间皮素
卵巢癌
癌症研究
CD28
T细胞
肿瘤微环境
细胞毒性T细胞
CD8型
免疫系统
医学
卵巢肿瘤
癌症
免疫学
抗原
生物
内科学
体外
生物化学
作者
Esther Schoutrop,Ibrahim El‐Serafi,Thomas Poiret,Ying Zhao,Okan Gultekin,Rui He,Lidia Moyano‐Galceran,Joseph W. Carlson,Kaisa Lehti,Moustapha Hassan,Isabelle Magalhaes,Jonas Mattsson
出处
期刊:Cancer Research
[American Association for Cancer Research]
日期:2021-04-01
卷期号:81 (11): 3022-3035
被引量:111
标识
DOI:10.1158/0008-5472.can-20-2701
摘要
New therapeutic options for patients with ovarian cancer are urgently needed. Therefore, we evaluated the efficacy of two second-generation mesothelin (MSLN)-directed CAR T cells in orthotopic mouse models of ovarian cancer. Treatment with CAR T cells expressing an MSLN CAR construct including the CD28 domain (M28z) significantly prolonged survival, but no persistent tumor control was observed. Despite lower response rates, MSLN-4-1BB (MBBz) CAR T cells induced long-term remission in some SKOV3-bearing mice. Tumor-infiltrating M28z and MBBz CAR T cells upregulated PD-1 and LAG3 in an antigen-dependent manner while MSLN+ tumor cells expressed the corresponding ligands (PD-L1 and HLA-DR), demonstrating that coinhibitory pathways impede CAR T-cell persistence in the ovarian tumor microenvironment. Furthermore, profiling plasma soluble factors identified a cluster of M28z- and MBBz-treated mice characterized by elevated T-cell secreted factors that had increased survival, higher CD8+ T-cell tumor infiltration, less exhausted CAR T-cell phenotypes, and increased HLA-DR expression by tumor cells. Altogether, our study demonstrates the therapeutic potential of MSLN-CAR T cells to treat ovarian cancer. SIGNIFICANCE: These findings demonstrate that MSLN-directed CAR T cells can provide antitumor immunity against ovarian cancer.
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