通过诱导 NKG2D 配体使原发性急性淋巴细胞白血病对自然杀伤细胞的识别敏感。
Sensitizing primary acute lymphoblastic leukemia to natural killer cell recognition by induction of NKG2D ligands.
机构信息
Institute of Cellular Medicine, Newcastle University, Newcastle upon Tyne, UK.
出版信息
Leuk Lymphoma. 2013 Jan;54(1):167-73. doi: 10.3109/10428194.2012.708026. Epub 2012 Sep 8.
Abstract
Natural killer (NK) cell immunosurveillance may be impaired by malignant disease, resulting in tumor escape and disease progression. Therapies that enhance NK cytotoxicity may therefore prove valuable in remission-induction and maintenance treatment regimens. Acute lymphoblastic leukemia (ALL) has previously been considered resistant to NK cell lysis and not tractable to this approach. Our study demonstrates that bortezomib, valproate and troglitazone can up-regulate NK activating ligands on a B-ALL cell line and on a proportion but not all adult primary B-ALL samples. Drug-treated ALL cells trigger higher levels of NK degranulation, as measured by CD107a expression, and this effect is dependent on signaling through the NK activating receptor NKG2D. These results suggest that bortezomib, valproate and troglitazone may have clinical utility in sensitizing ALL to NK mediated lysis in vivo.
摘要
自然杀伤 (NK) 细胞免疫监视可能因恶性疾病而受损,导致肿瘤逃逸和疾病进展。因此,增强 NK 细胞毒性的疗法可能在缓解诱导和维持治疗方案中具有重要价值。急性淋巴细胞白血病 (ALL) 以前被认为对 NK 细胞溶解具有抗性,并且不能通过这种方法治疗。我们的研究表明,硼替佐米、丙戊酸和曲格列酮可以上调 B-ALL 细胞系和一部分但不是所有成人原发性 B-ALL 样本上的 NK 激活配体。经药物处理的 ALL 细胞触发更高水平的 NK 脱颗粒,如 CD107a 表达所示,并且这种效应依赖于通过 NK 激活受体 NKG2D 的信号转导。这些结果表明,硼替佐米、丙戊酸和曲格列酮可能具有临床应用价值,可使 ALL 对 NK 介导的体内溶解敏感。
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