Effect of topoisomerase inhibitors and DNA-binding drugs on the cell proliferation and ultrastructure of Trypanosoma cruzi

Zuma, Aline Araújo; Cavalcanti, Danielle Pereira; Maia, Marina C.P.; Souza, Wanderley de; Motta, María Cristina M.

doi:10.1016/j.ijantimicag.2010.11.031

Cited by 37 publications

(25 citation statements)

References 54 publications

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“…1). Such an effect, as previously reported by Zuma et al (2011), may be related to the fact that this drug promotes remarkable modifications on kinetoplast DNA arrangement, but does not impair cell division. The control cells presented a typical organization, such as a nucleus containing condensed heterochromatin, one mitochondrion, a bar-shaped kinetoplast, a Golgi complex, and a flagellum (Fig.…”

Section: Resultssupporting

confidence: 74%

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Unveiling the effects of berenil, a DNA-binding drug, on Trypanosoma cruzi: implications for kDNA ultrastructure and replication

et al. 2014

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Section: Resultssupporting

confidence: 74%

“…The drug concentrations used in this work (2, 10, 20, and 50 μM) were determined according to data presented in previous reports (Portugal 1994;Witola et al 2005;Zuma et al 2011).…”

Section: Drug Treatmentmentioning

confidence: 99%

Unveiling the effects of berenil, a DNA-binding drug, on Trypanosoma cruzi: implications for kDNA ultrastructure and replication

et al. 2014

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“…The other subunit contains the catalytic amino acid (Tyr222), which acts by breaking one DNA strand by a specific nucleotide sequence (13). All of these features have also been found in the other protozoanborne NTDs pathogens: Trypanosoma brucei, the agent responsible for sleeping sickness in Africa (11), and T. cruzi, responsible for Chagas' disease in South America (36). However, despite the fact that these enzymes conserve their catalytic domains unchanged, they display two nonconserved regions, one at the C-terminal end of the large protomer and the other at the N-terminal end of the small protomer, which are extremely important in sensitivity to topoisomerase poisons (12).…”

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confidence: 95%

Indotecan (LMP400) and AM13-55: Two Novel Indenoisoquinolines Show Potential for Treating Visceral Leishmaniasis

Balaña‐Fouce

Fernández-Prada

Requena

et al. 2012

Antimicrob Agents Chemother

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dVisceral leishmaniasis is an emerging neglected tropical disease (NTD) caused by the protozoan Leishmania infantum in the countries bordering the Mediterranean Basin. Currently there is no effective vaccine against this disease, and the therapeutic approach is based on toxic derivatives of Sb V . Therefore, the discovery of new therapeutic targets and the development of drugs designed to inhibit them comprise an extremely important approach to fighting this disease. DNA topoisomerases (Top) have been identified as promising targets for therapy against leishmaniasis. These enzymes are involved in solving topological problems generated during replication, transcription, and recombination of DNA. Being unlike that of the mammalian host, type IB DNA topoisomerase (TopIB) from Leishmania spp. is a unique bisubunit protein, which makes it very interesting as a selective drug target. In the present investigation, we studied the effect of two TopIB poisons with indenoisoquinoline structure, indotecan and AM13-55, on a murine BALB/c model of infected splenocytes with L. infantum, comparing their effectiveness with that of the clinically tested leishmanicidal drug paromomycin. Both compounds have high selectivity indexes compared with uninfected splenocytes. SDS-KCl-precipitable DNA-protein complexes in Leishmania promastigotes and in vitro cleaving assays confirmed that these drugs are Top poisons. The inhibitory potency of both indenoisoquinolines on L. infantum recombinant TopIB was assessed in vitro, with results showing that indotecan was the most active compound, preventing the relaxation of supercoiled DNA. Experimental infections in susceptible BALB/c mice treated with 2.5 mg/kg body weight/day once every other day for a total of 15 days showed that indotecan cleared more than 80% of the parasite burden of the spleen and liver, indicating promising activity against visceral leishmaniasis.

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“…The type I enzymes make a transient single stranded nick in absence of any high energy cofactor, whereas the type II enzymes make double-stranded breaks in the presence of ATP, which allows supercoils to be removed from the circular DNAs. Both types of enzymes have been characterized in kinetoplastid hemoflagellated protozoan parasites [123].…”

Section: Dna Topoisomerase I and Iimentioning

confidence: 99%

New Treatments for Chagas Disease and the Relationship between Chagasic Patients and Cancers

Oliveira¹,

Mendes²,

Almeida³

et al. 2014

CRJ

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Abstract:Chagas disease is an infectious illness with a broad distribution throughout the South American and African continents, importantly influencing human morbidity and mortality and a controversial relationship with the onset of cancers, especially of the gastrointestinal tract system. In addition, it is listed by the World Health Organization (WHO) as one ofthe most neglected tropical diseases. Although Chagas disease (CD) was discovered more than 100 years ago, the existing therapies show low efficacy and serious side effects and developing safer and more effective drugs remains a hard challenge. Thus, this review highlights the main, novel and promising treatments against Trypanosoma cruzi, including biomacromolecules, natural products, vaccines, and metabolic pathway targets and highlights a worsening of esophageal cancer prognosis in chagasic patients. Moreover, we also discuss the perspectives of obtaining original optimized drugs that take advantage of organic and inorganic medicinal chemistry advances, as well as molecular modeling and biotechnology.

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Effect of topoisomerase inhibitors and DNA-binding drugs on the cell proliferation and ultrastructure of Trypanosoma cruzi

Cited by 37 publications

References 54 publications

Unveiling the effects of berenil, a DNA-binding drug, on Trypanosoma cruzi: implications for kDNA ultrastructure and replication

Unveiling the effects of berenil, a DNA-binding drug, on Trypanosoma cruzi: implications for kDNA ultrastructure and replication

Indotecan (LMP400) and AM13-55: Two Novel Indenoisoquinolines Show Potential for Treating Visceral Leishmaniasis

New Treatments for Chagas Disease and the Relationship between Chagasic Patients and Cancers

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