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Anti-myeloma activity and molecular logic operation by Natural Killer cells in microfluidic droplets

机译:微流液滴中自然杀伤细胞的抗骨髓瘤活性和分子逻辑操作

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Immune-targeted therapies that activate effector lymphocytes such as Natural Killer (NK) cells are currently being investigated for the treatment of Multiple myeloma (MM), the second most common form of hematological cancer. However, individual NK cells are highly heterogeneous in their cytolytic potential, making it difficult to detect, quantify and correlate the outcome of dynamic effector-target cell interactions at single cell resolution. Here, we present a microfluidic bioassay platform capable of activity-based screening of cellular and molecular immunotherapies. We identified distinct functional signatures associated with NK-MM cell interaction. The addition of immunomodulatory drug lenalidomide altered responses of NK-susceptible MM cells but not that of NK-tolerant MM cells. Antitumor cytotoxicity was significantly increased by the blockade of PD1/PDL1 axis as well as the clinically relevant cell line NK92, which were used to construct molecular logic functions (AND and NOT gates). A predictive agent-based mathematical model was developed to simulate progressive disease states and drug efficacy. The findings of the current study validate the applicability of this microfluidic cytotoxicity assay for immunotherapy screening, biocomputation and for future employment in detection of patient-specific cell response for precision medicine.
机译:目前正在研究激活效应淋巴细胞(例如自然杀手(NK)细胞)的免疫靶向疗法,以治疗第二种最常见的血液学癌症形式多发性骨髓瘤(MM)。但是,单个NK细胞的溶细胞潜力高度异质,因此难以在单个细胞分辨率下检测,量化和关联动态效应子-靶细胞相互作用的结果。在这里,我们介绍了一种能够基于活动的细胞和分子免疫治疗筛选的微流控生物检测平台。我们确定了与NK-MM细胞相互作用相关的独特功能签名。免疫调节药物来那度胺的添加改变了对NK敏感的MM细胞的反应,但没有改变对NK耐受的MM细胞的反应。通过阻断PD1 / PDL1轴以及临床上相关的细胞系NK92(可用于构建分子逻辑功能(AND和NOT门)),显着提高了抗肿瘤细胞毒性。建立了基于预测剂的数学模型来模拟疾病进展状态和药物疗效。当前研究的结果证实了这种微流体细胞毒性测定法在免疫疗法筛选,生物计算以及将来用于检测精确医学的患者特异性细胞反应方面的适用性。

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