Association Between Canine Leishmaniosis and Ehrlichia Canis Co-infection: a Prospective Case-control Study

Overview

Journal Parasit Vectors

Publisher Biomed Central

Specialties Parasitology
Tropical Medicine

Date 2018 Mar 21

PMID 29554932

Citations 18

Authors

Charalampos Attipa

Laia Solano-Gallego

Kostas Papasouliotis

Francesca Soutter

David Morris

Chris Helps

Scott Carver

Severine Tasker

Affiliations

Soon will be listed here.

Abstract

Background: In the Mediterranean basin, Leishmania infantum is a major cause of disease in dogs, which are frequently co-infected with other vector-borne pathogens (VBP). However, the associations between dogs with clinical leishmaniosis (ClinL) and VBP co-infections have not been studied. We assessed the risk of VBP infections in dogs with ClinL and healthy controls.

Methods: We conducted a prospective case-control study of dogs with ClinL (positive qPCR and ELISA antibody for L. infantum on peripheral blood) and clinically healthy, ideally breed-, sex- and age-matched, control dogs (negative qPCR and ELISA antibody for L. infantum on peripheral blood) from Paphos, Cyprus. We obtained demographic data and all dogs underwent PCR on EDTA-blood extracted DNA for haemoplasma species, Ehrlichia/Anaplasma spp., Babesia spp., and Hepatozoon spp., with DNA sequencing to identify infecting species. We used logistic regression analysis and structural equation modelling (SEM) to evaluate the risk of VBP infections between ClinL cases and controls.

Results: From the 50 enrolled dogs with ClinL, DNA was detected in 24 (48%) for Hepatozoon spp., 14 (28%) for Mycoplasma haemocanis, 6 (12%) for Ehrlichia canis and 2 (4%) for Anaplasma platys. In the 92 enrolled control dogs, DNA was detected in 41 (45%) for Hepatozoon spp., 18 (20%) for M. haemocanis, 1 (1%) for E. canis and 3 (3%) for A. platys. No Babesia spp. or "Candidatus Mycoplasma haematoparvum" DNA was detected in any dog. No statistical differences were found between the ClinL and controls regarding age, sex, breed, lifestyle and use of ectoparasitic prevention. A significant association between ClinL and E. canis infection (OR = 12.4, 95% CI: 1.5-106.0, P = 0.022) was found compared to controls by multivariate logistic regression. This association was confirmed using SEM, which further identified that younger dogs were more likely to be infected with each of Hepatozoon spp. and M. haemocanis, and dogs with Hepatozoon spp. were more likely to be co-infected with M. haemocanis.

Conclusions: Dogs with ClinL are at a higher risk of co-infection with E. canis than clinically healthy dogs. We recommend that dogs diagnosed with ClinL should be tested for E. canis co-infection using PCR.

Citing Articles

Meta-analysis of tick-borne and other pathogens: Co-infection or co-detection? That is the question.

Porcelli S, Deshuillers P, Moutailler S, Lagree A Curr Res Parasitol Vector Borne Dis. 2024; 6:100219.

PMID: 39483631 PMC: 11525461. DOI: 10.1016/j.crpvbd.2024.100219.

Ehrlichia spp. infection worsens cardiac damage in dogs with canine visceral leishmaniasis.

Zanfagnini L, Reis Junior J, Rocha V, Souza S, Hitara K, Marcondes M Rev Bras Parasitol Vet. 2024; 33(2):e018223.

PMID: 38836809 PMC: 11253817. DOI: 10.1590/S1984-29612024023.

Synthetic Peptides Selected by Immunoinformatics as Potential Tools for the Specific Diagnosis of Canine Visceral Leishmaniasis.

Moreira G, Maia R, Soares N, Ostolin T, Coura-Vital W, Aguiar-Soares R Microorganisms. 2024; 12(5).

PMID: 38792746 PMC: 11123790. DOI: 10.3390/microorganisms12050906.

Modulation of Macrophage Redox and Apoptotic Processes to during Coinfection with the Tick-Borne Bacteria .

Pessoa-Pereira D, Scorza B, Cyndari K, Beasley E, Petersen C Pathogens. 2023; 12(9).

PMID: 37764937 PMC: 10537792. DOI: 10.3390/pathogens12091128.

[Circulación de Leishmania infantum y Trypanosoma cruzi en perros domésticos de áreas urbanas de Sincelejo, región Caribe de Colombia].

Rueda-Concha K, Payares-Mercado A, Guerra-Castillo J, Melendrez J, Arroyo-Munive Y, Martinez-Abad L Biomedica. 2022; 42(4):633-649.

PMID: 36511676 PMC: 9814371. DOI: 10.7705/biomedica.6369.

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