Discovery of safe and orally effective 4-aminoquinaldine analogues as apoptotic inducers with activity against experimental visceral leishmaniasis

Palit, Palit ; Hazra, Abhijit ; Maity, Arindam ; Vijayan, R. S. K. ; Manoharan, Prabu ; Banerjee, Sukdeb ; Mondal, Nirup B. ; Ghoshal, Nanda ; Ali, Nahid (2012) Discovery of safe and orally effective 4-aminoquinaldine analogues as apoptotic inducers with activity against experimental visceral leishmaniasis Antimicrobial Agents and Chemotherapy, 56 (1). pp. 432-445. ISSN 0066-4804

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Official URL: http://aac.asm.org/content/56/1/432

Related URL: http://dx.doi.org/10.1128/AAC.00700-11

Abstract

Novel antileishmanials are urgently required to overcome emergence of drug resistance, cytotoxic effects, and difficulties in oral delivery. Toward this, we investigated a series of novel 4-aminoquinaldine derivatives, a new class of molecules, as potential antileishmanials. 4-Aminoquinaldine derivatives presented inhibitory effects on L. donovani promastigotes and amastigotes (50% inhibitory concentration range, 0.94 to 127 μM). Of these, PP-9 and PP-10 were the most effective in vitro and demonstrated strong efficacies in vivo through the intraperitoneal route. They were also found to be effective against both sodium antimony gluconate-sensitive and -resistant Leishmania donovani strains in BALB/c mice when treated orally, resulting in more than 95% protection. Investigation of their mode of action revealed that killing by PP-10 involved moderate inhibition of dihydrofolate reductase and elicitation of the apoptotic cascade. Our studies implicate that PP-10 augments reactive oxygen species generation, evidenced from decreased glutathione levels and increased lipid peroxidation. Subsequent disruption of Leishmania promastigote mitochondrial membrane potential and activation of cytosolic proteases initiated the apoptotic pathway, resulting in DNA fragmentation and parasite death. Our results demonstrate that PP-9 and PP-10 are promising lead compounds with the potential for treating visceral leishmaniasis (VL) through the oral route.

Item Type:Article
Source:Copyright of this article belongs to American Society for Microbiology.
ID Code:98444
Deposited On:23 Jul 2014 04:37
Last Modified:23 Jul 2014 04:37

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