4.7 Article

Role for early-differentiated natural killer cells in infectious mononucleosis

期刊

BLOOD
卷 124, 期 16, 页码 2533-2543

出版社

AMER SOC HEMATOLOGY
DOI: 10.1182/blood-2014-01-553024

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资金

  1. National Institutes of Health, National Cancer Institute [R01CA108609]
  2. Sassella Foundation [10/02, 11/02, 12/02]
  3. Cancer Research Switzerland [KFS-02652-08-2010]
  4. Cancer League of the Canton of Zurich
  5. Association for International Cancer Research [11-0516]
  6. KFSPMS of the University of Zurich
  7. KFSPHLD of the University of Zurich
  8. Vontobel Foundation
  9. Baugarten Foundation
  10. EMDO Foundation
  11. Sobek Foundation
  12. Fondation Acteria
  13. Novartis
  14. Walter L. and Johanna Wolf Foundation
  15. Swiss National Science Foundation [310030_143979, CRSII3_136241, 310030_135028]
  16. Children's Research Center of the University Children's Hospital Zurich [10353]
  17. Swiss National Science Foundation (SNF) [310030_135028] Funding Source: Swiss National Science Foundation (SNF)

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A growing body of evidence suggests that the human natural killer (NK)-cell compartment is phenotypically and functionally heterogeneous and is composed of several differentiation stages. Moreover, NK-cell subsets have been shown to exhibit adaptive immune features during herpes virus infection in experimental mice and to expand preferentially during viral infections in humans. However, both phenotype and role of NK cells during acute symptomatic Epstein-Barr virus (EBV) infection, termed infectious mononucleosis (IM), remain unclear. Here, we longitudinally assessed the kinetics, the differentiation, and the proliferation of subsets of NK cells in pediatric IM patients. Our results indicate that acute IM is characterized by the preferential proliferation of early-differentiated CD56(dim) NKG2A(+) immunoglobulin-like receptor NK cells. Moreover, this NK-cell subset exhibits features of terminal differentiation and persists at higher frequency during at least the first 6 months after acute IM. Finally, we demonstrate that this NK-cell subset preferentially degranulates and proliferates on exposure to EBV-infected B cells expressing lytic antigens. Thus, early-differentiated NK cells might play a key role in the immune control of primary infection with this persistent tumor-associated virus.

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