TY - JOUR
T1 - Humoral vaccine responses following Chimeric Antigen Receptor T-cell therapy for hematological malignancies
AU - Einarsdottir, Sigrun
AU - Lobaugh, Stephanie
AU - Luan, Danny
AU - Gomez-Llobell, Marina
AU - Subramanian, Padmapriya
AU - Devlin, Sean
AU - Chung, David
AU - Dahi, Parastoo B.
AU - Falchi, Lorenzo
AU - Giralt, Sergio
AU - Landau, Heather
AU - Lesokhin, Alexander M.
AU - Lin, Richard
AU - Lue, Jennifer
AU - Mailankody, Sham
AU - Palomba, M. Lia
AU - Park, Jae H.
AU - Salles, Gilles
AU - Scordo, Michael
AU - Escribano-Serrat, Silvia
AU - Sanz, Jaime
AU - Rejeski, Kai
AU - Shouval, Roni
AU - Usmani, Saad
AU - Perales, Miguel Angel
AU - Shah, Gunjan
AU - Shahid, Zainab
N1 - Publisher Copyright:
© The Author(s) 2025.
PY - 2025/7/2
Y1 - 2025/7/2
N2 - This single-center, retrospective study analyzed vaccine responses in patients who received post-Chimeric Antigen Receptor (CAR) T-cell therapy vaccination between 2018 and 2024. Vaccinations were administered according to EBMT/CIBMTR recommendations and pathogen-specific IgG responses to 12 vaccine-preventable infections were assessed. Seroprotection was defined by established cut-offs or a significant fold increase in titers. A total of 73 patients that had not received intravenous immunoglobulins within the eight weeks prior to pre- or post titer were included. The median time to vaccination initiation was 13 months (range 6–66) post-CAR T. Pre and post-vaccination titers were available for 49 patients. Pre-vaccination seroprotection was high (> 85%) for tetanus and poliovirus. Among patients not seroprotected prior to vaccination, vaccine response rates were high for tetanus and polio (100%), moderate for diphtheria (75%) and haemophilus influenzae type b (62%), and lower for pertussis (48%), hepatitis A (43%), hepatitis B (44%), and pneumococcal disease (33%). CD19 CAR T recipients had higher pre-vaccination seroprotection rates than BCMA recipients, but vaccine responses did not differ significantly between groups. Pre-vaccination IgA levels were significantly associated with vaccine response, and absolute B-cell counts trended higher among responders (p = 0.054). Our findings highlight the importance of immune reconstitution in vaccine responses post-CAR T.
AB - This single-center, retrospective study analyzed vaccine responses in patients who received post-Chimeric Antigen Receptor (CAR) T-cell therapy vaccination between 2018 and 2024. Vaccinations were administered according to EBMT/CIBMTR recommendations and pathogen-specific IgG responses to 12 vaccine-preventable infections were assessed. Seroprotection was defined by established cut-offs or a significant fold increase in titers. A total of 73 patients that had not received intravenous immunoglobulins within the eight weeks prior to pre- or post titer were included. The median time to vaccination initiation was 13 months (range 6–66) post-CAR T. Pre and post-vaccination titers were available for 49 patients. Pre-vaccination seroprotection was high (> 85%) for tetanus and poliovirus. Among patients not seroprotected prior to vaccination, vaccine response rates were high for tetanus and polio (100%), moderate for diphtheria (75%) and haemophilus influenzae type b (62%), and lower for pertussis (48%), hepatitis A (43%), hepatitis B (44%), and pneumococcal disease (33%). CD19 CAR T recipients had higher pre-vaccination seroprotection rates than BCMA recipients, but vaccine responses did not differ significantly between groups. Pre-vaccination IgA levels were significantly associated with vaccine response, and absolute B-cell counts trended higher among responders (p = 0.054). Our findings highlight the importance of immune reconstitution in vaccine responses post-CAR T.
UR - https://www.scopus.com/pages/publications/105010028186
U2 - 10.1038/s41408-025-01321-w
DO - 10.1038/s41408-025-01321-w
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C2 - 40603286
AN - SCOPUS:105010028186
SN - 2044-5385
VL - 15
JO - Blood Cancer Journal
JF - Blood Cancer Journal
IS - 1
M1 - 114
ER -
