The use of electrogenerated acetonitrile anion allows the alkylation of N-Boc-4-aminopyridine in very high yields, under mild conditions and without by-products. The high reactivity of this base is due to its large tetraethylammonium counterion, which leaves the acetonitrile anion "naked." The deprotection of the obtained compounds led to high yields in N-alkylated 4-aminopyridines. Nonsymmetrically dialkylated 4-aminopyridines were obtained by subsequent reaction of monoalkylated ones with t-BuOK and alkyl halides, while symmetrically dialkylated 4-aminopyridines were obtained by direct reaction of 4-aminopyridine with an excess of t-BuOK and alkyl halides. Some mono- and dialkyl-4-aminopyridines were selected to evaluate antifungal and antiprotozoal activity; the dialkylated 4-aminopyridines 3ac, 3ae and 3ff showed antifungal towards Cryptococcus neoformans; whereas 3cc, 3ee and 3ff showed antiprotozoal activity towards Leishmania infantum and Plasmodium falciparum.
Efficient electrochemical N-alkylation of N-boc-protected 4-aminopyridines: towards new biologically active compounds / Feroci, Marta; Chiarotto, Isabella; Forte, Gianpiero; Simonetti, Giovanna; D'Auria, Felicia Diodata; Diodata, ; Maes, Louis; Scipione, Luigi; Friggeri, Laura; DI SANTO, Roberto; DE VITA, Daniela; Tortorella, Silvano. - In: ISRN ORGANIC CHEMISTRY. - ISSN 2090-5149. - STAMPA. - 2014:(2014), pp. 1-10. [10.1155/2014/621592]
Efficient electrochemical N-alkylation of N-boc-protected 4-aminopyridines: towards new biologically active compounds.
FEROCI, Marta;CHIAROTTO, Isabella;FORTE, GIANPIERO;SIMONETTI, Giovanna;D'AURIA, Felicia Diodata;SCIPIONE, Luigi;FRIGGERI, LAURA;DI SANTO, Roberto;DE VITA, DANIELA;TORTORELLA, Silvano
2014
Abstract
The use of electrogenerated acetonitrile anion allows the alkylation of N-Boc-4-aminopyridine in very high yields, under mild conditions and without by-products. The high reactivity of this base is due to its large tetraethylammonium counterion, which leaves the acetonitrile anion "naked." The deprotection of the obtained compounds led to high yields in N-alkylated 4-aminopyridines. Nonsymmetrically dialkylated 4-aminopyridines were obtained by subsequent reaction of monoalkylated ones with t-BuOK and alkyl halides, while symmetrically dialkylated 4-aminopyridines were obtained by direct reaction of 4-aminopyridine with an excess of t-BuOK and alkyl halides. Some mono- and dialkyl-4-aminopyridines were selected to evaluate antifungal and antiprotozoal activity; the dialkylated 4-aminopyridines 3ac, 3ae and 3ff showed antifungal towards Cryptococcus neoformans; whereas 3cc, 3ee and 3ff showed antiprotozoal activity towards Leishmania infantum and Plasmodium falciparum.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
