Cell Reports (Jan 2018)

ICAMs Are Not Obligatory for Functional Immune Synapses between Naive CD4 T Cells and Lymph Node DCs

  • Sara W. Feigelson,
  • Adam Solomon,
  • Adi Biram,
  • Miki Hatzav,
  • Moria Lichtenstein,
  • Ofer Regev,
  • Stav Kozlovski,
  • Diana Varol,
  • Caterina Curato,
  • Dena Leshkowitz,
  • Steffen Jung,
  • Ziv Shulman,
  • Ronen Alon

DOI
https://doi.org/10.1016/j.celrep.2017.12.103
Journal volume & issue
Vol. 22, no. 4
pp. 849 – 859

Abstract

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Protective immune responses depend on the formation of immune synapses between T cells and antigen-presenting cells (APCs). The two main LFA-1 ligands, ICAM-1 and ICAM-2, are co-expressed on many cell types, including APCs and blood vessels. Although these molecules were suggested to be key players in immune synapses studied in vitro, their contribution to helper T cell priming in vivo is unclear. Here, we used transgenic mice and intravital imaging to examine the role of dendritic cell (DC) ICAM-1 and ICAM-2 in naive CD4 T cell priming and differentiation in skin-draining lymph nodes. Surprisingly, ICAM deficiency on endogenous CD40-stimulated lymph node DCs did not impair their ability to arrest and prime CD4 lymphocyte activation and differentiation into Th1 and Tfh effectors. Thus, functional T cell receptor (TCR)-specific helper T cell synapses with antigen-presenting DCs and subsequent proliferation and early differentiation into T effectors do not require LFA-1-mediated T cell adhesiveness to DC ICAMs.

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