Early assessment of IL8 and PD1+ Treg predicts response and guides treatment monitoring in cemiplimab-treated cutaneous squamous cell carcinoma

下调和上调 白细胞介素8 医学 免疫系统 CD8型 细胞因子 癌症研究 免疫学 内科学 生物 基因 生物化学
作者
Daniela Esposito,Fabiana Napolitano,Daniela Claudia Maresca,Marcello Scala,Annarita Amato,Stefania Belli,Claudia Maria Ascione,Angela Vallefuoco,Giuseppe Attanasio,Fabio Somma,Angela Ianaro,Daniela Russo,Silvia Varricchio,Massimo Mascolo,Cláudia Dias da Costa,Alessandro Villa,Massimiliano Scalvenzi,Gianfranco Orlandino,Teresa Troiani,Alberto Servetto,Roberto Bianco,Giuseppe Ercolano,Luigi Formisano
出处
期刊:Journal for ImmunoTherapy of Cancer [BMJ]
卷期号:13 (1): e010421-e010421
标识
DOI:10.1136/jitc-2024-010421
摘要

Purpose Anti-programmed cell death 1 (PD1) is the first-choice treatment in patients with advanced cutaneous squamous cell carcinoma (cSCC), when curative options are unavailable. However, reliable biomarkers for patient selection are still lacking. Experimental design In this translational study, clinical annotations, tissue and liquid biopsies were acquired to investigate the association between sustained objective responses and transcriptional profiles, immune cell dynamics in tumor tissue and peripheral blood samples, as well as circulating cytokine levels. Results First, we investigated the baseline characteristics of the immune landscape of cSCC biopsies. Gene Set Enrichment Analysis showed upregulation of interleukin (IL)2/STAT5 pathways and downregulation of Interferon signatures in non-responder patients compared with responders. Next, we studied the early changes induced by cemiplimab in tissue biopsies. Notably, after only three weeks, cemiplimab treatment induced an increase in B cells and CD8+ T cells in responders, whereas their abundance decreased in non-responder patients. Moreover, analyzing differentially expressed genes modulated early during treatment, compared with baseline biopsies, we found that IL1β and IL8 exhibited early downregulation in responder patients’ tumor specimens. We assessed whether changes in the local tumor microenvironment were mirrored in peripheral blood. Similar to tissue findings, no changes were observed in the whole T regulatory (Treg) population, although PD1+ Tregs, which were downregulated in responder patients (vs T0), showed a rebound enrichment in non-responders after three cycles of cemiplimab. Finally, IL8 mirrored the tissue results, unlike IL1β, with early (T1) and then sustained (T3) downregulation of its levels in responder patients, while increased in non-responders. Conclusions Taken together, these findings shed light on the significance of early transcriptomic and immune cell modulation in predicting responses to cemiplimab therapy. Additionally, our data suggest that IL8 levels in peripheral blood offer promising avenues for personalized treatment selection and response assessment in patients with cSCC receiving cemiplimab, while PD1+Tregs can be followed longitudinally to monitor response to therapy.

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