Literature DB >> 15927894

Blocking effect of a biotinylated protease inhibitor on the egress of Plasmodium falciparum merozoites from infected red blood cells.

Christoph Gelhaus1, Radim Vicik, Tanja Schirmeister, Matthias Leippe.   

Abstract

The malaria parasite Plasmodium falciparum invades human red blood cells. Before infecting new erythrocytes, the merozoites have to exit their host cell to get into the blood plasma. Knowledge about the mechanism of egress is scarce, but it is thought that proteases are basically involved in this step. We have introduced a biotinylated dibenzyl aziridine-2,3-dicarboxylate (bADA) as an irreversible cysteine protease inhibitor to study the mechanism of merozoite release and to identify the proteases involved. The compound acts on parasite proteins in the digestive vacuole and in the host cell cytosol, as judged by fluorescence microscopy. The inhibitor blocks rupture of the host cell membrane, leading to clustered merozoite structures, as evidenced by immunoelectron microscopy. Interestingly, bADA did not prevent rupture of the parasitophorous vacuole membrane (PVM) that surrounds the parasite during the period of intraerythrocytic maturation. The compound appears to be a valuable template for the development of inhibitors specific for individual plasmodial proteases, which would be useful tools to dissect the molecular mechanisms underlying the process of merozoite release and consequently to develop potent antimalarial drugs.

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Year:  2005        PMID: 15927894     DOI: 10.1515/BC.2005.059

Source DB:  PubMed          Journal:  Biol Chem        ISSN: 1431-6730            Impact factor:   3.915


  8 in total

1.  New stages in the program of malaria parasite egress imaged in normal and sickle erythrocytes.

Authors:  Svetlana Glushakova; Glen Humphrey; Evgenia Leikina; Amanda Balaban; Jeffrey Miller; Joshua Zimmerberg
Journal:  Curr Biol       Date:  2010-05-27       Impact factor: 10.834

2.  Aziridine-2,3-dicarboxylate-based cysteine cathepsin inhibitors induce cell death in Leishmania major associated with accumulation of debris in autophagy-related lysosome-like vacuoles.

Authors:  Uta Schurigt; Caroline Schad; Christin Glowa; Ulrike Baum; Katja Thomale; Johannes K Schnitzer; Martina Schultheis; Norbert Schaschke; Tanja Schirmeister; Heidrun Moll
Journal:  Antimicrob Agents Chemother       Date:  2010-09-20       Impact factor: 5.191

3.  Irreversible effect of cysteine protease inhibitors on the release of malaria parasites from infected erythrocytes.

Authors:  Svetlana Glushakova; Julia Mazar; Martin F Hohmann-Marriott; Erinn Hama; Joshua Zimmerberg
Journal:  Cell Microbiol       Date:  2008-10-22       Impact factor: 3.715

4.  A multifunctional serine protease primes the malaria parasite for red blood cell invasion.

Authors:  Konstantinos Koussis; Chrislaine Withers-Martinez; Sharon Yeoh; Matthew Child; Fiona Hackett; Ellen Knuepfer; Luiz Juliano; Ute Woehlbier; Hermann Bujard; Michael J Blackman
Journal:  EMBO J       Date:  2009-02-12       Impact factor: 11.598

5.  Protease inhibitors from marine actinobacteria as a potential source for antimalarial compound.

Authors:  L Karthik; Gaurav Kumar; Tarun Keswani; Arindam Bhattacharyya; S Sarath Chandar; K V Bhaskara Rao
Journal:  PLoS One       Date:  2014-03-11       Impact factor: 3.240

Review 6.  Protease inhibitors and their peptidomimetic derivatives as potential drugs.

Authors:  Georgie Fear; Slavko Komarnytsky; Ilya Raskin
Journal:  Pharmacol Ther       Date:  2006-09-22       Impact factor: 12.310

Review 7.  Malarial proteases and host cell egress: an 'emerging' cascade.

Authors:  Michael J Blackman
Journal:  Cell Microbiol       Date:  2008-06-28       Impact factor: 3.715

8.  The role of serine-type serine repeat antigen in Plasmodium yoelii blood stage development.

Authors:  Ximei Huang; Kingsley Liew; Onguma Natalang; Anthony Siau; Neng Zhang; Peter Rainer Preiser
Journal:  PLoS One       Date:  2013-04-25       Impact factor: 3.240

  8 in total

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