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Circulating inflammatory mediators as biomarkers of ocular toxoplasmosis in acute and in chronic infection

Ana Paula Trovatti Uetanabaro, Luara Isabela dos Santos, Priscilla Miranda Henriques, Ester Roffê, Daniel V. Vasconcelos-Santos, Alan Sher, Dragana Janković, Matheus de Souza Gomes, Laurence Rodrigues do Amaral, Ana Carolina Campi‐Azevedo, Andréa Teixeira‐Carvalho, Olindo Assis Martins‐Filho, Ricardo T. Gazzinelli, Lis Ribeiro do Valle Antonelli

2020Journal of Leukocyte Biology22 citationsDOI

Abstract

Toxoplasmosis is highly endemic worldwide. In Brazil, depending on the geographical region and socioeconomic status, 40-70% of individuals become seropositive at some point in their lives. A significant proportion of Toxoplasma gondii-chronically infected individuals who are otherwise immunocompetent develop recurrent ocular lesions. The inflammatory/immune mechanisms involved in development of ocular lesion are still unknown and, despite previous investigation, there are no reliable immune biomarkers to predict/follow disease outcome. To better understand the impact of the immune response on parasite control and immunopathology of ocular toxoplasmosis, and to provide insights on putative biomarkers for disease monitoring, we assessed the production of a large panel of circulating immune mediators in a longitudinal study of patients with postnatally acquired toxoplasmosis stratified by the presence of ocular involvement, both at the early acute stage and 6 months later during chronic infection, correlating them with presence of ocular involvement. We found that T. gondii-infected patients, especially during the acute stage of the disease, display high levels of chemokines, cytokines, and growth factors involved in the activation, proliferation, and migration of inflammatory cells to injured tissues. In particular, major increases were found in the IFN-induced chemokines CXCL9 and CXCL10 in T. gondii-infected patients regardless of disease stage or clinical manifestations. Moreover, a specific subgroup of circulating cytokines and chemokines including GM-CSF, CCL25, CCL11, CXCL12, CXCL13, and CCL2 was identified as potential biomarkers that accurately distinguish different stages of infection and predict the occurrence of ocular toxoplasmosis. In addition to serving as predictors of disease development, these host inflammatory molecules may offer promise as candidate targets for therapeutic intervention.

Topics & Concepts

ToxoplasmosisImmunologyChemokineToxoplasma gondiiImmune systemBiologyCXCL9DiseaseCXCL10MedicinePathologyAntibodyToxoplasma gondii Research StudiesHerpesvirus Infections and TreatmentsImmune Response and Inflammation
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