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经口接种不同发育阶段的克氏锥虫 I 和 II 对小鼠感染的演变。

Evolution of infection in mice inoculated by the oral route with different developmental forms of Trypanosoma cruzi I and II.

机构信息

Post-Graduate Program in Health Sciences at the State University of Maringá (UEM), Av. Colombo 5790, Bloco 126, CEP 87020-900 Maringá, Paraná, Brazil.

出版信息

Exp Parasitol. 2013 Nov;135(3):511-7. doi: 10.1016/j.exppara.2013.08.013. Epub 2013 Aug 29.

Abstract

Oral infection has become the most important transmission mechanism of Chagas disease in Brazil. For this study, the development of Trypanosoma cruzi infection in mice, induced by the oral and intraperitoneal (IP) routes, was compared. Four groups of Swiss mice were used to evaluate the influence of parasite genetics, number of parasites, inoculation volume and developmental stages on the development of the orally induced infection: 1 - blood trypomastigotes (BT) via oral; 2 - BT via IP; 3 - culture metacyclic trypomastigotes (MT) via oral; and 4 - culture MT via IP. Animals inoculated orally showed levels of parasitemia, as well as infectivity and mortality rates, lower than animals inoculated via IP, regardless of DTU (discrete typing unit) and inoculum. Animals infected with TcII showed higher levels of these parameters than did animals infected with TcI. The larger volume of inoculum showed a greater capacity to cause an infection when administered via the oral route. BT infection was more virulent than culture MT infection for both routes (oral and IP). However, mice inoculated orally with BT showed lower levels than via IP, while mice inoculated orally with culture MT showed similar levels of infection to those inoculated via IP. Mice inoculated with culture MT showed more histopathological changes than those inoculated with BT, regardless of the inoculation route. These results indicate that this alternative experimental model is useful for evaluating infection by T. cruzi isolates with subpatent parasitemia and low virulence, such as those belonging to the TcI and TcIV DTUs, which are prevalent in outbreaks of orally transmitted Chagas disease.

摘要

口腔感染已成为巴西恰加斯病最重要的传播机制。在这项研究中,比较了经口和腹腔内(IP)途径诱导的克氏锥虫感染在小鼠中的发展。使用四组瑞士小鼠来评估寄生虫遗传学、寄生虫数量、接种量和发育阶段对经口诱导感染发展的影响:1-经口血锥虫(BT);2-BT 经 IP;3-经口培养循环运动锥虫(MT);4-经 IP 培养 MT。经口接种的动物表现出比经 IP 接种的动物更低的寄生虫血症水平、感染率和死亡率,无论 DTU(离散分型单位)和接种物如何。感染 TcII 的动物比感染 TcI 的动物表现出更高的这些参数水平。通过口服途径接种更大体积的接种物显示出更大的感染能力。BT 感染比经口和 IP 途径的培养 MT 感染更具毒性。然而,经口接种 BT 的小鼠比经 IP 接种的小鼠表现出更低的水平,而经口接种培养 MT 的小鼠表现出与经 IP 接种的小鼠相似的感染水平。经口接种培养 MT 的小鼠比经口接种 BT 的小鼠表现出更多的组织病理学变化,无论接种途径如何。这些结果表明,这种替代实验模型可用于评估具有亚显性寄生虫血症和低毒力的 T. cruzi 分离物的感染,例如属于 TcI 和 TcIV DTU 的分离物,这些分离物在经口传播的恰加斯病暴发中很常见。

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