AI Article Synopsis
- The study investigates how estrogen signaling influences the effectiveness of immunotherapy in melanoma, aiming to create a gene signature for predicting treatment responses.
- Using RNA sequencing from various melanoma datasets, researchers identified 11 estrogen response-related genes that distinguish between immunotherapy responders and non-responders, leading to a predictive model.
- The findings suggest that a higher signature score correlates with better immune cell infiltration and improved patient outcomes, highlighting the potential for personalized immunotherapy approaches in melanoma based on estrogen-related genes.
Article Abstract
Background: Estrogen/estrogen receptor signaling influences the tumor microenvironment and affects the efficacy of immunotherapy in some tumors, including melanoma. This study aimed to construct an estrogen response-related gene signature for predicting response to immunotherapy in melanoma.
Methods: RNA sequencing data of 4 immunotherapy-treated melanoma datasets and TCGA melanoma was obtained from open access repository. Differential expression analysis and pathway analysis were performed between immunotherapy responders and non-responders. Using dataset GSE91061 as the training group, a multivariate logistic regression model was built from estrogen response-related differential expression genes to predict the response to immunotherapy. The other 3 datasets of immunotherapy-treated melanoma were used as the validation group. The correlation was also examined between the prediction score from the model and immune cell infiltration estimated by xCell in the immunotherapy-treated and TCGA melanoma cases.
Results: "Hallmark Estrogen Response Late" was significantly downregulated in immunotherapy responders. 11 estrogen response-related genes were significantly differentially expressed between immunotherapy responders and non-responders, and were included in the multivariate logistic regression model. The AUC was 0.888 in the training group and 0.654-0.720 in the validation group. A higher 11-gene signature score was significantly correlated to increased infiltration of CD8+ T cells (rho=0.32, p=0.02). TCGA melanoma with a high signature score showed a significantly higher proportion of immune-enriched/fibrotic and immune-enriched/non-fibrotic microenvironment subtypes (p<0.001)-subtypes with better response to immunotherapy-and significantly better progression-free interval (p=0.021).
Conclusion: In this study, we identified and verified an 11-gene signature that could predict response to immunotherapy in melanoma and was correlated with tumor-infiltrating lymphocytes. Our study suggests targeting estrogen-related pathways may serve as a combination strategy for immunotherapy in melanoma.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10213284 | PMC |
| http://dx.doi.org/10.3389/fimmu.2023.1109300 | DOI Listing |
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