In our search for new safe antiparasitic agents, an enzymatic
pathway
was applied to synthesize a series of N-pyridinylmethyl
amides derived from structurally different carboxylic acids. Thirty
derivatives, including 11 new compounds, were prepared through lipase-catalyzed
acylation in excellent yields. In order to optimize the synthetic
methodology, the impact of different reaction parameters was analyzed.
Some compounds were evaluated as antiproliferative agents against Trypanosoma cruzi, the parasite responsible for American
trypanosomiasis (Chagas’ disease). Some of them showed significant
activity as parasite proliferation inhibitors. Amides derived from
2-aminopicoline and stearic and elaidic acids were as potent as nifurtimox
against the amastigote form of T. cruzi, the clinically
relevant form of the parasite. Even more, a powerful synergism between
nifurtimox and N-(pyridin-2-ylmethyl)stereamide was
observed, almost completely inhibiting the proliferation of the parasite.
Besides, the obtained compounds showed no toxicity in Vero cells,
making them excellent potential candidates as lead drugs.
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