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In silico reconstruction of the amino acid metabolic pathways of Trypanosoma cruzi

Research Article Vol 7, Issue 3, 2008
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In silico reconstruction of the amino acid metabolic pathways of Trypanosoma cruzi

A.C.R. Guimarães, T.D. Otto, M. Alves-Ferreira, A.B. Miranda, W.M. Degrave
Published: September 23, 2008
Genet. Mol. Res. 7 (3) : 872-882
DOI: https://doi.org/10.4238/vol7-3x-meeting05

Cite this Article
A.C.R. Guimarães, T.D. Otto, M. Alves-Ferreira, A.B. Miranda, W.M. Degrave (2008). In silico reconstruction of the amino acid metabolic pathways of Trypanosoma cruzi. Genet. Mol. Res. 7(3): 872-882. https://doi.org/10.4238/vol7-3x-meeting05

About the Authors
A.C.R. Guimarães, T.D. Otto, M. Alves-Ferreira, A.B. Miranda, W.M. Degrave

Corresponding Author
A.C.R. Guimarães
Email: carolg@fiocruz.br

ABSTRACT

Trypanosoma cruzi is the epidemiological agent of Chagas’ disease, affecting most of Central and South America, constituting a significant health and socio-economic problem. The parasite has a metabolism largely based on the consumption of amino acids, which participate in a diversity of metabolic pathways, leading to many crucial compounds for the survival of this parasite. Study of its enzymes has the potential to disclose new therapeutic targets and foster the development of new drugs. In this study, we employed computational approaches to reconstruct in silico the amino acid metabolic pathways of T. cruzi, aiming to link genomic information with functional information. For that, protein sequences from 570 EC classes belonging to 25 different pathways in general amino acid metabolism were downloaded from KEGG. A subset of 471 EC classes had at least one sequence deposited. Clustering of the proteins belonging to each EC class was performed using a similarity-based approach implemented in the tool AnEnPi. Reconstruction of the metabolic pathways comprising the amino acid metabolism of T. cruzi was performed by analyzing the output of blastp, using as query the dataset of predicted proteins of T. cruzi against all sequences of each individual cluster. This approach allowed us to identify 764 T. cruzi proteins probably involved in the metabolism of amino acids as well as the identification of several putative cases of analogy. Furthermore, we were able to identify several enzymatic activities of T. cruzi that were not previously included in KEGG.

Key words: Metabolism, Trypanosoma cruzi, Amino acid, analogy.

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