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肠道上皮内淋巴细胞区室的综合表型分析:1型呼肠孤病毒急性感染胃肠道引起的扰动

Comprehensive phenotypic analysis of the gut intra-epithelial lymphocyte compartment: perturbations induced by acute reovirus 1/L infection of the gastrointestinal tract.

作者信息

Bharhani Mantej S, Grewal Jasvir S, Peppler Richard, Enockson Candace, London Lucille, London Steven D

机构信息

Department of Microbiology and Immunology, Medical University of South Carolina, PO Box 250504, 173 Ashley Avenue, Charleston, SC 29425, USA.

出版信息

Int Immunol. 2007 Apr;19(4):567-79. doi: 10.1093/intimm/dxm022. Epub 2007 Mar 15.

Abstract

Intestinal intra-epithelial lymphocytes (IELs) form a highly specialized lymphoid compartment. IELs consist primarily of T cells that are dispersed as single cells within the epithelial cell layer that surrounds the intestinal lumen. These lymphocytes along with lamina propria lymphocytes are considered to play an important role in the regulation of immune responses. IELs are heterogeneous with regard to phenotype, and they contain sub-populations with diverse functions. In our most recent study, we found that intra-duodenal inoculation of mice with reovirus serotype 1/strain Lang (reovirus 1/L) induced expression of both germinal center and T cell antigen and CD11c on IELs suggesting these cells to be the recently stimulated cells in gut mucosal tissue. We also demonstrated that IELs from these mice when cultured in vitro in the presence of reovirus 1/L-pulsed antigen-presenting cells generated reovirus 1/L-specific MHC-restricted CTL whose function was mediated utilizing perforin, Fas-FasL and TRAIL mechanisms. This present study provides a comprehensive analysis of the diverse subsets of IELs, which function with other mucosal cells to provide a strong, protective immunity in a highly regulated fashion inside the microenvironment of the intestinal epithelium. We demonstrated that the IEL population contains both thymus-dependent (TD) and thymus-independent (TI) lymphocytes in mice and that a complex phenotype is present when sub-populations are analyzed for TCR, Thy-1, CD4, CD8 and B220 expression in a comprehensive manner. In reovirus 1/L-inoculated mice, we found a decrease in the TI population and an increase in the TD population characterized by significant alterations in various sub-populations. This increase was largely due to an increase in CD4(+), CD8(+) and CD4/CD8 double-positive sub-populations of TD IELs. Intracellular cytokine analysis demonstrated induction of IFN-gamma and an increase in effector/cytotoxic CD8 and CD4 cells after reovirus 1/L infection. These results suggest that TD IELs may play an important role in the clearance of reovirus 1/L infection from gut.

摘要

肠道上皮内淋巴细胞(IELs)形成一个高度特化的淋巴区室。IELs主要由T细胞组成,这些T细胞以单个细胞的形式分散在围绕肠腔的上皮细胞层内。这些淋巴细胞与固有层淋巴细胞一起被认为在免疫反应的调节中发挥重要作用。IELs在表型上具有异质性,并且包含具有不同功能的亚群。在我们最近的研究中,我们发现用1型呼肠孤病毒/朗株(呼肠孤病毒1/L)对小鼠进行十二指肠内接种可诱导生发中心和T细胞抗原以及IELs上的CD11c表达,这表明这些细胞是肠道黏膜组织中最近受到刺激的细胞。我们还证明,当这些小鼠的IELs在体外与经呼肠孤病毒1/L脉冲处理的抗原呈递细胞一起培养时,会产生呼肠孤病毒1/L特异性的MHC限制性CTL,其功能通过穿孔素、Fas - FasL和TRAIL机制介导。本研究对IELs的不同亚群进行了全面分析,这些亚群与其他黏膜细胞一起发挥作用,以高度调控的方式在肠道上皮微环境中提供强大的保护性免疫。我们证明,在小鼠中IEL群体同时包含胸腺依赖性(TD)和胸腺非依赖性(TI)淋巴细胞,并且当全面分析亚群的TCR、Thy - 1、CD4、CD8和B220表达时,会出现复杂的表型。在接种呼肠孤病毒1/L的小鼠中,我们发现TI群体减少,TD群体增加,其特征是各个亚群发生显著变化。这种增加主要是由于TD IELs的CD4(+)、CD8(+)和CD4/CD8双阳性亚群增加。细胞内细胞因子分析表明,呼肠孤病毒1/L感染后可诱导IFN - γ产生,并且效应/细胞毒性CD8和CD4细胞增加。这些结果表明,TD IELs可能在清除肠道中的呼肠孤病毒1/L感染中发挥重要作用。

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