Molecular docking, synthesis and in vitro antimalarial evaluation of certain novel curcumin analogues

Autores

  • Chandrajit Dohutia Assam Down Town University; Department of Pharmaceutical Sciences
  • Dipak Chetia Dibrugarh University
  • Kabita Gogoi Indian Council of Medical Research; Regional Medical Research Centre NE
  • Dibya Ranjan Bhattacharyya Indian Council of Medical Research; Regional Medical Research Centre NE
  • Kishore Sarma Indian Council of Medical Research; Regional Medical Research Centre NE

DOI:

https://doi.org/10.1590/s2175-97902017000400084

Palavras-chave:

Curcumin/synthesis, Curcumin/antimalarial activity, Curcumin/Knoevenagel condensates, PfATP6, Malaria, Docking, In vitro, ADME/Tox.

Resumo

The receptor protein PfATP6 has been identified as the common target of artemisinin and curcumin. The work was initiated to assess the antimalarial activity of six curcumin derivatives based on their binding affinities and correlating the in silico docking outcome with in vitro antimalarial screening results. A ligand library of thirty two Knoevenagel condensates of curcumin were designed and docked against PfATP6 protein and six compounds with the best binding scores were synthesized and screened for their antimalarial activity against the sensitive 3D7 strain of Plasmodium falciparum. ADME/Tox, pharmacokinetic and pharmacodynamic profiles of the designed compounds were analyzed and reported. 4-FB was found to have similar binding energy to the standard artemisinin (-6.75 and -6.73 respectively) while 4-MB, 3-HB, 2-HB, B, 4-NB displayed better binding energy than curcumin (-5.95, -5.89, -5.68, -5.35, -5.29 and -5.25 respectively). At a dose of 50 µg/mL all the six compounds showed 100% schizont inhibition while at 5µg/ml, five showed more than 75% inhibition and better results than curcumin. 4-FB showed the best activity with 97.8% schizonticidal activity. The in vitro results superimpose the results obtained from the in silico study thereby encouraging development of promising curcumin leads in the battle against malaria.

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Publicado

2017-01-01

Edição

v. 53 n. 4 (2017)

Seção

Artigos

Licença

All content of the journal, except where identified, is licensed under a Creative Commons attribution-type BY.

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Como Citar

Molecular docking, synthesis and in vitro antimalarial evaluation of certain novel curcumin analogues. (2017). Brazilian Journal of Pharmaceutical Sciences, 53(4), e00084. https://doi.org/10.1590/s2175-97902017000400084