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经胃肠道接种和苯达唑治疗对瑞士小鼠感染克氏锥虫(Y 株,DTU TcII)的影响。

Impact of gastrointestinal inoculation and benznidazole treatment on infection by Trypanosoma cruzi (Y strain, DTU TcII) in Swiss mice.

机构信息

Postgraduate Program in Health Sciences, Health Sciences Center, State University of Maringá, Maringá, 87.020.900, Brazil.

Postgraduate Program in Biological Sciences, Biological Sciences Center, State University of Maringá, Maringá, 87.020.900, Brazil.

出版信息

Exp Parasitol. 2024 Oct;265:108810. doi: 10.1016/j.exppara.2024.108810. Epub 2024 Aug 10.

DOI:10.1016/j.exppara.2024.108810
PMID:39134115
Abstract

In Brazil, where Chagas disease is endemic, the most frequent form of transmission of the parasite is the oral route, associated with greater severity and worse response to benznidazole (BZ), the drug used in its treatment. This study aimed to evaluate the impact of gastrointestinal infection (GI) and BZ treatment on the parasitological and histopathological parameters in mice inoculated with a strain of T. cruzi II. Swiss mice were inoculated by GI and intraperitoneal (IP) routes with 2x10 culture-derived metacyclic trypomastigotes of the Y strain (TcII) of T. cruzi and were treated with BZ in the acute phase of the infection. Fresh blood examination, qPCR, histopathological and biochemical evaluations (enzymatic dosages and oxidative stress-OS) were performed. BZ treatment of uninfected animals caused changes in the liver, increased the activity of aspartate aminotransferase and alanine aminotransferase enzymes and OS, showing that the drug alone affects this organ. Inflammation and necrosis in the cardiac tissue were less intense and deaths occurred later in animals inoculated via the GI route than the animals inoculated via the IP route. BZ reduced the intensity of tissue lesions and avoided lethality in animals inoculated via the GI route, and decreased parasitemia and OS in those inoculated via both routes. Although BZ alone caused liver damage, it was less intense than that caused by both routes of inoculation. Infection with the Y strain of T. cruzi II via the GI route proved to be less virulent and pathogenic and responded better to treatment than the infection acquired via the IP route.

摘要

在恰加斯病流行的巴西,寄生虫最常见的传播途径是经口传播,与更严重的疾病和更差的苯并咪唑(BZ)治疗反应有关,BZ 是用于治疗的药物。本研究旨在评估胃肠道感染(GI)和 BZ 治疗对感染 T. cruzi II 株的小鼠寄生虫学和组织病理学参数的影响。瑞士小鼠通过 GI 和腹腔(IP)途径接种 2x10 个来源于培养的 Y 株(TcII)T. cruzi 的环二型滋养体,并在感染的急性阶段用 BZ 治疗。进行了新鲜血液检查、qPCR、组织病理学和生化评估(酶剂量和氧化应激-OS)。未感染动物的 BZ 治疗导致肝脏发生变化,增加天冬氨酸转氨酶和丙氨酸转氨酶酶的活性和 OS,表明药物单独影响该器官。与通过 IP 途径接种的动物相比,通过 GI 途径接种的动物的心脏组织中的炎症和坏死程度较轻,死亡发生较晚。BZ 降低了组织损伤的强度,并避免了通过 GI 途径接种的动物的致死性,同时降低了通过两种途径接种的动物的寄生虫血症和 OS。尽管 BZ 单独引起肝脏损伤,但与通过两种接种途径引起的损伤相比,其损伤程度较轻。通过 GI 途径感染 T. cruzi II 的 Y 株证明其毒力和致病性较低,对治疗的反应优于通过 IP 途径获得的感染。

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