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抗白血病 T 细胞反应可以通过特定调节性 T 细胞亚群的组成来预测。

Antileukemic T-cell responses can be predicted by the composition of specific regulatory T-cell subpopulations.

机构信息

Department for Hematopoietic Cell Transplantation, Medicine Department 3, University Hospital of Munich, Germany.

出版信息

J Immunother. 2013 May;36(4):223-37. doi: 10.1097/CJI.0b013e31829180e7.

Abstract

Regulatory T cells (Treg) are important regulators of immune responses. In acute myeloid leukemia (AML) patients before/after immunotherapy (stem cell transplantation or donor lymphocyte infusion), their suppressive role can contribute to suppress severe graft-versus-host reactions, but also to impair antileukemic reactions. As leukemia-derived dendritic cells (DCleu) are known to improve the antileukemic functionality of T cells, we evaluated the composition and development of distinct Treg subtypes in AML patients (n=12) compared with healthy probands (n=5) under unstimulated conditions and during stimulation with DCleu-containing DC (DC) or blast-containing mononuclear cells (MNC) in 0- to 7-day mixed lymphocyte cultures by flow cytometry. T-cell subgroups in AML patients were correlated with antileukemic functionality before and after DC or MNC stimulation by functional fluorolysis assays. (1) AML patients' T cells presented with significantly higher frequencies of Treg subgroups in unstimulated T cells compared with healthy probands. (2) After 7 days of DC or MNC stimulation, all Treg subtypes generally increased; significantly higher frequencies of Treg subtypes were still found in AML patients. (3) Antileukemic cytotoxicity was achieved in 36% of T cells after MNC compared with 64% after DC stimulation. Antileukemic activity after DC but not after MNC stimulation correlated with significantly lower frequencies of Treg subtypes (CD8Treg/Teff/em reg). Furthermore, cut-off values for Treg subpopulations could be defined, allowing a prediction of antileukemic response. We demonstrate a crucial role of special Treg subtypes in the mediation of antileukemic functionality. High CD8 Treg, Teff/em reg, and CD39 T cells correlated clearly with a reduced antileukemic activity of T cells. DC stimulation of T cells contributes to overcome impaired antileukemic T-cell reactivity. Refined analyses in the context of clinical responses to immunotherapies and graft versus host reactions are required.

摘要

调节性 T 细胞(Treg)是免疫反应的重要调节剂。在接受免疫治疗(干细胞移植或供体淋巴细胞输注)前后的急性髓系白血病(AML)患者中,其抑制作用既能抑制严重的移植物抗宿主反应,也能抑制抗白血病反应。由于白血病衍生的树突状细胞(DCleu)已知可改善 T 细胞的抗白血病功能,我们通过流式细胞术评估了 AML 患者(n=12)与健康对照者(n=5)在未刺激条件下以及在含有 DCleu 的树突状细胞(DC)或含 blast 的单核细胞(MNC)的 DC 或 MNC 刺激下,在 0 至 7 天混合淋巴细胞培养中不同 Treg 亚群的组成和发育情况。通过功能荧光溶解测定,将 AML 患者的 T 细胞亚群与 DC 或 MNC 刺激前后的抗白血病功能相关联。(1)与健康对照者相比,AML 患者的 T 细胞在未刺激的 T 细胞中表现出明显更高频率的 Treg 亚群。(2)7 天后,所有 Treg 亚群通常都会增加;但在 AML 患者中仍发现更高频率的 Treg 亚群。(3)与 MNC 刺激后相比,MNC 刺激后 36%的 T 细胞中可达到抗白血病细胞毒性,而 DC 刺激后则为 64%。DC 刺激而非 MNC 刺激后的抗白血病活性与 Treg 亚群(CD8Treg/Teff/em reg)的频率明显降低相关。此外,还可以定义 Treg 亚群的截止值,从而可以预测抗白血病反应。我们证明了特殊 Treg 亚群在介导抗白血病功能方面起着关键作用。高 CD8 Treg、Teff/em reg 和 CD39 T 细胞与 T 细胞抗白血病活性降低明显相关。T 细胞的 DC 刺激有助于克服抗白血病 T 细胞反应受损。需要在免疫治疗和移植物抗宿主反应的临床反应背景下进行更精细的分析。

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