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首页> 外文期刊>APMIS: Acta Pathologica, Microbiologica et Immunologica Scandinavica >Praziquantel efficacy in mice infected with PZQ non-susceptible S. mansoni isolate treated with artemether: parasitological, biochemical and immunohistochemical assessment.
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Praziquantel efficacy in mice infected with PZQ non-susceptible S. mansoni isolate treated with artemether: parasitological, biochemical and immunohistochemical assessment.

机译:吡喹酮在用蒿甲醚处理的感染了PZQ的非敏感曼氏沙门氏菌的小鼠中的功效:寄生虫学,生化和免疫组化评估。

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摘要

Based on the fact that artemether (ART) affects immature schistosomes and that the effect of praziquantel (PZQ) mainly targets mature schistosomes, this work investigates the possible enhanced efficacy of PZQ in combination with ART in mice harboring a PZQ non-susceptible Schistosoma mansoni isolate. Associated schistosomal, inflammatory, hepatic histopathological changes have been investigated by examining the tissue markers expressing apoptosis using FAS (CD95), anti-apoptosis (Bcl2) and angiogenesis [vascular endothelial growth factor (VEGF)]. A batch of Swiss albino mice infected with a PZQ non-susceptible (EE10) S. mansoni isolate was divided into 12 groups. Animals of the first group were left without treatment as infected controls, while groups 2-6 received PZQ in increasing doses. The animals of group 7 received ART in double doses. Those comprising groups 8-12 received combined therapy of PZQ and ART in the same doses and at the same timings postinfection (PI) as those belonging to groups 2-6. Parasitological parameters, liver function, and histopathological and immunohistochemical studies of FAS, Bcl2 and VEGF antibodies were assessed. Combined administration of ART and PZQ reduced the ED(50) (the dose at which the worm burden was decreased by 50%) of PZQ. Typical granulomas were not seen in animals treated with ART alone and combined with PZQ, with least expression of FAS and VEGF and increased expression of Bcl2. The minimal histopathological changes recorded in mice treated with both ART and PZQ could be related to a synergistic/additive effect of ART, markedly reducing the intensity of infection. Improved liver function tests support the less severe histopathological changes under the influence of this treatment protocol. This study encourages human trials especially in areas where malaria is not endemic, and differing combination doses should be investigated in view of the antagonistic effect noticed with some dose regimens.
机译:基于蒿甲醚(ART)影响未成熟的血吸虫和吡喹酮(PZQ)的作用主要针对成熟的血吸虫这一事实,这项工作研究了PZQ与ART联合在携带PZQ非易感性曼氏血吸虫分离株的小鼠中的增强功效。通过使用FAS(CD95),抗凋亡(Bcl2)和血管生成[血管内皮生长因子(VEGF)]检测表达凋亡的组织标志物,研究了相关的血吸虫,炎性,肝组织病理学改变。将一批感染了不易感染PZQ(EE10)曼氏沙门氏菌的瑞士白化病小鼠分为12组。第一组动物未经治疗即作为感染的对照组,而第2-6组动物则以递增剂量接受PZQ。第7组的动物接受双重剂量的ART。包含第8-12组的患者接受了与属于第2-6组的患者相同的剂量和感染后(PI)相同时间的PZQ和ART联合治疗。评估了FAS,Bcl2和VEGF抗体的寄生虫学参数,肝功能以及组织病理学和免疫组化研究。 ART和PZQ的联合给药可降低PZQ的ED(50)(蠕虫负担减少50%的剂量)。在单独用ART和PZQ联合治疗的动物中未见典型的肉芽肿,FAS和VEGF的表达最少,Bcl2的表达增加。用ART和PZQ治疗的小鼠中记录的最小组织病理学变化可能与ART的协同/累加作用有关,从而显着降低了感染强度。在该治疗方案的影响下,改善的肝功能测试可支持不太严重的组织病理学改变。这项研究鼓励人类进行试验,尤其是在疟疾不是地方流行的地区,鉴于某些剂量方案具有明显的拮抗作用,应研究不同的联合剂量。

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