The pentose phosphate pathway in Trypanosoma cruzi: A potential target for the chemotherapy of Chagas disease

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Abstract

Trypanosoma cruzi is highly sensitive to oxidative stress caused by reactive oxygen species. Trypanothione, the parasite's major protection against oxidative stress, is kept reduced by trypanothione reductase, using NADPH; the major source of the reduced coenzyme seems to be the pentose phosphate pathway. Its seven enzymes are present in the four major stages in the parasite's biological cycle; we have cloned and expressed them in Escherichia coli as active proteins. Glucose 6-phosphate dehydrogenase, which controls glucose flux through the pathway by its response to the NADP/NADPH ratio, is encoded by a number of genes per haploid genome, and is induced up to 46-fold by hydrogen peroxide in metacyclic trypomastigotes. The genes encoding 6- phosphogluconolactonase, 6phosphogluconate dehydrogenase, transaldolase and transketolase are present in the CL Brener clone as a single copy per haploid genome. 6-phosphogluconate dehydrogenase is very unstable, but was stabilized introducing two salt bridges by site-directed mutagenesis. Ribose-5-phosphate isomerase belongs to Type B; genes encoding Type A enzymes, present in mammals, are absent. Ribulose-5-phosphate epimerase is encoded by two genes. The enzymes of the pathway have a major cytosolic component, although several of them have a secondary glycosomal localization, and also minor localizations in other organelles.

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Igoillo-Esteve, M., Maugeri, D., Stern, A. L., Beluardi, P., & Cazzulo, J. J. (2007). The pentose phosphate pathway in Trypanosoma cruzi: A potential target for the chemotherapy of Chagas disease. Anais Da Academia Brasileira de Ciencias, 79(4), 649–663. https://doi.org/10.1590/s0001-37652007000400007

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