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Related Pentacyclic Triterpenes Have Immunomodulatory Activity in Chronic Experimental Visceral Leishmaniasis

机译:相关五环素三萜患者在慢性实验内脏Leishmaniaisis中具有免疫调节活性

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Leishmaniasis is a neglected tropical disease caused by the flagellated protozoa of the genus Leishmania that affects millions of people around the world. Drugs employed in the treatment of leishmaniasis have limited efficacy and induce local and systemic side effects to the patients. Natural products are an interesting alternative to treat leishmaniasis, because some purified molecules are selective toward parasites and not to the host cells. Thus, the aim of the present study was to compare the in vitro antileishmanial activity of the triterpenes betulin (Be), lupeol (Lu), and ursolic acid (UA); analyze the physiology and morphology of affected organelles; analyze the toxicity of selected triterpenes in golden hamsters; and study the therapeutic activity of triterpenes in hamsters infected with L. ( L. ) infantum as well as the cellular immunity induced by studied molecules. The triterpenes Lu and UA were active on promastigote ( and ? μ M, respectively) and amastigote forms ( and ? μ M, respectively) of L. ( L. ) infantum , and their selectivity indexes (SI) toward amastigote forms were higher (≥13.4 and 14, respectively) than SI of miltefosine (2.7). L. ( L. ) infantum promastigotes treated with Lu and UA showed cytoplasmic degradation, and in some of these areas, cell debris were identified, resembling autophagic vacuoles, and parasite mitochondria were swelled, fragmented, and displayed membrane potential altered over time. Parasite cell membrane was not affected by studied triterpenes. Studies of toxicity in golden hamster showed that Lu did not alter blood biochemical parameters associated with liver and kidney functions; however, a slight increase of aspartate aminotransferase level in animals treated with 2.5?mg/kg of UA was detected. Lu and UA triterpenes eliminated amastigote forms in the spleen (87.5 and 95.9% of reduction, respectively) and liver of infected hamster (95.9 and 99.7% of reduction, respectively); and UA showed similar activity at eliminating amastigote forms in the spleen and liver than amphotericin B (99.2 and 99.8% of reduction). The therapeutic activity of both triterpenes was associated with the elevation of IFN- γ and/or iNOS expression in infected treated animals. This is the first comparative work showing the in vitro activity, toxicity, and therapeutic activity of Lu and UA in the chronic model of visceral leishmaniasis caused by L. ( L. ) infantum ; additionally, both triterpenes activated cellular immune response in the hamster model of visceral leishmaniasis.
机译:利什曼病是由利什曼属影响数以百万计的世界各地的人们的鞭毛的原虫一个被忽视的热带疾病。在利什曼病的治疗中使用的药物具有有限的效力和诱导局部和全身性副作用的患者。天然产品是一个有趣的替代治疗利什曼病,因为有些纯化的分子是有选择性的对寄生虫和不宿主细胞。因此,本研究的目的是比较的三萜类化合物桦木醇的体外活性antileishmanial(BE),羽扇豆醇(路),和熊果酸(UA);分析生理学和影响细胞器的形态;分析金仓鼠选择三萜类化合物的毒性;并研究在感染了L.(L.)婴儿以及通过研究分子诱导细胞免疫的仓鼠三萜类化合物的治疗活性。所述三萜烯Lu和UA上的有效的前鞭毛体(和βμ男,分别地)和无鞭毛体的形式(和βμ男,分别地)的L.(L.)婴儿,和它们的选择性指数(SI)朝向无鞭毛体形式的较高( ≥13.4和14,分别地)比米替福新的SI(2.7)。与路和UA处理L.(L.)前鞭毛体的婴儿表明细胞质降解,并且在一些领域,细胞碎片被确定,类似自噬泡,和寄生虫线粒体肿胀,片段化,并显示随时间改变膜电位。寄生虫细胞膜并没有受到影响研究的三萜类化合物。金黄地鼠胚胎毒性的研究表明,鲁做肝肾功能相关不改变血液生化指标;然而,检测到天冬氨酸转氨酶水平的在2.5?毫克/千克UA的治疗的动物略有增加。路和UA三萜类化合物在脾(分别减少87.5和95.9%,)和被感染的仓鼠(分别减少95.9和99.7%,)的肝消除无鞭毛体形式;和UA表现出相似的活性,以消除在脾脏和肝脏比两性霉素B(减少99.2和99.8%)无鞭毛体形式。两个三萜类化合物的治疗活性与IFN-γ和/或iNOS的表达在感染治疗的动物的高度相关联。这是示出了体外活性,毒性的第一比较工作,并在引起L.(L.)婴儿内脏利什曼病的慢性模型路和UA的治疗活性;另外,无论是三萜类激活内脏利什曼病的仓鼠模型细胞免疫应答。

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