Annabel Meireson1,2, Simon J Tavernier3,4, Sofie Van Gassen5,6, Nora Sundahl1,7, Annelies Demeyer1,2, Mathieu Spaas1,7, Vibeke Kruse1,8, Liesbeth Ferdinande9, Jo Van Dorpe1,9, Benjamin Hennart10,11, Delphine Allorge10,11, Filomeen Haerynck3, Karel Decaestecker1,12, Sylvie Rottey1,8, Yvan Saeys1,5,6, Piet Ost1,7, Lieve Brochez1,2. 1. Cancer Research Institute Ghent (CRIG), Ghent University, 9000 Ghent, Belgium. 2. Dermatology Research Unit, Ghent University Hospital, 9000 Ghent, Belgium. 3. Centre for Primary Immunodeficiency Ghent, Primary Immune Deficiency Research Lab, Department of Internal Medicine and Pediatrics, Jeffrey Modell Diagnosis and Research Centre, Ghent University Hospital, 9000 Ghent, Belgium. 4. VIB Center for Inflammation Research, Unit of Molecular Signal Transduction in Inflammation, 9000 Ghent, Belgium. 5. VIB Center for Inflammation Research, Unit of Data Mining and Modeling for Biomedicine, 9000 Ghent, Belgium. 6. Department of Applied Mathematics, Computer Science and Statistics, Ghent University, 9000 Ghent, Belgium. 7. Department of Radiation Oncology and Experimental Cancer Research, Ghent University Hospital, 9000 Ghent, Belgium. 8. Department of Medical Oncology, Ghent University Hospital, 9000 Ghent, Belgium. 9. Department of Pathology, Ghent University Hospital, 9000 Ghent, Belgium. 10. Unité Fonctionnelle de Toxicologie, CHU Lille, F-59000 Lille, France. 11. ULR 4483-IMPact de l'Environnement Chimique sur la Santé Humaine (IMPECS), Université de Lille, F-59000 Lille, France. 12. Department of Urology, Ghent University Hospital, 9000 Ghent, Belgium.
Abstract
(1) Background: Blockade of the PD-1/PD-L1 pathway has revolutionized the oncology field in the last decade. However, the proportion of patients experiencing a durable response is still limited. In the current study, we performed an extensive immune monitoring in patients with stage III/IV melanoma and stage IV UC who received anti-PD-1 immunotherapy with SBRT. (2) Methods: In total 145 blood samples from 38 patients, collected at fixed time points before and during treatment, were phenotyped via high-parameter flow cytometry, luminex assay and UPLC-MS/MS. (3) Results: Baseline systemic immunity in melanoma and UC patients was different with a more prominent myeloid compartment and a higher neutrophil to lymphocyte ratio in UC. Proliferation (Ki67+) of CD8+ T-cells and of the PD-1+/PD-L1+ CD8+ subset at baseline correlated with progression free survival in melanoma. In contrast a higher frequency of PD-1/PD-L1 expressing non-proliferating (Ki67-) CD8+ and CD4+ T-cells before treatment was associated with worse outcome in melanoma. In UC, the expansion of Ki67+ CD8+ T-cells and of the PD-L1+ subset relative to tumor burden correlated with clinical outcome. (4) Conclusion: This study reveals a clearly different immune landscape in melanoma and UC at baseline, which may impact immunotherapy response. Signatures of proliferation in the CD8+ T-cell compartment prior to and early after anti-PD-1 initiation were positively correlated with clinical outcome in both cohorts. PD-1/PD-L1 expression on circulating immune cell subsets seems of clinical relevance in the melanoma cohort.
(1) Background: Blockade of the PD-1/PD-L1 pathway has revolutionized the oncology field in the last decade. However, the proportion of patients experiencing a durable response is still limited. In the current study, we performed an extensive immune monitoring in patients with stage III/IV melanoma and stage IV UC who received anti-PD-1 immunotherapy with SBRT. (2) Methods: In total 145 blood samples from 38 patients, collected at fixed time points before and during treatment, were phenotyped via high-parameter flow cytometry, luminex assay and UPLC-MS/MS. (3) Results: Baseline systemic immunity in melanoma and UCpatients was different with a more prominent myeloid compartment and a higher neutrophil to lymphocyte ratio in UC. Proliferation (Ki67+) of CD8+ T-cells and of the PD-1+/PD-L1+ CD8+ subset at baseline correlated with progression free survival in melanoma. In contrast a higher frequency of PD-1/PD-L1 expressing non-proliferating (Ki67-) CD8+ and CD4+ T-cells before treatment was associated with worse outcome in melanoma. In UC, the expansion of Ki67+ CD8+ T-cells and of the PD-L1+ subset relative to tumor burden correlated with clinical outcome. (4) Conclusion: This study reveals a clearly different immune landscape in melanoma and UC at baseline, which may impact immunotherapy response. Signatures of proliferation in the CD8+ T-cell compartment prior to and early after anti-PD-1 initiation were positively correlated with clinical outcome in both cohorts. PD-1/PD-L1 expression on circulating immune cell subsets seems of clinical relevance in the melanoma cohort.
Entities:
Keywords:
anti-PD-1; blood biomarkers; immune monitoring; immunotherapy; melanoma; urothelial cancer
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