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首页> 外文期刊>Gastroenterology >Notch-1 signaling regulates intestinal epithelial barrier function, through interaction with CD4+ T cells, in mice and humans.
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Notch-1 signaling regulates intestinal epithelial barrier function, through interaction with CD4+ T cells, in mice and humans.

机译:Notch-1信号传导通过与CD4 + T细胞,小鼠和人类的相互作用来调节肠上皮阻挡函数。

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BACKGROUND & AIMS: Interactions between lymphocytes and intestinal epithelial cells occur in the subepithelial space of the gastrointestinal tract. Normal human lamina propria lymphocytes (LPLs) induce differentiation of intestinal epithelial cells. The absence of LPLs in mice, such as in RAG1(-/-) mice, results in defects in epithelial cell differentiation. We investigated the role of lymphoepithelial interactions in epithelial differentiation and barrier function. METHODS: We used adoptive transfer to determine if CD4(+) T cells (CD4(+)CD62L(+)CD45Rb(Hi) and/or CD4(+)CD62L(+)CD45Rb(Lo)) could overcome permeability defect (quantified in Ussing chambers). Immunofluorescence staining was performed to determine expression of cleaved Notch-1, villin, and claudin 5 in colon samples from mice and humans. Caco-2 cells were infected with a lentivirus containing a specific Notch-1 or scrambled short hairpin RNA sequence. Tight junction assembly was analyzed by immunoblot and immunofluorescence analyses, and transepithelial resistance was monitored. RESULTS: Expression of cleaved Notch-1, villin, or claudin 5 was not detected in RAG1(-/-) colonocytes; their loss correlated with increased intestinal permeability. Transfer of CD45Rb(Hi) and/or CD45Rb(Lo) cells into RAG1(-/-) mice induced expression of cleaved Notch, villin, and claudin 5 in colonocytes and significantly reduced the permeability of the distal colon. Loss of Notch-1 expression in Caco-2 cells correlated with decreased transepithelial resistance and dysregulated expression and localization of tight junction proteins. Levels of cleaved Notch-1 were increased in colonic epithelium of patients with Crohn's disease. CONCLUSIONS: LPLs promote mucosal barrier function, which is associated with activation of the Notch-1 signaling pathway. LPLs maintain intestinal homeostasis by inducing intestinal epithelial cell differentiation, polarization, and barrier function.
机译:背景和目的:在胃肠道的耻骨上存在淋巴细胞和肠上皮细胞之间的相互作用。正常的人椎板丙氨酸淋巴细胞(LPLS)诱导肠上皮细胞的分化。小鼠中没有LPLS,例如Rag1( - / - )小鼠,导致上皮细胞分化中的缺陷。我们研究了淋巴上皮相互作用在上皮分化和屏障功能中的作用。方法:我们使用过继转移来确定CD4(+)T细胞(CD4(+)CD62L(+)CD45RB(HI)和/或CD4(+)CD62L(+)CD45RB(LO))可以克服渗透性缺陷(量化在USSing腔室中)。进行免疫荧光染色以确定来自小鼠和人类的结肠样品中裂解Notch-1,villin和Claudin 5的表达。用含有特定的Notch-1或炒短发夹RNA序列的慢病毒感染Caco-2细胞。通过免疫印迹和免疫荧光分析分析紧密的结组件,并监测Transepithelial抗性。结果:在RAG1( - / - )结肠单胞细胞中未检测到切割Notch-1,villin或Claudin 5的表达;它们的损失与肠道渗透性增加相关。将CD45RB(HI)和/或CD45RB(LO)细胞转移到RAG1( - / - )小鼠中诱导切割槽,绒毛蛋白和克劳丁蛋白5在结肠细胞中的表达,并显着降低了远端结肠的渗透性。 CaCO-2细胞中Notch-1表达的丧失与细胞抗性降低和狭义结蛋白的失调表达和局部化相关。克罗恩病患者的结肠上皮患者裂解Notch-1水平增加。结论:LPLS促进粘膜屏障功能,其与Notch-1信号通路的激活相关。 LPLS通过诱导肠上皮细胞分化,极化和屏障功能来保持肠道稳态。

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