Human peripheral blood natural killer progenitors represent a flexible, heterogeneous population whose phenotype and function are controlled by their membrane-bound IL-15. Indeed, reciprocal membrane-bond IL-15 trans-presentation commits these cells into NK differentiation, while membrane-bound IL-15 stimulation with its soluble ligand (sIL-15Rα) triggers a reverse signal (pERK1/2 and pFAK) that modifies the developmental program of at least two subsets of PB-NKPs. This treatment generates: i) the expansion of an immature NK subset growing in suspension; ii) the appearance of an unprecedented adherent non-proliferative subset with a dendritic morphology co-expressing marker, cytokines and functions typical of myeloid dendritic cells (CD1a(+)/BDCA1(+)/IL-12(+)) and NK cells (CD3-/NKp46(+)/ CD56(+)/IFNγ(+)). The generation of these putative NK/DCs is associated to the rapid inhibition of negative regulators of myelopoiesis (the transcription factors STAT6 and GATA-3) followed by the transient upregulation of inducers of myeloid development, such as the transcription factors (PU.1, GATA-1) and the anti-apoptotic molecule (MCL-1).
Membrane-bound IL-15 stimulation on peripheral blood natural kiler progenitors leads to the generation of an adherent subset co-expressing dendritic cells and natural kiler functional markers.
膜结合的 IL-15 刺激外周血天然杀伤细胞祖细胞,导致产生一种粘附亚群,该亚群共表达树突状细胞和天然杀伤细胞功能标志物
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作者:Negrini Simone, Giuliani Massimo, Durali Deniz, Chouaib Salem, Azzarone Bruno
| 期刊: | Haematologica | 影响因子: | 7.900 |
| 时间: | 2011 | 起止号: | 2011 May;96(5):762-6 |
| doi: | 10.3324/haematol.2010.033738 | 研究方向: | 细胞生物学 |
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