Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase

Prior to adoptive transfer, CAR T cells are activated, lentivirally infected with CAR transgenes, and expanded over 9 to 11 days. An unintended consequence of this process is the progressive differentiation of CAR T cells over time in culture. Differentiated T cells engraft poorly, which limits thei...

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Autores principales: Durgin, Joseph S., Thokala, Radhika, Johnson, Lexus, Song, Edward, Leferovich, John, Bhoj, Vijay, Ghassemi, Saba, Milone, Michael, Binder, Zev, O'Rourke, Donald M., O'Connor, Roddy S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society of Gene & Cell Therapy 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8899523/
https://www.ncbi.nlm.nih.gov/pubmed/34813961
http://dx.doi.org/10.1016/j.ymthe.2021.11.014
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author Durgin, Joseph S.
Thokala, Radhika
Johnson, Lexus
Song, Edward
Leferovich, John
Bhoj, Vijay
Ghassemi, Saba
Milone, Michael
Binder, Zev
O'Rourke, Donald M.
O'Connor, Roddy S.
author_facet Durgin, Joseph S.
Thokala, Radhika
Johnson, Lexus
Song, Edward
Leferovich, John
Bhoj, Vijay
Ghassemi, Saba
Milone, Michael
Binder, Zev
O'Rourke, Donald M.
O'Connor, Roddy S.
author_sort Durgin, Joseph S.
collection PubMed
description Prior to adoptive transfer, CAR T cells are activated, lentivirally infected with CAR transgenes, and expanded over 9 to 11 days. An unintended consequence of this process is the progressive differentiation of CAR T cells over time in culture. Differentiated T cells engraft poorly, which limits their ability to persist and provide sustained tumor control in hematologic as well as solid tumors. Solid tumors include other barriers to CAR T cell therapies, including immune and metabolic checkpoints that suppress effector function and durability. Sialic acids are ubiquitous surface molecules with known immune checkpoint functions. The enzyme C. perfringens neuraminidase (CpNA) removes sialic acid residues from target cells, with good activity at physiologic conditions. In combination with galactose oxidase (GO), NA has been found to stimulate T cell mitogenesis and cytotoxicity in vitro. Here we determine whether CpNA alone and in combination with GO promotes CAR T cell antitumor efficacy. We show that CpNA restrains CAR T cell differentiation during ex vivo culture, giving rise to progeny with enhanced therapeutic potential. CAR T cells expressing CpNA have superior effector function and cytotoxicity in vitro. In a Nalm-6 xenograft model of leukemia, CAR T cells expressing CpNA show enhanced antitumor efficacy. Arming CAR T cells with CpNA also enhanced tumor control in xenograft models of glioblastoma as well as a syngeneic model of melanoma. Given our findings, we hypothesize that charge repulsion via surface glycans is a regulatory parameter influencing differentiation. As T cells engage target cells within tumors and undergo constitutive activation through their CARs, critical thresholds of negative charge may impede cell-cell interactions underlying synapse formation and cytolysis. Removing the dense pool of negative cell-surface charge with CpNA is an effective approach to limit CAR T cell differentiation and enhance overall persistence and efficacy.
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spelling pubmed-88995232023-03-02 Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase Durgin, Joseph S. Thokala, Radhika Johnson, Lexus Song, Edward Leferovich, John Bhoj, Vijay Ghassemi, Saba Milone, Michael Binder, Zev O'Rourke, Donald M. O'Connor, Roddy S. Mol Ther Original Article Prior to adoptive transfer, CAR T cells are activated, lentivirally infected with CAR transgenes, and expanded over 9 to 11 days. An unintended consequence of this process is the progressive differentiation of CAR T cells over time in culture. Differentiated T cells engraft poorly, which limits their ability to persist and provide sustained tumor control in hematologic as well as solid tumors. Solid tumors include other barriers to CAR T cell therapies, including immune and metabolic checkpoints that suppress effector function and durability. Sialic acids are ubiquitous surface molecules with known immune checkpoint functions. The enzyme C. perfringens neuraminidase (CpNA) removes sialic acid residues from target cells, with good activity at physiologic conditions. In combination with galactose oxidase (GO), NA has been found to stimulate T cell mitogenesis and cytotoxicity in vitro. Here we determine whether CpNA alone and in combination with GO promotes CAR T cell antitumor efficacy. We show that CpNA restrains CAR T cell differentiation during ex vivo culture, giving rise to progeny with enhanced therapeutic potential. CAR T cells expressing CpNA have superior effector function and cytotoxicity in vitro. In a Nalm-6 xenograft model of leukemia, CAR T cells expressing CpNA show enhanced antitumor efficacy. Arming CAR T cells with CpNA also enhanced tumor control in xenograft models of glioblastoma as well as a syngeneic model of melanoma. Given our findings, we hypothesize that charge repulsion via surface glycans is a regulatory parameter influencing differentiation. As T cells engage target cells within tumors and undergo constitutive activation through their CARs, critical thresholds of negative charge may impede cell-cell interactions underlying synapse formation and cytolysis. Removing the dense pool of negative cell-surface charge with CpNA is an effective approach to limit CAR T cell differentiation and enhance overall persistence and efficacy. American Society of Gene & Cell Therapy 2022-03-02 2021-11-20 /pmc/articles/PMC8899523/ /pubmed/34813961 http://dx.doi.org/10.1016/j.ymthe.2021.11.014 Text en © 2021 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Article
Durgin, Joseph S.
Thokala, Radhika
Johnson, Lexus
Song, Edward
Leferovich, John
Bhoj, Vijay
Ghassemi, Saba
Milone, Michael
Binder, Zev
O'Rourke, Donald M.
O'Connor, Roddy S.
Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase
title Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase
title_full Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase
title_fullStr Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase
title_full_unstemmed Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase
title_short Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase
title_sort enhancing car t function with the engineered secretion of c. perfringens neuraminidase
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8899523/
https://www.ncbi.nlm.nih.gov/pubmed/34813961
http://dx.doi.org/10.1016/j.ymthe.2021.11.014
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