Trypanosoma cruzi synthesizes proline via a delta1-pyrroline-5-carboxylate reductase whose activity is fine-tuned by NADPH cytosolic pools

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dc.contributor(CeTICS) Centro de Toxinas, Resposta-imune e Sinalização Celularpt_BR
dc.contributor(LCC) Lab. Ciclo Celularpt_BR
dc.contributor.authorMarchese, Leticia Mpt_BR
dc.contributor.authorOlavarria, Karel Mpt_BR
dc.contributor.authorMantilla, Brian Spt_BR
dc.contributor.authorAvila, Carla Cristi Del Campopt_BR
dc.contributor.authorSouza, Rodolpho Ornitz Oliveirapt_BR
dc.contributor.authorDamasceno, Flávia Silvapt_BR
dc.contributor.authorElias, Maria Carolinapt_BR
dc.contributor.authorSilber, Ariel Marianopt_BR
dc.date.accessioned2020-07-09T21:27:36Z-
dc.date.available2020-07-09T21:27:36Z-
dc.date.issued2020pt_BR
dc.identifier.citationMarchese LM, Olavarria KM, Mantilla BS, Avila CCDC, Souza ROO, Damasceno FS, et al. Trypanosoma cruzi synthesizes proline via a delta1-pyrroline-5-carboxylate reductase whose activity is fine-tuned by NADPH cytosolic pools. Biochem. J.. 2020 Apr;477(10):1827-1845. doi:10.1042/BCJ20200232.pt_BR
dc.identifier.urihttps://repositorio.butantan.gov.br/handle/butantan/3024-
dc.description.abstractIn Trypanosoma cruzi, the etiological agent of Chagas disease, the amino acid proline participates in processes related to T. cruzi survival and infection, such as ATP production, cell differentiation, host-cell invasion, and in protection against osmotic, nutritional, and thermal stresses and oxidative imbalance. However, little is known about proline biosynthesis in this parasite. delta1-Pyrroline-5-carboxylate reductase (P5CR, EC 1.5.1.2) catalyzes the biosynthesis of proline from delta1-pyrroline-5-carboxylate (P5C) with concomitant NADPH oxidation. Herein, we show that unlike other eukaryotes, T. cruzi biosynthesizes proline from P5C, which is produced exclusively from glutamate. We found that TcP5CR is a NADPH-dependent cytosolic enzyme with a Km app for P5C of 23.9 mM and with a higher expression in the insect-resident form of parasite. High concentrations of the co-substrate NADPH partially inhibited TcP5CR activity, prompting us to analyze multiple kinetic inhibition models. The model that best explained the obtained data included a non-competitive substrate inhibition mechanism (Ki app = 45 ± 0.7 µM). Therefore, TcP5CR is a candidate as a regulatory factor of this pathway. Finally, we show that P5C can exit trypanosomatid mitochondria in conditions that do not compromise organelle integrity. These observations, together with previously reported results, lead us to propose that in T. cruzi TcP5CR participates in a redox shuttle between the mitochondria and the cytoplasm. In this model cytoplasmic redox equivalents from NADPH pools are transferred to the mitochondria using proline as a reduced metabolite and shuttling to fuel electrons to the respiratory chain through proline oxidation by its cognate dehydrogenasept_BR
dc.description.sponsorship(FAPESP) Fundação de Amparo à Pesquisa do Estado de São Paulopt_BR
dc.description.sponsorship(CNPq) Conselho Nacional de Desenvolvimento Científico e Tecnológicopt_BR
dc.description.sponsorship(GCRF) Global Challenges Research Fundpt_BR
dc.format.extent1827-1845pt_BR
dc.language.isoEnglishpt_BR
dc.relation.ispartofThe Biochemical Journalpt_BR
dc.rightsOpen accesspt_BR
dc.titleTrypanosoma cruzi synthesizes proline via a delta1-pyrroline-5-carboxylate reductase whose activity is fine-tuned by NADPH cytosolic poolspt_BR
dc.typeArticlept_BR
dc.identifier.doi10.1042/BCJ20200232pt_BR
dc.identifier.urlhttps://doi.org/10.1042/BCJ20200232pt_BR
dc.contributor.external(USP) Universidade de São Paulopt_BR
dc.identifier.citationvolume477pt_BR
dc.identifier.citationissue10pt_BR
dc.subject.keywordProline biosynthesispt_BR
dc.subject.keyword1D-Pyrroline-5-carboxylatept_BR
dc.subject.keywordmitochondrial shuttlept_BR
dc.subject.keywordsubstrate inhibitionpt_BR
dc.subject.keywordTrypanosoma cruzipt_BR
dc.relation.ispartofabbreviatedBiochem Jpt_BR
dc.identifier.citationabntv. 477, n. 10, p. 1827-1845, abr. 2020pt_BR
dc.identifier.citationvancouver2020 Apr;477(10):1827-1845pt_BR
dc.contributor.butantanAvila, Carla Cristi Del Campo|:Aluno|:Centro de Toxinas, Resposta-imune e Sinalização Celular (CeTICS)|:pt_BR
dc.contributor.butantanElias, Maria Carolina|:Pesquisador|:LCC - Laboratório de Ciclo Celular|:pt_BR
dc.sponsorship.butantan(CNPq) Conselho Nacional de Desenvolvimento Científico e Tecnológico¦¦308351/2013-4pt_BR
dc.sponsorship.butantan(CNPq) Conselho Nacional de Desenvolvimento Científico e Tecnológico¦¦404769/2018-7pt_BR
dc.sponsorship.butantan(FAPESP) Fundação de Amparo à Pesquisa do Estado de São Paulo¦¦2016/06034-2pt_BR
dc.sponsorship.butantanGlobal Challenges Research Fund (GCRF)¦¦MR/P027989/1pt_BR
dc.identifier.bvsccBR78.1pt_BR
dc.identifier.bvsdbIBProdpt_BR
dc.description.dbindexedYespt_BR
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