@article {Kimmane006364, author = {Thomas Kimman and Anne Slomp and Anne Martens and Sarah Grabherr and Shuang Li and Eline van Diest and Jan Meeldijk and Jurgen Kuball and Monique C Minnema and Eric Eldering and Niels Bovenschen and Zsolt Sebesty{\'e}n and Victor Peperzak}, title = {Serpin B9 controls tumor cell killing by CAR T cells}, volume = {11}, number = {3}, elocation-id = {e006364}, year = {2023}, doi = {10.1136/jitc-2022-006364}, publisher = {BMJ Specialist Journals}, abstract = {Background Initial clinical responses with gene engineered chimeric antigen receptor (CAR) T cells in cancer patients are highly encouraging; however, primary resistance and also relapse may prevent durable remission in a substantial part of the patients. One of the underlying causes is the resistance mechanisms in cancer cells that limit effective killing by CAR T cells. CAR T cells exert their cytotoxic function through secretion of granzymes and perforin. Inhibition of granzyme B (GrB) can underlie resistance to T cell-mediated killing, and it has been shown that serine proteinase inhibitor serpin B9 can effectively inhibit GrB. We aimed to determine whether expression of serpin B9 by cancer cells can lead to resistance toward CAR T cells.Methods Serpin B9 gene and protein expression were examined by R2 or DepMap database mining and by western blot or flow cytometric analysis, respectively. Coculture killing experiments were performed with melanoma cell line MeWo, diffuse large B cell lymphoma (DLBCL) cell line OCI-Ly7 or primary chronic lymphocytic leukemia (CLL) cells as target cells and natural killer cell line YT-Indy, CD20 CAR T cells or CD19 CAR T cells as effector cells and analyzed by flow cytometry.Results Serpin B9 protein expression was previously shown to be associated with clinical outcome in melanoma patients and in line with these observations we demonstrate that enforced serpin B9 expression in melanoma cells reduces sensitivity to GrB-mediated killing. Next, we examined serpin B9 expression in a wide array of primary tumor tissues and human cell lines to find that serpin B9 is uniformly expressed in B-cell lymphomas and most prominently in DLBCL and CLL. Subsequently, using small interfering RNA, we silenced serpin B9 expression in DLBCL cells, which increased their sensitivity to CD20 CAR T cell-mediated killing. In addition, we showed that co-ulture of primary CLL cells with CD20 CAR T cells results in selection of serpin B9-high CLL cells, suggesting these cells resist CAR T-cell killing.Conclusions Overall, the data indicate that serpin B9 is a resistance mediator for CAR T cell-mediated tumor cell killing that should be inhibited or bypassed to improve CAR T-cell responses.The datasets used in the current study are available from the corresponding author on reasonable request.}, URL = {https://jitc.bmj.com/content/11/3/e006364}, eprint = {https://jitc.bmj.com/content/11/3/e006364.full.pdf}, journal = {Journal for ImmunoTherapy of Cancer} }