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Longitudinal Blood Immune-Inflammatory and Radiomic Profiling to Decode Different Patterns of Acquired Resistance to Immunotherapy in Patients with NSCLC

Articolo
Data di Pubblicazione:
2024
Abstract:
Purpose: To uncover the underpinnings of acquired resistance (AR) to immunotherapy (IO), we determined whether distinctive clinico-pathological, radiomic and peripheral blood (PB) immune-inflammatory features reflect oligo- and systemic (sys)-AR in advanced NSCLC patients undergoing immune checkpoints inhibitors. Experimental design: On 105 consecutive IO-treated advanced NSCLC, PB immunophenotypes, cytokines and CT-derived radiomic features (RFs), extracted from primary and merged metastatic lesions, were prospectively collected at baseline (T0) and first disease assessment (T1, 9-12 weeks), and their delta (Δ) variation [(T1-T0)/T0] computed. AR, defined as progression after initial response (complete/partial) or stable disease ≥ 6 months, was subdivided according to the number of new and/or progressive lesions in oligoAR (≤3) and sysAR (>3). Clinico-pathological, PB and radiomic parameters and survival outcome were statistically correlated to AR patterns. Results: OligoAR and sysAR involved 24% and 12.4% of cases, respectively. While baseline PB immune profiles were comparable, a Δpos cytotoxic (NK, CD8+GnzB+) and Δneg immunosuppressive (CD14+ monocytes) dynamic coupled with different modulation of IL-6, TGF-β1, TNFα and sPD-L1 represented distinctive features of oligoAR vs sysAR (P<0.05). Significantly longer post-progression survival characterized oligoAR vs sysAR (median 20.3 vs 5.6 months;HR:0.22,P<0.001). The number and sites of oligoAR involvement appeared to condition blood immune background (P<0.05) and survival. Delta radiomic outperformed baseline RFs, with 15 ΔRFs sharply discriminating oligoAR from sysAR (P range:<0.001-0.04). ROC analysis confirmed the optimal performance of top-ranked ΔRFs (AUC range:0.88-0.99). Conclusions: Longitudinal analysis of blood immune hallmarks and radiomic descriptors may decipher distinct patterns of AR to IO in advanced NSCLC patients.
Tipologia CRIS:
03A-Articolo su Rivista
Elenco autori:
Mazzaschi, Giulia; Marrocchio, Cristina; Moron Dalla Tor, Lucas; Leo, Ludovica; Balbi, Maurizio; Milanese, Gianluca; Adebanjo, Ganiyat A.R.; Lorusso, Bruno; Monica, Gregorio; Pluchino, Monica; Minari, Roberta; D'Agnelli, Simona; Cardinale, Elisa; Perrone, Fabiana; Bordi, Paola; Leonetti, Alessandro; Ledda, Roberta E.; Silva, Mario; Buti, Sebastiano; Roti, Giovanni; Bettati, Stefano; Quaini, Federico; Tiseo, Marcello; Sverzellati, Nicola
Autori di Ateneo:
BALBI Maurizio
Link alla scheda completa:
https://iris.unito.it/handle/2318/2046411
Pubblicato in:
CLINICAL CANCER RESEARCH
Journal
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