Literature DB >> 20149108

Distinct subcellular localization in the cytosol and apicoplast, unexpected dimerization and inhibition of Plasmodium falciparum glyoxalases.

Miriam Urscher1, Jude M Przyborski, Masaya Imoto, Marcel Deponte.   

Abstract

The ubiquitous glyoxalase system removes methylglyoxal as a harmful by-product of glycolysis. Because malaria parasites have drastically increased glycolytic fluxes, they could be highly susceptible to the inhibition of this detoxification pathway. Here we analysed the intracellular localization, oligomerization and inhibition of the glyoxalases from Plasmodium falciparum. Glyoxalase I (GloI) and one of the two glyoxalases II (cGloII) were located in the cytosol of the blood stages. The second glyoxalase II (tGloII) was detected in the apicoplast pointing to alternative metabolic pathways. Using a variety of methods, cGloII was found to exist in a monomer-dimer equilibrium that might have been overlooked for homologues from other organisms and that could be of physiological importance. The compounds methyl-gerfelin and curcumin, which were previously shown to inhibit mammalian GloI, also inhibited P. falciparum GloI. Inhibition patterns were predominantly competitive but were complicated because of the two different active sites of the enzyme. This effect was neglected in previous inhibition studies of monomeric glyoxalases I, with consequences for the interpretation of inhibition constants. In summary, the present work reveals novel general glyoxalase properties that future research can build on and provides a significant advance in characterizing the glyoxalase system from P. falciparum.

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Year:  2010        PMID: 20149108     DOI: 10.1111/j.1365-2958.2010.07082.x

Source DB:  PubMed          Journal:  Mol Microbiol        ISSN: 0950-382X            Impact factor:   3.501


  10 in total

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4.  The cytosolic glyoxalases of Plasmodium falciparum are dispensable during asexual blood-stage development.

Authors:  Cletus A Wezena; Romy Alisch; Alexandra Golzmann; Linda Liedgens; Verena Staudacher; Gabriele Pradel; Marcel Deponte
Journal:  Microb Cell       Date:  2017-11-20

Review 5.  Characteristic Variations and Similarities in Biochemical, Molecular, and Functional Properties of Glyoxalases across Prokaryotes and Eukaryotes.

Authors:  Charanpreet Kaur; Shweta Sharma; Mohammad Rokebul Hasan; Ashwani Pareek; Sneh L Singla-Pareek; Sudhir K Sopory
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6.  Prokaryotic ancestry and gene fusion of a dual localized peroxiredoxin in malaria parasites.

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7.  Roles of Ferredoxin-Dependent Proteins in the Apicoplast of Plasmodium falciparum Parasites.

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8.  Cellular effects of curcumin on Plasmodium falciparum include disruption of microtubules.

Authors:  Rimi Chakrabarti; Parkash S Rawat; Brian M Cooke; Ross L Coppel; Swati Patankar
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9.  Episodes of horizontal gene-transfer and gene-fusion led to co-existence of different metal-ion specific glyoxalase I.

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10.  Hemolytic and antimalarial effects of tight-binding glyoxalase 1 inhibitors on the host-parasite unit of erythrocytes infected with Plasmodium falciparum.

Authors:  Cletus A Wezena; Miriam Urscher; Robert Vince; Swati S More; Marcel Deponte
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  10 in total

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