EGFR: New Insights on Its Activation and Mutation in Tumor and Tumor Immunotherapy

Abstract The success of immune checkpoint blockades (ICBs) has accelerated the clinical implementation of multiple single agents and combination immunotherapies, but the response rates vary. Reconsideration of immune‐oncology therapeutic failures via perspective from tumor‐intrinsic (such as oncogenic driver genes) and tumor‐extrinsic (the complexity of immune cell–cancer cell interactions) may help to better design more effective anticancer drugs and treatment strategies. Herein, in this review, introducing the frequently mutated gene EGFR in tumors and its abnormal activation are mainly focused on, highlighting that epidermal growth factor receptor (EGFR) wild‐type and mutants respond differently to ICBs via tumor‐intrinsic and tumor‐extrinsic manners. Through briefly reviewing how EGFR is activated and the current EGFR targeting strategy, the present clinical trials of combination with EGFR inhibitors and ICBs are summarized, and the mechanism by which EGFR affects immunotherapy and measures to improve the efficacy of immunotherapy are discussed.