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The Brain Microvascular Endothelium Supports T Cell Proliferation and Has Potential for Alloantigen Presentation

机译:脑微血管内皮细胞支持T细胞增殖,并具有呈递抗原的潜力

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Endothelial cells (EC) form the inner lining of blood vessels and are positioned between circulating lymphocytes and tissues. Hypotheses have formed that EC may act as antigen presenting cells based on the intimate interactions with T cells, which are seen in diseases like multiple sclerosis, cerebral malaria (CM) and viral neuropathologies. Here, we investigated how human brain microvascular EC (HBEC) interact with and support the proliferation of T cells. We found HBEC to express MHC II, CD40 and ICOSL, key molecules for antigen presentation and co-stimulation and to take up fluorescently labeled antigens via macropinocytosis. In co-cultures, we showed that HBEC support and promote the proliferation of CD4+ and CD8+ T cells, which both are key in CM pathogenesis, particularly following T cell receptor activation and co-stimulation. Our findings provide novel evidence that HBEC can trigger T cell activation, thereby providing a novel mechanism for neuroimmunological complications of infectious diseases.
机译:内皮细胞(EC)形成血管的内层,位于循环的淋巴细胞和组织之间。假说已经形成,EC可以基于与T细胞的紧密相互作用而充当抗原呈递细胞,这种现象在多发性硬化症,脑疟疾(CM)和病毒性神经病理学等疾病中可见。在这里,我们研究了人脑微血管EC(HBEC)如何与T细胞相互作用并支持T细胞的增殖。我们发现HBEC可以表达MHC II,CD40和ICOSL,它们是抗原呈递和共刺激的关键分子,并通过巨胞吞作用吸收荧光标记的抗原。在共培养物中,我们表明HBEC支持并促进CD4 +和CD8 + T细胞的增殖,这两者都是CM发病机理的关键,特别是在T细胞受体激活和共同刺激后。我们的发现为HBEC可以触发T细胞活化提供了新的证据,从而为传染性疾病的神经免疫并发症提供了新的机制。

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