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Non-equilibrium and differential function between intraepithelial and lamina propria virus-specific TCR alpha beta(+) CD8 alpha beta(+) T cells in the small intestinal mucosa

机译:小肠黏膜上皮内和固有层病毒特异性TCR alpha beta(+)CD8 alpha beta(+)T细胞之间的非平衡和差异功能

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摘要

The gastrointestinal mucosa regularly encounters commensal and pathogenic microbiota. Gut mucosal lymphocytes consist of two phenotypically different populations residing in the intestinal intraepithelial (IEL) compartment and lamina propria (LP). Little is known about compositional and functional differences of antigen-specific T cells from these mucosal compartments after mucosal infection, or the degree of trafficking between them. We here studied the B8R(20-27)-specific CD8 T-cell response in LP and IEL compartments after intrarectal immunization with modified vaccinia virus Ankara (MVA). CD8(+) T cells in the IEL compartment had much lower avidity than in the LP or spleen during acute and memory phases. Surprisingly, the TCR V beta-chain distribution of antigen-specific T cells and the length of the CDR3 region of the dominant V beta genes showed substantial dissimilarities between IEL and LP antigen-specific CD8 alpha beta T cells in individual mice, increasing with time. We show functional and compositional differences between these mucosal compartments during the effector and memory phases of the immune response, indicating limited crosstalk and microenvironmental differences between the IEL, LP, and spleen. The restricted migration of cells from each of these mucosal compartments could partly account for a founder effect we observed in the IEL TCR alpha beta CD8 alpha beta epitope-specific repertoire that might impact protective efficacy.
机译:胃肠道粘膜经常遇到共​​生和致病菌群。肠粘膜淋巴细胞由两个表型不同的种群组成,分别位于肠上皮内(IEL)和固有层(LP)。关于粘膜感染后这些粘膜区室的抗原特异性T细胞的组成和功能差异或它们之间的运输程度知之甚少。我们在这里用改良牛痘病毒安卡拉(MVA)直肠内免疫后研究了LP和IEL隔室中的B8R(20-27)特异性CD8 T细胞应答。在急性期和记忆期,IEL区室中的CD8(+)T细胞的亲和力比LP或脾脏中的低。出人意料的是,抗原特异性T细胞的TCR Vβ链分布和显性Vβ基因的CDR3区域的长度显示个别小鼠的IEL和LP抗原特异性CD8αβT细胞之间存在实质性差异,并随时间增加。我们显示在免疫反应的效应和记忆阶段,这些粘膜区室之间的功能和组成差异,表明IEL,LP和脾脏之间的有限的串扰和微环境差异。细胞从这些粘膜区室中的每个细胞的迁移受限可能部分解释了我们在IEL TCRαβCD8αβ表位特异性表述中观察到的可能影响保护功效的基础效应。

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