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The fate of autoreactive, GFP+ T cells in rat models of uveitis analyzed by intravital fluorescence microscopy and FACS.

机译:通过玻璃体内荧光显微镜和FACS分析了葡萄膜炎大鼠模型中自身反应性GFP + T细胞的命运。

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摘要

Experimental autoimmune uveitis (EAU) is an inflammatory disease of the immune privileged inner eye, mediated by CD4(+) Th1 cells specific for retinal autoantigens. To elucidate the fate of the T cells in the eye we adoptively transferred green fluorescent protein-positive (GFP(+)) T cells with specificity for R14, a peptide from interphotoreceptor retinoid-binding protein (IRBP) or OVA as foreign control antigen to naive Lewis rats. We also used the model of immunogenic uveitis, an inflammatory eye disease induced by intraocular injection of soluble OVA 1 day post transfer of OVA-specific GFP(+) cells. We investigated the timing of ocular T cell infiltration and their immunological activation state by intravital fluorescence microscopy (IVFM) of the iris until onset of intraocular inflammation. Within 30 min of injection, GFP(+) cells invaded the iris tissue, irrespective of their antigen specificity, whereas intraocular inflammation was only observed 3 days later, if cells recognized their respectiveantigen (R14-specific cells in EAU, OVA-specific cells in immunogenic uveitis). Using FACS analysis we found that activation markers were upregulated only on cells from uveitic eyes, but not from other sources, suggesting that intraocularly presented specific antigen is a prerequisite for T cell reactivation and subsequent recruitment of inflammatory cells.
机译:实验性自身免疫性葡萄膜炎(EAU)是一种免疫特权内眼的炎症性疾病,由针对视网膜自身抗原的CD4(+)Th1细胞介导。为了阐明眼睛中T细胞的命运,我们过继转移了对R14有特异性的绿色荧光蛋白阳性(GFP(+))T细胞,R14是一种由感光受体类视黄醇结合蛋白(IRBP)或OVA制成的肽,作为外源对照抗原天真的刘易斯老鼠。我们还使用了免疫原性葡萄膜炎的模型,这是由OVA特异性GFP(+)细胞转移后1天眼内注射可溶性OVA引起的炎症性眼病。我们通过虹膜的活体荧光显微镜(IVFM)研究了眼T细胞浸润的时间及其免疫激活状态,直到眼内炎症发作。注射后30分钟内,GFP(+)细胞侵入虹膜组织,无论其抗原特异性如何,而仅在3天后观察到眼内炎症,前提是细胞识别其各自的抗原(EAU中的R14特异性细胞,OVA特异性的OVA特异性细胞)。免疫原性葡萄膜炎)。使用FACS分析,我们发现活化标记仅在葡萄膜眼的细胞上调,而在其他来源则未上调,这表明眼内呈递的特异性抗原是T细胞活化和随后募集炎症细胞的先决条件。

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