Hevillyn Fernanda Lucas da Silva , Marcella Paula Mansano Sarto , Ana Paula de Abreu , Nilma de Souza Fernandes , Ingrid Giarola Matias dos Santos , João Vitor de Souza Trovo , Aline Francieli da Silva , Alice Maria Souza-Kaneshima , Jurandir Fernando Comar , Max Jean de Ornelas Toledo
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引用次数: 0
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 2x106 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.
在恰加斯病流行的巴西,最常见的寄生虫传播途径是口服,其严重程度更高,对治疗药物苯并咪唑(BZ)的反应更差。本研究的目的是评估胃肠道感染(GI)和 BZ 治疗对接种了 T. cruzi II 株系的小鼠的寄生虫学和组织病理学参数的影响。通过胃肠道和腹膜内(IP)途径给瑞士小鼠接种 2x106 株培养衍生的 Y 株(TcII)胰母细胞,并在感染的急性期用 BZ 治疗。进行了鲜血检查、qPCR、组织病理学和生化评估(酶剂量和氧化应激-OS)。用 BZ 治疗未感染的动物会导致肝脏发生变化,增加天冬氨酸氨基转移酶和丙氨酸氨基转移酶的活性以及氧化应激,这表明该药物会单独影响肝脏。与通过 IP 途径接种的动物相比,通过 GI 途径接种的动物心脏组织的炎症和坏死程度较轻,死亡时间较晚。BZ 可减轻胃肠道接种动物的组织病变程度,避免其死亡,并可降低两种途径接种动物的寄生虫血症和 OS。虽然单独使用 BZ 会造成肝脏损伤,但其强度低于两种接种途径造成的损伤。事实证明,通过消化道途径感染克柔兹Ⅱ号Y株的毒性和致病性较低,对治疗的反应也比通过IP途径感染要好。
期刊介绍:
Experimental Parasitology emphasizes modern approaches to parasitology, including molecular biology and immunology. The journal features original research papers on the physiological, metabolic, immunologic, biochemical, nutritional, and chemotherapeutic aspects of parasites and host-parasite relationships.