Protein kinase CK2 enables regulatory T cells to suppress excessive TH2 responses in vivo

蛋白激酶 CK2 可使调节性 T 细胞抑制体内过度的 TH2 反应

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作者:Alexander Ulges, Matthias Klein, Sebastian Reuter, Bastian Gerlitzki, Markus Hoffmann, Nadine Grebe, Valérie Staudt, Natascha Stergiou, Toszka Bohn, Till-Julius Brühl, Sabine Muth, Hajime Yurugi, Krishnaraj Rajalingam, Iris Bellinghausen, Andrea Tuettenberg, Susanne Hahn, Sonja Reißig, Irma Haben, F

Abstract

The quality of the adaptive immune response depends on the differentiation of distinct CD4(+) helper T cell subsets, and the magnitude of an immune response is controlled by CD4(+)Foxp3(+) regulatory T cells (Treg cells). However, how a tissue- and cell type-specific suppressor program of Treg cells is mechanistically orchestrated has remained largely unexplored. Through the use of Treg cell-specific gene targeting, we found that the suppression of allergic immune responses in the lungs mediated by T helper type 2 (TH2) cells was dependent on the activity of the protein kinase CK2. Genetic ablation of the β-subunit of CK2 specifically in Treg cells resulted in the proliferation of a hitherto-unexplored ILT3(+) Treg cell subpopulation that was unable to control the maturation of IRF4(+)PD-L2(+) dendritic cells required for the development of TH2 responses in vivo.

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