Liver-primed memory T cells generated under noninflammatory conditions provide anti-infectious immunity.

6533b838fe1ef96bd12a4811

RESEARCH PRODUCT

Liver-primed memory T cells generated under noninflammatory conditions provide anti-infectious immunity.

Edgar Schmitt Andrea Staratschek-jox Svenja Debey-pascher Zeinab Abdullah Imke Atreya Oliver Schanz Joachim Schultze Jan P. Böttcher Linda Diehl Jessica Grell Silke Hegenbarth Percy A Knolle Percy A. Knolle Dirk Wohlleber Peter Van Endert Dirk H. Busch Christian Kurts Markus F. Neurath Waldemar Kolanus Andreas Limmer Bastian Höchst

subject

T cell Receptors Antigen T-Cell Priming (immunology)chemical and pharmacologic phenomena Biology CD8-Positive T-Lymphocytes Lymphocyte Activation General Biochemistry Genetics and Molecular Biology Mice Cross-Priming Antigen CD28 Antigens medicine Animals lcsh:QH301-705.5 Innate immune system Gene Expression Profiling T-cell receptor Receptors Interleukin-12 CD28 Endothelial Cells hemic and immune systems Dendritic Cells Acquired immune system Listeria monocytogenes Immunity Innate Neuropilin-1 Mice Inbred C57BL medicine.anatomical_structure lcsh:Biology (General)Liver Immunology Immunologic Memory CD8

description

SummaryDevelopment of CD8+ T cell (CTL) immunity or tolerance is linked to the conditions during T cell priming. Dendritic cells (DCs) matured during inflammation generate effector/memory T cells, whereas immature DCs cause T cell deletion/anergy. We identify a third outcome of T cell priming in absence of inflammation enabled by cross-presenting liver sinusoidal endothelial cells. Such priming generated memory T cells that were spared from deletion by immature DCs. Similar to central memory T cells, liver-primed T cells differentiated into effector CTLs upon antigen re-encounter on matured DCs even after prolonged absence of antigen. Their reactivation required combinatorial signaling through the TCR, CD28, and IL-12R and controlled bacterial and viral infections. Gene expression profiling identified liver-primed T cells as a distinct Neuropilin-1+ memory population. Generation of liver-primed memory T cells may prevent pathogens that avoid DC maturation by innate immune escape from also escaping adaptive immunity through attrition of the T cell repertoire.

year	journal	country	edition	language
2013-03-01	Cell reports

10.1016/j.celrep.2013.02.008 https://pubmed.ncbi.nlm.nih.gov/23499443