Intrinsic factors and CD1d1 but not CD1d2 expression levels control invariant natural killer T cell subset differentiation

Author:

Amable Ludivine,Ferreira Martins Luis Antonio,Pierre Remi,Do Cruseiro Marcio,Chabab Ghita,Sergé ArnauldORCID,Kergaravat Camille,Delord Marc,Viret Christophe,Jaubert Jean,Liu Chaohong,Karray SaoussenORCID,Marie Julien C.ORCID,Irla MagaliORCID,Georgiev HristoORCID,Clave EmmanuelORCID,Toubert AntoineORCID,Lucas BrunoORCID,Klibi Jihene,Benlagha KamelORCID

Abstract

AbstractInvariant natural killer T (NKT) cell subsets are defined based on their cytokine-production profiles and transcription factors. Their distribution is different in C57BL/6 (B6) and BALB/c mice, with a bias for NKT1 and NKT2/NKT17 subsets, respectively. Here, we show that the non-classical class I-like major histocompatibility complex CD1 molecules CD1d2, expressed in BALB/c and not in B6 mice, could not account for this difference. We find however that NKT cell subset distribution is intrinsic to bone marrow derived NKT cells, regardless of syngeneic CD1d-ligand recognition, and that multiple intrinsic factors are likely involved. Finally, we find that CD1d expression levels in combination with T cell antigen receptor signal strength could also influence NKT cell distribution and function. Overall, this study indicates that CD1d-mediated TCR signals and other intrinsic signals integrate to influence strain-specific NKT cell differentiation programs and subset distributions.

Funder

INSERM

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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