The use of BRM-activated killer cells in adoptive immunotherapy: a pilot study with nine advanced cancer patients.

Biotherapy (Dordrecht, Netherlands) Pub Date : 1998-01-01 DOI:10.1023/a:1008047628284

T Ebina, Y Fujimiya, T Yamaguchi, N Ogama, H Sasaki, N Isono, Y Suzuki, R Katakura, K Tanaka, K Nagata, S Takano, K Tamura, K Uno, T Kishida

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引用次数: 12

Abstract

Adoptive immunotherapy using MHC-nonrestricted-lymphocytes, peripheral blood gammadelta T cells and NK cells was devised. Peripheral blood mononuclear cells (3 x 10(7)) were selected by immobilization to anti-CD3 monoclonal antibody for 4 days and cultured for 2 weeks in the presence of IL-2. Thereafter they were reactivated by 500 U/ml of IFN-alpha and 1000 U/ml of IL-2 for 1 hour. Enhancement of NK and LAK activities was confirmed. Peripheral blood gammadelta T cells proliferated in response to immobilized anti-CD3 antibody (3% to 30%). Approximately 6 x 10(9) BRM-activated killer (BAK) cells composed of CD56+ gammadelta T cells and CD56+ NK cells, were dispensed to cancer patients via intravenous drip infusion. Nine patients were treated with BAK cells every 2 weeks or every month on an outpatient basis. During the course of adoptive immunotherapy, the crossed affinity immunoelectrophoresis (CAIE) pattern of serum immunosuppressive acidic protein (IAP) was analysed. Both the production and glycosylation pattern of IAP is changed in response to tumor enlargement and may therefore act as a marker of the disease progression. During the course of BAK therapy, the glycosylation IAP pattern of 6 patients changed from tumor (T) to normal (N). In addition, the performance status of all patients was maintained at 90-100% of the Karnofsky scale and any side effects including fever were not observed during treatments with BAK cells. Moreover, the overall quality of life (QOL) of the patients, scored at the Face scale was favorable. In addition, blood levels of activated gammadelta T cells producing IFN-gamma were assayed as an indication marker of BAK therapy. The normal range of IFN-gamma producing gammadelta T cells comprised 6.9 +/- 0.9% of peripheral blood mononuclear cells (PBMC), according to a single cell FACScan analyses of PBMCs derived from normal individuals. IFN-gamma producing gammadelta T cells of Patients No. 8 and 9, who received extensive chemotherapy before initiation of BAK therapy, comprised only 0.2% and 2% of PBMC, respectively. These patients died 3 and 6 months after beginning BAK therapy. Peripheral blood gammadelta T cells of Patients Nos. 1-7 proliferated in response to immobilized anti-CD3 antibody and the frequency of IFN-gamma producing gammadelta T cells in PBMC preparation of these patients were over 3% before initiation of BAK therapy. Since our data show a positive correlation between survival time and initial gammadelta T cell counts, a low frequency of these cells may contraindicate BAK therapy.

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brm活化杀伤细胞在过继免疫治疗中的应用:一项针对9名晚期癌症患者的初步研究。

采用mhc非限制性淋巴细胞、外周血γ - T细胞和NK细胞进行过继免疫治疗。选择3 × 10(7)个外周血单个核细胞，用抗cd3单克隆抗体固定4天，在IL-2存在下培养2周。然后用500 U/ml的ifn - α和1000 U/ml的IL-2再激活1小时。证实NK和LAK活性增强。外周血γ - δ T细胞对固定的抗cd3抗体有增殖反应(3%至30%)。大约6 × 10(9)个brm激活的杀伤细胞(BAK)由CD56+ γ - T细胞和CD56+ NK细胞组成，通过静脉滴注的方式分配给癌症患者。9例患者在门诊基础上每2周或每月接受BAK细胞治疗。对过继免疫治疗过程中血清免疫抑制酸性蛋白(IAP)的交叉亲和免疫电泳(CAIE)谱进行分析。IAP的产生和糖基化模式都随着肿瘤增大而改变，因此可能作为疾病进展的标志。在BAK治疗过程中，6例患者的糖基化IAP模式由肿瘤(T)变为正常(N)。此外，所有患者的运动状态保持在Karnofsky量表的90-100%，在BAK细胞治疗期间未观察到任何副作用，包括发烧。此外，患者的整体生活质量(QOL)，在脸量表得分是良好的。此外，血液中产生ifn - γ的活化γ δ T细胞水平作为BAK治疗的适应症标志物进行检测。根据来自正常人的外周血单核细胞的单细胞FACScan分析，正常范围内产生ifn - γ的γ δ T细胞占外周血单核细胞(PBMC)的6.9 +/- 0.9%。8号和9号患者在开始BAK治疗前接受了广泛的化疗，产生ifn - γ的γ - T细胞分别仅占PBMC的0.2%和2%。这些患者在开始BAK治疗3个月和6个月后死亡。1-7号患者的外周血γ - T细胞对固定的抗cd3抗体有增殖反应，在BAK治疗开始前，这些患者的PBMC制备中产生ifn - γ的γ - T细胞的频率超过3%。由于我们的数据显示生存时间与初始γ δ T细胞计数呈正相关，因此这些细胞的低频率可能是BAK治疗的禁忌。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Biotherapy (Dordrecht, Netherlands)

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