Synthesis electrophilic attack

In the section dealing with electrophilic attack at carbon some results on indazole homocyclic reactivity were presented nitration at position 5 (Section 4.04.2.1.4(ii)), sulfon-ation at position 7 (Section 4.04.2.1.4(iii)) and bromination at positions 5 and 7 (Section 4.04.2.1.4(v)). The orientation depends on the nature (cationic, neutral or anionic) of the indazole. Protonation, for instance, deactivates the heterocycle and directs the attack towards the fused benzene ring. A careful study of the nitration of indazoles at positions 2, 3, 5 or 7 has been published by Habraken (7UOC3084) who described the synthesis of several dinitroindazoles (5,7 5,6 3,5 3,6 3,4 3,7). The kinetics of the nitration of indazole to form the 5-nitro derivative have been determined (72JCS(P2)632). The rate profile at acidities below 90% sulfuric acid shows that the reaction involves the conjugate acid of indazole. 

Pyrazolopyrimidines, amino-acidity, 5, 309 alkylation, 5, 310 N-oxide synthesis, 5, 324 synthesis, 4, 525 5, 328 Pyrazolopyrimidines, dimethyl-synthesis, 5, 316 Pyrazolo[ 1,5-a]pyrimidines electrophilic attack, 5,311 synthesis, 5, 271, 320, 331 Pyrazolo[ 1,5-c]pyrimidines electrophilic attack, 5, 312 Pyrazolo[3,4- d]pyrimidines nucleophilic attack, 5, 313 synthesis, 5, 161, 272, 323, 334 tautomerism, 5, 309 Pyrazolo[4,3-d]pyrimidines alkylation, 5, 310 synthesis, 5, 272... 

Thiazolin-5-one, 2-alkoxy-4-arylazo-rearrangements, 5, 777 2-Thiazolin-5-one, 4-methyl-2-phenyl-protomeric equilibrium, 6, 249 4-Thiazolin-2-one, 4-aryl-reactions, 6, 286 4-Thiazolin-2-one, 3,4-dimethyl-protonation, 6, 286 4-Thiazolin-2-one, 4-methyl-reactions, 6, 286 Thiazolinones electrophilic attack, 5, 99 Thiazolin-2-ones IR spectroscopy, 6, 241 nucleophilic displacement, 5, 100 2-Thiazolin-4-ones reactions, 6, 287 2-substituted synthesis, 6, 306 synthesis, 5, 129 6, 309, 310 tautomerism, 6, 248 2-Thiazolin-5-ones IR spectroscopy, 6, 242 reactions, 6, 288 synthesis, 5, 138 tautomerism, 6, 249 4-Thiazolin-2-ones synthesis, 6, 314 4-Thiazolin-3-ylacetic acid esters... 

The synthesis of the 2-acyloxathianes 3 makes use of the fact that for stereoelectronic reasons1, electrophilic attack on conformationally locked 2-lithiated oxathianes 1 leads exclusively to equatorially substituted products 2. A subsequent oxidation step completes the synthesis. 

The CO-X bond breaking is the result of an electrophilic attack (on the carbonyl oxygen atom, hence the catalytic role of acids in these rupture reactions) or a nucleophilic one (on the carbonyl carbon atom whose positive property is due to the X electron-withdrawing property). The dangers of this type of reaction come from its speed and high exothermicity and/or instability of the products obtained in some cases. The accidents that are described below can make one believe that acid anhydrides in general and acetic anhydride in particular represent greater risks than acid chlorides since they constitute the accident factor of almost all accidents described. This is obviously related to their frequent use in synthesis rather than acid chlorides, that are rarely used. 

Complex 169 is very susceptible to electrophilic attack, as shown in Scheme 32. The protonation of 169 with PyHCl gave back 166. In this reaction, the assistance of one of the oxygens as the primary site of the protonation cannot be excluded. The alkylation with MeOTf, unlike in the case of 161 (see Scheme 29),22 occurs at the alkylidene carbon as well, forming the 2,3-dimethyl-2-butene-W derivative 167, which was obtained also by the direct synthesis given in Scheme 31. 

As a second approach to stabilizing the pz-diols, bulky substituents at appropriate positions were employed to hinder electrophilic attack. The first synthesis of pz-diols was accomplished by removal of the dispiroketal protecting group from the centrally metalated porphyrazines, M[pz(AB3)], A = di-ferf-butyl phenyl, B = dipiroketal (197) (M = Ni) 198 (M = Cu) with acetic acid to form the stable, iso-lable porphyrazines, M [pz(AB3)], A = di-ferf-butyl phenyl, B = diol (203) (M = Ni) 204 (M = Cu) (Scheme 41) (10). 

