Perturbation of NK cell peripheral homeostasis accelerates prostate carcinoma metastasis
Gang Liu, … , Zihai Li, Jennifer D. Wu
Gang Liu, … , Zihai Li, Jennifer D. Wu
Published September 9, 2013
Citation Information: J Clin Invest. 2013;123(10):4410-4422. https://doi.org/10.1172/JCI69369.
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Research Article Oncology

Perturbation of NK cell peripheral homeostasis accelerates prostate carcinoma metastasis

Abstract

The activating receptor NK cell group 2 member D (NKG2D) mediates antitumor immunity in experimental animal models. However, whether NKG2D ligands contribute to tumor suppression or progression clinically remains controversial. Here, we have described 2 novel lines of “humanized” bi-transgenic (bi-Tg) mice in which native human NKG2D ligand MHC class I polypeptide-related sequence B (MICB) or the engineered membrane-restricted MICB (MICB.A2) was expressed in the prostate of the transgenic adenocarcinoma of the mouse prostate (TRAMP) model of spontaneous carcinogenesis. Bi-Tg TRAMP/MICB mice exhibited a markedly increased incidence of progressed carcinomas and metastasis, whereas TRAMP/MICB.A2 mice enjoyed long-term tumor-free survival conferred by sustained NKG2D-mediated antitumor immunity. Mechanistically, we found that cancer progression in TRAMP/MICB mice was associated with loss of the peripheral NK cell pool owing to high serum levels of tumor-derived soluble MICB (sMICB). Prostate cancer patients also displayed reduction of peripheral NK cells and high sMIC levels. Our study has not only provided direct evidence in “humanized” mouse models that soluble and membrane-restricted NKG2D ligands pose opposite impacts on cancer progression, but also uncovered a mechanism of sMIC-induced impairment of NK cell antitumor immunity. Our findings suggest that the impact of soluble NKG2D ligands should be considered in NK cell–based cancer immunotherapy and that our unique mouse models should be valuable for therapy optimization.

Authors

Gang Liu, Shengjun Lu, Xuanjun Wang, Stephanie T. Page, Celestia S. Higano, Stephen R. Plymate, Norman M. Greenberg, Shaoli Sun, Zihai Li, Jennifer D. Wu

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Figure 2

Accelerated progression to PD carcinomas in TRAMP/MICB mice is associated with elevated serum sMICB and loss of surface MICB.

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Accelerated progression to PD carcinomas in TRAMP/MICB mice is associate...
(A) Representative IHC staining demonstrating the pattern of MICB expression (brown) in TRAMP/MICB mice. Scale bars: 100 μm. (B) Summary IHC score of surface MICB expression on tumor cells. (C) Quantitative RT-PCR showing comparable levels of MICB expression in PD and WD tumors at the mRNA level. (D) ELISA measurement of serum levels of sMICB in the cohorts of 24-week-old TRAMP/MICB mice at various ages during carcinoma development. *P < 0.01; **P < 0.001. Note that development of PD carcinomas is associated with marked elevation of serum levels of sMICB. (E) Correlation of serum sMICB with tumor volume in TRAMP/MICB mice at the age of 24 weeks. (F) Quantitative RT-PCR showing comparable levels of endogenous NKG2D ligand RAE-1 expression in PD and WD tumors at the mRNA level. (G) Representative micrograph and added summary scores of IHC staining demonstrating pattern of endogenous NKG2D ligand RAE-1 expression in TRAMP/MICB carcinomas. Scale bars: 100 μm. Data represent results from 4 independent analyses.