Systematic review and meta-analysis on NY-ESO-1 expression in triple-negative breast cancer
Photo by National Cancer Institute / Unsplash
Key Takeaway
Consider the reported NY-ESO-1 prevalence in TNBC as variable and method-dependent.
This is a systematic review and meta-analysis of observational studies on NY-ESO-1 expression in triple-negative breast cancer (TNBC). The scope was to synthesize prevalence data from 12 studies comprising 1,545 TNBC patients.
The main synthesized finding is a pooled NY-ESO-1 expression prevalence of 16.1% (95% CI: 11.4-22.2%). The analysis showed high heterogeneity (I²=83.7%). Expression rates varied significantly by antibody clone (E978: 15.1% vs. D8.38: 32.6%, p<0.0001) and by scoring method (composite scoring: 15.9% vs. dual scoring: 16.9% vs. H-score: 10.1% vs. simple threshold: 32.6%, p<0.001).
The authors acknowledge limitations including NY-ESO-1 expression heterogeneity, a lack of TNBC-specific clinical trials, and inadequate immunogenicity data. Safety was reported as manageable, but specific adverse event rates were not reported.
Practice relevance is restrained; the authors suggest future research should standardize NY-ESO-1 detection protocols to identify patients for NY-ESO-1-targeted immunotherapy and prioritize TNBC-specific trials. This is an observational synthesis and does not establish causation.
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View Original Abstract ↓
Breast cancer remains one of the most common types of cancer, including the subtype triple-negative breast cancer (TNBC) which is challenging to treat due to its aggressiveness. Cancer-testis antigens (CTAs), especially New York Esophageal Squamous Cell Carcinoma 1 (NY-ESO-1), have become promising immunotherapeutic targets attributable to their restricted expression profile in normal tissues but overexpressed in TNBC, leading to immunogenicity. This review provides comprehensive discussion of NY-ESO-1 including its structural basis of NY-ESO-1 recognition by T cell receptors (TCRs) and antibodies, epigenetic regulation via DNA methylation or histone modifications, and expression patterns or clinical relevance in TNBC. A systematic meta-analysis of 12 studies comprising 1,545 TNBC patients showed a pooled NY-ESO-1 expression prevalence of 16.1% (95% CI: 11.4-22.2%), with heterogeneity (I=83.7%) attributable to antibody clone used for NY-ESO-1 detection (E978: 15.1% vs. D8.38: 32.6%, p<0.0001) and scoring methods (composite scoring: 15.9% vs. dual scoring: 16.9% vs. H-score: 10.1% vs. simple threshold: 32.6%, p<0.001). Structural analyses reveal NY-ESO-1 recognition by TCRs, antibodies, and engineered binding scaffolds. We examine preclinical and clinical evidence for NY-ESO-1-targeted therapies, including adoptive cell therapy and peptide vaccines, which show manageable safety profiles and induce immunological responses. Epigenetic regulation is a therapeutic avenue, whereby hypomethylating agents and histone deacetylase inhibitors can upregulate NY-ESO-1 expressions that promote tumor immunogenicity. Nonetheless, challenges persist such as NY-ESO-1 expression heterogeneity, lack of TNBC-specific clinical trials, and inadequate immunogenicity. Future research should standardize NY-ESO-1 detection protocols to identify TNBC patients for NY-ESO-1-targeted immunotherapy, prioritize TNBC-specific trials and combinations with epigenetic priming agents.
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