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骨髓移植后的CD16-CD56+自然杀伤细胞。

CD16- CD56+ natural killer cells after bone marrow transplantation.

作者信息

Jacobs R, Stoll M, Stratmann G, Leo R, Link H, Schmidt R E

机构信息

Abt. für Klinische Immunologie und Transfusionsmedizin, Medizinische Hochschule Hannover, Germany.

出版信息

Blood. 1992 Jun 15;79(12):3239-44.

PMID:1375847
Abstract

Natural killer (NK) cells are phenotypically defined as lymphocytes expressing the antigens CD56 and mostly CD16 (Fc gamma RIII), but lacking CD3. A small CD3- CD16- CD56+ NK cell subset has been described in normal individuals representing less than 2% of peripheral blood lymphocytes. We analyzed here 70 patients for their reconstitution of the immune system during follow-up after autologous or allogeneic bone marrow transplantation. In 35% of these patients, two different NK cell subsets, namely CD56+dim and CD56+bright cells, were observed. The mean duration of these two subsets after transplant was 4 months. Sixty-five percent of the patients exhibited an increased number of NK cells, but only the typical CD16+ CD56+dim population. The CD56+bright subpopulation represented a particular CD3- CD16- NK subset, with posttransplant frequencies up to 70% of all NK cells and 40% of peripheral blood lymphocytes, respectively. In contrast to normal CD56+dim NK cells, CD56+bright cells coexpressed the activation antigens p75 beta-chain of interleukin-2 receptor (IL-2R), CD2R, and CD26, but were negative for CD16. NK and antibody-dependent cellular cytotoxicity activity of CD56+bright cells was low compared with CD56+dim NK cells. But using IL-2 and interferon gamma, their cytotoxicity could be enhanced even more than in CD56+dim lymphocytes. These different subsets may reflect distinct activation or differentiation steps of NK cells during reconstitution of the immune system. Their differential response to IL-2 may be of functional importance for posttransplant cytokine therapy.

摘要

自然杀伤(NK)细胞在表型上被定义为表达抗原CD56且大多表达CD16(FcγRIII)但缺乏CD3的淋巴细胞。在正常个体中已描述了一个小的CD3-CD16-CD56+NK细胞亚群,其在外周血淋巴细胞中所占比例不到2%。我们在此分析了70例患者在自体或异基因骨髓移植后的随访期间免疫系统的重建情况。在这些患者中,35%观察到两种不同的NK细胞亚群,即CD56+dim和CD56+bright细胞。移植后这两个亚群的平均持续时间为4个月。65%的患者NK细胞数量增加,但只有典型的CD16+CD56+dim群体。CD56+bright亚群代表一个特殊的CD3-CD16-NK亚群,移植后的频率分别高达所有NK细胞的70%和外周血淋巴细胞的40%。与正常的CD56+dim NK细胞相比,CD56+bright细胞共表达白细胞介素-2受体(IL-2R)的激活抗原p75β链、CD2R和CD26,但CD16呈阴性。与CD56+dim NK细胞相比,CD56+bright细胞的NK和抗体依赖性细胞毒性活性较低。但使用IL-2和干扰素γ,它们的细胞毒性甚至可比CD56+dim淋巴细胞增强得更多。这些不同的亚群可能反映了免疫系统重建过程中NK细胞不同的激活或分化阶段。它们对IL-2的不同反应可能对移植后细胞因子治疗具有功能重要性。

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