Abstract
Myeloid progenitor cells have generally been considered the predominant source of myeloid cells under steady-state conditions. Here we show that NK cells contributed to a myeloid cell lineage pool in naïve and tumor-bearing mice. Using fate tracing of NKp46+ cells, we found that myeloid cells could be derived from NK cells. Notably, among mature CD11b+CD27+ NK cells, c-Kit+CD24+ NK cells were capable of differentiating into a range of myeloid lineages in vitro and produced neutrophils and monocytes in vivo. The differentiation was completely inhibited by NK-stimulating cytokines. In addition to the potential for differentiation into myeloid cells, c-Kit+CD24+ NK cells retained NK cell phenotypes and effector functions. Mechanistically, GATA-2 was necessary for the differentiation of c-Kit+CD24+ NK cells. Therefore, we discovered that GATA-2-dependent differentiation of c-Kit+CD24+ NK cells contributes to myeloid cell development and identified a novel pathway for myeloid lineage commitment under physiological conditions.
Original language | English |
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Pages (from-to) | 4462-4481 |
Number of pages | 20 |
Journal | FASEB Journal |
Volume | 34 |
Issue number | 3 |
DOIs | |
State | Published - 1 Mar 2020 |
Externally published | Yes |
Bibliographical note
Publisher Copyright:© 2020 Federation of American Societies for Experimental Biology
Keywords
- CD24
- GATA-2
- c-Kit
- myeloid cell development
- natural killer cell