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This research investigates the role of THRB in immune regulation and its potential as a biomarker in clear cell renal cell carcinoma (ccRCC).

April 16, 2026Open Access

Downregulation of THRB drives immune microenvironment suppression and poor outcomes, acting as a dual biomarker for clear cell renal cell carcinoma

Key Points

This research investigates the role of THRB in immune regulation and its potential as a biomarker in clear cell renal cell carcinoma (ccRCC).
Analyzed TCGA-KIRC and validation cohorts for THRB expression and correlations with clinical data
Conducted survival analysis using Kaplan-Meier and Cox regression
Assessed immune infiltration with CIBERSORT and ESTIMATE methods
Evaluated functional enrichment via GO, KEGG, GSEA
Examined drug sensitivity predictions with pRRophetic
THRB is downregulated in ccRCC and correlates with advanced stage and poorer survival outcomes
Multivariate analysis confirms THRB's independent prognostic value
Low-THRB tumors exhibit higher immune activation with increased CD8⁺ T cells and Treg markers
THRB correlates negatively with tumor mutational burden and positive with inhibitory checkpoints
Predictions indicate lower sensitivity to sunitinib/pazopanib in low-THRB patients

Abstract

Clear cell renal cell carcinoma (ccRCC) frequently resists targeted and immune therapies, necessitating predictive biomarkers. Thyroid hormone receptor beta (THRB), a nuclear transcription factor at 3p21-25, shows tumor-suppressive roles in other cancers but its immunomodulatory function in ccRCC remains unclear. Using TCGA-KIRC data (535 tumors, 72 normals) and validation cohorts (GSE46699/53757), we analyzed THRB expression, clinical correlations, and immune associations via differential expression (limma), survival analysis (Kaplan-Meier/Cox regression), immune infiltration (CIBERSORT/ESTIMATE), functional enrichment (GO/KEGG/GSEA), and drug sensitivity (pRRophetic). THRB was significantly downregulated in ccRCCand 11 other cancers (P < 0.05), correlating with advanced stage/grade (P < 0.001) and poorer survival (OS HR = 2.33, DSS HR = 3.43; P < 0.001). Multivariate analysis confirmed its independent prognostic value (HR = 0.69, P = 0.007). Functionally, THRB associated with immune regulation (T-cell activation, PD-1/PD-L1 pathways) and distinct immune infiltration patterns. High-THRB tumors were enriched for resting immune cells and M2 macrophages, while low-THRB tumors showed higher fractions of CD8⁺ T cells and regulatory T cells (Tregs), along with elevated expression of T-cell exhaustion markers (all P < 0.01). This suggests a complex role for THRB in shaping the immune landscape. THRB negatively correlated with TMB (r=-0.26, P < 0.001) and inhibitory checkpoints (LGALS9, CD70), but positively with VTCN1. In silico analysis predicted that low-THRB patients might exhibit reduced sensitivity to sunitinib/pazopanib (higher IC50, P < 0.001). THRB downregulation is associated with poor prognosis, an immunosuppressive microenvironment, and resistance to targeted therapies in ccRCC. These findings suggest its potential as a dual biomarker, implying that THRB loss may contribute to immune dysregulation and therapy resistance. Restoring THRB-mediated pathways may offer novel therapeutic strategies, though its predictive value for immunotherapy requires future clinic validation.

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Downregulation of THRB drives immune microenvironment suppression and poor outcomes, acting as a dual biomarker for clear cell renal cell carcinoma

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Abstract

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