Novel Imidazole‐based Hydrazonoyl Cyanides and Amidrazones Containing N(N,O)‐Heterocycles: Selective Synthesis, Reaction Mechanisms and Preliminary Anticancer Evaluation

Author:

Fernandes Soraia P. S.12,Gonçalves Jorge M.1ORCID,Silva Bruna F.1ORCID,Pereira Eva Q.1,Coutinho Paulo J. G.34ORCID,Pereira‐Wilson Cristina25ORCID,Dias Alice M.1ORCID

Affiliation:

1. CQUM – Chemistry Centre, Department of Chemistry University of Minho 4710-057 Braga Portugal

2. CEB - Centre of Biological Engineering, Department of Biology University of Minho 4710-057 Braga Portugal

3. CF-UM-UP – Physics Centre of Minho and Porto Universities University of Minho 4710-057 Braga Portugal

4. LaPMET – Laboratory of Physics for Materials and Emergent Technologies University of Minho 4710-057 Braga Portugal

5. LABBELS – Associate Laboratory Guimarães Braga Portugal

Abstract

AbstractTwo series of novel hybrid heterocyclic compounds that combine the imidazole ring with bioactive piperidine, morpholine or piperazine heterosystems, through a hydrazone unit, were easily obtained by two competitive pathways. Starting from 5‐amino‐4‐cyanoformimidoyl imidazoles and 1‐aminopiperidine, 4‐aminomorpholine or 1‐amino‐4‐methylpiperazine under mild acidic media led to the selective synthesis of 5‐aminoimidazole 4‐carboxamidrazones, whereas the corresponding 4‐hydrazonoyl cyanide derivatives were obtained under stronger acidic conditions. These highly functionalized imidazoles provide convenient synthetic precursors to a vast array of heterocycles with potential pharmaceutical applications. The reaction mechanisms were elucidated on the basis of experimental assays and in silico calculations. The compounds were screened against colorectal cancer HCT116‐p53 wt cell line, and significant IC50 values of 3.69 μM and 4.83 μM were obtained.

Publisher

Wiley

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