Evaluation of phthalazinone phosphodiesterase inhibitors with improved activity and selectivity against Trypanosoma cruzi

Araújo, Julianna Siciliano de; Silva, Patrícia Bernardino da; Batista, Marcos Meuser; Peres, Raiza Brandão; Cardoso-Santos, Camila; Kalejaiye, Titilola D.; Munday, Jane C.; Heuvel, Erik de; Sterk, Geert Jan; Augustyns, Koen; Salado, Irene G.; Matheeussen, An; Esch, Iwan J. P. de; Koning, Harry P. de; Leurs, Rob; Maes, Louis; Soeiro, Maria de Nazaré Correia

doi:10.1093/jac/dkz516

Cited by 8 publications

(17 citation statements)

References 54 publications

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“…These observations are suggestive of osmotic stress and may be related to increased levels of cAMP. In this context, we investigated the possibility of a PDE target for NPD-227 and observed that it induced a significant increase in the cellular cAMP concentration, confirming the targeting of at least one PDE parasite isoform, consistent with reports on other PDE inhibitor chemotypes (25,26).…”

Section: Discussionsupporting

confidence: 85%

“…The rounding of parasites induced by NPD-227 suggests an impact on the osmoregulation system, already described as an outcome of PDEC inhibition in T. cruzi (9). Indeed, we have previously shown that exposure to other classes of PDE inhibitors, specifically imidazoles (25) and phthalazinones (26), causes profound ultrastructural damage in the Golgi, flagellar pocket, and plasma membrane of T. cruzi. These observations are suggestive of osmotic stress and may be related to increased levels of cAMP.…”

Section: Discussionmentioning

confidence: 74%

“…Combined therapy has been proposed as an ideal approach, considering its potential to enhance efficacy and delay drug resistance by acting upon different cellular targets (28,29). This strategy represents an important tool to optimize the potential of PDE inhibitors within combined approaches, particularly in view of their incomplete effects on trypomastigotes, and our successful experience with some combination approaches (26,(30)(31)(32). In the in vivo efficacy proof of concept, coadministration of Bz and NPD-227 resulted in improved efficacy in acute mouse models of T. cruzi infection, leading to ϳ90% reduction in parasitemia and lower mortality rates (0 to 17%) than seen with either drug alone (Bz and NPD monotherapy: 40 to 63% and 40 to 50%, respectively).…”

Section: Discussionmentioning

confidence: 99%

“…Following 48 h of interaction, the infected cultures were rinsed, fixed with Bouin for 5 min, stained with Giemsa, and evaluated by light microscopy. The percentage of infected host cells and the number of parasites per cell were determined for the calculation of the infection index as reported (26).…”

Section: Trypanocidal Activitymentioning

confidence: 99%

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Efficacy of Novel Pyrazolone Phosphodiesterase Inhibitors in Experimental Mouse Models of Trypanosoma cruzi

Araújo

Silva

Batista

et al. 2020

Antimicrob Agents Chemother

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Pyrazolones are heterocyclic compounds with interesting biological properties. Some derivatives inhibit phosphodiesterases (PDEs) and thereby increase the cellular concentration of cyclic AMP (cAMP), which plays a vital role in the control of metabolism in eukaryotic cells, including the protozoan Trypanosoma cruzi, the etiological agent of Chagas disease (CD), a major Neglected Tropical Disease. In vitro phenotypic screening identified a 4-bromophenyl-dihydropyrazole dimer as anti-T. cruzi hit and 17 novel pyrazolone analogues with variations on the phenyl ring were investigated in a panel of phenotypic laboratory models. Potent activity against the intracellular forms (Tulahuen and Y strains) was obtained with EC50 values within the 0.17 - 3.3 μM range. Although most were not active against bloodstream trypomastigotes, an altered morphology and loss of infectivity were observed. Pretreatment of the mammalian host cells with pyrazolones did not interfere with infection and proliferation, showing that the drug activity was not the result of changes to host cell metabolism. The pyrazolone NPD-227 increased the intracellular cAMP levels and was able to sterilize of T. cruzi-infected cell cultures. Thus, due to its high potency and selectivity in vitro, and its additive interaction with benznidazole (Bz), NPD-227 was next assessed in the acute mouse model. Oral dosing for 5 days of NPD-227 at 10 mg/kg + BZ at 10 mg/kg not only reduced parasitaemia (>87 %) but also protected against mortality (>83% survival), hence demonstrating superiority to the monotherapy schemes. These data support these pyrazolone molecules as potential novel therapeutic alternatives for Chagas disease.

