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[淋巴因子激活的杀伤细胞(LAK)疗法治疗晚期肾细胞癌:动脉内LAK疗法的临床研究及LAK细胞活性的实验研究]

[Lymphokine-activated killer (LAK) therapy for advanced renal cell carcinoma: clinical study on arterial LAK therapy and experimental study on LAK cell activity].

作者信息

Hayakawa M

机构信息

Department of Urology, School of Medicine, University of the Ryukyus.

出版信息

Hinyokika Kiyo. 1992 Nov;38(11):1311-8.

PMID:1485587
Abstract

Experimental and clinical studies were conducted on lymphokine-activated killer (LAK) cell therapy for advanced renal cell carcinoma (RCC). The traffic assay using radiolabeled LAK cells indicated short-term but appreciable accumulation of LAK cells in the tumor site when trans-arterially infused. By contrast, systemically infused LAK cells were localized not to the tumor tissue but to the lung. Therefore, we began treatment of the patients with extrapulmonary metastases by means of regional arterial administration of LAK cells and those who had pulmonary metastases by a systemic LAK therapy. Regimen of Interleukin-2 (IL-2) administration was bolus infusion of 5 x 10 U IL-2 twice daily. Frequency of LAK cell administration varied from one to three times a week depending upon the patient's condition. Eight out of 16 metastases, such as bone, muscle, and lymph node metastases, in 9 patients treated by arterial LAK therapy showed regression. Side effects during LAK therapy were not serious. Past history of having chemotherapy was an unfavorable factor that could reduce the sensitivity to LAK therapy. Our laboratory study showed the production of Interferon (IFN)-gamma and Tumor Necrosis Factor (TNF)-alpha by LAK cells when preincubated with RCC cells, which may indicate the mechanism of LAK cell-mediated antitumor activity in vivo. The study also showed that LAK cells as well as monocytes preincubated with the supernatant of LAK cells damaged normal endothelial cells in vitro, which suggested the possibility that LAK therapy risks increasing the frequency of brain metastasis by damaging the blood-brain barrier.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

针对晚期肾细胞癌(RCC)的淋巴因子激活的杀伤细胞(LAK)疗法进行了实验和临床研究。使用放射性标记的LAK细胞进行的示踪分析表明,经动脉注入时,LAK细胞在肿瘤部位有短期但明显的聚集。相比之下,全身注入的LAK细胞并非定位于肿瘤组织,而是定位于肺部。因此,我们开始对肺外转移患者采用LAK细胞区域动脉给药治疗,对肺转移患者采用全身LAK疗法治疗。白细胞介素-2(IL-2)的给药方案是每日两次大剂量注入5×10单位IL-2。LAK细胞的给药频率根据患者情况每周从1次到3次不等。在接受动脉LAK疗法治疗的9名患者中,16处转移灶(如骨、肌肉和淋巴结转移)中的8处出现消退。LAK疗法期间的副作用并不严重。既往有化疗史是一个不利因素,可能会降低对LAK疗法的敏感性。我们的实验室研究表明,LAK细胞与RCC细胞预孵育时会产生干扰素(IFN)-γ和肿瘤坏死因子(TNF)-α,这可能表明LAK细胞在体内介导抗肿瘤活性的机制。该研究还表明,LAK细胞以及与LAK细胞上清液预孵育的单核细胞在体外会损伤正常内皮细胞,这提示LAK疗法可能存在通过破坏血脑屏障增加脑转移频率的风险。(摘要截断于250字)

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[Lymphokine-activated killer (LAK) therapy for advanced renal cell carcinoma: clinical study on arterial LAK therapy and experimental study on LAK cell activity].[淋巴因子激活的杀伤细胞(LAK)疗法治疗晚期肾细胞癌:动脉内LAK疗法的临床研究及LAK细胞活性的实验研究]
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Lymphokine-activated killer traffic assay and our preliminary clinical results of regional arterial infusion of lymphokine-activated killer cells for renal cell carcinoma.淋巴因子激活的杀伤细胞迁移试验以及我们对肾细胞癌进行区域动脉内输注淋巴因子激活的杀伤细胞的初步临床结果。
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[Study of adoptive immunotherapy for metastatic renal cell carcinoma with lymphokine-activated killer (LAK) cells and interleukin-2. II. Clinical evaluation].[用淋巴因子激活的杀伤细胞(LAK细胞)和白细胞介素-2对转移性肾细胞癌进行过继性免疫治疗的研究。II. 临床评估]
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Interleukin 2 and lymphokine-activated killer cell therapy: analysis of a bolus interleukin 2 and a continuous infusion interleukin 2 regimen.白细胞介素2与淋巴因子激活的杀伤细胞疗法:大剂量白细胞介素2与持续输注白细胞介素2方案的分析
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Immunotherapy with lymphokine-activated natural killer cells and recombinant interleukin-2: a feasibility trial in metastatic renal cell carcinoma.淋巴因子激活的自然杀伤细胞与重组白细胞介素-2免疫疗法:转移性肾细胞癌的可行性试验
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Endogenous and adoptively transferred A-NK and T-LAK cells continuously accumulate within murine metastases up to 48 h after inoculation.内源性和过继转移的A-NK细胞及T-LAK细胞在接种后48小时内持续在小鼠转移灶中积聚。
In Vivo. 1999 May-Jun;13(3):199-204.
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The anti-tumor efficacy of lymphokine-activated killer cells and recombinant interleukin 2 in vivo: direct correlation between reduction of established metastases and cytolytic activity of lymphokine-activated killer cells.淋巴因子激活的杀伤细胞和重组白细胞介素2在体内的抗肿瘤疗效:已形成转移灶的减少与淋巴因子激活的杀伤细胞的细胞溶解活性之间的直接相关性。
J Immunol. 1986 May 15;136(10):3899-909.

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