Abstracts of the 13th International Conference on Thrombosis and Hemostasis Issues in Cancer, 2026

PO18 | THE THROMBO-INFLAMMATION AXIS AS PREDICTOR OF TOXICITY IN PATIENTS TREATED WITH CAR-T CELLS

C. Fernández-Arias1, M. Marcos-Jubilar1, M. Panizo1, C. Vázquez-Puerta2, J.R. González-Porras2, M. Ibáñez1, A. Queralt1, M. Carrasco1, M.B. Villacrés1, C. Conde1, P. Elizalde1, S. Huerga1, A. Alfonso1, P. Rodríguez-Otero1, S. Villar1, M.A. Canales1, J. Rifón1, F. Prósper1, J.A. Páramo1, J. Orbe1, R. Lecumberri1 | 1Clínica Universidad de Navarra, Pamplona; 2Hospital Clínico Universitario de Salamanca, Salamanca, Spain

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Published: 16 April 2026
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Introduction. CAR-T cell therapy has transformed hematologic malignancies treatment. Cytokine release syndrome (CRS) and immune effector cell–associated neurotoxicity syndrome (ICANS) are its major toxicities. Thromboinflammation, involving neutrophil extracellular traps (NETs) and extracellular vesicles (EVs), remains unexplored in this setting.

Aim. To characterize thromboinflammatory-related biomarkers and EVs of distinct cellular origin, assess temporal dynamics and evaluate their potential as predictors of toxicity after CAR-T therapy.

Methods. Prospective study in adult patients with hematologic malignancies treated with anti-CD19 or anti-BCMA CAR-T at two centers. Samples were collected before lymphodepletion, at infusion, at 48 hours, and 14 days post-infusion. Elastase, double-strand circulating DNA (dsDNAc) and P-selectin were quantified using ELISA and fluorescence-based assays. EVs of red blood cell, platelet, endothelial, and myeloid origin were characterized by flow cytometry. The study analyzed associations between the occurrence of ICANS, clinically significant CRS (grade ≥ 2), and major or clinically relevant bleeding events within 30 days post-infusion.

Results. Sixty-two patients were included (median age 62 years; 65% male): 29 with multiple myeloma and 33 with B-cell malignancies. Clinically significant CRS occurred in 20 patients (31%), and ICANS in 24 (26%), with median onset at days 3 and 6, respectively. Eight major or clinically relevant bleeding events (13%) were observed, all but one after day 14. Only one thrombotic event (1.6%) occurred. Elastase and P-selectin levels decreased after lymphodepletion with partial recovery, while dsDNAc levels remained stable. All EV subtypes declined significantly over time. No biomarker, including EVs, was associated with clinically relevant CRS. In univariate analysis, dsDNAc levels were significantly higher in patients who developed ICANS. DsDNAc at 48 hours remained independently associated with ICANS (OR 24, 95% CI 1.01–570; p=0.049), yielding an AUC of 0.78. At 48 hours, platelet-derived EVs (CD41/61+) and P-selectin levels were associated with bleeding risk, although not independently of platelet count.

Conclusions. Early elevation of circulating dsDNAc may serve as an independent predictor of ICANS and could help in the risk stratification and monitoring of patients undergoing CAR-T cell therapy.
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Emostasi e Trombosi SI di. PO18 | THE THROMBO-INFLAMMATION AXIS AS PREDICTOR OF TOXICITY IN PATIENTS TREATED WITH CAR-T CELLS: C. Fernández-Arias1, M. Marcos-Jubilar1, M. Panizo1, C. Vázquez-Puerta2, J.R. González-Porras2, M. Ibáñez1, A. Queralt1, M. Carrasco1, M.B. Villacrés1, C. Conde1, P. Elizalde1, S. Huerga1, A. Alfonso1, P. Rodríguez-Otero1, S. Villar1, M.A. Canales1, J. Rifón1, F. Prósper1, J.A. Páramo1, J. Orbe1, R. Lecumberri1 | 1Clínica Universidad de Navarra, Pamplona; 2Hospital Clínico Universitario de Salamanca, Salamanca, Spain. Bleeding Thromb Vasc Biol [Internet]. 2026 Apr. 16 [cited 2026 Apr. 17];5(s1). Available from: https://www.btvb.org/btvb/article/view/513

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