| Literature DB >> 32049052 |
Simon Zenke1, Margriet M Palm2, Julia Braun1, Alina Gavrilov3, Philippa Meiser4, Jan P Böttcher4, Niklas Beyersdorf5, Stephan Ehl6, Audrey Gerard7, Tim Lämmermann3, Ton N Schumacher8, Joost B Beltman2, Jan C Rohr9.
Abstract
T cell responses upon infection display a remarkably reproducible pattern of expansion, contraction, and memory formation. If the robustness of this pattern builds entirely on signals derived from other cell types or if activated T cells themselves contribute to the orchestration of these population dynamics-akin to bacterial quorum regulation-is unclear. Here, we examined this question using time-lapse microscopy, genetic perturbation, bioinformatic predictions, and mathematical modeling. We found that ICAM-1-mediated cell clustering enabled CD8+ T cells to collectively regulate the balance between proliferation and apoptosis. Mechanistically, T cell expressed CD80 and CD86 interacted with the receptors CD28 and CTLA-4 on neighboring T cells; these interactions fed two nested antagonistic feedback circuits that regulated interleukin 2 production in a manner dependent on T cell density as confirmed by in vivo modulation of this network. Thus, CD8+ T cell-population-intrinsic mechanisms regulate cellular behavior, thereby promoting robustness of population dynamics.Entities:
Keywords: CD28; CD80; CTLA-4; IL-2; T lymphocyte; feedback; population dynamics; quorum regulation; robustness
Year: 2020 PMID: 32049052 DOI: 10.1016/j.immuni.2020.01.018
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745