首页> 外文期刊>Clinical immunology: The official journal of the Clinical Immunology Society >Reduced IFN-alpha secretion by blood dendritic cells in human diabetes.
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Reduced IFN-alpha secretion by blood dendritic cells in human diabetes.

机译:在人类糖尿病中血液树突状细胞的IFN-α分泌减少。

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Characterization of dendritic cells (DC) in human diabetes has been restricted to monocyte-derived DC in type 1 diabetes, whose physiological relevance to endogenous DC is uncertain. Here, we provide the first report characterizing the phenotype and function of endogenous DC subsets in type 1 and type 2 diabetes. We show that DC subsets in each diabetic group exhibit normal properties concerning frequency and activation state, as determined using 4-color flow cytometry of whole blood cells. DC maturation is also intact as confirmed by their efficacious ability to stimulate T cell proliferation in an allogeneic MLR assay. Yet we found that DC are poor producers of IFN-alpha (P < 0.05) in human diabetes. IFN-alpha is a potent antiviral agent and therefore its reduced levels may interfere with T cell-mediated immune responses leading to increased susceptibility and persistence of infections in persons with diabetes.
机译:人类糖尿病中树突状细胞(DC)的表征仅限于1型糖尿病的单核细胞衍生DC,其与内源性DC的生理相关性尚不确定。在这里,我们提供了第一个描述1型和2型糖尿病的内源性DC亚型的表型和功能的报告。我们显示每个糖尿病组中的DC子集表现出有关频率和激活状态的正常属性,这是使用全血细胞的4色流式细胞术确定的。 DC在同种异体MLR分析中刺激T细胞增殖的有效能力也证实了DC成熟。然而,我们发现DC在人类糖尿病中是IFN-α的不良生产者(P <0.05)。 IFN-α是有效的抗病毒药,因此其降低的水平可能会干扰T细胞介导的免疫反应,从而导致糖尿病患者感染的易感性和持久性升高。

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