首页> 外文期刊>Anticancer Research: International Journal of Cancer Research and Treatment >Feasibility study of adoptive immunotherapy for metastatic lung tumors using peptide-pulsed dendritic cell-activated killer (PDAK) cells.
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Feasibility study of adoptive immunotherapy for metastatic lung tumors using peptide-pulsed dendritic cell-activated killer (PDAK) cells.

机译:采用肽脉冲树突状细胞激活的杀伤细胞(PDAK)对转移性肺肿瘤进行过继免疫治疗的可行性研究。

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We have established a novel culture system to generate effector lymphocytes designated as peptide-pulsed dendritic cell-activated killer (PDAK) cells using cultured dendritic cells (DCs), synthetic peptide, peripheral blood lymphocytes, and interleukin-2 plus immobilized anti-CD3 antibody. A feasibility study of an adoptive immunotherapy trial using PDAK cells was conducted on HLA-A2 and HLA-A24 cancer patients with antigen-positive lung metastasis that was defined by serological analysis or PCR analysis. Eleven patients with lung metastasis participated in the study: 6 with colorectal cancer, 2 with pancreatic cancer, 1 each with breast and lung cancer, and 1 with melanoma. The patients received either Muc-1, CEA, gpl00, Her-2 or SART-3-PDAK cells generated in vitro, intravenously in combination with 350,000 U IL-2 weekly for 9 weeks, together with a planned dose-escalation schedule of three transfers each of 1 x 10(7), 3 x 10(7) and 1 x 10(8) PDAK cells/kg for 6 patients, and with a uniform dose of 3x 10(7) PDAK cells/kg for the remaining 5 patients. Peptide/HLA-specific cytotoxic activity and TCRVbeta gene usage of PDAK cells were analyzed. All transfers of PDAK cells, which showed peptide/HLA-specific lysis, were well-tolerated in all patients, and adverse effects (elevation of transaminase, fever, and headache) were observed primarily at grade 1, but in no case greater than grade 2. The generation of sufficient cells to treat the patients with 3 x 10(7) PDAK cells/kg was feasible using our culture system, but we were able to generate and administer the dose of 1 x 10(8) PDAK cells/kg in only one patient. One partial response (PR) of lung metastasis occurred in a pancreatic cancer patient who received 3 x 10(7) Muc-1-PDAK cells/kg. The cytolytic units of PDAK cells in this patient appeared to be substantially higher compared to those in PD patients. TCR gene usage analysis on PDAK cells revealed preferential usage of TCRVbeta segments. These results suggest that adoptive immunotherapy using PDAK cells for cancer patients with antigen-positive lung metastasis is safe and feasible, and tumor response should be examined in a future clinical trial
机译:我们已经建立了一种新型的培养系统,可以使用培养的树突状细胞(DC),合成肽,外周血淋巴细胞,白细胞介素2以及固定化的抗CD3抗体来生成称为淋巴细胞脉冲的树突状细胞激活的杀伤(PDAK)细胞的效应淋巴细胞。 。对通过血清学分析或PCR分析确定的抗原阳性肺转移的HLA-A2和HLA-A24癌症患者进行了使用PDAK细胞的过继免疫疗法试验的可行性研究。 11名肺转移患者参加了该研究:6例结直肠癌,2例胰腺癌,1例乳腺癌和肺癌以及1例黑素瘤。患者接受了体外产生的Muc-1,CEA,gp100,Her-2或SART-3-PDAK细胞,静脉内联合350,000 U IL-2进行了9周的每周静脉注射,并计划了3次剂量递增计划每6例患者转移1 x 10(7),3 x 10(7)和1 x 10(8)PDAK细胞/千克,其余5例均匀转移3x 10(7)PDAK细胞/千克耐心。分析了PDAK细胞的肽/ HLA特异性细胞毒性活性和TCRVbeta基因使用情况。所有表现出肽/ HLA特异性裂解的PDAK细胞的转移均在所有患者中均得到良好耐受,并且主要在1级观察到不良反应(转氨酶升高,发烧和头痛),但不超过1级2.使用我们的培养系统可以产生足够的细胞来治疗3 x 10(7)PDAK细胞/ kg的患者,但是我们能够产生和施用1 x 10(8)PDAK细胞/ kg的剂量仅一名患者。接受3 x 10(7)Muc-1-PDAK细胞/ kg的胰腺癌患者发生肺转移的部分反应(PR)。与PD患者相比,该患者中PDAK细胞的溶细胞单位似乎要高得多。对PDAK细胞的TCR基因使用情况分析显示,优先使用TCRVbeta片段。这些结果表明,使用PDAK细胞进行的过继免疫疗法对于抗原阳性的肺转移癌患者是安全可行的,应在以后的临床试验中检查肿瘤反应

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