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首页> 外文期刊>Immunobiology: Zeitschrift fur Immunitatsforschung >Impaired phagocytic capacity driven by downregulation of major phagocytosis-related cell surface molecules elicits an overall modulatory cytokine profile in neutrophils and monocytes from the indeterminate clinical form of Chagas disease
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Impaired phagocytic capacity driven by downregulation of major phagocytosis-related cell surface molecules elicits an overall modulatory cytokine profile in neutrophils and monocytes from the indeterminate clinical form of Chagas disease

机译:由吞噬作用相关的细胞表面主要分子的下调驱动的吞噬能力受损,导致恰加斯病的不确定临床形式导致嗜中性粒细胞和单核细胞的整体调节性细胞因子谱

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摘要

The distinct ability of phagocytes to present antigens, produce cytokines and provide co-stimulatory signals may contribute to the severity of the outcome of Chagas disease. In this paper, we evaluate the phenotypic features of phagocytes along with the cytokine signature of circulating T-cells from Chagas disease patients with indeterminate (IND) and cardiac (CARD) clinical forms of the disease. Our data demonstrated that neutrophils from IND patients displayed an impaired ability to produce cytokines. A lower Trypanosoma cruzi phagocytic index and higher nitric oxide levels were characteristics of monocytes from IND. The impaired phagocytic capacity did not reflect on the levels of anti-. T. cruzi IgG, but was detectable in the downregulation of Fc-γR, TLR and CR1 molecules. The monocyte-derived cytokine signature demonstrated that a down-regulated synthesis of IL-12 and a modulatory state were evidenced by a positive correlation between IL-12 and IL-10 with a lower synthesis of TNF-α. The down-regulation of MHC-II and CD86 in monocytes supports the occurrence of particularities in the APC-activation-arm in IND, and may be involved in the T-cell pro-inflammatory pattern counterbalanced by a potent IL-10 response. Our findings support the hypothesis that differential phenotypic features of monocytes from IND may be committed to the induction of a distinct immune response related to low morbidity in chronic Chagas disease.
机译:吞噬细胞呈现抗原,产生细胞因子和提供共刺激信号的独特能力可能会导致南美锥虫病的严重程度。在本文中,我们评估了具有不确定(IND)和心脏(CARD)临床形式的恰加斯病患者的吞噬细胞的表型特征以及循环T细胞的细胞因子特征。我们的数据表明,来自IND患者的中性粒细胞显示出产生细胞因子的能力受损。克鲁氏锥虫吞噬指数较低和一氧化氮水平较高是IND单核细胞的特征。吞噬能力受损未反映抗-抗药水平。 T. cruzi IgG,但可在Fc-γR,TLR和CR1分子的下调中检测到。单核细胞衍生的细胞因子特征表明,IL-12和IL-10与TNF-α的合成呈正相关,从而证明了IL-12的合成被下调和调节状态。 MHC-II和CD86在单核细胞中的下调支持了IND中APC激活臂的特殊性,并且可能参与了有效的IL-10反应所抵消的T细胞促炎模式。我们的发现支持以下假说:来自IND的单核细胞的不同表型特征可能致力于诱导与慢性Chagas病低发病率相关的独特免疫反应。

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