Literature DB >> 14530966

Targeting enzymes involved in spermidine metabolism of parasitic protozoa--a possible new strategy for anti-parasitic treatment.

A Kaiser1, A Gottwald, W Maier, H M Seitz.   

Abstract

Sequencing data obtained from the Plasmodium, Anopheles gambiae and human genome projects provide a new basis for drug and vaccine development. One of the most characteristic features in the process of drug development against parasitic protozoa is target identification in a biological pathway. The next step must be a structure-based rational drug design if the target is not only present in the parasite. In mouse models of malaria, such drugs should be tested for efficacy of the new therapies. Here, we present data that pinpoint the existence of two enzymes of the polyamine pathway involved in spermidine metabolism in P. falciparum, i.e. deoxyhypusine synthase (DHS; EC 1.1.1.249) and homospermidine synthase (HSS; EC 2.5.1.45). Recent data obtained from the malaria genome databases showed that at least a putative gene encoding DHS is present in the parasite. Sequencing data from the P. falciparum genome project prove that the eukaryotic initiation factor eIF5A (the substrate for DHS) exists in P. falciparum. Here, we present the amino acid sequence of eIF5A from P. vivax, which causes tertiary malaria. EIF5A from P. vivax shows 82% nucleic acid and 97% amino acid identity to its homologue from P. falciparum. GC/MS data and inhibitor studies with agmatine prove that the triamine homospermidine occurs in the parasite. These data suggest a separate locus encoding HSS in P. falciparum. The hss gene recruits from the dhs gene in eukaryotes. Here, we present genomic DNA fragments obtained by amplification with primers of a conserved region (amino acid positions 550-1,043) between the putative P. falciparum DHS gene ( dhs) and the HSS gene ( hss) from the plant Senecio vulgaris (Asteraceae). The amplification product from different P. falciparum strains reveals differences in sequence identity, compared with the putative dhs gene from P. falciparum strain 3D7. Expression of the full-length clone and determination of HSS-specific activity will finally prove whether a separate region encoding HSS exists.

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Year:  2003        PMID: 14530966     DOI: 10.1007/s00436-003-0970-y

Source DB:  PubMed          Journal:  Parasitol Res        ISSN: 0932-0113            Impact factor:   2.289


  47 in total

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3.  Homospermidine synthase, the first pathway-specific enzyme of pyrrolizidine alkaloid biosynthesis, evolved from deoxyhypusine synthase.

Authors:  D Ober; T Hartmann
Journal:  Proc Natl Acad Sci U S A       Date:  1999-12-21       Impact factor: 11.205

4.  Chlorella virus PBCV-1 encodes a functional homospermidine synthase.

Authors:  A Kaiser; M Vollmert; D Tholl; M V Graves; J R Gurnon; W Xing; A D Lisec; K W Nickerson; J L Van Etten
Journal:  Virology       Date:  1999-10-10       Impact factor: 3.616

5.  The crystal structure of spermidine synthase with a multisubstrate adduct inhibitor.

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Authors:  D Bevec; J Hauber
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Authors:  D Chamot; C Kuhlemeier
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Authors:  Paul M J Clement; Hartmut M Hanauske-Abel; Edith C Wolff; Hynda K Kleinman; Myung Hee Park
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3.  Piperidones with activity against Plasmodium falciparum.

Authors:  Michael Saeftel; Ramadan Salem Sarite; Tujo Njuguna; Ulrike Holzgrabe; Daniela Ulmer; Achim Hoerauf; Annette Kaiser
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4.  The guanylhydrazone CNI-1493: an inhibitor with dual activity against malaria-inhibition of host cell pro-inflammatory cytokine release and parasitic deoxyhypusine synthase.

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5.  In vitro and in vivo silencing of plasmodial dhs and eIf-5a genes in a putative, non-canonical RNAi-related pathway.

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7.  Cloning, expression and functional activity of deoxyhypusine synthase from Plasmodium vivax.

Authors:  James T Njuguna; Marwa Nassar; Achim Hoerauf; Annette E Kaiser
Journal:  BMC Microbiol       Date:  2006-10-16       Impact factor: 3.605

8.  A suggested vital function for eIF-5A and dhs genes during murine malaria blood-stage infection.

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  8 in total

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