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Mesothelin antigen density influences anti-mesothelin chimeric antigen receptor T cell cytotoxicity

间皮素 细胞毒性 抗原 嵌合抗原受体 流式细胞术 细胞毒性T细胞 胰腺癌 癌细胞 抗体 癌症研究 细胞 分子生物学 化学 癌症 免疫学 生物 医学 T细胞 免疫系统 生物化学 内科学 体外
作者
Grace Chu,Charles G. Bailey,Rajini Nagarajah,Oei Ban Liang,Cynthia Metierre,Sharon M. Sagnella,Laura Castelletti,Dannel Yeo,Stephen Adelstein,John E.J. Rasko
出处
期刊:Cytotherapy [Elsevier]
卷期号:26 (4): 325-333
标识
DOI:10.1016/j.jcyt.2024.01.011
摘要

Several anti-mesothelin (MSLN) chimeric antigen receptor (CAR) T cells are in phase 1/2 clinical trials to treat solid-organ malignancies. The effect of MSLN antigen density on MSLN CAR cytotoxicity against tumor cells has not been examined previously, nor are there data regarding the effect of agents that increase MSLN antigen density on anti-MSLN CAR T cell efficacy.MSLN antigen density was measured on a panel of pancreatic cancer and mesothelioma cell lines by flow cytometry. In parallel, the cytotoxicity and specificity of two anti-MSLN CAR T cells (m912 and SS1) were compared against these cell lines using a real-time impedance-based assay. The effect of two MSLN 'sheddase' inhibitors (lanabecestat and TMI-1) that increase MSLN surface expression was also tested in combination with CAR T cells.SS1 CAR T cells were more cytotoxic compared with m912 CAR T cells against cell lines that expressed fewer than ∼170 000 MSLN molecules/cell. A comparison of the m912 and amatuximab (humanized SS1) antibodies identified that amatuximab could detect and bind to lower levels of MSLN on pancreatic cancer and mesothelioma cell lines, suggesting that superior antibody/scFv affinity was the reason for the SS1 CAR's superior cytotoxicity. The cytotoxicity of m912 CAR T cells was improved in the presence of sheddase inhibitors, which increased MSLN antigen density.These data highlight the value of assessing CAR constructs against a panel of cells expressing varying degrees of target tumor antigen as occurs in human tumors. Furthermore, the problem of low antigen density may be overcome by concomitant administration of drugs that inhibit enzymatic shedding of MSLN.
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