RNA sequencing of MC38 tumor cells from control-diet- and high-fat-diet-fed C57BL/6J mice

Multiple cancers, including colorectal cancer (CRC), are more frequent and often more aggressive in obese individuals. Here, we show that macrophages accumulate within tumors of obese CRC patients and in obese CRC mice and promote accelerated tumor growth. These changes are initiated by oleic acid accumulation and subsequent tumor cell-derived acid production, and driven by signaling through GPR65, an acid-sensing receptor on CRC-associated macrophages. We demonstrate a similar role for GPR65 in hepatocellular carcinoma (HCC) in obese mice. Tumors in obese patients with CRC or HCC also exhibit increased GPR65 expression, suggesting that the mechanism revealed here likely contributes to tumor growth in a range of obesity-associated cancers and represents a potential therapeutic target. Gene expression profiling of MC38 tumor cells, characterized as CD45-negative cells and dTomato-positive via sorting, from 5 control-diet-fed and 5 high-fat-diet-fed mice 21 days post implantation.