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重组白细胞介素-2的体内效应。I. 从接受重组白细胞介素-2的癌症患者中分离循环Leu-19+淋巴因子激活的杀伤效应细胞。

In vivo effects of recombinant IL-2. I. Isolation of circulating Leu-19+ lymphokine-activated killer effector cells from cancer patients receiving recombinant IL-2.

作者信息

McMannis J D, Fisher R I, Creekmore S P, Braun D P, Harris J E, Ellis T M

机构信息

Section of Hematology/Oncology, Loyola University Stritch School of Medicine, Maywood, IL 60153.

出版信息

J Immunol. 1988 Feb 15;140(4):1335-40.

PMID:3257776
Abstract

This study was designed to isolate and phenotypically characterize lymphokine-activated killer (LAK) cells generated in vivo during administration of high dose rIL-2 to cancer patients. The development of circulating LAK effector cells in these patients was demonstrated by the ability of fresh PBL to exhibit lytic activity against the NK-resistant Daudi cell line and fresh tumor cells without prior in vitro culture with rIL-2. Kinetic studies demonstrated that circulating LAK effector cells are detectable 4 to 6 wk after the initiation of rIL-2 therapy. Cells isolated by FACS revealed that circulating LAK cells are Leu-19+, Leu-17+ but CD5-. We have previously reported that circulating Leu-19+ cells are heterogeneous with regard to the expression of CD16 and CD8. Since sorting of cells expressing Leu-19 and either low quantities of CD8 or CD16 resulted in cytolytic activity in both the positive and negative fractions, these latter two markers do not identify subpopulations of Leu-19+ cells with or without LAK cytolytic activity. Although all LAK cells generated in vivo were Leu-19+, we generated LAK cells from the Leu-19- subpopulation after in vitro culture with rIL-2, suggesting that at least some of in vitro generated LAK cells are derived from Leu-19- precursor cells. These LAK cells did not, however, express the Leu-19 surface marker. Based on the functional data reported in this paper, we conclude that circulating LAK effector cells are a phenotypically heterogeneous population that express surface Ag in association with NK cells and not T lymphocytes.

摘要

本研究旨在分离并从表型上鉴定癌症患者在大剂量重组白细胞介素-2(rIL-2)给药期间体内产生的淋巴因子激活的杀伤细胞(LAK细胞)。这些患者循环中LAK效应细胞的出现通过新鲜外周血淋巴细胞(PBL)对NK抗性的Daudi细胞系和新鲜肿瘤细胞表现出裂解活性得以证明,且无需事先用rIL-2进行体外培养。动力学研究表明,在rIL-2治疗开始后4至6周可检测到循环中的LAK效应细胞。通过荧光激活细胞分选术(FACS)分离的细胞显示,循环中的LAK细胞为Leu-19+、Leu-17+但CD5-。我们之前报道过,循环中的Leu-19+细胞在CD16和CD8表达方面是异质性的。由于对表达Leu-19以及低量CD8或CD16的细胞进行分选后,阳性和阴性组分均具有细胞溶解活性,所以后两个标志物并不能识别具有或不具有LAK细胞溶解活性的Leu-19+细胞亚群。尽管体内产生的所有LAK细胞均为Leu-19+,但我们在用rIL-2进行体外培养后从Leu-19-亚群中产生了LAK细胞,这表明至少一些体外产生的LAK细胞源自Leu-19-前体细胞。然而,这些LAK细胞并不表达Leu-19表面标志物。基于本文报道的功能数据,我们得出结论,循环中的LAK效应细胞是一个表型异质性群体,其表达与NK细胞而非T淋巴细胞相关的表面抗原。

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