Sensitivity to immune checkpoint inhibitors in BRAF/MEK inhibitor refractory melanoma

Patel, RP; Lim, LRJ; Saleh, R; Schenk, D; Lee, MK; Lelliott, E; Rao, AD; Arabi, S; Smith, L; Trigos, AS; Haynes, N; McArthur, GA; Sheppard, KE

Author(s): Patel, RP; Lim, LRJ; Saleh, R; Schenk, D; Lee, MK; Lelliott, E; Rao, AD; Arabi, S; Smith, L; Trigos, AS; Haynes, N; McArthur, GA; Sheppard, KE;
Details: Publication Year 2025-05-15,Volume 13,Issue #5,Page e011551
Journal Title: Journal for ImmunoTherapy of Cancer
Publication Type: Research article
Abstract: BACKGROUND: Resistance to BRAF and MEK inhibitors (BRAFi/MEKi) in metastatic melanoma frequently results in cross-resistance to immune checkpoint inhibitors (ICI), limiting effective treatment options. However, a subset of BRAFi/MEKi-resistant patients remains responsive to second-line ICI, suggesting heterogeneous underlying resistance mechanisms. This study aimed to explore the tumor immune microenvironment in BRAFi/MEKi-resistant melanoma to uncover factors influencing sensitivity to second-line ICI therapy. METHOD: To investigate mechanisms underlying resistance and responsiveness to second-line ICIs, BRAFi/MEKi-resistant melanoma mouse models were used. Flow cytometry was employed to analyze immune cell populations within the tumor microenvironment, focusing on changes in CD8+T effector cells and other key immune subsets. RNA sequencing was performed to profile transcriptomic changes in resistant tumors, providing insights into the signaling pathways associated with resistance. Clinical samples from BRAFi/MEKi-resistant patients were further evaluated for correlations between immune profiles and key signaling pathways to support findings from the preclinical models. RESULTS: Using BRAFi/MEKi-resistant melanoma mouse models, we observed distinct alterations in the tumor-immune microenvironment. Tumors exhibiting resistance showed a significant increase in CD8+T effector cells following BRAFi/MEKi treatment, suggesting an immune-stimulatory response. Mechanistic analysis identified the activation of the EGFR-STAT signaling pathway as a key driver of intrinsic resistance in these models. Notably, these tumors retained sensitivity to second-line ICI therapy, contrasting with NRAS-driven BRAFi/MEKi-resistant tumors, which demonstrated cross-resistance to ICIs. Supporting these findings, clinical samples from BRAFi/MEKi-resistant patients revealed a correlation between elevated EGFR activation and higher immune scores, indicating potential sensitivity to ICI therapy in this subset of patients. CONCLUSION: EGFR overexpression emerges as a potential predictive biomarker for responsiveness to second-line ICIs in BRAFi/MEKi-resistant melanoma. These findings underscore the need for stratified therapeutic approaches and highlight EGFR as a target for improving outcomes in ICI therapy.
Publisher: BMJ
Keywords: *Immune Checkpoint Inhibitors/pharmacology/therapeutic use; Animals; Mice; Humans; *Melanoma/drug therapy/pathology/genetics/immunology; *Proto-Oncogene Proteins B-raf/antagonists & inhibitors; *Drug Resistance, Neoplasm; *Protein Kinase Inhibitors/pharmacology/therapeutic use; Tumor Microenvironment; Female; Cell Line, Tumor; Immune Checkpoint Inhibitors; Skin Cancer; Subcutaneous; Tumor infiltrating lymphocyte - TIL; Tumor microenvironment - TME
Department(s): Laboratory Research
Publisher's Version: https://doi.org/10.1136/jitc-2025-011551
Open Access at Publisher's Site: https://doi.org/10.1136/jitc-2025-011551
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 2025-06-03 03:44:11

Last Modified: 2025-06-03 03:44:24