TRAIL-R deficiency in mice promotes susceptibility to chronic inflammation and tumorigenesis
Niklas Finnberg, … , Andres J.P. Klein-Szanto, Wafik S. El-Deiry
Niklas Finnberg, … , Andres J.P. Klein-Szanto, Wafik S. El-Deiry
Published December 13, 2007
Citation Information: J Clin Invest. 2008;118(1):111-123. https://doi.org/10.1172/JCI29900.
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TRAIL-R deficiency in mice promotes susceptibility to chronic inflammation and tumorigenesis

Abstract

Preclinical data support the potential of the death-signaling receptors for TRAIL as targets for cancer therapy. However, it is unclear whether these death-signaling receptors suppress the emergence and growth of malignant tumors in vivo. Herein we show that TNF-related apoptosis-inducing ligand receptor (TRAIL-R), the only proapoptotic death-signaling receptor for TRAIL in the mouse, suppresses inflammation and tumorigenesis. Loss of a single TRAIL-R allele on the lymphoma-prone Eμ-myc genetic background significantly reduced median lymphoma-free survival. TRAIL-R–deficient lymphomas developed with equal frequency irrespective of mono- or biallelic loss of TRAIL-R, had increased metastatic potential, and showed apoptotic defects relative to WT littermates. In addition, TRAIL-R–/– mice showed decreased long-term survival following a sublethal dose of ionizing radiation. Histological evaluation of moribund irradiated TRAIL-R–/– animals showed hallmarks of bronchopneumonia as well as tumor formation with increased NF-κB p65 expression. TRAIL-R also suppressed diethylnitrosamine-induced (DEN-induced) hepatocarcinogenesis, as an increased number of large tumors with apoptotic defects developed in the livers of DEN-treated TRAIL-R–/– mice. Thus TRAIL-R may function as an inflammation and tumor suppressor in multiple tissues in vivo.

Authors

Niklas Finnberg, Andres J.P. Klein-Szanto, Wafik S. El-Deiry

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Figure 1

Monoallelic loss of TRAIL-R promotes c-myc–driven lymphomagenesis.

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Monoallelic loss of TRAIL-R promotes c-myc–driven lymphomagenesis. ...
(A) Kaplan-Meier survival curves for the different genotypes (TRAIL-R–/–, n = 14; TRAIL-R+/–, n = 30; and WT, n = 11) on the Eμ-myc genetic background. Survival was markedly decreased in TRAIL-R+/– and TRAIL-R–/– mice (log rank test, P = 0.023 and P = 0.003, respectively) relative to WT littermates. Immunohistochemistry for c-myc+ (α-myc) (B and C) and B220+ showed increased metastasis of lymphoma cells (B and data not shown; n = 6/genotype) to liver (n = 5/genotype; average tumor emboli area percentage ± SEM; Student’s t test, P < 0.05) and lung (box-and-whisker plot shows relative median number of B220+ cells/field; Mann-Whitney U test, P < 0.05) in both TRAIL-R+/– and TRAIL-R–/– animals relative to WT animals on the Eμ-myc genetic background.