DOCK8 enforces immunological tolerance by promoting IL-2 signaling and immune synapse formation in Tregs
Erin Janssen, Sudha Kumari, Mira Tohme, Sumana Ullas, Victor Barrera, Jeroen M.J. Tas, Marcela Castillo-Rama, Roderick T. Bronson, Shariq M. Usmani, Darrell J. Irvine, Thorsten R. Mempel, Raif S. Geha
Erin Janssen, Sudha Kumari, Mira Tohme, Sumana Ullas, Victor Barrera, Jeroen M.J. Tas, Marcela Castillo-Rama, Roderick T. Bronson, Shariq M. Usmani, Darrell J. Irvine, Thorsten R. Mempel, Raif S. Geha
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Research Article Immunology

DOCK8 enforces immunological tolerance by promoting IL-2 signaling and immune synapse formation in Tregs

Abstract

Patients deficient in the guanine nucleotide exchange factor DOCK8 have decreased numbers and impaired in vitro function of Tregs and make autoantibodies, but they seldom develop autoimmunity. We show that, similarly, Dock8–/– mice have decreased numbers and impaired in vitro function of Tregs but do not develop autoimmunity. In contrast, mice with selective DOCK8 deficiency in Tregs develop lymphoproliferation, autoantibodies, and gastrointestinal inflammation, despite a normal percentage and in vitro function of Tregs, suggesting that deficient T effector cell function might protect DOCK8-deficient patients from autoimmunity. We demonstrate that DOCK8 associates with STAT5 and is important for IL-2–driven STAT5 phosphorylation in Tregs. DOCK8 localizes within the lamellar actin ring of the Treg immune synapse (IS). Dock8–/– Tregs have abnormal TCR-driven actin dynamics, decreased adhesiveness, an altered gene expression profile, an unstable IS with decreased recruitment of signaling molecules, and impaired transendocytosis of the costimulatory molecule CD86. These data suggest that DOCK8 enforces immunological tolerance by promoting IL-2 signaling, TCR-driven actin dynamics, and the IS in Tregs.

Authors

Erin Janssen, Sudha Kumari, Mira Tohme, Sumana Ullas, Victor Barrera, Jeroen M.J. Tas, Marcela Castillo-Rama, Roderick T. Bronson, Shariq M. Usmani, Darrell J. Irvine, Thorsten R. Mempel, Raif S. Geha

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Figure 3

Mice with a Treg-specific DOCK8 deficiency develop gastrointestinal inflammation.

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Mice with a Treg-specific DOCK8 deficiency develop gastrointestinal infl...
(A) Representative photographs of the MLNs from 30-week-old Foxp3YFP–Cre/Dock8flox/flox mice and Foxp3YFP–Cre controls. (B) Total cellularity, number of CD4+ T cells, and percentage of activated CD69+ T cells of CD4+ T cells in MLNs from 30-week-old Foxp3YFP–Cre/Dock8flox/flox mice and Foxp3YFP–Cre controls. (C and D) Representative photographs of the stomachs (C) and representative H&E-stained sections of the forestomach and glandular stomach (original magnification, ×10) (D) from 30-week-old Foxp3YFP–Cre/Dock8flox/flox mice and Foxp3YFP–Cre controls. Scale bar: 100 μm (D). (E) Representative images (original magnification, ×20) of indirect immunofluorescent staining of stomach sections for IgG using dilutions of serum from a 28-week-old Foxp3YFP–Cre/Dock8flox/flox mouse and Foxp3YFP–Cre controls. (F and G) Representative H&E-stained sections (original magnification, ×20) (F) and enteritis pathology score (G) of the small intestine (SI) from 30-week-old Foxp3YFP–Cre/Dock8flox/flox mice and Foxp3YFP–Cre controls. Scale bar: 100 μm. (H) qPCR analysis of cytokine mRNA expression in the SI of 30-week-old Foxp3YFP–Cre/Dock8flox/flox mice and Foxp3YFP–Cre controls. Results are expressed as fold increase of the cytokine mRNA/b2microglobulin mRNA ratio relative to control. (I and J) Representative H&E-stained sections (original magnification, ×20) (I) and colitis pathology score (J) of the mid colon from 30-week-old Foxp3YFP–Cre/Dock8flox/flox mice and Foxp3YFP–Cre controls. (K) Fecal lipocalin-2 concentrations in the stools of 30-week-old Foxp3YFP–Cre/Dock8flox/flox mice and Foxp3YFP–Cre controls. (L) qPCR analysis of cytokine mRNA expression in the colons from 30-week-old Foxp3YFP–Cre/Dock8flox/flox mice and Foxp3YFP–Cre controls. Results are expressed as fold increase of the cytokine mRNA/b2microglobulin mRNA ratio relative to control. Symbols represent individual mice, and error bars in B, G, H, J, and K represent mean and SEM. t test, *P < 0.05, **P < 0.01, ***P < 0.001.