Parasite, Compartments, and Molecules: Trick versus Treatment on Chagas Disease

Vannier‐Santos, Marcos Andre; Brunoro, Giselle Villa Flor; Soeiro, Maria de Nazaré Correia; DeCastro, Solange L.; Menna-Barreto, Rubem F.S.

doi:10.5772/intechopen.84472

Cited by 4 publications

(8 citation statements)

References 175 publications

(189 reference statements)

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“…1). (6,7,8,9) Despite this promising scenario, mitochondrial phenotypes are commonly observed only by electron microscopy, with few reports assessing the real impact of these compounds in the organelle physiology.…”

Section: Potential Drug Targets In Trypanosomatid Mitochondrion and O...mentioning

confidence: 99%

Is the mitochondrion a promising drug target in trypanosomatids?

Pedra-Rezende

Bombaça

Menna-Barreto

2022

Mem. Inst. Oswaldo Cruz

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The trypanosomatids Trypanosoma brucei, Trypanosoma cruzi and Leishmania spp. are etiological agents of important neglected tropical diseases, affecting millions of people worldwide, and the drugs available for these diseases present several limitations. Novel efficient and nontoxic drugs are necessary as an alternative to the current chemotherapy. The unique mitochondrion of trypanosomatids and its peculiar features turn this organelle a potential drug target. Several phenotypic studies describe the damage in the parasite mitochondrial ultrastructure, but the molecular target is unknown. Few reports demonstrated the electron transport system (ETS) as a target due to the high similarities to mammalian orthologues, hence ETS is not a good candidate for drug intervention. On the other hand, antioxidant enzymes, such as trypanothione reductase, and an alternative oxidase (AOX) seem to be interesting targets; however no high active inhibitors were developed up to now. Finally, due to the remarkable differences to mammalian machinery, together with the high biological importance for the parasite survival, the mitochondrial import system stands out as a very promising target in trypanosomatids. Archaic translocase of the outer membrane (ATOM) and translocase of the inner membrane (TIM) complexes, which mediate both protein and tRNA import, composed by specific subunits of these parasites, could be excellent candidates, deserving studies focused on the development of specific drugs.

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Section: Potential Drug Targets In Trypanosomatid Mitochondrion and O...mentioning

confidence: 99%

Is the mitochondrion a promising drug target in trypanosomatids?

Pedra-Rezende

Bombaça

Menna-Barreto

2022

Mem. Inst. Oswaldo Cruz

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“…CD therapy is based on two old antiparasitic drugs that are in clinical use for at least half a century: nifurtimox (Nif)(5-nitrofurane, Bayer 2502; Bayer, Germany) and benznidazole (Bz) (2-nitroimidazole; Pharmaceutical Laboratory of the State of Pernambuco [LAFEPE], Brazil, ELEA/Mundo Sano, Argentina). 9 Both present low efficacies especially in the later chronic stage, are contraindicated during pregnancy, cause severe side effects leading to high drop-out rates (treatment discontinuation ≈ 20%), and are inactive against parasite strains naturally resistant to both nitroderivatives. 9 In fact, T. cruzi display high genetic diversity with multiple strains belonging to seven discrete type units (DTUs) and that result in different naturally resistance profile and distinct drug efficacy.…”

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confidence: 99%

“… 9 Both present low efficacies especially in the later chronic stage, are contraindicated during pregnancy, cause severe side effects leading to high drop-out rates (treatment discontinuation ≈ 20%), and are inactive against parasite strains naturally resistant to both nitroderivatives. 9 In fact, T. cruzi display high genetic diversity with multiple strains belonging to seven discrete type units (DTUs) and that result in different naturally resistance profile and distinct drug efficacy. 10 , 11 Also, the recent pandemic Coronavirus disease 2019 (COVID-19) brought additional concerns adding a potential worsen prognostic for the chagasic carriers, impacting the most vulnerable populations who need public policies for health services.…”

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confidence: 99%

“…However, despite the large amount of pre-clinical studies screening different classes of natural products and synthetic compounds, only few drugs moved to clinical trials, which included repurposing studies with two anti-fungi triazoles inhibitors of the sterol 14a-demethylase (CYP51): Posaconazole (POSA) and E1224, the later a prodrug of fosravuconazole, an antifungal discovered by Eisai Ltd (Japan). 9 Although showing very promising in in vitro and in vivo assays, both CYP51 inhibitors fail to sustain efficacy in clinical trials. 13 , 14 , 18 The discrepancy of pre-clinical and clinical outcomes of both azoles raised several concerns regarding the lack of translation of pre-clinical ( in vitro and in vivo ) and clinical trials.…”

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confidence: 99%

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Perspectives for a new drug candidate for Chagas disease therapy

Soeiro

2022

Mem. Inst. Oswaldo Cruz

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Chagas disease (CD), a neglected tropical illness caused by the protozoan Trypanosoma cruzi , affects more than 6 million people mostly in poor areas of Latin America. CD has two phases: an acute, short phase mainly oligosymptomatic followed to the chronic phase, a long-lasting stage that may trigger cardiac and/or digestive disorders and death. Only two old drugs are available and both present low efficacy in the chronic stage, display side effects and are inactive against parasite strains naturally resistant to these nitroderivatives. These shortcomings justify the search for novel therapeutic options considering the target product profile for CD that will be presently reviewed besides briefly revisiting the data on phosphodiesterase inhibitors upon T. cruzi .

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“…Organelles: Kp: kinetoplast, f: flagellum, fp: flagellar pocket, mt: mitochondrion, nu: nucleus, ER: endoplasmic reticulum, Go: golgi apparatus, Ac: acidocalcisomes, Gl: glycosomes, Ap: autophagosomes. The drawing is based on data from Benaim et al and Vannier-Santos et al163,228…”

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confidence: 99%

Review on Experimental Treatment Strategies Against Trypanosoma cruzi

Mazzeti

Capelari-Oliveira

Bahia

et al. 2021

JEP

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Chagas disease is a neglected tropical disease caused by the protozoan Trypanosoma cruzi . Currently, only nitroheterocyclic nifurtimox (NFX) and benznidazole (BNZ) are available for the treatment of Chagas disease, with limitations such as variable efficacy, long treatment regimens and toxicity. Different strategies have been used to discover new active molecules for the treatment of Chagas disease. Target-based and phenotypic screening led to thousands of compounds with anti- T. cruzi activity, notably the nitroheterocyclic compounds, fexinidazole and its metabolites. In addition, drug repurposing, drug combinations, re-dosing regimens and the development of new formulations have been evaluated. The CYP51 antifungal azoles, as posaconazole, ravuconazole and its prodrug fosravuconazole presented promising results in experimental Chagas disease. Drug combinations of nitroheterocyclic and azoles were able to induce cure in murine infection. New treatment schemes using BNZ showed efficacy in the experimental chronic stage, including against dormant forms of T. cruzi . And finally, sesquiterpene lactone formulated in nanocarriers displayed outstanding efficacy against different strains of T. cruzi , susceptible or resistant to BNZ, the reference drug. These pre-clinical results are encouraging and provide interesting evidence to improve the treatment of patients with Chagas disease.

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Parasite, Compartments, and Molecules: Trick versus Treatment on Chagas Disease

Cited by 4 publications

References 175 publications

Is the mitochondrion a promising drug target in trypanosomatids?

Is the mitochondrion a promising drug target in trypanosomatids?

Perspectives for a new drug candidate for Chagas disease therapy

Review on Experimental Treatment Strategies Against Trypanosoma cruzi

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