Your search keyword '"D. Yanguas-Pérez"' showing total 2 results

1. The route of Besnoitia besnoiti tachyzoites inoculation does not influence the clinical outcome of the infection in calves

Author

P.L. Brum, Luis Miguel Ortega-Mora, Javier Blanco-Murcia, Carlos Diezma-Díaz, D. Yanguas-Pérez, Marta González-Huecas, Ignacio Ferre, Gema Álvarez-García, Alejandro Jiménez-Meléndez, M. Pizarro-Díaz, Enrique Tabanera, and Michela Re

Subjects

0301 basic medicine, Male, Pathology, medicine.medical_specialty, Injections, Intradermal, 030231 tropical medicine, Antibodies, Protozoan, Cattle Diseases, Lymphadenopathy, Biology, 03 medical and health sciences, 0302 clinical medicine, Immune system, Subcutaneous Absorption, medicine, Animals, Respiratory system, Besnoitiosis, Innate immune system, General Veterinary, Intradermal route, Experimental model, Inoculation, Coccidiosis, General Medicine, 030108 mycology & parasitology, Besnoitia besnoiti, biology.organism_classification, Immunity, Humoral, Disease Models, Animal, Immunoglobulin G, Sarcocystidae, Parasitology, Cattle

Abstract

In a previous attempt, an experimental model of bovine besnoitiosis was established in calves that were intravenously inoculated with different doses of Besnoitia besnoiti tachyzoites. Despite the fact that all infected calves developed the acute stage of disease, only microscopic findings characteristic of chronic besnoitiosis were reported. In the present study, calves were inoculated by subcutaneous and intradermal routes with B. besnoiti tachyzoites with the aim of developing clinical signs and macroscopic lesions characteristic of chronic besnoitiosis. Nine 3-month-old male calves were randomly distributed into three groups of three animals each. Next, 106 tachyzoites were inoculated by either the subcutaneous (G1) or intradermal route (G2). The negative control group (G3) was inoculated with PBS. Daily clinical monitoring and regular blood collection were performed. At 70 days post-infection (pi), animals were euthanized, and tissues were collected to investigate lesions and parasites. Infected animals developed mild-moderate acute besnoitiosis characterized by lymphadenopathy from four days to 47 days pi, and sporadic fever peaks were only observed in one calf from G2. However, other clinical signs and macroscopic lesions characteristic of chronic besnoitiosis were not detected. Only nine tissue samples were B. besnoiti-DNA-positive, eight of which belonged to reproductive and respiratory tracts tissues from G1. Finally, the kinetics of the immune responses were similar in both infected groups. However, delayed and lower cellular and humoral immune responses were observed in G1 followed by G2 and were compared with intravenously inoculated calves. The differences observed among the three inoculation routes could be due to different effector mechanisms of the host early innate immune response against B. besnoiti. Accordingly, the inoculation route of B. besnoiti tachyzoites does not significantly influence the clinical outcome of the infection in calves. Thus, a further refinement of this experimental model of bovine besnoitiosis is needed to reproduce macroscopic lesions characteristic of chronic stage disease.

Published

2018

2. The route of Besnoitia besnoiti tachyzoites inoculation does not influence the clinical outcome of the infection in calves.

Author

Diezma-Díaz C, Ferre I, Re M, Jiménez-Meléndez A, Tabanera E, González-Huecas M, Pizarro-Díaz M, Yanguas-Pérez D, Brum PL, Blanco-Murcia J, Ortega-Mora LM, and Álvarez-García G

Subjects

Animals, Antibodies, Protozoan blood, Cattle, Cattle Diseases parasitology, Immunity, Humoral, Immunoglobulin G blood, Injections, Intradermal, Lymphadenopathy etiology, Lymphadenopathy parasitology, Male, Sarcocystidae, Subcutaneous Absorption, Cattle Diseases prevention & control, Coccidiosis veterinary, Disease Models, Animal

Abstract

In a previous attempt, an experimental model of bovine besnoitiosis was established in calves that were intravenously inoculated with different doses of Besnoitia besnoiti tachyzoites. Despite the fact that all infected calves developed the acute stage of disease, only microscopic findings characteristic of chronic besnoitiosis were reported. In the present study, calves were inoculated by subcutaneous and intradermal routes with B. besnoiti tachyzoites with the aim of developing clinical signs and macroscopic lesions characteristic of chronic besnoitiosis. Nine 3-month-old male calves were randomly distributed into three groups of three animals each. Next, 10 6 tachyzoites were inoculated by either the subcutaneous (G1) or intradermal route (G2). The negative control group (G3) was inoculated with PBS. Daily clinical monitoring and regular blood collection were performed. At 70 days post-infection (pi), animals were euthanized, and tissues were collected to investigate lesions and parasites. Infected animals developed mild-moderate acute besnoitiosis characterized by lymphadenopathy from four days to 47 days pi, and sporadic fever peaks were only observed in one calf from G2. However, other clinical signs and macroscopic lesions characteristic of chronic besnoitiosis were not detected. Only nine tissue samples were B. besnoiti-DNA-positive, eight of which belonged to reproductive and respiratory tracts tissues from G1. Finally, the kinetics of the immune responses were similar in both infected groups. However, delayed and lower cellular and humoral immune responses were observed in G1 followed by G2 and were compared with intravenously inoculated calves. The differences observed among the three inoculation routes could be due to different effector mechanisms of the host early innate immune response against B. besnoiti. Accordingly, the inoculation route of B. besnoiti tachyzoites does not significantly influence the clinical outcome of the infection in calves. Thus, a further refinement of this experimental model of bovine besnoitiosis is needed to reproduce macroscopic lesions characteristic of chronic stage disease., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019