RAG recombinase expression discriminates the development of natural killer cells.

INTRODUCTION

V(D)J recombination, initiated by recombination-activating gene (RAG) endonucleases, is a crucial process for the generation of diversified antigen receptors of T and B lymphocytes but regarded dispensable for innate natural killer (NK) lymphocytes lacking clonotypic receptors.

METHODS

To explore the impact of potential rearrangements on NK cell maturation, RAG-fate mapping reporter human induced pluripotent stem cell (iPSC) lines were generated by introduction of RSS-invEGFP constructs into the AAVS1 locus using CRISPR/Cas9 and differentiated into NK cells .

RESULTS

GFP expression was observed in up to 14% of mature NK cells characterized by a CD45 CD56CD57NKG2CKIR phenotype and unproductive genetic rearrangements in the locus. Advanced maturation was further revealed by transcriptomic studies using RNA sequencing. Despite their strong effector function, DNA damage response and survival to ionizing radiation were compromised.

DISCUSSION

These findings suggest a role of RAG expression in NK cell ontogeny supporting the development of a terminally differentiated effector population.