Simões-Mattos L, Teixeira M J, Costa D C, Prata J R C, Bevilaqua C M L, Sidrim J J C, Rocha M F G
Faculdade de Veterinária (FAVET), Universidade Estadual do Ceará (UECE), Av. Paranjana 1700, Campus do Itaperi, Fortaleza, Ceará, Brazil.
Vet Parasitol. 2002 Jan 28;103(3):207-16. doi: 10.1016/s0304-4017(01)00595-7.
The objective of the present study was to assess the effect of terbinafine treatment in hamsters infected with Leishmania chagasi. Four of five groups of hamsters were infected with 3 x 10(7) L. chagasi promastigotes by the intracardiac route and submitted to different treatments of 30 days duration starting on the 30th day after inoculation. Group 1 was treated with 100mg/kg terbinafine PO, group 2 was treated with 80 mg/kg Glucantime IM, and group 3 was treated with a combination of the same dose of each drug by the same routes. Group 4 (control) received vehicle (Tween 80 [0.1%]+CMC[0.5%]+H(2)O [0.5 ml], PO). Spleen parasite burden and spleen relative weight were determined 3 days after the end of the treatment. The results were analyzed by the Kruskal-Wallis test (P < 0.05). There was no difference between the infected untreated and terbinafine-treated groups in spleen parasite burden (15.81+/-15.81 vs. 13.00+/-12.94, respectively). Terbinafine plus Glucantime (6.11+/-5.90) and Glucantime alone (4.83+/-4.82) significantly reduced spleen parasite burden compared to the infected untreated group (15.81+/-15.81, P<0.01). There was a difference in the relative weight of the spleen between the naïve and the infected untreated groups (2.5+/-0.2 vs. 9.8+/-1.0, respectively) as well as between the naïve and terbinafine groups (2.5+/-0.2 vs. 10.0+/-1.4, respectively). Glucantime alone and Glucantime plus terbinafine (2.5+/-0.2 and 4.2+/-0.6) significantly reduced the weight of the spleen in comparison with the infected untreated group. Even so, the spleen parasite burden was directly related to spleen weight. Terbinafine alone at the dose and schedule used had no effect on spleen parasite burden or relative spleen weight of L. chagasi-infected hamsters.
本研究的目的是评估特比萘芬治疗对感染恰加斯利什曼原虫的仓鼠的影响。五组仓鼠中有四组通过心脏内途径感染3×10⁷个恰加斯利什曼原虫前鞭毛体,并在接种后第30天开始接受为期30天的不同治疗。第1组口服100mg/kg特比萘芬,第2组肌肉注射80mg/kg葡糖胺锑钠,第3组通过相同途径接受相同剂量的两种药物联合治疗。第4组(对照组)接受赋形剂(吐温80[0.1%]+羧甲基纤维素[0.5%]+水[0.5ml],口服)。在治疗结束后3天测定脾脏寄生虫负荷和脾脏相对重量。结果采用Kruskal-Wallis检验进行分析(P<0.05)。未治疗的感染组和特比萘芬治疗组之间的脾脏寄生虫负荷无差异(分别为15.81±15.81和13.00±12.94)。与未治疗的感染组(15.81±15.81)相比,特比萘芬加葡糖胺锑钠(6.11±5.90)和单独使用葡糖胺锑钠(4.83±4.82)显著降低了脾脏寄生虫负荷(P<0.01)。未感染组与未治疗的感染组之间的脾脏相对重量存在差异(分别为2.5±0.2和9.8±1.0),未感染组与特比萘芬组之间也存在差异(分别为2.5±0.2和10.0±1.4)。与未治疗的感染组相比,单独使用葡糖胺锑钠以及葡糖胺锑钠加特比萘芬(2.5±0.2和4.2±0.6)显著降低了脾脏重量。即便如此,脾脏寄生虫负荷与脾脏重量直接相关。按所用剂量和疗程单独使用特比萘芬对感染恰加斯利什曼原虫的仓鼠的脾脏寄生虫负荷或脾脏相对重量没有影响。
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