NKp46 identifies an NKT cell subset susceptible to leukemic transformation in mouse and human
Jianhua Yu, … , Susheela Tridandapani, Michael A. Caligiuri
Jianhua Yu, … , Susheela Tridandapani, Michael A. Caligiuri
Published March 1, 2011
Citation Information: J Clin Invest. 2011;121(4):1456-1470. https://doi.org/10.1172/JCI43242.
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Research Article Hematology

NKp46 identifies an NKT cell subset susceptible to leukemic transformation in mouse and human

Abstract

IL-15 may have a role in the development of T cell large granular lymphocyte (T-LGL) or NKT leukemias. However, the mechanisms of action and the identity of the cell subset that undergoes leukemic transformation remain elusive. Here we show that in both mice and humans, NKp46 expression marks a minute population of WT NKT cells with higher activity and potency to become leukemic. Virtually 100% of T-LGL leukemias in IL-15 transgenic mice expressed NKp46, as did a majority of human T-LGL leukemias. The minute NKp46+ NKT population, but not the NKp46– NKT population, was selectively expanded by overexpression of endogenous IL-15. Importantly, IL-15 transgenic NKp46– NKT cells did not become NKp46+ in vivo, suggesting that NKp46+ T-LGL leukemia cells were the malignant counterpart of the minute WT NKp46+ NKT population. Mechanistically, NKp46+ NKT cells possessed higher responsiveness to IL-15 in vitro and in vivo compared with that of their NKp46– NKT counterparts. Furthermore, interruption of IL-15 signaling using a neutralizing antibody could prevent LGL leukemia in IL-15 transgenic mice. Collectively, our data demonstrate that NKp46 identifies a functionally distinct NKT subset in mice and humans that appears to be directly susceptible to leukemic transformation when IL-15 is overexpressed. Thus, IL-15 signaling and NKp46 may be useful targets in the treatment of patients with T-LGL or NKT leukemia.

Authors

Jianhua Yu, Takeki Mitsui, Min Wei, Hsiaoyin Mao, Jonathan P. Butchar, Mithun Vinod Shah, Jianying Zhang, Anjali Mishra, Christopher Alvarez-Breckenridge, Xingluo Liu, Shujun Liu, Akihiko Yokohama, Rossana Trotta, Guido Marcucci, Don M. Benson Jr., Thomas P. Loughran Jr., Susheela Tridandapani, Michael A. Caligiuri

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Figure 1

Flow cytometric analysis of NKp46 expression on mouse T cells.

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Flow cytometric analysis of NKp46 expression on mouse T cells. (A) CD3 v...
(A) CD3 versus NKp46 staining of splenocytes isolated from WT FvB/NJ mice, IL-15tg polyclonal mice, and leukemic mice (n = 5/group). The T-LGL leukemic mice show a vastly expanded CD3+NKp46+ fraction, with a total white blood cell count in peripheral blood of over 1 × 108/ml (normal white blood cell count = 1~3 × 106/ml). (B) A representative example of NKp46 expression on monoclonal NK1.1+CD3+ T-LGL leukemic cells. NKp46 was expressed in all cases of mouse T-LGL leukemia examined (n = 10) (data not shown). (C) CD3 versus NKp46 staining for WT FvB/NJ leukocytes from different organs. Results are summarized in Supplemental Table 1. A lymphocyte was used for these experiments, and percentages of cells in the respective quadrants are indicated in AC.