Details

Autor(en) / Beteiligte

• Pionnier, Nicolas
• Sjoberg, Hanna
• Furlong-Silva, Julio
• Marriott, Amy
• Halliday, Alice
• Archer, John
• Steven, Andrew
• Taylor, Mark J
• Turner, Joseph D

Titel

Eosinophil-Mediated Immune Control of Adult Filarial Nematode Infection Can Proceed in the Absence of IL-4 Receptor Signaling

Ist Teil von

• The Journal of immunology (1950), 2020-08, Vol.205 (3), p.731-740

Ort / Verlag

United States: AAI

Erscheinungsjahr

2020

Link zum Volltext

Quelle

MEDLINE

Beschreibungen/Notizen

• Helminth infections are accompanied by eosinophilia in parasitized tissues. Eosinophils are effectors of immunity to tissue helminths. We previously reported that in the context of experimental filarial nematode infection, optimum tissue eosinophil recruitment was coordinated by local macrophage populations following IL-4R-dependent in situ proliferation and alternative activation. However, in the current study, we identify that control of chronic adult filarial worm infection is evident in IL-4Rα-deficient (IL-4Rα ) mice, whereby the majority of infections do not achieve patency. An associated residual eosinophilia was apparent in infected IL-4Rα mice. By treating IL-4Rα mice serially with anti-CCR3 Ab or introducing a compound deficiency in CCR3 within IL-4Rα mice, residual eosinophilia was ablated, and susceptibility to chronic adult infection was established, promoting a functional role for CCR3-dependent eosinophil influx in immune control in the absence of IL-4/IL-13-dependent immune mechanisms. We investigated additional cytokine signals involved in residual eosinophilia in the absence IL-4Rα signaling and defined that IL-4Rα /IL-5 double-knockout mice displayed significant eosinophil deficiency compared with IL-4Rα mice and were susceptible to chronic fecund adult filarial infections. Contrastingly, there was no evidence that either IL-4R-dependent or IL-4R-independent/CCR3/IL-5-dependent immunity influenced microfilarial loads in the blood. Our data demonstrate multiplicity of Th2-cytokine control of eosinophil tissue recruitment during chronic filarial infection and that IL-4R-independent/IL-5- and CCR3-dependent pathways are sufficient to control filarial adult infection via an eosinophil-dependent effector response prior to patency.