Abstract
L-Amino acid esters, such as L-Leu-OMe, kill Leishmania amazonensis amastigotes by a mechanism which appears to involve ester hydrolysis by cysteine proteinases located in the parasite megasomes. We have examined the killing of isolated amastigotes by L-dipeptide esters and derived some structure-activity correlations. Toxicity of the compounds for the parasites was measured by a tetrazolium (MTT) reduction assay. The results show that active dipeptide esters contained at least 1 hydrophobic amino acid (Leu, lle, Val, Phe or Trp). The activity of homodipeptide methyl esters depended on the nature of the amino acid, as indicated by the following series: Phe-Phe-OMe> Val-Val-OMe> Leu-Leu-OMe> Trp-Trp-OMe> Ile-Ile-OMe. The nature of the amino acids in Leu-X-OMe and X-Leu-OMe was relatively unimportant when X was Phe, Trp or Val. However, when X was Ala or Gly, Leu-X-OMe was several-fold more active than X-Leu-OMe. A similar preference for the more hydrophobic residue in the amino terminal position was also found in esters containing a single phenylalanine or valine. Protection of the amino group by benzyloxycarbonyl (Z) or t-butyloxycarbonyl (BOC) substituents markedly enhanced the activity of the esters. An-mPhe-Gly-OEt, a retro-inverso analogue of Bz-Phe-Gly-OEt, was several-fold more active than the parent compound. Selected esters were assayed on infected macrophages and concentrations that induced minimal toxicity to the host cells were estimated. The ED50 s for intracellular parasites were 1–5 to 5-fold higher than those for isolated amastigotes. Therapeutic ratios (concentration for detectable toxicity for macrophages/ED90) ranged from 1–6 (for Z-Leu-Gly-OMe) to 8 (for Val-Val-OMe). © 1990, Cambridge University Press. All rights reserved.
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Ramazeilles, C., Rabinovitch, M., Juliano, L., & Chagas, J. R. (1990). The anti-leishmanial activity of dipeptide esters on leishmania amazonensis amastigotes. Parasitology, 100(2), 201–207. https://doi.org/10.1017/S0031182000061205
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