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B细胞的调节能力决定了慢性淋巴细胞白血病的侵袭性。

The regulatory capacity of B cells directs the aggressiveness of CLL.

作者信息

Mohr Audrey, Cumin Marie, Bagacean Cristina, Pochard Pierre, Le Dantec Christelle, Hillion Sophie, Renaudineau Yves, Berthou Christian, Tempescul Adrian, Saad Hussam, Pers Jacques-Olivier, Bordron Anne, Jamin Christophe

机构信息

UMR1227, Lymphocytes B et Autoimmunité, Univ Brest, INSERM, Brest, France.

Laboratoire d'Immunologie et Immunothérapie, CHRU Morvan, Brest, France.

出版信息

Oncoimmunology. 2018 Dec 12;8(3):1554968. doi: 10.1080/2162402X.2018.1554968. eCollection 2019.

Abstract

Chronic lymphocytic leukemia (CLL) is associated with abnormal T-cell responses responsible for defective anti-tumor activities. Intriguingly, CLL B cells share phenotypical characteristics with regulatory B (Breg) cells suggesting that they might negatively control the T-cell activation and immune responses. We elaborated an co-culture system with T cells to evaluate the Breg capacities of CLL B cells following innate Toll-like receptor 9 (TLR9) engagement. We demonstrated that B cells from half of the patients exhibited regulatory capacities, whilst B cells from the remaining patients were unable to develop a Breg function. The T cell sensitivities of all patients were normal suggesting that defective Breg activities were due to intrinsic CLL B cell deficiencies. Thus, TLR-dedicated gene assays highlighted differential signature of the TLR9 negative regulation pathway between the two groups of patients. Furthermore, correlations of the doubling time of lymphocytosis, the time to first treatment, the mutational status of IgVH and the Breg functions indicate that patients with efficient Breg activities have more aggressive CLL than patients with defective Breg cells. Our observations may open new approaches for adjusting therapeutic strategies targeting the Breg along with the evolution of the disease.

摘要

慢性淋巴细胞白血病(CLL)与负责抗肿瘤活性缺陷的异常T细胞反应有关。有趣的是,CLL B细胞与调节性B(Breg)细胞具有相同的表型特征,这表明它们可能会对T细胞活化和免疫反应产生负向控制作用。我们构建了一个与T细胞共培养的系统,以评估天然Toll样受体9(TLR9)激活后CLL B细胞的Breg功能。我们发现,半数患者的B细胞表现出调节功能,而其余患者的B细胞则无法发挥Breg功能。所有患者的T细胞敏感性均正常,这表明Breg活性缺陷是由于CLL B细胞内在缺陷所致。因此,针对TLR的基因检测突出了两组患者之间TLR9负调控途径的差异特征。此外,淋巴细胞增多的倍增时间、首次治疗时间、IgVH突变状态与Breg功能之间的相关性表明,具有高效Breg活性的患者比Breg细胞功能缺陷的患者患有更具侵袭性的CLL。我们的观察结果可能为随着疾病进展调整针对Breg的治疗策略开辟新途径。

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