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Electroporation of NKG2D RNA CAR Improves V?9V?2 T Cell Responses against Human Solid Tumor Xenografts.


ABSTRACT: V?9V?2 T cell-based anticancer immunotherapy has shown some promise in early-phase clinical trials but there is still large room for improvement. Using the extracellular domain of the human NKG2D, a stimulatory receptor expressed by V?9V?2 T cells, we constructed NKG2D ligand-specific chimeric antigen receptors (CARs). We adopted a non-viral CAR approach via mRNA electroporation to modify V?9V?2 T cells and demonstrated that, upon interaction with the NKG2D ligand-positive cancer cells, the CARs substantially enhanced the cytotoxic activity of the modified cells toward multiple cultured solid tumor cell lines, including those resistant to Zometa treatment. Repeated doses of the CAR-expressing cells resulted in tumor regression in mice with established tumors, extending median survival time by up to 132% as compared to the PBS control group. The findings suggest clinical potential for RNA CAR-modified V?9V?2 T cells to treat a wide variety of NKG2D ligand-expressing cancers.

SUBMITTER: Ang WX 

PROVIDER: S-EPMC7240063 | biostudies-literature | 2020 Jun

REPOSITORIES: biostudies-literature

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Electroporation of NKG2D RNA CAR Improves Vγ9Vδ2 T Cell Responses against Human Solid Tumor Xenografts.

Ang Wei Xia WX   Ng Yu Yang YY   Xiao Lin L   Chen Can C   Li Zhendong Z   Chi Zhixia Z   Tay Johan Chin-Kang JC   Tan Wee Kiat WK   Zeng Jieming J   Toh Han Chong HC   Wang Shu S  

Molecular therapy oncolytics 20200504


Vγ9Vδ2 T cell-based anticancer immunotherapy has shown some promise in early-phase clinical trials but there is still large room for improvement. Using the extracellular domain of the human NKG2D, a stimulatory receptor expressed by Vγ9Vδ2 T cells, we constructed NKG2D ligand-specific chimeric antigen receptors (CARs). We adopted a non-viral CAR approach via mRNA electroporation to modify Vγ9Vδ2 T cells and demonstrated that, upon interaction with the NKG2D ligand-positive cancer cells, the CARs  ...[more]

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