Chronic infection with the protozoan Toxoplasma gondii prevents the development of experimental atopic dermatitis in mice

•Study of T. gondii immune-modulation in an atopic dermatitis mouse model.•Sensitization during chronic toxoplasmosis results in a lower atopic dermatitis.•Chronic infection prevents TH2 and TH1 allergen specific response.•Infection decrease type 2 innate cytokines during allergen sensitization. Sup...

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Veröffentlicht in:Journal of dermatological science 2019-12, Vol.96 (3), p.143-150
Hauptverfasser: Perrone Sibilia, Matías Damián, Aldirico, María de los ängeles, Soto, Ariadna Soledad, Picchio, Mariano Sergio, Sánchez, Vanesa Roxana, Arcón, Nadia, Moretta, Rosalía, Martín, Valentina, Vanzulli, Silvia, Fenoy, Ignacio Martín, Goldman, Alejandra
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Sprache:eng
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Zusammenfassung:•Study of T. gondii immune-modulation in an atopic dermatitis mouse model.•Sensitization during chronic toxoplasmosis results in a lower atopic dermatitis.•Chronic infection prevents TH2 and TH1 allergen specific response.•Infection decrease type 2 innate cytokines during allergen sensitization. Supporting the hypothesis thatT. gondii infection protects against allergy in humans we previously demonstrated that this infection can modulate not only the susceptibility to develop respiratory allergies in mice but also suppresses allergic responses at systemic level. This latter finding suggests that T. gondii infection could prevent the onset of other allergic diseases, such as atopic dermatitis. At present, few studies have investigated the modulation of atopic dermatitis by parasite infections. Here, we sought to investigate whether chronic infection with T. gondii is capable of modulating the development of atopic dermatitis. Chronically infected mice were sensitized by repeated epicutaneous ovalbumin administration. Skin histopathology, humoral response, cytokine production and innate type-II lymphoid cells (ILC2) were assessed. A marked reduction in epidermal thickness and dermal inflammatory infiltrate along with a reduction in mast cell count was observed in infected mice compared to non-infected mice. These results correlated with a diminished TH2 and TH1 allergen specific response. Reduced type-II IL-4 and IL-5 cytokines were already detected during the first 24 h of allergen sensitization in splenocytes and draining lymph nodes from infected mice. Moreover, this reduced type-II profile in chronically infected animals correlated with diminished ILC2 number in draining lymph nodes. Chronic infection withT. gondii prevents the development of atopic dermatitis. The diminished susceptibility seems to result from changes in type-II innate immune response that may lead to the induction of a deficient TH2 response and consequently to a lower susceptibility to develop atopic dermatitis.
ISSN:0923-1811
1873-569X
DOI:10.1016/j.jdermsci.2019.10.007