Lentiviral delivery of combinatorial CAR/CRISPRi circuit into human primary T cells is enhanced by TBK1/IKKɛ complex inhibitor BX795

Lingyu Li; Yuan Gao; Richa Srivastava; Wei Wang; Qinghui Xiong; Zhiming Fang; Alejandra Pelayo; Carolyn Denson; Angshumala Goswami; Rona Harari-Steinfeld; Zhifen Yang; Lihong Weng; Lei Stanley Qi; Francesco M. Marincola

doi:10.1186/s12967-020-02526-2

Journal of Translational Medicine (Sep 2020)

Lentiviral delivery of combinatorial CAR/CRISPRi circuit into human primary T cells is enhanced by TBK1/IKKɛ complex inhibitor BX795

Lingyu Li,
Yuan Gao,
Richa Srivastava,
Wei Wang,
Qinghui Xiong,
Zhiming Fang,
Alejandra Pelayo,
Carolyn Denson,
Angshumala Goswami,
Rona Harari-Steinfeld,
Zhifen Yang,
Lihong Weng,
Lei Stanley Qi,
Francesco M. Marincola

Affiliations

Lingyu Li: Refuge Biotechnologies Inc.
Yuan Gao: Refuge Biotechnologies Inc.
Richa Srivastava: Refuge Biotechnologies Inc.
Wei Wang: Hangzhou Juwu Biotech Co., Ltd.
Qinghui Xiong: Hangzhou Juwu Biotech Co., Ltd.
Zhiming Fang: Hangzhou Juwu Biotech Co., Ltd.
Alejandra Pelayo: Refuge Biotechnologies Inc.
Carolyn Denson: Refuge Biotechnologies Inc.
Angshumala Goswami: Refuge Biotechnologies Inc.
Rona Harari-Steinfeld: Refuge Biotechnologies Inc.
Zhifen Yang: Refuge Biotechnologies Inc.
Lihong Weng: Hangzhou Juwu Biotech Co., Ltd.
Lei Stanley Qi: Department of Bioengineering, Department of Chemical and Systems Biology, ChEM-H, Stanford University
Francesco M. Marincola: Refuge Biotechnologies Inc.

DOI: https://doi.org/10.1186/s12967-020-02526-2
Journal volume & issue: Vol. 18, no. 1
pp. 1 – 12

Abstract

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Abstract Background Adoptive transfer of engineered immune cells is a promising strategy for cancer treatment. However, low transduction efficiency particularly when large payload lentiviral vectors are used on primary T cells is a limitation for the development of cell therapy platforms that include multiple constructs bearing long DNA sequences. RB-340-1 is a new CAR T cell that combines two strategies in one product through a CRISPR interference (CRISPRi) circuit. Because multiple regulatory components are included in the circuit, RB-340-1 production needs delivery of two lentiviral vectors into human primary T cells, both containing long DNA sequences. To improve lentiviral transduction efficiency, we looked for inhibitors of receptors involved in antiviral response. BX795 is a pharmacological inhibitor of the TBK1/IKKɛ complex, which has been reported to augment lentiviral transduction of human NK cells and some cell lines, but it has not been tested with human primary T cells. The purpose of this study was to test if BX795 treatment promotes large payload RB-340-1 lentiviral transduction of human primary T cells. Methods To make the detection of gene delivery more convenient, we constructed another set of RB-340-1 constructs containing fluorescent labels named RB-340-1F. We incorporated BX795 treatment into the human primary T cell transduction procedure that was optimized for RB-340-1F. We tested BX795 with T cells collected from multiple donors, and detected the effect of BX795 on T cell transduction, phenotype, cell growth and cell function. Results We found that BX795 promotes RB-340-1F lentiviral transduction of human primary T cells, without dramatic change in cell growth and T cell functions. Meanwhile, BX795 treatment increased CD8+ T cell ratios in transduced T cells. Conclusions These results indicate that BX795 treatment is effective, and might be a safe approach to promote RB-340-1F lentiviral transduction of human primary T cells. This approach might also be helpful for other T cell therapy products that need delivery of complicated platform via large payload lentiviral vectors.

Published in Journal of Translational Medicine

ISSN: 1479-5876 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://translational-medicine.biomedcentral.com/

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