Molecular phenotypic linkage between N-methyladenosine methylation and tumor immune microenvironment in hepatocellular carcinoma.

PURPOSE

The crucial role of N-methyladenosine (mA) methylation in anti-tumor immunity and immunotherapy has been broadly depicted. However, the molecular phenotypic linkages between mA modification pattern and immunological ecosystem are expected to be disentangled in hepatocellular carcinoma (HCC), for immunotherapeutic unresponsiveness circumvention and combination with promising drug agents.

METHODS

Modification patterns of mA methylation were qualitatively dissected according to the large-scale HCC samples profiling. We then determined the immune phenotypic linkages by systematically evaluating their tumor microenvironment composition, immune/stromal-relevant signature, immune checkpoints correlation, and prognostic value. Individual quantification of mA methylation pattern was achieved by mAscore construction, intensified by longitudinal single-cell analysis of immunotherapy cohort and validated by the transcriptomic profiles of our in-hospital GDPH-HCC cohort. Candidate therapeutic agents were also screened out.

RESULTS

Three distinct mA methylation patterns were determined in high accordance with inflamed-, excluded-, and desert-immunophenotype. To be precise, Immune-inflamed high-mAscore group was characterized by activated immunity with favorable prognosis. Stromal activation and absence of immune cell infiltration were observed in low-mAscore phenotype, linked to impaired outcome. Patients with low-mAscore demonstrated diminished responses and clinical benefits for cohorts receiving immunotherapy. The above credible linkage between mA methylation pattern and tumor immune microenvironment was robustly validated in our GDPH-HCC cohort. Single-cell dynamic change of mA methylation level in exhausted CD8 T cell and fibroblast was depicted in immunotherapy cohort fore and art. Derived from mA methylation pattern, seven potential frontline drug agents were recognized as promising choice for high-mAscore patients.

CONCLUSION

Our work bridged the credible linkage between epigenetics and anti-tumor immunity in HCC, unraveling mA modification pattern as immunological indicator and predictor for immunotherapy. Individualized mAscore facilitated strategic choices to maximize therapy-responsive possibility.