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Curcumin Enhances the Anti-Trypanosoma cruzi Activity of Benznidazole-Based Chemotherapy in Acute Experimental Chagas Disease

机译:姜黄素增强急性实验性南美锥虫病基于苯并咪唑的化学疗法的克氏锥虫活性

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摘要

Although curcumin can increase the effectiveness of drugs against malaria, combination therapies using the molecule have never been investigated in Chagas disease (ChD). Therefore, we evaluated the efficacy of curcumin as a complementary strategy to benznidazole (Bz)-based chemotherapy in mice acutely infected with Trypanosoma cruzi. Eighty-four 12-week-old Swiss mice were equally randomized into seven groups: uninfected (NI), T. cruzi infected and untreated (INF), infected and treated with 100 mg/kg of body weight Bz (B100), 50 mg/kg Bz (B50), 100 mg/kg curcumin (C100), 100 mg/kg Bz plus 100 mg/kg curcumin (B100 plus C100), and 50 mg/kg Bz plus 100 mg/kg curcumin (B50 plus C100). After microscopic identification of blood trypomastigotes (4 days after inoculation), both drugs were administered by gavage once a day for 20 days. Curcumin showed limited antiparasitic, anti-inflammatory, and antioxidant effects when administered alone. When curcumin and Bz were combined, there was a drastic reduction in parasitemia, parasite load, mortality, anti-T. cruzi IgG reactivity, circulating levels of cytokines (gamma interferon [IFN-γ], interleukin 4 [IL-4], and MIP1-α), myocardial inflammation, and morphological and oxidative cardiac injury; these results exceeded the isolated effects of Bz. The combination of Bz and curcumin was also effective at mitigating liver toxicity triggered by Bz, increasing the parasitological cure rate, and preventing infection recrudescence in noncured animals, even when the animals were treated with 50% of the recommended therapeutic dose of Bz. By limiting the toxic effects of Bz and enhancing its antiparasitic efficiency, the combination of the drug with curcumin may be a relevant therapeutic strategy that is possibly better tolerated in ChD treatment than Bz-based monotherapy.
机译:尽管姜黄素可以提高抗疟疾药物的功效,但尚未在南美锥虫病(ChD)中研究使用该分子的联合疗法。因此,我们评估了姜黄素作为基于苯并硝唑(Bz)的化学疗法在急性感染克鲁斯锥虫的小鼠中的补充策略的功效。将84只12周龄的瑞士小鼠随机分为7组:未感染(NI),克氏锥虫感染和未治疗(INF),用100 mg / kg体重Bz(B100),50 mg感染和治疗/ kg Bz(B50),100 mg / kg姜黄素(C100),100 mg / kg Bz加100 mg / kg姜黄素(B100加C100)和50 mg / kg Bz加100 mg / kg姜黄素(B50加C100) 。在显微镜下鉴定出血液中的锥虫病后(接种后4天),两种药物每天一次经管饲法给药,共20天。姜黄素单独给药时显示出有限的抗寄生虫,抗炎和抗氧化作用。当姜黄素和Bz合并使用时,寄生虫血症,寄生虫负荷,死亡率和抗T素都大大降低。 cruzi IgG反应性,细胞因子(γ干扰素[IFN-γ],白介素4 [IL-4]和MIP1-α)的循环水平,心肌炎症以及形态和氧化性心脏损伤;这些结果超出了Bz的孤立作用。 Bz和姜黄素的组合还可以有效减轻Bz触发的肝毒性,提高寄生虫治愈率,并在未治愈的动物中预防感染复发,即使使用50%推荐治疗剂量的Bz治疗动物。通过限制Bz的毒性作用并增强其抗寄生虫功效,该药物与姜黄素的组合可能是一种相关的治疗策略,在ChD治疗中可能比基于Bz的单一疗法耐受性更好。

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