Liver Histopathological and Immunohistochemical Evaluation from Fasciola hepatica Experimentally Infected and Reinfected Sheep

Author:

Herrera-Torres Guillem1ORCID,Ruiz-Campillo María T.1ORCID,Bautista María J.1ORCID,Martínez-Moreno Francisco J.2ORCID,Zafra Rafael2ORCID,Buffoni Leandro2ORCID,Rufino-Moya Pablo J.2,Martínez-Moreno Álvaro2ORCID,Molina-Hernández Verónica1ORCID,Pérez José1ORCID

Affiliation:

1. Departamento de Anatomía y Anatomía Patológica Comparadas y Toxicología, UIC Zoonosis y Enfermedades Emergentes (ENZOEM), Universidad de Córdoba, 14014 Córdoba, Spain

2. Departamento de Sanidad Animal, Área de Parasitología, UIC Zoonosis y Enfermedades Emergentes (ENZOEM), Universidad de Córdoba, 14014 Córdoba, Spain

Abstract

Fasciolosis is an important economic disease of livestock. There is a global interest in the development of protective vaccines since the current anthelmintic therapy is no longer sustainable. A better knowledge of the host–parasite interaction is needed to design effective vaccines. To date, few studies have evaluated host–parasite interaction by comparing infected and reinfected animals. The present study evaluates the microscopical hepatic lesions in sheep infected and reinfected with Fasciola hepatica during the acute and chronic stages of infection. The histopathological study revealed the presence of necrotizing foci (NF1) associated with larvae migration during the early stages of infection in the primoinfected (PI) and reinfected (RI) groups. In the late stages of infection of the PI group and at the early and late stages of infection in the RI groups, extensive necrotizing/hemorrhagic foci (NF2) were found in the vicinity of enlarged bile ducts, some containing adult flukes, suggesting parasites may have caused NF2 while feeding. The immunohistochemical study revealed an increase in Foxp3+ T cells in both PI and RI groups with respect to the UC group and in the infiltrates adjacent to NF1 in the RI groups with respect to the PI group, suggesting the F. hepatica induce Foxp3 T cell expansion to facilitate parasite survival. In addition, in both the PI and RI groups, and during acute and chronic stages of the infection, a poor expression of iNOS was found accompanied by a strong expression of CD163, suggesting a marked M2 activation of macrophages in the hepatic lesions, which may be related with healing processes, and it also may facilitate parasite survival. The main differences between PI and RI animals were the more severe infiltration of eosinophils and Foxp3+ T cells, whereas RI did not modify M2 activation of macrophages which occurs since the early stages of primoinfection.

Funder

Spanish Ministry of Science and Innovation

Regional Government of Andalusia-FEDER

Publisher

MDPI AG

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