Induction of resistance to chimeric antigen receptor T cell therapy by transduction of a single leukemic B cell

Ruella, Marco; Xu, Jun; Barrett, David M.; Fraietta, Joseph A.; Reich, Tyler J.; Ambrose, David E; Klichinsky, Michael; Shestova, Olga; Patel, Prachi; Kulikovskaya, Irina; Nazimuddin, Farzana; Bhoj, Vijay; Orlando, Elena; Fry, Terry J.; Bitter, Hans; Maude, Shannon L.; Levine, Bruce L.; Nobles, Christopher L.; Bushman, Frederic D.; Young, Regina M.; Scholler, John; Gill, Saar; June, Carl H.; Grupp, Stephan A.; Lacey, Simon F.; Melenhorst, J. Joseph

doi:10.1038/s41591-018-0201-9

Cited by 467 publications

(374 citation statements)

References 36 publications

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“…Surprisingly, a recent report uncovered an unexpected resistance mechanism to CD19-CAR-T cell therapy: Ruella et al showed that during the cell production process, a contaminating lymphoma B-cell underwent transduction leading to CD19-CAR expression. Cis interactions with surface CD19 resulted in its shielding by the CAR, making the antigen inaccessible to CAR-T cells [363]. While this phenomenon was not reported elsewhere, it does underscore the need to care for stringent production processes but more importantly, it demonstrates to what extent the development and mechanisms of resistance to engineered lymphocyte treatments may be unusal.…”

Section: Resultsmentioning

confidence: 89%

T-cells “à la CAR-T(e)” – Genetically engineering T-cell response against cancer

Eisenberg

Hoogi

Shamul

et al. 2019

Advanced Drug Delivery Reviews

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Section: Resultsmentioning

confidence: 89%

T-cells “à la CAR-T(e)” – Genetically engineering T-cell response against cancer

Eisenberg

Hoogi

Shamul

et al. 2019

Advanced Drug Delivery Reviews

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“…A report of the incidental CAR transduction of B cells, which conferred resistance to subsequent CAR T cell therapy 38 , highlights the importance of having a purified starting product. Strategies to optimize the input apheresis product before CAR T cell manufacturing, generally through T cell selection and enrichment, have been First, CAR T cell failures have several causes: for some patients, the CAR T cell product cannot be successfully manufactured or the generated CAR T cells do not expand sufficiently (either during manufacturing in vitro or after administration in vivo); in other patients, the problem of limited persistence in vivo is a potential mechanism underlying disease relapse.…”

Section: Wwwnaturecom/nrclinoncmentioning

confidence: 99%

Mechanisms of resistance to CAR T cell therapy

2019

Self Cite

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“…However, it has been recognized recently they may induce immunoreaction and insertional oncogenesis . Ruella et al . reported that the CAR gene was unintentionally introduced into a single leukemic B cell during T cell manufacture via lentiviral transduction, which caused the patient to relapse 9 months after CD19‐targeted CAR T cell (CTL019) infusion.…”

Section: Introductionmentioning

confidence: 99%

AAVS1 site‐specific integration of the CAR gene into human primary T cells using a linear closed‐ended AAV‐based DNA vector

Chen

Tan

Zhou

et al. 2020

The Journal of Gene Medicine

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Background Use of chimeric antigen receptor (CAR) T cells has become a promising strategy in cancer immunotherapy. However, safety in clinical application is also one of the most controversial issues. Methods In the present study, we investigated the application of a non‐viral site‐directed vector (CELiD [closed‐ended linear duplex DNA]) dependent on adeno‐associated virus (AAV) genomes for the purpose of safe CAR‐T engineering. We co‐electroporated CD19‐CAR encoding “CELiD” vectors with plasmid pCMV‐Rep into human T cells and ensured stably transfected CAR‐T cells by G418 selection. The efficiency of AAVS1 site‐specific integration was analyzed by a real‐time polymerase chain reaction. Results CAR‐T cells engineered by CELiD vectors could be established within 20 days with up to 22.8% AAVS1 site‐specific integration efficiency. CAR expression and cytokine secretion of CAR modified T cells were evaluated in vitro. Abundant effector cytokines were produced by the CAR‐T cells engineered by CELiD vectors compared to control T cells and the killing efficiency of target cells was estimated to as high as 75% in vitro. Conclusions With the help of the AAV‐derived CELiD vector, CAR genes were preferentially integrated into the AAVS1 site. This technology could be utilized in human T cell modification and remove the safety constraints of CAR‐T therapy.

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Induction of resistance to chimeric antigen receptor T cell therapy by transduction of a single leukemic B cell

Cited by 467 publications

References 36 publications

T-cells “à la CAR-T(e)” – Genetically engineering T-cell response against cancer

T-cells “à la CAR-T(e)” – Genetically engineering T-cell response against cancer

Mechanisms of resistance to CAR T cell therapy

AAVS1 site‐specific integration of the CAR gene into human primary T cells using a linear closed‐ended AAV‐based DNA vector

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