| Literature DB >> 35852466 |
Malte Deseke1,2, Francesca Rampoldi1, Inga Sandrock1, Eva Borst3, Heike Böning3, George Liam Ssebyatika4, Carina Jürgens3, Nina Plückebaum3, Maleen Beck1,5, Ahmed Hassan1, Likai Tan1,6, Abdi Demera1, Anika Janssen1, Peter Steinberger7, Christian Koenecke1,5, Abel Viejo-Borbolla3,8, Martin Messerle3,8, Thomas Krey2,3,4,9,8, Immo Prinz1,2,6,10.
Abstract
The innate and adaptive roles of γδ T cells and their clonal γδ T cell receptors (TCRs) in immune responses are still unclear. Recent studies of γδ TCR repertoire dynamics showed massive expansion of individual Vδ1+ γδ T cell clones during viral infection. To judge whether such expansion is random or actually represents TCR-dependent adaptive immune responses, information about their cognate TCR ligands is required. Here, we used CRISPR/Cas9-mediated screening to identify HLA-DRA, RFXAP, RFX5, and CIITA as required for target cell recognition of a CMV-induced Vγ3Vδ1+ TCR, and further characterization revealed a direct interaction of this Vδ1+ TCR with the MHC II complex HLA-DR. Since MHC II is strongly upregulated by interferon-γ, these results suggest an inflammation-induced MHC-dependent immune response of γδ T cells.Entities:
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Year: 2022 PMID: 35852466 PMCID: PMC9301659 DOI: 10.1084/jem.20212525
Source DB: PubMed Journal: J Exp Med ISSN: 0022-1007 Impact factor: 17.579