Abstract 2315P
Background
To uncover the underpinnings of acquired resistance (AR) to Immune Checkpoint Inhibitors (ICIs), we determined whether distinctive clinicopathological and peripheral blood (PB) immune-inflammatory features reflect oligo and systemic (sys) AR in advanced NSCLC patients undergoing ICIs.
Methods
On PB collected at baseline (T0) and first disease assessment (T1) from 105 ICI-treated NSCLC, we prospectively assessed LDH, derived Neutrophil-to-Lymphocyte ratio (dNLR), LIPI score, relevant immunophenotypes (flow-cytometry) and their respective delta (Δ) % variation [(T1-T0)/T0]. AR, defined as progression after initial response (CR/PR/SD ≥ 6 mos.), was subdivided according to the number of new and/or progressive lesions in oligoAR (≤ 3) and sysAR (> 3). Initial PD or SD < 6 mos. embodied non responders (NR), while absence of progression or PFS ≥ 12 mos. enclosed long-term/not progressors (LT/NP). Clinicopathological, PB parameters and survival outcome were statistically evaluated according to AR pattern.
Results
OligoAR involved 24% of cases, while sysAR 12.4%. Compared to NR, oligoAR pattern was associated with significantly lower T0 and Δ LDH, dNLR and LIPI, whereas no differences were observed vs sysAR and LT/NP. While baseline PB immune profiles were comparable, a Δ positive cytotoxic (NK, NKT, CD8+Ki67+, CD8+Gnz+) and Δ negative immunosuppressive (CD14+ monocytes, CD4+CD25+FOXP3+ Tregs) dynamics was distinctive of oligoAR vs sysAR (P < 0.05). Conversely, compared to LT/NP, oligoAR cases showed a lower cytotoxic/proliferating CD8 response coupled with higher CD14+/Tregs feedback (P < 0.05). Within oligoAR, patients with 1 progressive lesion, compared to those with ≥ 2, exhibited baseline lower LDH and higher NK/CD8+Gnz+ cytotoxic cells (P < 0.05) which in turn appeared to condition longer OS (HR: 4.90; P=0.04). Importantly, despite similar clinical profile, prolonged post-progression survival characterized oligoAR vs sysAR (median OS not reached vs 11.3 mos.; HR: 0.21, 95% CI: 0.08-0.59; P = 0.001).
Conclusions
The longitudinal analysis of blood immune hallmarks intersected with clinicopathological features may decipher the distinct patterns of AR in ICI-treated NSCLC patients.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
University Hospital of Parma.
Funding
AIRC - Italian Association for Cancer Research.
Disclosure
All authors have declared no conflicts of interest.
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