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慢性淋巴细胞白血病患者的循环树突状细胞区室存在严重缺陷,无法刺激有效的T细胞反应。

The circulating dendritic cell compartment in patients with chronic lymphocytic leukemia is severely defective and unable to stimulate an effective T-cell response.

作者信息

Orsini Enrica, Guarini Anna, Chiaretti Sabina, Mauro Francesca Romana, Foa Robert

机构信息

Dipartimento di Biotecnologie Cellulari ed Ematologia, University La Sapienza, Via Benevento 6, 00161 Rome, Italy.

出版信息

Cancer Res. 2003 Aug 1;63(15):4497-506.

PMID:12907623
Abstract

Chronic lymphocytic leukemia (CLL), the most frequent leukemia in the Western world, is characterized by a profound dysregulation of the host immune system that has a marked impact on the clinical course of the disease. To date, the competence of the circulating dendritic cell (DC) compartment in CLL patients has not been investigated. To address this issue, we sorted DC precursors from the peripheral blood of CLL patients and found a profoundly altered compartment as compared with normal donors. CLL DCs proved a morphologically and phenotypically immature population, lacking the maturation antigen CD83 and the costimulatory molecule CD80, unable to induce a significant proliferative response in allo-mixed lymphocyte reaction, with a reduced ability to release interleukin 12 and to drive a type 1 T-cell response. To investigate whether these defects could be ascribed to inhibiting soluble factors released by the leukemic clone, DCs were generated in vitro from normal monocytes in the presence of allogeneic CLL cells. The addition of CLL cells induced similar markers of abnormal maturation and functional impairment with an inhibition in the expression of costimulatory molecules and a reduction of their allo-stimulatory ability. The blocking of interleukin 6 activity was able to revert the inhibition in a proportion of patients. Taken together, these findings indicate that mechanisms of tumor-induced DC inhibition are operational in CLL patients, resulting in both maturative and functional defects in the circulating DC compartment, with a potential functional impact in the regulation of in vivo T-cell immune responses.

摘要

慢性淋巴细胞白血病(CLL)是西方世界最常见的白血病,其特征是宿主免疫系统严重失调,这对疾病的临床进程有显著影响。迄今为止,尚未对CLL患者循环树突状细胞(DC)区室的功能进行研究。为了解决这个问题,我们从CLL患者的外周血中分选了DC前体,发现与正常供体相比,该区室发生了深刻改变。CLL DCs在形态和表型上被证明是未成熟群体,缺乏成熟抗原CD83和共刺激分子CD80,在同种异体混合淋巴细胞反应中无法诱导显著的增殖反应,释放白细胞介素12的能力降低,且驱动1型T细胞反应的能力下降。为了研究这些缺陷是否可归因于白血病克隆释放的抑制性可溶性因子,在同种异体CLL细胞存在的情况下,从正常单核细胞体外生成DCs。添加CLL细胞会诱导类似的异常成熟和功能损害标志物,共刺激分子的表达受到抑制,其同种异体刺激能力降低。在一部分患者中,阻断白细胞介素6的活性能够逆转这种抑制作用。综上所述,这些发现表明肿瘤诱导的DC抑制机制在CLL患者中起作用,导致循环DC区室出现成熟和功能缺陷,对体内T细胞免疫反应的调节具有潜在的功能影响。

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