B细胞慢性淋巴细胞白血病中T细胞和B细胞的细胞内肿瘤坏死因子产生

Intracellular tumor necrosis factor production by T- and B-cells in B-cell chronic lymphocytic leukemia.

作者信息

Bojarska-Junak Agnieszka, Rolinski Jacek, Wasik-Szczepaneko Ewa, Kaluzny Zbigniew, Dmoszynska Anna

机构信息

Department of Clinical Immunology, University School of Medicine, Jaczewskiego 8, 20-950 Lublin, Poland.

出版信息

Haematologica. 2002 May;87(5):490-9.

PMID:12010662

Abstract

BACKGROUND AND OBJECTIVES

The pathogenesis of B-cell chronic lymphocytic leukemia (B-CLL) has been linked with the production and activity of certain growth factors. Tumor necrosis factor (TNF-alpha) is important for the growth and survival of B-CLL cells. TNF-alpha promotes the proliferation of the malignant cell clone and is believed to play a role in the progression of B-CLL. The aim of our study was to examine the level of production and intracellular expression of TNF-alpha by T- and B-cells in B-CLL in correlation with stage of disease and clinical parameters.

DESIGN AND METHODS

Using a three-color flow cytometry technique we analyzed intracellular TNF-alpha expression by B-cells (CD19+) and by T-cell subsets (CD3+/CD4+ and CD3+/CD8+) in peripheral blood (PB) and bone marrow (BM) from 40 patients with B-CLL and 24 healthy controls.

RESULTS

A higher number of TNF-a-positive B-cells were found in PB and BM in B-CLL patients than in normal controls. In BM this difference was statistically significant (p<0.007). Likewise, in PB and BM the percentage of T-cells expressing TNF-alpha was significantly higher in B-CLL patients than in normal controls (PB: p<0.00001; BM: p<0.007). CD3+/CD4+ cells from patients displayed a lower level of intracellular TNF-alpha expression than did CD3+/CD8+ cells (PB: p<0.0001; BM: p<0.04). The number of T-cells expressing TNF-alpha in B-CLL patients was higher in those with stages III-IV than in patients with early stage disease (PB: p<0.007; BM: p<0.01). Additionally, PB and BM T-cell subsets from patients in stages III-IV had a statistically significant higher level of cytoplasmic TNF-a expression than the corresponding cells from healthy controls (PB: p<0.02; BM: p<0.05). In PB the percentage of CD4+ and CD8+ T-cells expressing cytoplasmic TNF-alpha positively correlated with the stage of disease, total tumor mass (TTM) score and lymphocytosis. In BM only the percentage of CD8 T-cells positively correlated with TTM score and lymphocytosis. The expression of TNF-alpha in leukemic B-cells did not correlate with any progression parameters of disease.

INTERPRETATION AND CONCLUSIONS

The results obtained suggest that malignant B-cells are exposed to large numbers of T-cells able to synthesize and secrete TNF-alpha. Moreover, T-cells even though fewer than B-cells may be an important source of TNF-a in advanced stages of disease. This indicates that the TNF-alpha can be associated with progression of B-CLL and may be implicated in some side-effects associated with this disease.

摘要

背景与目的

B 细胞慢性淋巴细胞白血病（B-CLL）的发病机制与某些生长因子的产生及活性有关。肿瘤坏死因子（TNF-α）对 B-CLL 细胞的生长和存活至关重要。TNF-α促进恶性细胞克隆的增殖，并被认为在 B-CLL 的进展中起作用。我们研究的目的是检测 B-CLL 患者 T 细胞和 B 细胞中 TNF-α的产生水平及细胞内表达情况，并与疾病分期和临床参数进行相关性分析。

设计与方法

采用三色流式细胞术分析 40 例 B-CLL 患者外周血（PB）和骨髓（BM）中 B 细胞（CD19+）以及 T 细胞亚群（CD3+/CD4+和 CD3+/CD8+）的细胞内 TNF-α表达情况，并与 24 名健康对照者进行比较。

结果

B-CLL 患者 PB 和 BM 中 TNF-α阳性 B 细胞数量高于正常对照。在 BM 中，这种差异具有统计学意义（p<0.007）。同样，B-CLL 患者 PB 和 BM 中表达 TNF-α的 T 细胞百分比显著高于正常对照（PB：p<0.00001；BM：p<0.007）。患者的 CD3+/CD4+细胞内 TNF-α表达水平低于 CD3+/CD8+细胞（PB：p<0.0001；BM：p<0.04）。B-CLL 患者中，Ⅲ-Ⅳ期患者表达 TNF-α的 T 细胞数量高于疾病早期患者（PB：p<0.007；BM：p<0.01）。此外，Ⅲ-Ⅳ期患者 PB 和 BM 的 T 细胞亚群中细胞质 TNF-α表达水平在统计学上显著高于健康对照者相应细胞（PB：p<0.02；BM：p<0.05）。在 PB 中，表达细胞质 TNF-α的 CD4+和 CD8+T 细胞百分比与疾病分期、总肿瘤质量（TTM）评分及淋巴细胞增多症呈正相关。在 BM 中，仅 CD8 T 细胞百分比与 TTM 评分及淋巴细胞增多症呈正相关。白血病 B 细胞中 TNF-α的表达与疾病的任何进展参数均无相关性。