| Literature DB >> 30518876 |
Ryan Kolb1,2, Paige Kluz3,4, Zhen Wei Tan5, Nicholas Borcherding3,6,7, Nicholas Bormann8, Ajaykumar Vishwakarma3,7, Louis Balcziak9, Pengcheng Zhu5, Brandon Sj Davies10, Francoise Gourronc11, Ling-Zhi Liu3, Xin Ge3, Bing-Hua Jiang3, Katherine Gibson-Corley3, Aloysius Klingelhutz11, Nguan Soon Tan5,12,13,14, Yuwen Zhu15, Fayyaz S Sutterwala16, Xian Shen17, Weizhou Zhang18,19,20,21,22.
Abstract
Obesity is a risk factor for breast cancer and also predicts poor clinical outcomes regardless of menopausal status. Contributing to the poor clinical outcomes is the suboptimal efficacy of standard therapies due to dose limiting toxicities and obesity-related complications, highlighting the need to develop novel therapeutic approaches for treating obese patients. We recently found that obesity leads to an increase in tumor-infiltrating macrophages with activated NLRC4 inflammasome and increased interleukin (IL)-1β production. IL-1β, in turn, leads to increased angiogenesis and cancer progression. Using Next Generation RNA sequencing, we identified an NLRC4/IL-1β-dependent upregulation of angiopoietin-like 4 (ANGPTL4), a known angiogenic factor in cancer, in tumors from obese mice. ANGPTL4-deficiency by genetic knockout or treatment with a neutralizing antibody led to a significant reduction in obesity-induced angiogenesis and tumor growth. At a mechanistic level, ANGPTL4 expression is induced by IL-1β from primary adipocytes in a manner dependent on NF-κB- and MAP kinase-activation, which is further enhanced by hypoxia. This report shows that adipocyte-derived ANGPTL4 drives disease progression under obese conditions and is a potential therapeutic target for treating obese breast cancer patients.Entities:
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Year: 2018 PMID: 30518876 PMCID: PMC6440811 DOI: 10.1038/s41388-018-0592-6
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867