Converging TLR9 and PI3Kgamma signaling induces sterile inflammation and organ damage

Braulio Henrique Freire Lima,Emilio Hirsch,Mark Lennon,Lindisley Ferreira Gomides,Mauro Martins Teixeira,Remo Castro Russo,Celso M Queiroz-Junior,Augustin Amour,Edith M Hessel,Gustavo Batista Menezes,Matheus Silvério Mattos,Pedro Elias Marques,Lucas Kraemer

doi:10.1038/s41598-019-55504-0

Abstract

Toll-like receptor 9 (TLR9) and Phosphatidylinositol-3-kinase gamma (PI3Kγ) are very important effectors of the immune response, however, the importance of such crosstalk for disease development is still a matter of discussion. Here we show that PI3Kγ is required for immune responses in which TLR9 is a relevant trigger. We demonstrate the requirement of PI3Kγ for TLR9-induced inflammation in a model of CpG-induced pleurisy. Such requirement was further observed in inflammatory models where DNA sensing via TLR9 contributes to disease, such as silicosis and drug-induced liver injury. Using adoptive transfer, we demonstrate that PI3Kγ is important not only in leukocytes but also in parenchymal cells for the progression of inflammation. We demonstrate this crosstalk between TLR9 and PI3Kγ in vitro using human PBMCs. The inhibition of PI3Kγ in CpG-stimulated PBMCs resulted in reduction of both cytokine production and phosphorylated Akt. Therefore, drugs that target PI3Kγ have the potential to treat diseases mediated by excessive TLR9 signalling.

Highlights

Lima et al. demonstrate that PI3Kγ is necessary for TLR9-dependent cellular activation
The presence of PI3Kγ is shown to be as important in leukocytes as in non-hematopoietic cells for the development of diseases that are caused/exacerbated by the recognition of DNA via TLR9
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