Impact of Glucocorticoids on Immune Checkpoint Inhibitor Efficacy and Circulating Biomarkers in Non-Small Cell Lung Cancer Patients

Non-Small Cell Lung Cancer (NSCLC) / Leave a Comment

Source: Cancer Research Communications

Baseline corticosteroid use, particularly at high doses (>30 mg prednisone equivalent), significantly reduces the efficacy of immune checkpoint inhibitor (ICI) therapy in non-small cell lung cancer (NSCLC) patients and serves as the strongest independent predictor of poor outcomes. Oncologists should exercise caution when interpreting blood-based immune biomarkers in steroid-treated patients, as steroids impair T-cell maturation and confound predictive markers.

Study Design & Population

  • Study type: Retrospective cohort analysis with preclinical validation
  • Sample size: 277 NSCLC patients receiving ICI therapy at two academic centers
  • Key characteristics: 21 patients (8%) on baseline steroids for ≥12 weeks
  • Institutions: University of Southern California (n=189) and Roswell Park Comprehensive Cancer Center (n=88)

Key Findings

  • Overall response rate: Lower in steroid users versus non-users (specific rates not provided)
  • Progression-free survival: 3.2 vs 10.7 months (USC cohort) and 3.0 vs 6.6 months (RPCCC cohort)
  • Overall survival: 7.7 vs 21.0 months (USC) and 3.7 vs 16.4 months (RPCCC)
  • Independent risk factor: Steroid use was the only significant predictor in multivariate analysis across both cohorts
  • Mechanism: Steroids inhibit T-cell maturation and reduce CX3CR1+CD8+ T cell frequency
  • Biomarker impact: Neutrophil-to-lymphocyte ratio lost prognostic value in steroid-treated patients

Clinical Implications

  • Consider postponing ICI initiation until steroids can be discontinued or tapered to lowest effective dose
  • Standard blood-based biomarkers (NLR, CX3CR1+ CD8+ T cells) may be unreliable in steroid-treated patients
  • High-dose steroids (>30 mg prednisone equivalent) pose greater risk than lower doses
  • Preclinical data suggests stopping steroids at ICI initiation may restore efficacy

Limitations

  • Small steroid cohort: Only 8% of patients on baseline steroids
  • Incomplete biomarker data for NLR and CX3CR1+ CD8+ T cells
  • Limited dose analysis: Small medium-dose group (7.5-30 mg prednisone equivalent)
  • Single mouse model used for preclinical validation
  • 30-day exposure window: Analysis limited to steroid use within 30 days of ICI initiation
  • Higher brain metastases rate (24.2%) than prior studies may confound results

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