Computer assisted design of potentially active anti-trypanosomal compounds

Paulino, M.; Iribarne, F.; Hansz, M.; Vega, M.; Seoane, G.; Cerecetto, Hugo; Di Maio, R.; Caracelli, I.; Zukerman-Schpector, J.; Olea Azar, Claudio; Stoppani, A. O. M.; Berriman, M.; Fairlamb, A. H.; Tapia, O.

Artículo de revista

Fecha

2002-04-26

Registro en:

JOURNAL OF MOLECULAR STRUCTURE-THEOCHEM 584 Pages: 95-105

0166-1280

https://repositorio.uchile.cl/handle/2250/120965

Autor

Paulino, M.

Iribarne, F.

Hansz, M.

Vega, M.

Seoane, G.

Cerecetto, Hugo

Di Maio, R.

Caracelli, I.

Zukerman-Schpector, J.

Olea Azar, Claudio

Stoppani, A. O. M.

Berriman, M.

Fairlamb, A. H.

Tapia, O.

Institución

Universidad de Chile

Resumen

A computer assisted molecular modeling was used to design molecules having a shape complementary to the active site of glutathione reductase (GR) and trypanothione reductase (TR). The designed 5-nitro compound derivatives. were obtained from structural knowledge gleaned on glutathione (GSSG), trypanothione (T[S](2)) and GSP disulfide (glutathionylspermidine disulfide). These molecules form complexes with the enzymes GR and TR. The theoretical lead compound was: N1-[1-(5-nitro-2-furyl)methylidene]-N4-(4-[3-(2,2,2-trifluoroacetyl)hexahydro-1-1-pyrimidynil]butyl) semicarbazide (NPIPCO). A multidisciplinary team developed around the efforts to synthesize this lead. In this work we report on eight compounds that were synthesized in the pathway to NPIPCO: 4-(2-methoxyethyl)-1-, 4-butyl-1-, 4-hexyl-1- and 2-methoxphenyl-1-(5-nitrofurfurilidene) semicarbazides and the corresponding 5-nitrothiophenes. These substances are expected to act as pro-transition state analogues. Enzymologic studies proved that many of these compounds are inhibitors of TR. Furthermore, they showed inhibitory activity on Tripanosoma cruzi growth in vitro.

Materias

Anti-trypanosomal compounds

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