Please use this identifier to cite or link to this item: http://hdl.handle.net/10773/20646
Title: Toward the discovery of inhibitors of babesipain-1, a Babesia bigemina cysteine protease: in vitro evaluation, homology modeling and molecular docking studies
Author: Perez, Bianca
Antunes, Sandra
Goncalves, Lidia M.
Domingos, Ana
Gomes, Jose R. B.
Gomes, Paula
Teixeira, Catia
Keywords: 3-DIMENSIONAL STRUCTURES
QUALITY
PROTEINS
RECOGNITION
EXPRESSION
PREDICTION
PAPAIN
ERRORS
BOVIS
Issue Date: 2013
Publisher: SPRINGER
Abstract: Babesia bigemina is a protozoan parasite that causes babesiosis, a disease with a world-wide distribution in mammals, principally affecting cattle and man. The unveiling of the genome of B. bigemina is a project in active progress that has already revealed a number of new targets with potential interest for the design of anti-babesiosis drugs. In this context, babesipain-1 has been identified as a proteolytically active enzyme whose three-dimensional structure has not been resolved yet, but which is known to be inhibited by cysteine proteases inhibitors such as E64, ALLN, leupeptin, and vinyl sulfones. In this work, we introduce (1) a homology model of babesipain-1; (2) a comparison between babesipain-1 and falcipain-2, a cysteine protease of the malaria parasite Plasmodium falciparum; (3) in vitro data for babesipain-1 inhibition by HEDICINs and HECINs, previously reported as modest inhibitors of falcipain-2; and (4) the docked binding conformations of HEDICINs and HECINs in the model of babesipain-1. HEDICINs presented similar preferred binding conformations for both babesipain-1 and falcipain-2. However, in vitro bioassay shows that HEDICINs and HECINs are better inhibitors of babesipain-1 than of falcipain-2, which could be explained by observed differences between the active pockets of these proteins in silico. Results presented herein provide a valuable contribution to future computer-aided molecular design of new babesipain-1 inhibitors.
Peer review: yes
URI: http://hdl.handle.net/10773/20646
DOI: 10.1007/s10822-013-9682-2
ISSN: 0920-654X
Publisher Version: 10.1007/s10822-013-9682-2
Appears in Collections:CICECO - Artigos



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