Chlorotoxin-directed CAR T cells for specific and effective targeting of glioblastoma.
Dongrui WangRenate StarrWen-Chung ChangBrenda AguilarDarya AlizadehSarah L WrightXin YangAlfonso BritoAniee SarkissianJulie R OstbergLi LiYanhong ShiMargarita GutovaKaren S AboodyBehnam BadieStephen J FormanMichael E BarishChristine E BrownPublished in: Science translational medicine (2021)
Although chimeric antigen receptor (CAR) T cells have demonstrated signs of antitumor activity against glioblastoma (GBM), tumor heterogeneity remains a critical challenge. To achieve broader and more effective GBM targeting, we developed a peptide-bearing CAR exploiting the GBM-binding potential of chlorotoxin (CLTX). We find that CLTX peptide binds a great proportion of tumors and constituent tumor cells. CAR T cells using CLTX as the targeting domain (CLTX-CAR T cells) mediate potent anti-GBM activity and efficiently target tumors lacking expression of other GBM-associated antigens. Treatment with CLTX-CAR T cells resulted in tumor regression in orthotopic xenograft GBM tumor models. CLTX-CAR T cells do not exhibit observable off-target effector activity against normal cells or after adoptive transfer into mice. Effective targeting by CLTX-CAR T cells requires cell surface expression of matrix metalloproteinase-2. Our results pioneer a peptide toxin in CAR design, expanding the repertoire of tumor-selective CAR T cells with the potential to reduce antigen escape.
Keyphrases
- cancer therapy
- poor prognosis
- escherichia coli
- binding protein
- type diabetes
- metabolic syndrome
- dendritic cells
- single cell
- immune response
- oxidative stress
- cell surface
- induced apoptosis
- transcription factor
- cell therapy
- cell cycle arrest
- human health
- anti inflammatory
- endoplasmic reticulum stress
- pi k akt
- dna binding