyl halide may also extend to reaction with the phenolic hydroxyl. The reaction with phosphoms tri- and pentachlorides is not restricted to the formation of the acid chloride. Further interaction of the phosphoms halide and the phenolic hydroxyl results in the formation of the phosphoric or phosphorous esters. 

The formation of amides can be accomplished by dehydration of the ammonium salts of salicylic acid. The more common method for amines is the reaction of the ester, acyl halide, or anhydride with an amine or ammonia. Each step is fast and essentially irreversible. 

We have previously seen (0-96) that dianions of carboxylic acids can be alkylated in the a position. These ions can also be acylated on treatment with a carboxylic ester1705 to give salts of p-keto acids. As in 0-96, the carboxylic acid can be of the form RCH2COOH or RR"CHCOOH. Since p-keto acids are so easily converted to ketones (2-40), this is also a method for the preparation of ketones R COCHiR and R COCHRR", where R can be primary, secondary, or tertiary alkyl, or aryl. If the ester is ethyl formate, an a-formyl carboxylate salt (R = H) is formed, which on acidification spontaneously de-carboxylates into an aldehyde.1706 This is a method, therefore, for achieving the conversion RCH2COOH — RCH2CHO, and as such is an alternative to the reduction methods discussed in 0-83. When the carboxylic acid is of the form RR CHCOOH. better yields are obtained by acylating with acyl halides rather than esters.1707... 

Acyl cations are now well-established chemical species. They can be prepared in quantity in solution, and several have been isolated as their crystalline salts. Recent papers have described their formation from carboxylic acids and esters under strongly acidic conditions81214, but they are most conveniently available from the reactions of acyl halides with L.ewis acids21 well-defined Lewis acid-base complexes are formed, which decompose in a second stage to the acyl cations21-23, viz. 

The primary and secondary alcohol functionalities have different reactivities, as exemplified by the slower reaction rate for secondary hydroxyls in the formation of esters from acids and alcohols (8). 1,2-Propylene glycol undeigoes most of the typical alcohol reactions, such as reaction with a free acid, acyl halide, or acid anhydride to form an ester reaction with alkali metal hydroxide to form metal salts and reaction with aldehydes or ketones to form acetals and ketals (9,10). The most important commercial application of propylene glycol is in the manufacture of polyesters by reaction with a dibasic or polybasic acid. 

Less reactive than acyl halides, but still suitable for difficult couplings, are symmetric or mixed anhydrides (e.g. with pivalic or 2,6-dichlorobenzoic acid) and HOAt-derived active esters. HOBt esters smoothly acylate primary or secondary aliphatic amines, including amino acid esters or amides, without concomitant esterification of alcohols or phenols [34], HOBt esters are the most commonly used type of activated esters in automated solid-phase peptide synthesis. For reasons not yet fully understood, acylations with HOBt esters or halophenyl esters can be effectively catalyzed by HOBt and HOAt [3], and mixtures of BOP (in situ formation of HOBt esters) and HOBt are among the most efficient coupling agents for solid-phase peptide synthesis [2]. In acylations with activated amino acid derivatives, the addition of HOBt or HOAt also retards racemization [4,12,35]. 

The esterification of support-bound carboxylic acids has not been investigated as thoroughly as the esterification of support-bound alcohols. Resin-bound activated acid derivatives that are well suited to the preparation of esters include O-acylisoureas (formed from acids and carbodiimides), acyl halides [23,226-228], and mixed anhydrides (Table 13.15). A-Acylurea formation does not compete with esterifications as efficiently as it does with the formation of amides from support-bound acids. Esters can also be prepared from carboxylic acids on insoluble supports by acid-catalyzed esterification [152,229]. Alternatively, support-bound carboxylic acids can be esteri-fied by O-alkylation, either with primary or secondary aliphatic alcohols under Mitsu-nobu conditions or with reactive alkyl halides or sulfonates (Table 13.15). 

It is this equilibrium which renders difficult the explanation of the course of the reactions which take place when metallic sodium or sodium ethoxide and then alkyl or acyl halide are added to these compounds. At first it was thought that the sodio compound formed with acetoacetic ester was CH3.CO.CHNa.COOC2H5, because the reaction with alkyl and acyl halides always yielded a C-derivative, CH3.CO.CHR.COOC2H5. The first example of a different course of reaction was found in the formation of an O-derivative—/3-carhethoxyhydroxycrotonic ester from sodio-acetoacetic ester and chloroformic ester (J. pr., [2], 37, 473 B., 25,1760 A., 277, 64). This could only be explained by assigning an enol formula to the sodium salt—... 

Carboalkoxy acyl halides are made from mono esters of dibasic acids and thionyl chloride or phosphorus pentachloride. Examples are numerous. Halides with the ester group in the beta position are unstable to prolonged heating. Alkyl halide is eliminated with the formation of an anhydride. Under certain conditions a rearrangement occurs in the preparation of ester acid chlorides. The product obtained is a mixture of the expected compound and its isomer in which the ester and acid chloride groups are interchanged, viz., ROjCCHR (CI ) CO,H — RO,C(CH,) CHR COQ. The cyclic anhydride is a likely intermediate. ... 

Acyl halides such as acetyl chloride react with water to regenerate the starting acid and they react with alcohols to yield esters. The reaction is often facilitated by the presence of a tertiary amine catalyst. Although this may function purely as a base to neutralize the hydrochloric acid which is formed in the reaction, bases such as dimethylaminopyridine can also activate the carboxyl group via the formation of the intermediate shown in Scheme 3.66. 

Lateral metallation at C-2(a) of l-/ftt-butoxycarbonyl-2-methylimidazoline 709 (Scheme 173) with r f-BuLi results in the formation of a bright yellow lithiated intermediate that reacts with alkyl halides, diphenyldiselenide, and phosphoryl chlorides to give 710. In the case of reaction with esters, the conjugated ketones 711 are formed <2000T2061>. In the case of acylation with esters, conjugated enamino-ketones were the tautomer isolated. Further alkylation is also possible under similar conditions, to give 712. 

Electrogenerated nickel(O) bipyridine complexes serve as catalysts for a number of syntheses (a) formation of ketones from acyl halides and either alkyl or aryl halides [319], (b) production of, )/-unsaturated esters via coupling of a -haloesters with aryl or vinyl halides [320], (c) coupling of a-chloroesters or a-chloronitriles with carbonyl... 

Schotten-Baumann reaction The formation of an ester or amide from an acyl halide with an alcohol or an amine respectively when reacted with aqueous alkali. 

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