Litcius/Paper detail

IL-6 promotes tumor growth through immune evasion but is dispensable for cachexia

Young‐Yon Kwon, Sheng Hui

2024EMBO Reports17 citationsDOIOpen Access PDF

Abstract

Various cytokines have been implicated in cancer cachexia. One such cytokine is IL-6, deemed as a key cachectic factor in mice inoculated with colon carcinoma 26 (C26) cells, a widely used cancer cachexia model. Here we tested the causal role of IL-6 in cancer cachexia by knocking out the IL-6 gene in C26 cells. We found that the growth of IL-6 KO tumors was dramatically delayed. More strikingly, while IL-6 KO tumors eventually reached the similar size as wild-type tumors, cachexia still took place, despite no elevation in circulating IL-6. In addition, the knockout of leukemia inhibitory factor (LIF), another IL-6 family cytokine proposed as a cachectic factor in the model, also affected tumor growth but not cachexia. We further showed an increase in the infiltration of immune cell population in the IL-6 KO tumors compared with wild-type controls and the defective IL-6 KO tumor growth was rescued in immunodeficient mice while cachexia was not. Thus, IL-6 promotes tumor growth by facilitating immune evasion but is dispensable for cachexia.

Topics & Concepts

CachexiaCytokineImmune systemBiologyCancer researchImmunologyLeukemia inhibitory factorPopulationCancerInterleukin 6MedicineGeneticsEnvironmental healthCytokine Signaling Pathways and Interactionsinterferon and immune responsesCancer, Hypoxia, and Metabolism