Monocyte recruitment and activated inflammation are associated with thyroid carcinogenesis in a mouse model

Sunmi Park; Jack Zhu; Grégoire Altan-Bonnet; Sheue-Yann Cheng

Monocyte recruitment and activated inflammation are associated with thyroid carcinogenesis in a mouse model

Am J Cancer Res. 2019 Jul 1;9(7):1439-1453. eCollection 2019.

Authors

Sunmi Park¹, Jack Zhu², Grégoire Altan-Bonnet³, Sheue-Yann Cheng¹

Affiliations

¹ Laboratory of Molecular Biology, Cancer and Inflammation Program, Center for Cancer Research, National Cancer Institute Bethesda, Maryland 20892-4264, USA.
² Cancer Genetics Branch, Cancer and Inflammation Program, Center for Cancer Research, National Cancer Institute Bethesda, Maryland 20892-4264, USA.
³ Immunodynamics Group, Cancer and Inflammation Program, Center for Cancer Research, National Cancer Institute Bethesda, Maryland 20892-4264, USA.

PMID: 31392080
PMCID: PMC6682719

Abstract

Thyroid cancer is the most common endocrine malignancy. Although an association between inflammation and thyroid cancer has long been recognized, a cause-effect relationship at the molecular level has yet to be elucidated. We explored how inflammation could contribute to thyroid carcinogenesis in Thrb^PV/PVPten^+/- mice. The Thrb^PV/PVPten^+/- mouse expresses a dominantly negative thyroid hormone receptor β (denoted as PV) and a deletion of one single allele of the Pten gene. This mutant mouse exhibits aggressive follicular thyroid cancer similarly as in patients. We found significantly increased infiltration of inflammatory monocytes in thyroid tumors of Thrb^PV/PVPten^+/- mice, while no apparent changes in monocyte homeostasis in the bone marrow and blood of tumor-bearing mice. Using global gene expression profiling, we found altered expression of inflammation mediators in that the expression of Ptgs1, Sphk1, OPN, Chil1, Tnfrsf18, IL6, and Ccl12 genes was significantly increased and expression of Kit, Ly96, Ephx2, CD163, IL15, and Ccr2 was significantly decreased. Subsequent validation of the gene expression by mRNA analysis prompted us to further delineate the inflammatory role of osteopontin (OPN) in thyroid carcinogenesis because of its critical role in monocyte/macrophage functions and proinflammatory responses. We found that the protein abundance of OPN and its receptor, integrin β1, was highly increased and, concurrently, the downstream effectors AKT and NF-κB were significantly elevated to drive thyroid tumor progression of Thrb^PV/PVPten^+/- mice. These results demonstrated that increased inflammation driven by elevated expression of immune-related genes and cytokines promoted thyroid cancer progression. Importantly, we uncovered OPN as a novel regulator in inflammatory response during thyroid carcinogenesis. These preclinical findings suggested that OPN can be a potential target for thyroid cancer therapy via modulation of inflammatory signaling.

Keywords: AKT signaling; Inflammation; activated monocytes; apoptosis; cDNA microarrays; integrins; osteopontin; thyroid cancer.