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Tissue factor as a new target for CAR-NK cell immunotherapy of triple-negative breast cancer

机译:组织因子作为三重阴性乳腺癌的汽车NK细胞免疫治疗的新靶标

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Triple-negative breast cancer (TNBC), representing ~15% of globally diagnosed breast cancer, is typically an incurable malignancy due to the lack of targetable surface targets for development of effective therapy. To address the unmet need for TNBC treatment, we recently determined that tissue factor (TF) is a useful surface target in 50–85% of patients with TNBC and developed a second-generation TF-targeting antibody-like immunoconjugate (called L-ICON) for preclinical treatment of TNBC. Using the chimeric antigen receptor (CAR) approach, here we develop and test TF-targeting CAR-engineered natural killer (TF-CAR-NK) cells that co-express CD16, the Fc receptor (FcγIII) to mediate antibody-dependent cellular toxicity (ADCC), for a preclinical assessment of immunotherapy of TNBC using TF-CAR-NK cell as single agent therapy and in combination with L-ICON. Our preclinical results demonstrate that TF-CAR-NK cells alone could kill TNBC cells and its efficacy was enhanced with L-ICON ADCC in vitro. Moreover, TF-CAR-NK cells were effective in vivo for the treatment of TNBC in cell line- and patient’s tumor-derived xenograft mouse models. Thus, this study established the proof of concept of targeting TF as a new target in CAR-NK immunotherapy for effective treatment of TNBC and may warrant further preclinical study and potentially future investigation in TNBC patients.
机译:代表〜15%的全球诊断乳腺癌的三阴性乳腺癌(TNBC)通常是由于缺乏有效治疗的疗效靶向而导致的恶性肿瘤。为了解决对TNBC治疗的未满足需求,我们最近确定组织因子(TF)是50-85%的TNBC患者的有用表面靶标,并开发出第二代TF靶向抗体样免疫缀合物(称为L-图标)对于TNBC的临床前治疗。使用嵌合抗原受体(轿厢)方法,在这里,我们开发和测试TF靶向汽车工程化的天然杀伤(TF-CAR-NK)细胞,其共同表达CD16,FC受体(FCγIII)以介导抗体依赖性细胞毒性(ADCC),用于使用TF-CAR-NK细胞作为单孕疗法的TNBC免疫疗法的临床前评估,并与L-ICON组合。我们的临床前结果表明,单独的TF-CAR-NK细胞可以杀死TNBC细胞,并且其在体外用L-ICON ADCC增强其疗效。此外,TF-CAR-NK细胞在细胞系和患者肿瘤衍生的异种移植小鼠模型中有效地用于治疗TNBC。因此,本研究确立了靶向TF作为汽车 - NK免疫疗法的新靶标的概念证明,用于有效治疗TNBC,并且可能需要进一步的临床前研究和在TNBC患者的未来未来调查。

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    《Scientific reports.》 |2020年第1期|共13页
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    Zhiwei Hu;

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