2009
DOI: 10.1021/jm8013663
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Structures of Falcipain-2 and Falcipain-3 Bound to Small Molecule Inhibitors: Implications for Substrate Specificity

Abstract: Falcipain-2 and falcipain-3 are critical hemoglobinases of Plasmodium falciparum, the most virulent human malaria parasite. We have determined the 2.9 Å crystal structure of falcipain-2 in complex with the epoxysuccinate E64 and the 2.5 Å crystal structure of falcipain-3 in complex with the aldehyde leupeptin. These complexes represent the first crystal structures of plasmodial cysteine proteases with small molecule inhibitors and the first reported crystal structure of falcipain-3. Our structural analyses ind… Show more

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Cited by 158 publications
(178 citation statements)
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“…Compounds 8 and 9 were evaluated in vitro concerning their ability to inhibit (i) heme polymerization to hemozoin; (ii) falcipain activity; and (iii) development of blood-stage P. falciparum. In order to support observed SAR and to rationalize the activity profile of the novel compounds, we also performed molecular modeling calculations on computational models derived from X-ray structures of FP2 (PDB code: 3BPF) and FP3 (PDB code: 3BWK) co-crystalized with E64 and K11017, respectively [7,16].…”
Section: Rationalementioning
confidence: 99%
See 1 more Smart Citation
“…Compounds 8 and 9 were evaluated in vitro concerning their ability to inhibit (i) heme polymerization to hemozoin; (ii) falcipain activity; and (iii) development of blood-stage P. falciparum. In order to support observed SAR and to rationalize the activity profile of the novel compounds, we also performed molecular modeling calculations on computational models derived from X-ray structures of FP2 (PDB code: 3BPF) and FP3 (PDB code: 3BWK) co-crystalized with E64 and K11017, respectively [7,16].…”
Section: Rationalementioning
confidence: 99%
“…Amongst them, cysteine proteases, especially falcipain-2 (FP2) and falcipain-3 (FP3), are key therapeutic targets [7]. Therefore, compounds able to simultaneously impair hemozoin formation and falcipain proteolytic activity may be potent agents against blood-stage plasmodia with reduced propensity to elicit parasite resistance [11].…”
Section: Introductionmentioning
confidence: 99%
“…For this process, we used the molecular docking program GOLD (Genetic Optimization for Ligand Docking) [19,20] from the Cambridge Crystallographic Data Center. The X-ray structure of FP2 with its bound inhibitor E64 (PDB code: 3BPF) [21] was used and prepared for docking with Sybyl X 1.3 software. The original ligand, ions and solvent molecules were removed and the protein was protonated to a pH = 5.5.…”
Section: Molecular Dockingmentioning
confidence: 99%
“…For this validation, we selected the available complex of FP3 with K11017 inhibitor from the PDB databank (PDB code: 3BWK) [24]. The selection of FP3 structure (PDB code: 3BWK) to establish a docking protocol was based on the following reasons: (i) FP2 and FP3 are both cysteine proteases of Plasmodium Falciparum and contribute more or less equally to the digestion of hemoglobin in the food vacuole [21]; (ii) the superimposition of FP2 (3BPF, chainB) and FP3 (3BWK, chainA) using DaliLite server [25], matches 240 a-carbons with an RMSD of 1.1 Å , a Z score of 38.9 and a sequence of identity of 66% and (iii) FP3 X-ray structure (3BWK) give us access to the bioactive conformation of one of the peptidyl vinyl sulfones derivatives of this study (ligand 14). The X-ray FP3 structure presented a missing residue, the C-terminal GLU243, which was added with the module Biopolymer in Sybyl X 1.3 molecular modeling program.…”
Section: Molecular Dockingmentioning
confidence: 99%
“…Hydrophobic residues usually constitute the S2 pocket, but the key residue (residue 205 in papain) present at the bottom of the pocket is not conserved [32]. In this critical position of falcipain-2 and of babesipain-1, we find the polar residue Asp234 [40] and the bulky hydrophobic Phe206 residue, respectively. This difference was suggested to be responsible for a narrower S2 pocket in babesipain-1 compared to that in falcipain-2 and, hence, responsible for the P2 rank ordering observed for babesipain-1, Val [ Leu [ Phe, in contrast with that in falcipain-2 following Leu [ Phe [ Val ordering [6].…”
Section: Babesipain-1 Structurementioning
confidence: 84%