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Importance of antibody isotypes in antitumor immunity by monocytes and complement using human-immune tumor models

机译:在抗肿瘤抗体同形像的重要性由单核细胞和免疫补充使用人类免疫肿瘤模型

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Monoclonal antibodies (mAbs) have revolutionized clinical medicine, especially in the field of cancer immunotherapy. The challenge now is to improve the response rates, as immunotherapy still fails for many patients. Strategies to enhance tumor cell death is a fundamental aim, but relevant model systems for human tumor immunology are lacking. Herein, we have developed a preclinical human immune - three-dimensional (3D) tumor model (spheroids) to map the efficiency of tumor-specific isotypes for improved tumor cell killing. Different anti-CD20 Rituximab (RTX) isotypes alone or in combination, were evaluated for mediating complement-dependent cytotoxicity and antibody-dependent phagocytosis by human monocytic cells in 3D spheroids, in parallel with monolayer cultures, of human CD20~+ B-cell lymphomas. We demonstrate that the IgG3 variant of RTX has the greatest tumoricidal effect over other isotypes, and when combined with apoptosis-inducing RTX-IgG2 isotype the therapeutic effect can be substantially enhanced. The results show further that the treatment outcome by RTX isotypes is influenced by tumor morphology and expression of the complement inhibitor CD59. Hence, the human immune-3D tumor model is a clinical relevant and attractive ex vivo system to predict mAbs for best efficacy in cancer immunotherapy.
机译:单克隆抗体(mab)已经彻底改变了临床医学,尤其是领域的癌症免疫疗法。提高响应率,免疫疗法仍未对许多病人。增强肿瘤细胞死亡是一个基本的目的,但相关的人类肿瘤模型系统免疫学是缺乏。临床前人类免疫——三维(3 d)肿瘤模型(球状体)的映射肿瘤特异性的同形像的效率改善肿瘤细胞死亡。单独或者联合美罗华(RTX)同形像,进行评估中介补体依赖细胞毒性和锁定吞噬作用在三维球状体,由人类单核细胞的细胞与单层文化,人类的CD20 ~ +b细胞淋巴瘤。RTX的变异最大的杀肿瘤的效果比其他同形像,当总和与凋亡诱导RTX-IgG2同形像治疗效果可以大大增强。结果表明进一步的治疗结果RTX同形像受到肿瘤形态和表达的补充抑制剂CD59。模型是一个临床相关的和有吸引力的前女友体内系统预测马伯最佳功效癌症免疫疗法。

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