AUTHOR=Melsen Janine E. , van Ostaijen-ten Dam Monique M. , Schoorl Dorenda J. A. , Schol Pieter J. , van den Homberg Daphne A. L. , Lankester Arjan C. , Lugthart Gertjan , Schilham Marco W. 

TITLE=Single-cell transcriptomics in bone marrow delineates CD56dimGranzymeK+ subset as intermediate stage in NK cell differentiation

JOURNAL=Frontiers in Immunology

VOLUME=13

YEAR=2022

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2022.1044398

DOI=10.3389/fimmu.2022.1044398

ISSN=1664-3224

ABSTRACT=<p>Human natural killer (NK) cells in lymphoid tissues can be categorized into three subsets: CD56<sup>bright</sup>CD16<sup>+</sup>, CD56<sup>dim</sup>CD16<sup>+</sup> and CD69<sup>+</sup>CXCR6<sup>+</sup> lymphoid tissue-resident (lt)NK cells. How the three subsets are functionally and developmentally related is currently unknown. Therefore, we performed single-cell RNA sequencing combined with oligonucleotide-conjugated antibodies against CD56, CXCR6, CD117 and CD34 on fresh bone marrow NK cells. A minor CD56<sup>dim</sup>GzmK<sup>+</sup> subset was identified that shared features with CD56<sup>bright</sup> and CD56<sup>dim</sup>GzmK<sup>-</sup> NK cells based on transcriptome, phenotype (NKG2A<sup>high</sup>CD16<sup>low</sup>KLRG1<sup>high</sup>TIGIT<sup>high</sup>) and functional analysis in bone marrow and blood, supportive for an intermediate subset. Pseudotime analysis positioned CD56<sup>bright</sup>, CD56<sup>dim</sup>GzmK<sup>+</sup> and CD56<sup>dim</sup>GzmK<sup>-</sup> cells in one differentiation trajectory, while ltNK cells were developmentally separated. Integrative analysis with bone marrow cells from the Human Cell Atlas did not demonstrate a developmental connection between CD34<sup>+</sup> progenitor and NK cells, suggesting absence of early NK cell stages in bone marrow. In conclusion, single-cell transcriptomics provide new insights on development and differentiation of human NK cells.</p>