Control of RelB during dendritic cell activation integrates canonical and noncanonical NF-κB pathways

树突状细胞活化过程中对 RelB 的控制整合了典型和非典型 NF-κB 通路

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作者:Vincent F-S Shih, Jeremy Davis-Turak, Monica Macal, Jenny Q Huang, Julia Ponomarenko, Jeffrey D Kearns, Tony Yu, Riku Fagerlund, Masataka Asagiri, Elina I Zuniga, Alexander Hoffmann

Abstract

The NF-κB protein RelB controls dendritic cell (DC) maturation and may be targeted therapeutically to manipulate T cell responses in disease. Here we report that RelB promoted DC activation not as the expected RelB-p52 effector of the noncanonical NF-κB pathway, but as a RelB-p50 dimer regulated by canonical IκBs, IκBα and IκBɛ. IκB control of RelB minimized spontaneous maturation but enabled rapid pathogen-responsive maturation. Computational modeling of the NF-κB signaling module identified control points of this unexpected cell type-specific regulation. Fibroblasts that we engineered accordingly showed DC-like RelB control. Canonical pathway control of RelB regulated pathogen-responsive gene expression programs. This work illustrates the potential utility of systems analyses in guiding the development of combination therapeutics for modulating DC-dependent T cell responses.

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