Preclinical evaluation of antigen-sensitive B7-H3-targeting nanobody-based CAR-T cells in glioblastoma cautions for on-target, off-tumor toxicity

Fien Meeus; Cyprine Neba Funeh; Robin Maximilian Awad; Katty Zeven; Dorien Autaers; Ann De Becker; Ivan Van Riet; Cleo Goyvaerts; Sandra Tuyaerts; Bart Neyns; Nick Devoogdt; Yannick De Vlaeminck; Karine Breckpot

doi:10.1136/jitc-2024-009110

Preclinical evaluation of antigen-sensitive B7-H3-targeting nanobody-based CAR-T cells in glioblastoma cautions for on-target, off-tumor toxicity

J Immunother Cancer. 2024 Nov 19;12(11):e009110. doi: 10.1136/jitc-2024-009110.

Authors

Fien Meeus^{1

2}, Cyprine Neba Funeh², Robin Maximilian Awad³, Katty Zeven², Dorien Autaers³, Ann De Becker⁴, Ivan Van Riet^{4

5}, Cleo Goyvaerts², Sandra Tuyaerts^{6

7}, Bart Neyns^{6

7}, Nick Devoogdt², Yannick De Vlaeminck³, Karine Breckpot³

Affiliations

¹ Translational Oncology Research Center (TORC), Department of Biomedical Sciences, Laboratory for Molecular and Cellular Therapy (LMCT), Vrije Universiteit Brussel, Brussels, Belgium [email protected].
² Department of Medical Imaging (MIMA), Molecular Imaging and Therapy (MITH) research group, Vrije Universiteit Brussel, Brussels, Belgium.
³ Translational Oncology Research Center (TORC), Department of Biomedical Sciences, Laboratory for Molecular and Cellular Therapy (LMCT), Vrije Universiteit Brussel, Brussels, Belgium.
⁴ Department of Hematology, Cellular Therapy Laboratory, University Hospital Brussels, Universitair Ziekenhuis Brussel, Brussels, Belgium.
⁵ Translational Oncology Research Center (TORC), Department of Biomedical Sciences, Hematology and Immunology Research Team (HEIM), Vrije Universiteit Brussel, Brussels, Belgium.
⁶ Department of Medical Oncology, University Hospital Brussels, Universitair Ziekenhuis Brussel, Brussels, Belgium.
⁷ Translational Oncology Research Center (TORC), Department of Biomedical Sciences, Laboratory for Medical and Molecular Oncology (LMMO), Vrije Universiteit Brussel, Brussels, Belgium.

PMID: 39562005
DOI: 10.1136/jitc-2024-009110

Abstract

Background: Glioblastoma is the most common lethal primary brain tumor, urging evaluation of new treatment options. Chimeric antigen receptor (CAR)-T cells targeting B7 homolog 3 (B7-H3) are promising because of the overexpression of B7-H3 on glioblastoma cells but not on healthy brain tissue. Nanobody-based (nano)CARs are gaining increasing attention as promising alternatives to classical single-chain variable fragment-based (scFv)CARs, because of their single-domain nature and low immunogenicity. Still, B7-H3 nanoCAR-T cells have not been extensively studied in glioblastoma.

Methods: B7-H3 nanoCAR- and scFvCAR-T cells were developed and evaluated in human glioblastoma models. NanoCAR-T cells targeting an irrelevant antigen served as control. T cell activation, cytokine secretion and killing capacity were evaluated in vitro using ELISA, live cell imaging and flow cytometry. Antigen-specific killing was assessed by generating B7-H3 knock-out cells using Clustered Regularly Interspaced Short Palindromic Repeats (CRISPR)/Cas9-genome editing. The tumor tracing capacity of the B7-H3 nanobody was first evaluated in vivo using nuclear imaging. Then, the therapeutic potential of the nanoCAR-T cells was evaluated in a xenograft glioblastoma model.

Results: We showed that B7-H3 nanoCAR-T cells were most efficient in lysing B7-H3^pos glioblastoma cells in vitro. Lack of glioblastoma killing by control nanoCAR-T cells and lack of B7-H3^neg glioblastoma killing by B7-H3 nanoCAR-T cells showed antigen-specificity. We showed in vivo tumor targeting capacity of the B7-H3 nanobody-used for the nanoCAR design-in nuclear imaging experiments. Evaluation of the nanoCAR-T cells in vivo showed tumor control in mice treated with B7-H3 nanoCAR-T cells in contrast to progressive disease in mice treated with control nanoCAR-T cells. However, we observed limiting toxicity in mice treated with B7-H3 nanoCAR-T cells and showed that the B7-H3 nanoCAR-T cells are activated even by low levels of mouse B7-H3 expression.

Conclusions: B7-H3 nanoCAR-T cells showed promise for glioblastoma therapy following in vitro characterization, but limiting in vivo toxicity was observed. Off-tumor recognition of healthy mouse tissue by the cross-reactive B7-H3 nanoCAR-T cells was identified as a potential cause for this toxicity, warranting caution when using highly sensitive nanoCAR-T cells, recognizing the low-level expression of B7-H3 on healthy tissue.

Keywords: Adoptive cell therapy - ACT; Chimeric antigen receptor - CAR; Immunotherapy; Solid tumor; T cell.

MeSH terms

Animals
B7 Antigens* / immunology
Brain Neoplasms / immunology
Brain Neoplasms / therapy
Cell Line, Tumor
Glioblastoma* / immunology
Glioblastoma* / therapy
Humans
Immunotherapy, Adoptive / methods
Mice
Receptors, Chimeric Antigen / immunology
Receptors, Chimeric Antigen / metabolism
Single-Domain Antibodies* / immunology
Single-Domain Antibodies* / pharmacology
T-Lymphocytes / immunology
Xenograft Model Antitumor Assays

Substances

B7 Antigens
CD276 protein, human
Single-Domain Antibodies
Receptors, Chimeric Antigen