1. The glycosomal ATP-dependent phosphofructokinase of <em>Trypanosoma brucei</em> must have evolved from an ancestral pyrophosphate-dependent enzyme.
- Author
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Michels, Paul A. M., Chevalier, Nathalie, Opperdoes, Fred R., Rider, Mark H., and Rigden, Daniel J.
- Subjects
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TRYPANOSOMA , *PHOSPHOFRUCTOKINASE 1 , *ENZYMES , *ADENOSINE triphosphate , *AMINO acids , *PROTEINS - Abstract
Trypanosoma brucei contains an ATP-dependent phosphofructokinase (PFK), located in its glycosomes, which are peroxisome-like organelles sequestering the majority of its glycolytic enzymes. In this paper, we report the cloning and sequencing of the single-copy gene encoding this enzyme. Its amino-acid sequence is more similar to pyrophosphate (PPi)-dependent PFKs than to other ATP-dependent PFKs. a phylogenetic analysis suggests that the enzyme must have been derived from a PPi-dependent ancestral PFK, which changed its phospho-donor specificity during evolution. The enzyme is no longer capable of using PPi as phospho substrate, nor can it catalyze the reverse reaction as PPi-PFKs generally can. Moreover, the presence of a high pyrophosphatase activity in the cell renders it unlikely that PPi can function as free-energy source in present-day trypanosomes. It remains to be determined which mutations were responsible for the chage in phospho-substrate specificity of the trypanosomatid PFK. As a result of its particular evolutionary hitory, the T. brucei PFK shows many structural differences, even at the active site, when compared with other ATP-dependent PFKs. These differences offer great potential for the structure-based design of trypanocidal drugs. [ABSTRACT FROM AUTHOR]
- Published
- 1997
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