Absence of CD4+T Lymphocytes, CD8+T Lymphocytes, or B Lymphocytes Has Different Effects on the Efficacy of Posaconazole and Benznidazole in Treatment of Experimental AcuteTrypanosoma cruziInfection

Ferraz, Marcela Lencine; Gazzinelli, Ricardo T.; Alves, Rosana; Urbina, Julio A.; Romanha, Álvaro J.

doi:10.1128/aac.00779-08

Cited by 32 publications

(34 citation statements)

References 40 publications

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“…Several factors could be in play. A majority of studies that previously reported successful clearance of murine T. cruzi infections by posaconazole employed mice in early acute phase, with treatment starting as early as 1 day after the infection (8,9,33,34,37,38). It is possible that T. cruzi parasites in longer-term infections respond differently to treatment with posaconazole than parasites in early acute infections.…”

Section: Discussionmentioning

confidence: 95%

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Antitrypanosomal Treatment with Benznidazole Is Superior to Posaconazole Regimens in Mouse Models of Chagas Disease

Khare

Liu

Stinson

et al. 2015

Antimicrob Agents Chemother

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Two CYP51 inhibitors, posaconazole and the ravuconazole prodrug E1224, were recently tested in clinical trials for efficacy in indeterminate Chagas disease. The results from these studies show that both drugs cleared parasites from the blood of infected patients at the end of the treatment but that parasitemia rebounded over the following months. In the current study, we sought to identify a dosing regimen of posaconazole that could permanently clear Trypanosoma cruzi from mice with experimental Chagas disease. Infected mice were treated with posaconazole or benznidazole, an established Chagas disease drug, and parasitological cure was defined as an absence of parasitemia recrudescence after immunosuppression. Twenty-day therapy with benznidazole (10 to 100 mg/kg of body weight/day) resulted in a dose-dependent increase in antiparasitic activity, and the 100-mg/kg regimen effected parasitological cure in all treated mice. In contrast, all mice remained infected after a 25-day treatment with posaconazole at all tested doses (10 to 100 mg/kg/day). Further extension of posaconazole therapy to 40 days resulted in only a marginal improvement of treatment outcome. We also observed similar differences in antiparasitic activity between benznidazole and posaconazole in acute T. cruzi heart infections. While benznidazole induced rapid, dose-dependent reductions in heart parasite burdens, the antiparasitic activity of posaconazole plateaued at low doses (3 to 10 mg/kg/day) despite increasing drug exposure in plasma. These observations are in good agreement with the outcomes of recent phase 2 trials with posaconazole and suggest that the efficacy models combined with the pharmacokinetic analysis employed here will be useful in predicting clinical outcomes of new drug candidates.

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Section: Discussionmentioning

confidence: 95%

“…In that study, treatment failure was not evaluated by using an immunosuppression protocol, and it is possible that the sensitivity of parasite detection in that study was lower than in the current study. Failure to perform immunosuppression after the treatment also limits the sensitivity of three other studies from this list (33,34,38).…”

Section: Discussionmentioning

confidence: 99%

Antitrypanosomal Treatment with Benznidazole Is Superior to Posaconazole Regimens in Mouse Models of Chagas Disease

Khare

Liu

Stinson

et al. 2015

Antimicrob Agents Chemother

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“…Other studies have demonstrated that the anti-T. cruzi activity of POS in a murine model of acute Chagas disease is much less dependent on interferon-γ than that of BZN (Ferraz et al 2007). It has also been shown that ablation of TCD4 + , TCD8 + and B lymphocytes has distinct effects on POS and BZN activity in the same experimental model (Ferraz et al 2009). POS efficacy was especially dependent on the presence of functional TCD8 + cells, but relatively insensitive to the absence of LB cells, yet the reverse was true for BZN; the activity of both drugs was markedly reduced in the absence of TCD4 + cells.…”

Section: Ergosterol Biosynthesis Inhibitors (Ebi) As Potential New Thmentioning

confidence: 99%

“…POS efficacy was especially dependent on the presence of functional TCD8 + cells, but relatively insensitive to the absence of LB cells, yet the reverse was true for BZN; the activity of both drugs was markedly reduced in the absence of TCD4 + cells. These results were interpreted in terms of the different parasite stages preferentially targeted by the two drugs (intracellular amastigotes by POS, extracellular trypomastigotes by BZN) and distinct cooperation patterns with the host's immune system (Ferraz et al 2009). An independent study in a similar experimental model found that POS was more effective than BZN in preventing heart damage and promoting a trypanocidal immune response (Olivieri et al, unpublished observations).…”

Section: Ergosterol Biosynthesis Inhibitors (Ebi) As Potential New Thmentioning

confidence: 99%

Ergosterol biosynthesis and drug development for Chagas disease

Urbina

2009

Mem. Inst. Oswaldo Cruz

188

153

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“…O Nifurtimox é produzido pela Bayer para tratamento da doença de Chagas em alguns países da América Latina e, além disso, para tratamento da tripanossomíase africana Gambiense no continente africano (Jannin e Villa, 2007). A ação antiparasitária do nifurtimox está associada à geração de espécies reativas de oxigênio (EROs), tais como ânion superóxido e peróxido de hidrogênio (Docampo, 1990;Maya et al, 2007;Dias et al, 2009) (Urbina et al, 1998;Ferraz et al, 2007Ferraz et al, , 2009) e o ravuconazol (Urbina e Docampo, 2003;Diniz Lde et al, 2010) dos quais são os candidatos mais avançados para o desenvolvimento da nova droga anti -T. cruzi, partindo para ensaios clínicos dentro de pouco tempo (Urbina, 2010). Compostos que inibem a enzima cisteína protease, ou mais precisamente, a cruzipaína, também são canditados para o desenvolvimento de quimioterapias.…”

Section: Drogas Disponíveisunclassified

Avaliação das perspectivas terapêuticas do ácido L-tiazolidina-4-carboxílico, um análogo de prolina, na infecção de camundongos pelo Trypanosoma cruzi.

Rocha¹

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Absence of CD4⁺T Lymphocytes, CD8⁺T Lymphocytes, or B Lymphocytes Has Different Effects on the Efficacy of Posaconazole and Benznidazole in Treatment of Experimental AcuteTrypanosoma cruziInfection

Cited by 32 publications

References 40 publications

Antitrypanosomal Treatment with Benznidazole Is Superior to Posaconazole Regimens in Mouse Models of Chagas Disease

Antitrypanosomal Treatment with Benznidazole Is Superior to Posaconazole Regimens in Mouse Models of Chagas Disease

Ergosterol biosynthesis and drug development for Chagas disease

Avaliação das perspectivas terapêuticas do ácido L-tiazolidina-4-carboxílico, um análogo de prolina, na infecção de camundongos pelo Trypanosoma cruzi.

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