T and B lymphocytes in the brains of dogs with concomitant seropositivity to three pathogenic protozoans: Leishmania chagasi, Toxoplasma gondii and Neospora caninum.

BMC Res Notes

Laboratory of Applied Pathology-LAPAP, College of Veterinary Medicine, UNESP-Univ Estadual Paulista, Rua Clóvis Pestana 739, CEP 16050-680, Araçatuba, São Paulo, Brazil.

Published: June 2013

AI Article Synopsis

  • Visceral leishmaniasis can cause variable clinical symptoms in humans and dogs, and may lead to neurological disorders in infected dogs, which prompted a study comparing lymphocyte populations in the brains of dogs infected with different pathogens.
  • Inflammatory lesions characterized by the accumulation of CD3+ T lymphocytes were found in various brain regions across all infected groups, while CD79α+ B lymphocytes were present in low quantities with no significant differences among the groups.
  • The study concludes that L. chagasi infection alone can lead to lymphocyte influx in the brain, and co-infections with T. gondii and N. caninum do not worsen brain lesions or inflammation, highlighting the brain as a potentially affected organ in visceral leishmaniasis

Article Abstract

Background: Visceral leishmaniasis is a disease with great variability regarding the clinical manifestations in humans and dogs. Chronically infected dogs may develop neurological disorders, however, there are few reports that characterize the lesions and make clear the pathogenesis of the canine cerebral leishmaniasis. Concomitant with Leishmania chagasi, dogs may be infected by opportunistic pathogens, such as Toxoplasma gondii and Neospora caninum, which may contribute to the occurrence of lesions in the central nervous system. Hence, we aimed to compare the T and B lymphocytes population in the brains of infected dogs with seropositivity to L. chagasi, T. gondii and N. caninum concurrently (n = 24), seropositivity only to L. chagasi (n = 31), and seropositivity to T. gondii and N. caninum (n = 16). Uninfected dogs were used as control (n = 10).

Results: Inflammatory lesions, characterised by mononuclear cell accumulation, composed mainly of CD3+ T lymphocytes predominated in several encephalic regions of the dogs from all the three infected groups, with no difference among them (P = 0.0004), whereas CD79α+ B lymphocytes were detected in very small intensity and presented no difference among groups (P = 0.5313). Furthermore, no association among diseases was detected at the serological enquire.

Conclusions: We demonstrate that the peripheral infection by L. chagasi per se can promote the influx of lymphocytes within the nervous milieu as occurs during Toxoplasma and Neospora infections, and the concomitant seropositivity against these pathogens does not exacerbate the inflammatory brain lesions. Therefore, these findings give additional support that the brain should be included in the list of organs affected by visceral leishmaniasis and that even asymptomatic infected dogs may develop brain lesions.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3701587PMC
http://dx.doi.org/10.1186/1756-0500-6-226DOI Listing

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