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  4. New antiparasitic flexible triaryl diamidines, their prodrugs and aza analogues: synthesis,; in vitro; and; in vivo; biological evaluation, and molecular modelling studies
 
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New antiparasitic flexible triaryl diamidines, their prodrugs and aza analogues: synthesis,; in vitro; and; in vivo; biological evaluation, and molecular modelling studies

Date Issued
2021-01-01
Author(s)
Arafa, R. K.
Ismail, M. A.
Wenzler, T.  
Brun, R.  
Paul, A.
Wilson, W. D.
Alakhdar, A. A.
Boykin, D. W.
DOI
10.1016/j.ejmech.2021.113625
Abstract
Dicationic diamidines have been well established as potent antiparasitic agents with proven activity against tropical diseases like trypanosomiasis and malaria. This work presents the synthesis of new mono and diflexible triaryl amidines (6a-c, 13a,b and 17), their aza analogues (23 and 27) and respective methoxyamidine prodrugs (5, 7, 12a,b, 22 and 26). All diamidines were assessed in vitro against Trypanosoma brucei rhodesiense (T. b. r.) and Plasmodium falciparum (P. f.) where they displayed potent to moderate activities at the nanomolar level with IC(50)s = 11-378 nM for T. b. r. and 4-323 nM against P. f.. In vivo efficacy testing against T. b. r. STIB900 has shown the monoflexible diamidine 6c as the most potent derivative in this study eliciting 4/4 cures of infected mice for a treatment period of >60 days upon a 4 × 5 mg/kg dose i. p. treatment. Moreover, thermal melting analysis measurement ΔT(m) for this series of diamidines/poly (dA-dT) complexes fell between 0.5 and 19 °C with 6c showing the highest binding to the DNA minor groove. Finally, a 50 ns molecular dynamics study of an AT-rich DNA dodecamer with compound 6c revealed a strong binding complex supported by vdW and electrostatic interactions.
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