Proteome analysis of distinct developmental stages of human natural killer (NK) cells.
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Authors
Scheiter, MaxiLau, Ulrike
van Ham, Marco
Bulitta, Björn
Gröbe, Lothar
Garritsen, Henk
Klawonn, Frank
König, Sebastian
Jänsch, Lothar
Issue Date
2013-05
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Show full item recordAbstract
The recent Natural Killer (NK) cell maturation model postulates that CD34(+) hematopoietic stem cells (HSC) first develop into CD56(bright) NK cells, then into CD56(dim)CD57(-) and finally into terminally maturated CD56(dim)CD57(+). The molecular mechanisms of human NK cell differentiation and maturation however are incompletely characterized. Here we present a proteome analysis of distinct developmental stages of human primary NK cells, isolated from healthy human blood donors. Peptide sequencing was used to comparatively analyze CD56(bright) NK cells versus CD56(dim) NK cells and CD56(dim)CD57(-) NK cells versus CD56(dim)CD57(+) NK cells and revealed distinct protein signatures for all of these subsets. Quantitative data for about 3400 proteins were obtained and support the current differentiation model. Furthermore, 11 donor-independently, but developmental stage specifically regulated proteins so far undescribed in NK cells were revealed, which may contribute to NK cell development and may elucidate a molecular source for NK cell effector functions. Among those proteins, S100A4 (Calvasculin) and S100A6 (Calcyclin) were selected to study their dynamic subcellular localization. Upon activation of human primary NK cells, both proteins are recruited into the immune synapse (NKIS), where they colocalize with myosin IIa.Citation
Proteome analysis of distinct developmental stages of human natural killer (NK) cells. 2013, 12 (5):1099-114 Mol. Cell ProteomicsAffiliation
Research Group Cellular Proteomics, Helmholtz Centre for Infection Research, HZI, Inhoffenstraβe 7, D-38124 Braunschweig, Germany.PubMed ID
23315794Type
ArticleLanguage
enISSN
1535-9484ae974a485f413a2113503eed53cd6c53
10.1074/mcp.M112.024596
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