| Literature DB >> 34157301 |
Harikesh S Wong1, Kyemyung Park2, Anita Gola3, Antonio P Baptista4, Christine H Miller5, Deeksha Deep6, Meng Lou3, Lisa F Boyd7, Alexander Y Rudensky6, Peter A Savage5, Grégoire Altan-Bonnet8, John S Tsang9, Ronald N Germain10.
Abstract
A fraction of mature T cells can be activated by peripheral self-antigens, potentially eliciting host autoimmunity. We investigated homeostatic control of self-activated T cells within unperturbed tissue environments by combining high-resolution multiplexed and volumetric imaging with computational modeling. In lymph nodes, self-activated T cells produced interleukin (IL)-2, which enhanced local regulatory T cell (Treg) proliferation and inhibitory functionality. The resulting micro-domains reciprocally constrained inputs required for damaging effector responses, including CD28 co-stimulation and IL-2 signaling, constituting a negative feedback circuit. Due to these local constraints, self-activated T cells underwent transient clonal expansion, followed by rapid death ("pruning"). Computational simulations and experimental manipulations revealed the feedback machinery's quantitative limits: modest reductions in Treg micro-domain density or functionality produced non-linear breakdowns in control, enabling self-activated T cells to subvert pruning. This fine-tuned, paracrine feedback process not only enforces immune homeostasis but also establishes a sharp boundary between autoimmune and host-protective T cell responses. Published by Elsevier Inc.Entities:
Keywords: CTLA-4; IL-2; IL-2Rα; apoptosis; autoimmunity; computational modeling; feedback control; immune homeostasis; quantitative tissue imaging; regulatory T cells
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Year: 2021 PMID: 34157301 PMCID: PMC8390950 DOI: 10.1016/j.cell.2021.05.028
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 66.850