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克罗恩病改变了 CD4+T 细胞中的 MHC-rafts。

Crohn's disease alters MHC-rafts in CD4+ T-cells.

机构信息

Department of Surgery, Medical and Health Science Center, University of Debrecen, Debrecen, Hungary.

出版信息

Cytometry A. 2012 Feb;81(2):149-64. doi: 10.1002/cyto.a.21173. Epub 2011 Nov 29.

DOI:10.1002/cyto.a.21173
PMID:22128034
Abstract

Clusters of MHCI, ICAM-1, CD44, CD59, IL-2R, and IL-15R molecules have been studied on the surface of CD4(+) T-cells from peripheral blood and lymph nodes of patients in Crohn's disease and healthy individuals as controls by using a dual-laser flow cytometric fluorescence resonance energy transfer (FRET) technique and fluorescently stained Fabs. When cells from patients in Crohn's disease are compared to those of controls, the surface expression level for the MHCI reduced by ∼45%, for CD44 enhanced by ∼100%, and for IL-2Rα, IL-15Rα, and common γ(c) enhanced by ∼50%, ∼70%, and ∼130%, respectively. Efficiencies of FRET monitoring homoassociation for the MHCI and CD44 reduced, that for IL-2Rα enhanced. While efficiencies of FRET monitoring the association of γ(c) and ICAM-1 with the MHCI reduced, those monitoring association of IL-2/15Rα, CD44, and CD59 with MHCI enhanced. Efficiencies of FRET measured between the MHCI and IL-2Rα, IL-15Rα differently enhanced to the advantage of IL-15Rα, the one measured between γ(c) and IL-2Rα reduced, suggesting modulations in the strength of interaction of MHCI with IL-2R, IL-15R, and γ(c). The increases in density of surface bound cTx and in the associations of the receptors with the G(M1)-ganglioside lipid molecules suggest stronger lipid raft interactions of the receptors. The observed alterations of MHC-rafts in Crohn's disease--summarized in models of receptor patterns of diseased and control cells--may have functional consequences regarding signaling by the raft components.

摘要

使用双激光流式细胞荧光共振能量转移(FRET)技术和荧光标记 Fab,研究了克罗恩病患者外周血和淋巴结中的 CD4(+) T 细胞表面的 MHC I、ICAM-1、CD44、CD59、IL-2R 和 IL-15R 分子簇。将克罗恩病患者的细胞与对照组进行比较时,MHC I 的表面表达水平降低了约 45%,CD44 增强了约 100%,IL-2Rα、IL-15Rα 和共同γ(c)分别增强了约 50%、约 70%和约 130%。MHC I 和 CD44 的 FRET 监测同型结合效率降低,而 IL-2Rα 的增强。虽然 ICAM-1 与 MHC I 的结合的 FRET 监测效率降低,但监测 IL-2/15Rα、CD44 和 CD59 与 MHC I 的结合的 FRET 监测效率增强。MHC I 和 IL-2Rα、IL-15Rα 之间测量的 FRET 效率以有利于 IL-15Rα 的方式不同增强,而 γ(c)和 IL-2Rα 之间测量的 FRET 效率降低,表明 MHC I 与 IL-2R、IL-15R 和 γ(c)之间相互作用强度的调节。表面结合的 cTx 密度增加和受体与 G(M1)-神经节苷脂脂质分子的缔合增加表明受体的脂质筏相互作用更强。在克罗恩病中观察到的 MHC-筏的改变——总结为患病和对照细胞的受体模式模型——可能对筏成分的信号转导具有功能后果。

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