Identifiers
HUGO:CTNNB1
Maps_Modules
MODULE:CORE_SIGNALING_PATHWAYS MODULE:MIRNA_TF_IMMUNOSUPPRESSIVE
References
DENDRITIC_CELL
CASCADE:CATENINB
PMID:24023259
β-Catenin mediates tumor-induced immunosuppression by inhibiting cross-priming of CD8+ T cells
PMID:25730849
L-10 Mediates β-Catenin–Dependent Inhibition of Cross-Priming,β-catenin enhanced IL-10 induction through mTOR pathway.
β-Catenin up-regulates level of mTOR in DCs and activates mTOR signaling.
PMID:20705860
β-catenin signaling in DCs is required to induce Treg cells and suppress TH1/TH17 responses.
β-catenin signaling in intestinal DCs promotes the expression of Raldh and suppresses the expression of proinflammatory cytokines (IL6, IL23a,IL12p40)
but induces IL10 production.
PMID:15001769, PMID:17936032
GSK3B phosphorylates beta-catenin and inhibits its activity.
Beta-catenin signaling prevents production of inflammatory cytokines IL6, IL-1α, IL-6, TNF-α, and IL-12 p40,
But upregulates CCR7, both at the mRNA level and on the plasma membrane.
CCR7 is a chemokine receptor important for the migration of DCs from the periphery to T cell areas of lymph nodes.
DCs matured by CD activation of beta-catenin signaling alone failed to prime CD4 T cells to produce IFN-γ but did generate high levels of IL10 (Fig. 6A) together with other cytokines (not shown) consistent with type I regulatory T cells
→ _beta_-Catenin*|pho|active@INNATE_IMMUNE_CELL_Cytosol
→ degraded
→ _beta_-Catenin*@INNATE_IMMUNE_CELL_Cytosol + E-Cadherin*@INNATE_IMMUNE_CELL_Cytosol + _alpha_-Catenin*@INNATE_IMMUNE_CELL_Cytosol