Acetoacetyl

When both building block units are m place on the acyl carrier protein carbon-carbon bond formation occurs between the a carbon atom of the malonyl group and the carbonyl carbon of the acetyl group This is shown m step 1 of Figure 26 3 Carbon-carbon bond formation is accompanied by decarboxylation and produces a four carbon acetoacetyl (3 oxobutanoyl) group bound to acyl earner protein... 

The acetoacetyl group is then transformed to a butanoyl group by the reaction sequence illustrated m steps 2 to 4... 

Step 2 The ketone carbonyl of the acetoacetyl group is reduced to an alcohol function This reduction requires NADPH as a coenzyme (NADPH is the phosphate ester of NADH and reacts similarly to it)... 

S Acetoacetyl Reduced Hydronium iS 3 Hydroxybutanoyl Oxidized Water... 

The introduction to Section 26 8 pointed out that mevalonic acid is the biosynthetic pre cursor of isopentenyl pyrophosphate The early steps m the biosynthesis of mevalonate from three molecules of acetic acid are analogous to those m fatty acid biosynthesis (Sec tion 26 3) except that they do not involve acyl earner protein Thus the reaction of acetyl coenzyme A with malonyl coenzyme A yields a molecule of acetoacetyl coenzyme A... 

Carbon-carbon bond formation then occurs between the ketone carbonyl of acetoacetyl coenzyme A and the a carbon of a molecule of acetyl coenzyme A... 

In the presence of strong acid, such as boron trifluoride [7637-07-2] appropriately substituted acyl chlorides (7, R = CCl ) add to ketene to form the corresponding acetoacetyl chlorides, which can further react with alcohols to form the corresponding acetoacetates. 

Acetoiicetyliition Reactions. The best known and commercially most important reaction of diketene is the aceto acetylation of nucleophiles to give derivatives of acetoacetic acid (Fig. 2) (1,5,6). A wide variety of substances with acidic hydrogens can be acetoacetylated. This includes alcohols, amines, phenols, thiols, carboxyHc acids, amides, ureas, thioureas, urethanes, and sulfonamides. Where more than one functional group is present, ring closure often follows aceto acetylation, giving access to a variety of heterocycHc compounds. These reactions often require catalysts in the form of tertiary amines, acids, and mercury salts. Acetoacetate esters and acetoacetamides are the most important industrial intermediates prepared from diketene. 

Diketene is used to C-acetoacetylate aromatic compounds in the presence of aluminum trichloride [7446-70-0]. Benzene [71-43-2] and diketene react to produce acetoacet5lben2ene [93-91-4]. Pyrrole [109-97-7] and diketene react to produce 2-acetoacet5lpyrrole [22441-25-4]. The C-acetoacetyl derivatives of active methylene compounds such as cyanoacetates, malonodinitrile [109-77-3] and Meldmm s acid [2033-24-1], and olefins can be prepared using diketene. 

A shippable but somewhat less reactive form of diketene is its acetone adduct, 2,2,6-trimethyl-4JT-l,3-dioxin-4-one (15) (103,104). Thermolysis of this safer to handle compound provides acetylketene, a reactive intermediate that can be used for acetoacetylation and cycloaddition reactions. The diketene—acetone adduct as weH as / fZ-butylaceto acetate [1694-31 -1] (also used for aceto acetylations by the trans aceto acetylation reaction) (130), are offered commercially. 

As the most reactive and economical source of the acetoacetyl moiety, diketene is used as a valuable synthetic intermediate in the manufacture of acetoacetic acid derivatives and heterocycHc compounds which are used as intermediates in the manufacture of dyestuffs, agrochemicals, pharmaceuticals, and polymers. 

Hydroxyalkyl acrylates and polyols are acetoacetylated with diketene to give comonomers used in adhesives, polymers, and coatings, especially the new low solvent coatings, and for emulsion polymeri2ation. The most widely used compound is 2-acetoacetoxyethyl methacrylate (A ARM A) (152). 

A range of acetoacetylated lesins has been intioduced (68,69). The acetoacetoxy functionahty can be cioss-linked with melamine—formaldehyde resins, isocyanates, polyacrylates, and polyamines. There is particular interest for possible corrosion protection on steel because the acetoacetoxy group can form coordination compounds (qv) with iron, perhaps enhancing the adhesion to steel surfaces (see Chelating agents). 

Ketone body synthesis occurs only in the mitochondrial matrix. The reactions responsible for the formation of ketone bodies are shown in Figure 24.28. The first reaction—the condensation of two molecules of acetyl-CoA to form acetoacetyl-CoA—is catalyzed by thiolase, which is also known as acetoacetyl-CoA thiolase or acetyl-CoA acetyltransferase. This is the same enzyme that carries out the thiolase reaction in /3-oxidation, but here it runs in reverse. The second reaction adds another molecule of acetyl-CoA to give (i-hydroxy-(i-methyl-glutaryl-CoA, commonly abbreviated HMG-CoA. These two mitochondrial matrix reactions are analogous to the first two steps in cholesterol biosynthesis, a cytosolic process, as we shall see in Chapter 25. HMG-CoA is converted to acetoacetate and acetyl-CoA by the action of HMG-CoA lyase in a mixed aldol-Claisen ester cleavage reaction. This reaction is mechanistically similar to the reverse of the citrate synthase reaction in the TCA cycle. A membrane-bound enzyme, /3-hydroxybutyrate dehydrogenase, then can reduce acetoacetate to /3-hydroxybutyrate. 

It is also worth noting that the carbon of the carboxyl group that was added to drive this reaction is the one removed by the condensing enzyme. Thus, all the carbons of acetoacetyl-ACP (and of the fatty acids to be made) are derived from acetate units of acetyl-CoA. 

A/-2-Methyl-2-(o-phenylazophenoxy)propionyl, 562 A/-4-Chlorobutyryl, 563 A/-Acetoacetyl, 563 A/-3-(p-Hydroxyphenyl)propionyl, 563 (A/ -Dithiobenzyloxycarbonylamino)acetyl, 563 A/-Acetylmethionine Derivative. 563 4,5-Diphenyl-3-oxazolin-2-one, 564... 

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