Selective heteroarylation

Thienyl(phenyl)iodonium salts and other heteroaryl(phenyl)iodonium salts can be used as the selective heteroaryl transfer agents in reactions with phenol ethers. These heteroarylations occur at room temperature in the hexafluoroisopropanol solution in the presence of trimethylsilyl triflate via a SET mechanism [876]. 

The observed enhanced reactivity of aryl chlorides in mechanochanical conditions was employed in solid-state Suzuki cross-coupling of selected heteroaryl chlorides 39 and 40 with phenylboronic acid (Scheme 2.13), affording high yields of cross-coupling products 41 and 42. 

The reaction conditions (neutral, acidic or basic) do have an affect on the regioselectivity of the reaction. Acidic reaction conditions have also been shown to preferentially provide one regioisomer over basic conditions for reactions of aryl hydrazines. Extensive studies with 2-perfluoroacylcycloalkanones and mono-substituted hydrazines were studied to determine the selectivity of various alkyl-, aryl-, and heteroaryl-substituted hydrazines. Reactions of the aryl hydrazine 21 with the trifluoromethyl-substituted cycloalkanone 22 under neutral conditions (methanol, reflux) gave a mixture of isomers 23 and 24, whereas the reaction of the pyridyl hydrazine 25 was shown to give exclusively 26. 

Hence, microwave irradiation in DMA for 12 min at 120 °C or 30 min at 140 °C, depending on the substrate, resulted in 20 or 21 in 90-96% yields, compared to yields around 50% and a 24 h reaction time for conventional heating. As can be seen in Eq. 2 in Fig. 5, two possibilities exist to connect the heteroaryl bromide part with the five-membered heterocycle (indicated by a and fi. Table 2) that results in a six-membered 2-pyridone ring. Still, a very high selectivity was obtained yielding the 2-pyridones 21, in which the new bond had been introduced at Ca. It should be noted that the obtained structures 20 and 21 represent heterocyclic derivatives of 2-quinolones rather than true 2-quinolones. 

Chang et al. reported a mild tandem intramolecular hydroamination of yne amines to form an endo-adduct intermediate, which reacts with electron-deficient azides to produce cyclic amidines <06JA12366>. Selected examples of an interesting synthetic route to tropene derivatives 165 via a dual hydroamination strategy is shown below. This one-step reaction makes use of a palladium catalyst and takes place by sequential intermolecular hydroamination of cycloheptatriene with aryl, heteroaryl, and primary alkyl amines to generate intermediate 166, followed by transannular intramolecular hydroamination <06JA8134>. 

In a slightly less convenient procedure, but one which has general versatility, carbonylation of aryl (or vinyl) palladium compounds produces aryl, heteroaryl, and vinyl carboxylic acids. As with the other procedures, immediate upon its formation, the carboxylate anion migrates to the aqueous phase. Consequently, haloaromatic acids can be obtained from dihaloarenes, without further reaction of the second halogen atom, e.g. 1,4-dibromobenzene has been carbonylated (90% conversion) to yield 4-bromobenzoic acid with a selectivity for the monocarbonylation product of 95%. Additionally, the process is economically attractive, as the organic phase containing the catalyst can be cycled with virtually no loss of activity and ca. 4000 moles of acid can be produced for each mole of the palladium complex used [4],... 

The resolution was then based on the enzymatic propanolysis of this derivative in dioxane as solvent. Lip Novozyme 435 selectively cleaves the L-form of the oxazolone producing an L-enriched (81-87% ee) 2-acetamido-3-(heteroaryl)propionic acid propyl ester, the dynamic aspect of the process being based on the continual racemization of the residual oxazolone. The propyl group was then removed with alkali and a second selective enzymatic step to remove the acetyl protecting group with Fluka Acylase 1 produced the L-amino acid at better than 99% ee (Scheme 13). 

Delavirdine mesylate is a member of the /7w(heteroaryl)piperazine (BHAP) class of nonnucleoside HIV-1 reverse transcriptase inhibitors (Adams et al., 1998 Romero et al., 1993 Romero, 1994). This class of compounds was discovered by Upjohn scientists from a computer-directed dissimilarity analysis of the Pharmacia Upjohn chemical library to select compounds for screening against HIV-1 RT. The result of the in vitro assay (Deibel et al., 1990) is an IC50 of 0.260 p,M, which is comparable to AZT. In accordance with the previous NNRTIs, delavirdine is a noncompetitive inhibitor of reverse transcriptase, and has a synergistic effect with nucleoside transcriptase and protease inhibitors (Chong et al., 1994). 

By using the hypersensitive molecular mechanistic probe 2-(2-methoxy-3-phenylcy-clopropyl)-5-methylhexa-2,4-diene in the 2 + 2-photocycloaddition of [60]fullerene, it was shown that the reaction proceeds via a biradical and not a dipolar intermediate.6 Zirconium-induced cyclodimerization of heteroaryl-substituted alkynes produces tetrasubstituted cyclobutenes with high regio- and stereo-selectivity.7 The ruthenium-... 

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