Mesothelin-targeting chimeric antigen receptor-modified T cells by piggyBac transposon system suppress the growth of bile duct carcinoma

Jie-Ying Xu; Zhen-Long Ye; Du-Qing Jiang; Jiang-Chuan He; Yong-Mei Ding; Lin-Fang Li; Sai-Qun Lv; Ying Wang; Hua-Jun Jin; Qi-Jun Qian

doi:10.1177/1010428317695949

Mesothelin-targeting chimeric antigen receptor-modified T cells by piggyBac transposon system suppress the growth of bile duct carcinoma

Tumour Biol. 2017 Apr;39(4):1010428317695949. doi: 10.1177/1010428317695949.

Authors

Jie-Ying Xu¹, Zhen-Long Ye², Du-Qing Jiang¹, Jiang-Chuan He¹, Yong-Mei Ding³, Lin-Fang Li², Sai-Qun Lv², Ying Wang², Hua-Jun Jin², Qi-Jun Qian^{1

2

3}

Affiliations

¹ 1 Xinyuan Institute of Medicine and Biotechnology, College of Life Sciences, Zhejiang Sci-Tech University, Hangzhou, China.
² 2 Laboratory of Gene and Viral Therapy, Eastern Hepatobiliary Surgery Hospital, The Second Military Medical University of Chinese PLA, Shanghai, China.
³ 3 Department of Biotherapy, Eastern Hepatobiliary Surgery Hospital, The Second Military Medical University of Chinese PLA, Shanghai, China.

PMID: 28381173
DOI: 10.1177/1010428317695949

Abstract

Chimeric antigen receptor modified T cell-based immunotherapy is revolutionizing the field of cancer treatment. However, its potential in treating bile duct carcinoma has not been fully explored. Herein, we developed the second-generation mesothelin-targeting chimeric antigen receptor-modified T cells with the 4-1BB co-stimulatory module by the piggyBac transposon system. Mesothelin-targeting chimeric antigen receptor was expressed by 66.0% of mesothelin-targeting chimeric antigen receptor-modified T cells post electrophoretic transfection and stimulation with K562-meso cells; the expressions of activation markers were tested by flow cytometry assay and showed greater activation of mesothelin-targeting chimeric antigen receptor-modified T cells than control T cells (CD107α: 71.9% vs 48.6%; CD27: 92.1% vs 61.8%; CD137: 55.5% vs 8.4%; CD28: 98.0% vs 82.1%; CD134: 37.5% vs 10.4%). Furthermore, mesothelin-targeting chimeric antigen receptor-modified T cells exerted cytotoxicity toward mesothelin-expressing EH-CA1b and EH-CA1a cells in an effector-to-target ratio-dependent manner, while leaving mesothelin-negative GSC-SD and EH-GB1 cells and normal liver L02 cells almost unharmed. Mesothelin-targeting chimeric antigen receptor-modified T cells secreted cytokines at higher levels when co-cultured with mesothelin-positive EH-CA1a and EH-CA1b cells than with mesothelin-negative GSC-SD and EH-GB1 cells. Enhanced cytotoxicity and cytokine secretion of mesothelin-targeting chimeric antigen receptor-modified T cells compared to control T cells were also observed when co-cultured with 293-meso cells (interferon γ: 85.1% ± 1.47% vs 8.3% ± 2.50%, p = 0.000; tumor necrosis factor α: 90.9% ± 4.67% vs 18.5% ± 3.62%, p = 0.0004; interleukin 2: 60.8% ± 2.00% vs 15.6% ± 2.06%, p = 0.002; interleukin 6: 6.4% ± 2.95% vs 1.7% ± 0.63%, p = 0.055). In addition, mesothelin-targeting chimeric antigen receptor-modified T cells showed greater inhibitory and proliferative capability than control T cells within EH-CA1a cell xenografts. This study shows the potential of mesothelin-targeting chimeric antigen receptor-modified T cells in treating bile duct carcinoma.

Keywords: Chimeric antigen receptor; bile duct carcinoma; immunotherapy; mesothelin; piggyBac.

MeSH terms

Animals
Bile Duct Neoplasms / pathology
Bile Duct Neoplasms / therapy*
Cells, Cultured
DNA Transposable Elements*
GPI-Linked Proteins / immunology*
Humans
Immunotherapy / methods*
Mesothelin
Mice
Receptors, Antigen, T-Cell / immunology*
Recombinant Fusion Proteins
T-Lymphocytes / immunology*

Substances

DNA Transposable Elements
GPI-Linked Proteins
Msln protein, mouse
Receptors, Antigen, T-Cell
Recombinant Fusion Proteins
Mesothelin