Author: Walti, Carla S.; Loes, Andrea N.; Shuey, Kiel; Krantz, Elizabeth M.; Boonyaratanakornkit, Jim; Keane-Candib, Jacob; Loeffelholz, Tillie; Wolf, Caitlin R.; Taylor, Justin J.; Gardner, Rebecca A.; Green, Damian J.; Cowan, Andrew J.; Maloney, David G.; Turtle, Cameron J.; Pergam, Steven A.; Chu, Helen Y.; Bloom, Jesse D.; Hill, Joshua A.
Title: Humoral immunogenicity of the seasonal influenza vaccine before and after CAR-T-cell therapy Cord-id: ffdmrt6m Document date: 2021_5_11
ID: ffdmrt6m
Snippet: Recipients of chimeric antigen receptor-modified T (CAR-T) cell therapies for B-cell malignancies are immunocompromised and at risk for serious infections. Vaccine immunogenicity is unknown in this population. We conducted a prospective observational study of the humoral immunogenicity of 2019–2020 inactivated influenza vaccines (IIV) in children and adults immediately prior to (n=7) or 13–57 months after (n=15) CD19-, CD20-, or BCMA-targeted CAR-T-cell therapy, as well as controls (n=8). In
Document: Recipients of chimeric antigen receptor-modified T (CAR-T) cell therapies for B-cell malignancies are immunocompromised and at risk for serious infections. Vaccine immunogenicity is unknown in this population. We conducted a prospective observational study of the humoral immunogenicity of 2019–2020 inactivated influenza vaccines (IIV) in children and adults immediately prior to (n=7) or 13–57 months after (n=15) CD19-, CD20-, or BCMA-targeted CAR-T-cell therapy, as well as controls (n=8). Individuals post-CAR-T-cell therapy were in remission. We tested for antibodies to 4 vaccine strains at baseline and ≥1 time point after IIV using neutralization and hemagglutination inhibition assays. An antibody response was defined as a ≥4-fold titer increase from baseline at the first post-vaccine time point. Baseline A(H1N1) titers in the CAR-T cohorts were significantly lower compared to controls. Antibody responses to ≥1 vaccine strain occurred in 2 (29%) individuals before CAR-T-cell therapy; one individual maintained a response for >3 months post-CAR-T-cell therapy. Antibody responses to ≥1 vaccine strain occurred in 6 (40%) individuals vaccinated after CAR-T-cell therapy. An additional 2 (29%) and 6 (40%) individuals had ≥2-fold increases (at any time) in the pre- and post-CAR-T cohorts, respectively. There were no identified clinical or immunologic predictors of antibody responses. Neither severe hypogammaglobulinemia nor B-cell aplasia precluded antibody responses. These data support consideration for vaccination before and after CAR-T-cell therapy for influenza and other relevant pathogens such as SARS-CoV-2, irrespective of hypogammaglobulinemia or B-cell aplasia. Larger studies are needed to determine correlates of vaccine immunogenicity and durability in CAR-T-cell therapy recipients.
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