Inhibition of CXCR2 profoundly suppresses inflammation-driven and spontaneous tumorigenesis
Thomas Jamieson, … , Robert J.B. Nibbs, Owen J. Sansom
Thomas Jamieson, … , Robert J.B. Nibbs, Owen J. Sansom
Published August 27, 2012
Citation Information: J Clin Invest. 2012;122(9):3127-3144. https://doi.org/10.1172/JCI61067.
View: Text | PDF
Research Article Oncology

Inhibition of CXCR2 profoundly suppresses inflammation-driven and spontaneous tumorigenesis

Abstract

The chemokine receptor CXCR2 is a key mediator of neutrophil migration that also plays a role in tumor development. However, CXCR2 influences tumors through multiple mechanisms and might promote or inhibit tumor development depending on context. Here, we used several mouse models of spontaneous and inflammation-driven neoplasia to define indispensable roles for CXCR2 in benign and malignant tumors. CXCR2-activating chemokines were part of the secretome of cultured primary benign intestinal adenomas (ApcMin/+) and highly expressed by all tumors in all models. CXCR2 deficiency profoundly suppressed inflammation-driven tumorigenesis in skin and intestine as well as spontaneous adenocarcinoma formation in a model of invasive intestinal adenocarcinoma (AhCreER;Apcfl/+;Ptenfl/fl mice). Pepducin-mediated CXCR2 inhibition reduced tumorigenesis in ApcMin/+ mice. Ly6G+ neutrophils were the dominant source of CXCR2 in blood, and CXCR2 deficiency attenuated neutrophil recruitment. Moreover, systemic Ly6G+ cell depletion purged CXCR2-dependent tumor-associated leukocytes, suppressed established skin tumor growth and colitis-associated tumorigenesis, and reduced ApcMin/+ adenoma formation. CXCR2 is thus a potent protumorigenic chemokine receptor that directs recruitment of tumor-promoting leukocytes into tissues during tumor-inducing and tumor-driven inflammation. Similar leukocyte populations were also found in human intestinal adenomas, which suggests that CXCR2 antagonists may have therapeutic and prophylactic potential in the treatment of cancer.

Authors

Thomas Jamieson, Mairi Clarke, Colin W. Steele, Michael S. Samuel, Jens Neumann, Andreas Jung, David Huels, Michael F. Olson, Sudipto Das, Robert J.B. Nibbs, Owen J. Sansom

×

Figure 4

AOM/DSS-induced adenomas express CXCR2 ligands and are infiltrated by MPO+ cells.

Options: View larger image (or click on image) Download as PowerPoint
AOM/DSS-induced adenomas express CXCR2 ligands and are infiltrated by MP...
WT Balb/c mice were treated once i.p. with AOM and then underwent 3 5-day periods of 2% DSS feeding, interspersed by 16 days on normal water. Animals were sacrificed 70 days after AOM injection. (A) Relative abundance of transcripts for Cxcr2 and its ligands in AOM/DSS-induced adenomas, as determined by Q-RT-PCR; mean expression in normal colon of untreated mice is set to 1. **P < 0.01, ***P < 0.001, Mann-Whitney test. (B) Representative adenoma section stained with anti-MPO Ab (brown), counterstained with hematoxylin, and visualized by light microscopy. Scale bar: 100 μm.