Efficacy and safety of bendamustine‐containing bridging therapy in R/R LBCL patients receiving CD19 CAR T‐cells
Gloria Iacoboni,
Mario A. Sánchez‐Salinas,
Kai Rejeski,
Ana Á. Martín‐López,
Mi Kwon,
Víctor Navarro,
Katarzyna A. Jalowiec,
Rafael Hernani,
Juan L. Reguera‐Ortega,
Laura Gallur,
Viktoria Blumenberg,
María Herrero‐García,
Claire Roddie,
Ana Benzaquén,
Javier Delgado‐Serrano,
Rebeca Bailén,
Cecilia Carpio,
Paula Amat,
Lucia López‐Corral,
Lourdes Martín‐Martín,
Mariana Bastos,
Marion Subklewe,
Maeve O'Reilly,
Pere Barba
Affiliations
Gloria Iacoboni
Department of Hematology University Hospital Vall d'Hebron Barcelona Spain
Mario A. Sánchez‐Salinas
Department of Hematology University Hospital Vall d'Hebron Barcelona Spain
Kai Rejeski
Department of Medicine III University Hospital, LMU Munich Munich Germany
Ana Á. Martín‐López
Hematology Department Hospital Clínico Universitario de Salamanca, IBSAL, CIBERONC Salamanca Spain
Mi Kwon
Department of Hematology Hospital General Universitario Gregorio Marañón Madrid Spain
Víctor Navarro
Oncology Data Science (ODySey) Group, Vall d'Hebron Institute of Oncology (VHIO) Barcelona Spain
Katarzyna A. Jalowiec
Hematology Department University College London Cancer Institute London United Kingdom
Rafael Hernani
Haematology Department Hospital Clínico Universitario Valencia Spain
Juan L. Reguera‐Ortega
Hematology Department, Hospital Virgen del Rocío, Instituto de Biomedicina de Sevilla (IBIS)/CSIC Universidad de Sevilla Sevilla Spain
Laura Gallur
Department of Hematology University Hospital Vall d'Hebron Barcelona Spain
Viktoria Blumenberg
Department of Medicine III University Hospital, LMU Munich Munich Germany
María Herrero‐García
Cancer Research Centre (IBMCC, USAL‐CSIC), Institute for Biomedical Research of Salamanca (IBSAL) and Department of Medicine and Cytometry Service (NUCLEUS Research Support Platform) University of Salamanca (USAL) Salamanca Spain
Claire Roddie
Hematology Department University College London Cancer Institute London United Kingdom
Ana Benzaquén
Haematology Department Hospital Clínico Universitario Valencia Spain
Javier Delgado‐Serrano
Hematology Department, Hospital Virgen del Rocío, Instituto de Biomedicina de Sevilla (IBIS)/CSIC Universidad de Sevilla Sevilla Spain
Rebeca Bailén
Department of Hematology Hospital General Universitario Gregorio Marañón Madrid Spain
Cecilia Carpio
Department of Hematology University Hospital Vall d'Hebron Barcelona Spain
Paula Amat
Haematology Department Hospital Clínico Universitario Valencia Spain
Lucia López‐Corral
Hematology Department Hospital Clínico Universitario de Salamanca, IBSAL, CIBERONC Salamanca Spain
Lourdes Martín‐Martín
Cancer Research Centre (IBMCC, USAL‐CSIC), Institute for Biomedical Research of Salamanca (IBSAL) and Department of Medicine and Cytometry Service (NUCLEUS Research Support Platform) University of Salamanca (USAL) Salamanca Spain
Mariana Bastos
Department of Hematology Hospital General Universitario Gregorio Marañón Madrid Spain
Marion Subklewe
Department of Medicine III University Hospital, LMU Munich Munich Germany
Maeve O'Reilly
Hematology Department University College London Cancer Institute London United Kingdom
Pere Barba
Department of Hematology University Hospital Vall d'Hebron Barcelona Spain
Abstract Bridging therapy (BT) after leukapheresis is required in most relapsed/refractory (R/R) large B‐cell lymphoma (LBCL) patients receiving chimeric antigen receptor (CAR) T cells. Bendamustine‐containing regimens are a potential BT option. We aimed to assess if this agent had a negative impact on CAR‐T outcomes when it was administered as BT. We included R/R LBCL patients from six centers who received systemic BT after leukapheresis from February 2019 to September 2022; patients who only received steroids or had pre‐apheresis bendamustine exposure were excluded. Patients were divided into two BT groups, with and without bendamustine. Separate safety and efficacy analyses were carried out for axi‐cel and tisa‐cel. Of 243 patients who received BT, bendamustine (benda) was included in 62 (26%). There was a higher rate of BT progressors in the non‐benda group (62% vs. 45%, p = 0.02). Concerning CAR‐T efficacy, complete responses were comparable for benda versus non‐benda BT cohorts with axi‐cel (70% vs. 53%, p = 0.12) and tisa‐cel (44% vs. 36%, p = 0.70). Also, 12‐month progression‐free and overall survival were not significantly different between BT groups with axi‐cel (56% vs. 43% and 71% vs. 63%) and tisa‐cel (25% vs. 26% and 52% vs. 48%); there were no differences when BT response was considered. CAR T‐cell expansion for each construct was similar between BT groups. Regarding safety, CRS G ≥3 (6% vs. 6%, p = 0.79), ICANS G ≥3 (15% vs. 17%, p = 0.68), severe infections, and neutropenia post‐infusion were comparable among BT regimens. BT with bendamustine‐containing regimens is safe for patients requiring disease control during CAR T‐cell manufacturing.
