Plasmepsin inhibitors: design, synthesis, inhibitory studies and crystal structure analysis

Kesavulu, M. M. ; Gowda, A. S. Prakasha ; Ramya, T. N. C. ; Surolia, N. ; Suguna, K. (2005) Plasmepsin inhibitors: design, synthesis, inhibitory studies and crystal structure analysis The Journal of Peptide Research, 66 (4). pp. 211-219. ISSN 1397-002X

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Official URL: http://onlinelibrary.wiley.com/doi/10.1111/j.1399-...

Related URL: http://dx.doi.org/10.1111/j.1399-3011.2005.00288.x

Abstract

Plasmepsin group of enzymes are key enzymes in the life cycle of malarial parasites. As inhibition of plasmepsins leads to the parasite's death, these enzymes can be utilized as potential drug targets. Although many drugs are available, it has been observed that Plasmodium falciparum, the species that causes most of the malarial infections and subsequent death, has developed resistance against most of the drugs. Based on the cleavage sites of hemglobin, the substrate for plasmepsins, we have designed two compounds (p-nitrobenzoyl-leucine-β -alanine and p-nitrobenzoyl-leucine-isonipecotic acid), synthesized them, solved their crystal structures and studied their inhibitory effect using experimental and theoretical (docking) methods. In this paper, we discuss the synthesis, crystal structures and inhibitory nature of these two compounds which have a potential to inhibit plasmepsins.

Item Type:Article
Source:Copyright of this article belongs to John Wiley and Sons.
Keywords:Malaria; Plasmepsins; Plasmodium falciparum; Plasmepsin Inhibition; Aspartic Protease
ID Code:61592
Deposited On:15 Sep 2011 12:45
Last Modified:18 May 2016 11:14

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