Successful Aspects of the Coadministration of Sterol 14α-Demethylase Inhibitor VFV and Benznidazole in Experimental Mouse Models of Chagas Disease Caused by the Drug-Resistant Strain of Trypanosoma cruzi

被引:15
|
作者
Guedes-da-Silva, Francisca Hildemagna [1 ]
Jaen Batista, Denise da Gama [1 ]
Da Silva, Cristiane Franca [1 ]
Pavao, Beatriz Philot [1 ]
Batista, Marcos Meuser [1 ]
Moreira, Otacilio Cruz [2 ]
Souza, Leticia Rocha Quintino [2 ]
Britto, Constanca [2 ]
Rachakonda, Girish [3 ]
Villalta, Fernando [3 ]
Lepesheva, Galina I. [4 ]
Correia Soeiro, Maria de Nazare [1 ]
机构
[1] Fundacao Oswaldo Cruz, Inst Oswaldo Cruz, Lab Biol Celular, BR-21040360 Rio De Janeiro, Brazil
[2] Fundacao Oswaldo Cruz, Inst Oswaldo Cruz, Lab Biol Mol & Doencas Endem, BR-21040360 Rio De Janeiro, Brazil
[3] Meharry Med Coll, Dept Microbiol Immunol & Physiol, 1005 Dr DB Todd Jr Blvd, Nashville, TN 37208 USA
[4] Vanderbilt Univ, Inst Global Hlth, Sch Med, Dept Biochem, 622A RRB,2200 Pierce Ave, Nashville, TN 37232 USA
来源
ACS INFECTIOUS DISEASES | 2019年 / 5卷 / 03期
基金
美国国家卫生研究院;
关键词
coadministration; benznidazole; VFV; VNI; Colombiana strain; Trypanosoma cruzi; Chagas disease; IN-VITRO; COMBINATION THERAPY; CYP51; POSACONAZOLE; CANDIDATE; TARGET;
D O I
10.1021/acsinfecdis.8b00253
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Up to now, no vaccines are available for Chagas disease, and the current therapy is largely unsatisfactory. Novel imidazole-based scaffolds of protozoan sterol 14 alpha-demethylase (CYPS1) inhibitors have demonstrated potent antiparasitic activity with no acute toxicity. Presently our aim was to investigate the effectiveness of the experimental 14a-demethylase inhibitor VFV in the mouse models of Trypanosoma cruzi infection using a naturally drug-resistant Colombiana strain, under monotherapy and in association with the reference drug, benznidazole (Bz). The treatment with VFV resulted in complete parasitemia suppression and 100% animal survival when administered orally (given in 10% DMSO plus 5% Arabic gum) at 2S mg/kg (bid) for 60 days. However, as parasite relapse was found using VFV alone under this treatment scheme, the coadministration of VFV with Bz was assayed giving simultaneously (for 60 days, bid) by oral route, under two different drug vehicles (10% DMSO plus 5% Gum Arabic with or without 3% Tween 80). All tested mice groups resulted in >99.9% of parasitemia decrease and 100% animal survival. qPCR analysis performed on cyclophosphamide immunosuppressed mice revealed that, although presenting lack of cure, VFV given as monotherapy was 14-fold more active than Bz, and the coadministration of Bz plus VFV (given simultaneously, using 10% DMSO plus 5% Gum Arabic as vehicle) resulted in 106-fold lower blood parasitism as compared to the monotherapy of Bz. Another interesting finding was the parasitological cure in 70% of the animals treated with Bz and VFV when the coadministration was given using the VFV suspension in 10% DMSO + Arabic gum + Tween 80 (a formulation that we have found to provide a better pharmacokinetics), even after immunosuppression using cyclophosphamide cycles, supporting the promising aspect of the drug coadministration in improving the efficacy of therapeutic arsenal against T. cruzi.
引用
收藏
页码:365 / 371
页数:13
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