Literature DB >> 24558036

Structural basis for inactivation of Giardia lamblia carbamate kinase by disulfiram.

Andrey Galkin1, Liudmila Kulakova, Kap Lim, Catherine Z Chen, Wei Zheng, Illarion V Turko, Osnat Herzberg.   

Abstract

Carbamate kinase from Giardia lamblia is an essential enzyme for the survival of the organism. The enzyme catalyzes the final step in the arginine dihydrolase pathway converting ADP and carbamoyl phosphate to ATP and carbamate. We previously reported that disulfiram, a drug used to treat chronic alcoholism, inhibits G. lamblia CK and kills G. lamblia trophozoites in vitro at submicromolar IC50 values. Here, we examine the structural basis for G. lamblia CK inhibition of disulfiram and its analog, thiram, their activities against both metronidazole-susceptible and metronidazole-resistant G. lamblia isolates, and their efficacy in a mouse model of giardiasis. The crystal structure of G. lamblia CK soaked with disulfiram revealed that the compound thiocarbamoylated Cys-242, a residue located at the edge of the active site. The modified Cys-242 prevents a conformational transition of a loop adjacent to the ADP/ATP binding site, which is required for the stacking of Tyr-245 side chain against the adenine moiety, an interaction seen in the structure of G. lamblia CK in complex with AMP-PNP. Mass spectrometry coupled with trypsin digestion confirmed the selective covalent thiocarbamoylation of Cys-242 in solution. The Giardia viability studies in the metronidazole-resistant strain and the G. lamblia CK irreversible inactivation mechanism show that the thiuram compounds can circumvent the resistance mechanism that renders metronidazole ineffectiveness in drug resistance cases of giardiasis. Together, the studies suggest that G. lamblia CK is an attractive drug target for development of novel antigiardial therapies and that disulfiram, an FDA-approved drug, is a promising candidate for drug repurposing.

Entities:  

Keywords:  Animal Models; Carbamate Kinase; Crystallography; Disulfiram; Drug Discovery; Enzyme Inhibitors; Enzyme Structure; Giardia lamblia; Parasite

Mesh:

Substances:

Year:  2014        PMID: 24558036      PMCID: PMC4036171          DOI: 10.1074/jbc.M114.553123

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  30 in total

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Journal:  Acta Crystallogr Sect F Struct Biol Cryst Commun       Date:  2010-03-26

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2.  Discovery of novel antigiardiasis drug candidates.

Authors:  Liudmila Kulakova; Andrey Galkin; Catherine Z Chen; Noel Southall; Juan J Marugan; Wei Zheng; Osnat Herzberg
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7.  Hyperthermophilic Carbamate Kinase Stability and Anabolic In Vitro Activity at Alkaline pH.

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Review 9.  Parasitic diarrheal disease: drug development and targets.

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10.  Disulfiram as a novel inactivator of Giardia lamblia triosephosphate isomerase with antigiardial potential.

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Journal:  Int J Parasitol Drugs Drug Resist       Date:  2017-12-01       Impact factor: 4.077

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