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

Igoillo-Esteve, Mariana; Maugeri, Dante; Stern, A.L.; Beluardi, Paula; Cazzulo, Juán José

doi:10.1590/s0001-37652007000400007

Cited by 46 publications

(32 citation statements)

References 35 publications

(20 reference statements)

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“…mainly a response to the oxidative stress conditions, because NADPH provides the redox power for antioxidant systems (Nogae & Johnston, 1990;Pollak et al, 2007). An enhanced supply of NADPH is found under conditions of oxidative stress in various prokaryotic and eukaryotic cells (Boada et al, 2000;Igoillo-Esteve et al, 2007;Ralser et al, 2007;Williams & Ford, 2004). Clearly, the flux rearrangement in the central metabolism leads to greater NADPH formation, but is not sufficient for recovery from the oxidative stress conditions, as indicated by the perturbed redox state and the reduced metabolic activity.…”

Section: Metabolic Flux Reroutingmentioning

confidence: 99%

Physiological response of Corynebacterium glutamicum to oxidative stress induced by deletion of the transcriptional repressor McbR

et al. 2008

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In the present work the metabolic response of Corynebacterium glutamicum to deletion of the global transcriptional regulator McbR, which controls, e.g. the expression of enzymes of Lmethionine and L-cysteine biosynthesis and sulfur assimilation, was studied. Several oxidative stress proteins were significantly upregulated among about 40 proteins in response to deletion of McbR. Linked to this oxidative stress, the mutant exhibited a 50 % reduced growth rate, a 30 % reduced glucose uptake rate and a 30 % reduced biomass yield. It also showed metabolic flux rerouting in response to the deletion. NADPH metabolism was strongly altered. In contrast to the wild-type, the deletion strain supplied significantly more NADPH than required for anabolism, indicating the activity of additional NADPH-consuming reactions. These involved enzymes of oxidative stress protection. Through redirection of metabolic carbon flux in the central catabolism, including a 40 % increased tricarboxylic acid (TCA) cycle flux, the mutant revealed an enhanced NADPH supply to provide redox power for the antioxidant systems. This, however, was not sufficient to compensate for the oxidative stress, as indicated by the drastically disturbed redox equilibrium. The NADPH/NADP + ratio in C. glutamicum DmcbR was only 0.29, and thus much lower than that of the wild-type (2.35). Similarly, the NADH/NAD + ratio was substantially reduced from 0.18 in the wild-type to 0.08 in the mutant. Deletion of McbR is regarded as a key step towards biotechnological L-methionine overproduction in C. glutamicum. C. glutamicum DmcbR, however, did not overproduce L-methionine; this was very likely linked to the low availability of NADPH. Since oxidative stress is often observed in industrial production processes, engineering of NADPH metabolism could be a general strategy for improvement of production strains. Unlike the wild-type, C. glutamicum DmcbR contained large granules with high phosphorus content. The storage of these energy-rich polyphosphates is probably the result of a large excess of formation of ATP, as revealed by estimation of the underlying fluxes linked to energy metabolism.

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Section: Metabolic Flux Reroutingmentioning

confidence: 99%

Physiological response of Corynebacterium glutamicum to oxidative stress induced by deletion of the transcriptional repressor McbR

et al. 2008

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“…The pentose phosphate shunt -The pentose phosphate shunt is the most studied pathway in T. cruzi and the participating enzymes have been well characterised both molecularly and biochemically (Igoillo-Esteve et al 2007). The enzymes of this pathway were identified as cytoplasmic, but with secondary localisation in the glycosome.…”

Section: The Energy Metabolismmentioning

confidence: 99%

“…This enzyme has several copies in the T. cruzi genome, while the 6-phosphogluconolactonase, the 6-phosphogluconate dehydrogenase (6PGD) and the ribose 5-phosphate isomerase are present as only one copy. The latter enzyme is analogous to the human enzyme, which makes it an interesting therapeutic target (Igoillo-Esteve et al 2007). Recently, Stern et al (2007), using site directed mutagenesis, revealed details on the reaction mechanism of this enzyme, which acts via the formation of the 1,2-cis-enediol.…”

Section: The Energy Metabolismmentioning

confidence: 99%

“…The non-oxidative branch complements the pathway and the enzymes involved are ribulose-5-phosphate epimerase, with two gene copies in T. cruzi and the transaldolase and transketolase, each with one copy per haploid genome (Igoillo-Esteve et al 2007). One of the copies of ribulose-5-phophate isomerase presents a C-terminal (PTS1) signal for glycosome targeting but the cytosol also showed activity (Maugeri & Cazzulo 2004).…”

Section: The Energy Metabolismmentioning

confidence: 99%

“…A transaldolase is responsible for the transfer of the dihydroxyacetone group from fructose-6-phosphate to erythrose-4-phosphate, leading to the synthesis of sedoheptulose-7-phosphate and glyceraldeyde-3-P. The biochemical characterisation of the recombinant enzyme was reported (Igoillo-Esteve et al 2007). The transketolase of T. cruzi contains the PTS1 signal peptide, which possibly permits its distribution both in the glycosome and in the cytoplasm.…”

Section: The Energy Metabolismmentioning

confidence: 99%

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