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Section: Discussionsupporting

confidence: 85%

Section: Discussionmentioning

confidence: 74%

Section: Discussionmentioning

confidence: 99%

Section: Trypanocidal Activitymentioning

confidence: 99%

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Efficacy of Novel Pyrazolone Phosphodiesterase Inhibitors in Experimental Mouse Models of Trypanosoma cruzi

Araújo

Silva

Batista

et al. 2020

Antimicrob Agents Chemother

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“…The essentiality of the cAMP signaling pathways, including PKA, prompted us to extend our work on cAMP phosphodiesterases of protozoan parasites [ 28 – 32 ] to S . mansoni , anticipating that, as in human-infective protozoa, inhibition of PDEs leads to a fatal increase and imbalance in cellular cAMP levels.…”

Section: Introductionmentioning

confidence: 99%

Cloning and functional complementation of ten Schistosoma mansoni phosphodiesterases expressed in the mammalian host stages

et al. 2020

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Only a single drug against schistosomiasis is currently available and new drug development is urgently required but very few drug targets have been validated and characterised. However, regulatory systems including cyclic nucleotide metabolism are emerging as primary candidates for drug discovery. Here, we report the cloning of ten cyclic nucleotide phosphodiesterase (PDE) genes of S. mansoni, out of a total of 11 identified in its genome. We classify these PDEs by homology to human PDEs. Male worms displayed higher expression levels for all PDEs, in mature and juvenile worms, and schistosomula. Several functional complementation approaches were used to characterise these genes. We constructed a Trypanosoma brucei cell line in which expression of a cAMP-degrading PDE complements the deletion of TbrPDEB1/B2. Inhibitor screens of these cells expressing only either SmPDE4A, TbrPDEB1 or TbrPDEB2, identified highly potent inhibitors of the S. mansoni enzyme that elevated the cellular cAMP concentration. We further expressed most of the cloned SmPDEs in two pde1Δ/pde2Δ strains of Saccharomyces cerevisiae and some also in a specialised strain of Schizosacharomyces pombe. Five PDEs, SmPDE1, SmPDE4A, SmPDE8, SmPDE9A and SmPDE11 successfully complemented the S. cerevisiae strains, and SmPDE7var also complemented to a lesser degree, in liquid culture. SmPDE4A, SmPDE8 and SmPDE11 were further assessed in S. pombe for hydrolysis of cAMP and cGMP; SmPDE11 displayed considerable preferrence for cGMP over cAMP. These results and tools enable the pursuit of a rigorous drug discovery program based on inhibitors of S. mansoni PDEs.

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Benznidazole modulates release of inflammatory mediators by cardiac spheroids infected with Trypanosoma cruzi

Fiuza

Batista

Nunes

et al. 2021

Experimental Parasitology

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Evaluation of phthalazinone phosphodiesterase inhibitors with improved activity and selectivity against Trypanosoma cruzi

Cited by 8 publications

References 54 publications

Efficacy of Novel Pyrazolone Phosphodiesterase Inhibitors in Experimental Mouse Models of Trypanosoma cruzi

Efficacy of Novel Pyrazolone Phosphodiesterase Inhibitors in Experimental Mouse Models of Trypanosoma cruzi

Cloning and functional complementation of ten Schistosoma mansoni phosphodiesterases expressed in the mammalian host stages

Benznidazole modulates release of inflammatory mediators by cardiac spheroids infected with Trypanosoma cruzi

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