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Monocytes are activated in patients with myelodysplastic syndromes and can contribute to bone marrow failure through CD40-CD40L interactions with T helper cells

机译:单核细胞在骨髓增生异常综合症患者中被激活,并可能通过CD40-CD40L与T辅助细胞的相互作用而导致骨髓衰竭

摘要

Immune mechanisms have been shown to contribute to the process of myelodysplastic syndromes (MDS)-related bone marrow (BM) failure. The aim of this study was to evaluate the possible contribution of activated monocytes through CD40-CD40L(CD154) interactions with activated T helper cells. We demonstrated in 77 predominantly lower risk MDS patients that the CD40 receptor was expressed significantly higher on monocytes and that CD40L was expressed significantly higher on T helper cells in peripheral blood (PB) and BM. Increased levels of CD40 and CD40L were detected in the same patients. In addition, stimulation of the CD40 receptor on purified PB monocytes led to a significantly higher tumor necrosis factor alpha production in patients. Co-culture of BM mononuclear cells of 21 patients in the presence of a blocking CD40 monoclonal antibody (ch5D12) led to a significant increase in the number of colony-forming units. A correlation was seen between increased CD40 expression on monocytes with patients' age below 60 years and with the cytogenetic abnormality trisomy 8. These results demonstrate that CD40 expression on monocytes may identify a subgroup of MDS patients in whom immune-mediated hematopoietic failure is part of the disease process. As such, the CD40-CD40L-based activation of monocytes might be a target to counteract MDS-related BM failure.
机译:免疫机制已显示出与骨髓增生异常综合症(MDS)相关的骨髓(BM)衰竭的过程。这项研究的目的是评估活化的单核细胞通过CD40-CD40L(CD154)与活化的T辅助细胞相互作用的可能贡献。我们在77位主要是低危MDS患者中证明,外周血(PB)和BM中CD40受体在单核细胞上的表达明显较高,而CD40L在T辅助细胞上的表达明显较高。在同一例患者中检测到CD40和CD40L水平升高。此外,纯化的PB单核细胞上CD40受体的刺激导致患者体内明显增加的肿瘤坏死因子α产生。在存在封闭性CD40单克隆抗体(ch5D12)的情况下,共培养21位患者的BM单核细胞,导致菌落形成单位数量显着增加。在年龄小于60岁的患者中,单核细胞上CD40表达的增加与细胞遗传学异常三体性8之间存在相关性。这些结果表明,单核细胞上CD40的表达可能确定了MDS患者的一个亚组,其中免疫介导的造血功能衰竭是其中的一部分疾病过程。因此,基于CD40-CD40L的单核细胞活化可能是抵消MDS相关BM衰竭的靶标。

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