The l-arylpyrazol-5-ones (4.9), prepared by the two-step condensation of an arylhydrazine with ethyl acetoacetate, are the most commonly used coupling components for the synthesis of greenish yellow azo dyes. Coupling occurs at the 4-position of the pyrazolone ring which, as in the case of the acetoacetarylamides discussed above, is activated towards electrophilic attack by the two flanking unsaturated carbon atoms (Scheme 4.14). 

The utility of chiral oxazoline enolates in asymmetric synthesis has elegantly been demonstrated by Myers (106,120). The stereoselective aldol condensations of these enolates have been examined in a hmited number of cases (eq. [107]) (32,121). Assuming that the enolate formed has the geometry indicated in 164 (120b), the diastereoselection observed for both the aldol condensation and the previously reported alkylations favors electrophile attack on the Re face as indicated. In contrast, the unsubstituted enolate 163b exhibits significantly poorer diastereoface selection with a range of aldehydes (eq. [108]) (121). 

As the last point in Sect. IV, we discuss briefly the reactions of chiral sulfur compounds with electrophilic reagents. In contrast to nucleophilic substitution reactions, the number of known electrophilic reactions at sulfur is very small and practically limited to chiral tricoordinate sulfur compounds that on reacting with electrophilic reagents produce more stable tetracoordinate derivatives. It is generally assumed that the electrophilic attack is directed on the lone electron pair on sulfur and that the reaction is accompanied by retention of configuration. As typical examples of electrophilic reactions at tricoordinate sulfur, we mention oxidation, imination, alkylation, and halogenation. All these reactions were touched on in the section dealing with the synthesis of chiral tetracoordinate sulfur compounds. 

This approach to the isoquinoline ring, albeit a reduced isoquinoline, is mechanistically similar to the Bischler-Napieralski synthesis, in that it involves electrophilic attack of an iminium cation on to an aromatic ring. In this case, the imine intermediate is formed by reacting a phenylethylamine with an aldehyde. 

Alkynes, although not as prevalent as alkenes, have a number of important uses in synthesis. In general, alkynes are somewhat less reactive than alkenes toward many electrophiles. A major reason for this difference in reactivity is the substantially higher energy of the vinyl cation intermediate that is formed by an electrophilic attack on an alkyne. It is estimated that vinyl cations are about lOkcal/mol less stable than an alkyl cation with similar substitution. The observed differences in rate of addition in direct comparisons between alkenes and alkynes depend upon the specific electrophile and the reaction conditions.111 112 Table 4.4 summarizes some illustrative rate comparisons. A more complete discussion of the mechanistic aspects of addition to alkynes can be found in Section 6.5 of Part A. 

As a rule, the annular nitrogen atoms in 1,3,4-thiadiazoles are very reactive towards electrophiles as shown by facile alkylation reactions and quaternary salt formation. A thorough study on the quaternization of 2,5-disubstituted thiadiazoles, and its comparison with pyridazines has been published <84CHEC-i(4)545>. Electrophilic attack by benzyl chloride on 2-aminothiadiazole to give (44) in a regiospecific manner was utilized in the synthesis of an antiviral candidate <92MI 4io-oi>. 

The reaction of A2-piperideine (115) with methyl vinyl ketone to give (124) is another example of how initial electrophilic attack on the enamine double bond can be used in heterocyclic synthesis (77ACR193). This overall process is an enamine analog of the Robinson annelation and is a useful approach to the perhydroquinoline ring system. 

Although the reaction of dihydropyridinium ions produced by the electrophilic attack of dihydropyridines has promise in organic synthesis, this reaction has not been extensively exploited. Some examples of their potential are provided by the acid-catalyzed reactions with indoles (80TL2341). An application of this reaction for an efficient synthesis of ( )-deplancheine is shown in Scheme 25. An interesting feature of this reaction was the use of the alkoxy-substituted dihydropyridine as a carbonyl precursor. 

A very large group of syntheses in which the /3,y-bond is formed are those in which a side chain electrophile attacks the benzene ring. These include the Skraup and Doebner-von Miller syntheses (dealt with in Section 2.08.2.2.3(ii)), the Knorr, Conrad-Limpach and Combes syntheses of quinolines (dealt with here), the Pomerantz-Fritsch synthesis of isoquinolines, and many syntheses of phenanthridines and of acridines. 

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