n -boc保护的4-氨基吡啶的高效电化学n -烷基化:生成新的生物活性化合物。

ISRN Organic Chemistry Pub Date : 2014-03-05 eCollection Date: 2014-01-01 DOI:10.1155/2014/621592
Marta Feroci, Isabella Chiarotto, Gianpiero Forte, Giovanna Simonetti, Felicia Diodata D'Auria, Louis Maes, Daniela De Vita, Luigi Scipione, Laura Friggeri, Roberto Di Santo, Silvano Tortorella
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引用次数: 3

摘要

利用电生成的乙腈阴离子可以在温和的条件下以非常高的收率烷基化n - boc -4-氨基吡啶,并且没有副产物。这种碱的高反应性是由于它的大的四乙基铵反离子,使乙腈阴离子“裸露”。得到的化合物的脱保护导致n -烷基化4-氨基吡啶的高产率。单烷基化后的4-氨基吡啶与t-BuOK和卤化烷基反应得到不对称二烷基化的4-氨基吡啶,与过量的t-BuOK和卤化烷基直接反应得到对称二烷基化的4-氨基吡啶。选取单酰基-4-氨基吡啶和二烷基-4-氨基吡啶进行抗真菌和抗原虫活性评价;二烷基化的4-氨基吡啶3ac、3ae和3ff对新型隐球菌具有抗真菌作用;而3cc、3ee和3ff对婴儿利什曼原虫和恶性疟原虫表现出抗体活性。
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Efficient electrochemical N-alkylation of N-boc-protected 4-aminopyridines: towards new biologically active compounds.

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.

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