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Combination Cancer Therapy Using Chimeric Antigen Receptor-Engineered Natural Killer Cells as Drug Carriers

机译:使用嵌合抗原受体工程化的自然杀伤细胞作为药物载体的联合癌症治疗

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摘要

The therapeutic limitations of conventional chemotherapeutic drugs include chemo-resistance, tumor recurrence, and metastasis. Numerous nanoparticle-based active targeting approaches have emerged to enhance the intracellular concentration of drugs in tumor cells; however, efficient delivery of these systems to the tumor site while sparing healthy tissue remains elusive. Recently, much attention has been given to human immune-cell-directed nanoparticle drug delivery, because immune cells can traffic to the tumor and inflammatory sites. Natural killer cells are a subset of cytotoxic lymphocytes that play critical roles in cancer immunosurveillance. Engineering of the human natural killer cell line, NK92, to express chimeric antigen receptors to redirect their antitumor specificity has shown significant promise. We demonstrate that the efficacy of chemotherapy can be enhanced in vitro and in vivo while reducing off-target toxicity by using chimeric antigen receptor-engineered NK92 cells as carriers to direct drug-loaded nanoparticles to the target site.
机译:常规化疗药物的治疗局限性包括化学耐药性,肿瘤复发和转移。已经出现了许多基于纳米粒子的主动靶向方法来增强肿瘤细胞中药物的细胞内浓度。然而,在保留健康组织的同时,将这些系统有效地递送至肿瘤部位仍然遥不可及。近来,由于免疫细胞可以运输到肿瘤和炎症部位,因此已经对人类免疫细胞指导的纳米颗粒药物递送给予了很多关注。天然杀伤细胞是细胞毒性淋巴细胞的子集,其在癌症免疫监测中起关键作用。表达嵌合抗原受体以重定向其抗肿瘤特异性的人类天然杀伤细胞系NK92的工程设计已显示出巨大的希望。我们证明,通过使用嵌合抗原受体工程化的NK92细胞作为载体将载有药物的纳米颗粒导向靶位点,可以提高体外和体内化疗的功效,同时降低脱靶毒性。

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