T cell-dependent protective effects of CpG motifs of bacterial DNA in experimental colitis are mediated by CD11c+ dendritic cells.

Hofmann C; Dunger N; Grunwald N; Hammerling GJ; Hoffmann P; Scholmerich J; Falk W; Obermeier F

首页> 外文期刊>Gut: Journal of the British Society of Gastroenterology >T cell-dependent protective effects of CpG motifs of bacterial DNA in experimental colitis are mediated by CD11c+ dendritic cells.

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T cell-dependent protective effects of CpG motifs of bacterial DNA in experimental colitis are mediated by CD11c+ dendritic cells.

机译：实验性结肠炎中细菌DNA CpG基序的T细胞依赖性保护作用是由CD11c +树突状细胞介导的。

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BACKGROUND: Oligodeoxynucleotides (ODNs) containing unmethylated cytosine-guanosine (CpG) sequence motifs constitute the immunostimulatory components of bacterial DNA which potently activate innate immunity. Administration of CpG-ODNs before the onset of experimental colitis prevents intestinal inflammation by induction of colitis-suppressing T cells. AIMS: To identify the interplay between innate and adaptive immune cells finally leading to protective CpG-ODN effects in intestinal inflammation. METHODS: Total splenic cells or purified selected cell types (CD4(+)CD62L(+) T cells alone or with B cells or dendritic cells (DCs)) from BALB/c mice were (co)-incubated in vitro with CpG-ODN for 5 days and CD4(+)CD62L(+) cells were injected intraperitoneally into C.B.-17 SCID (severe combined immunodeficiency) mice. Splenic CD4(+)CD62L(+) T cells were isolated from transgenic donor mice in which CD11c(+) DCs were depleted by diphtheria toxin administration during CpG-ODN treatment and injected into C57BL/6 Rag2(-/-) recipients. Intestinal inflammation was evaluated by histological scoring and cytokine secretion of mesenteric lymph node cells. RESULTS: CpG-ODN treatment of total splenic cells but not of purified CD4(+)CD62L(+) cells reduced the colitogenic potential of transferred T cells. While CpG-ODN stimulation of co-cultured CD4(+)CD62L(+) and B-cells did not alter the colitogenic potential of T cells, co-incubation of CpG-ODN-stimulated DCs and CD4(+)CD62L(+) cells reduced the colitogenic potential of the T cell population. Depletion of CD11c(+) DCs during CpG-ODN administration in vivo abolished the protective CpG-ODN effects. CONCLUSIONS: CpG-ODN-dependent protective effects in experimental colitis act indirectly on CD4(+)CD62L(+) T cells. While the involvement of B cells could be excluded, CD11c(+) DCs were identified as key mediators of CpG-ODN-induced protection in experimental colitis.

机译：背景：含有未甲基化胞嘧啶-鸟苷（CpG）序列基序的寡脱氧核苷酸（ODN）构成了细菌DNA的免疫刺激成分，可有效激活先天免疫力。在实验性结肠炎发作前给予CpG-ODN可通过诱导抑制结肠炎的T细胞来预防肠道炎症。目的：确定先天性和适应性免疫细胞之间的相互作用，最终导致肠道炎症中的保护性CpG-ODN效应。方法：将来自BALB / c小鼠的总脾细胞或纯化的选定细胞类型（单独的CD4（+）CD62L（+）T细胞或与B细胞或树突状细胞（DC））与CpG-ODN进行体外（共）孵育。持续5天，将CD4（+）CD62L（+）细胞腹膜内注射到CB-17 SCID（严重的联合免疫缺陷）小鼠中。从转基因供体小鼠中分离出脾脏CD4（+）CD62L（+）T细胞，在该小鼠中CD11c（+）DC在CpG-ODN处理期间通过白喉毒素施用而耗尽，并注入C57BL / 6 Rag2（-/-）受体中。通过组织学评分和肠系膜淋巴结细胞的细胞因子分泌来评估肠道炎症。结果：CpG-ODN处理总的脾细胞而不是纯化的CD4（+）CD62L（+）细胞降低了转移的T细胞的致菌潜力。虽然共培养的CD4（+）CD62L（+）和B细胞的CpG-ODN刺激不会改变T细胞的致大肠杆菌潜力，但CpG-ODN刺激的DC和CD4（+）CD62L（+）的共孵育细胞降低了T细胞群体的致生力。在体内施用CpG-ODN期间耗尽CD11c（+）DC消除了保护性CpG-ODN效应。结论：实验性结肠炎中CpG-ODN依赖性保护作用间接作用于CD4（+）CD62L（+）T细胞。虽然可以排除B细胞的参与，但CD11c（+）DC被确定为实验性结肠炎中CpG-ODN诱导的保护的关键介质。

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《Gut: Journal of the British Society of Gastroenterology》 |2010年第10期|共8页
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Hofmann C; Dunger N; Grunwald N; Hammerling GJ; Hoffmann P; Scholmerich J; Falk W; Obermeier F;
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专利

1. T cell-dependent protective effects of CpG motifs of bacterial DNA in experimental colitis are mediated by CD11c+ dendritic cells. [J] . Hofmann C, Dunger N, Grunwald N, Gut: Journal of the British Society of Gastroenterology . 2010,第10期

机译：实验性结肠炎中细菌DNA CpG基序的T细胞依赖性保护作用是由CD11c +树突状细胞介导的。
2. CpG motifs of bacterial DNA exert protective effects in mouse models of IBD by antigen-independent tolerance induction. [J] . Bleich A, Janus LM, Smoczek A, Gastroenterology . 2009,第1期

机译：细菌DNA的CpG基序通过不依赖抗原的耐受诱导在IBD小鼠模型中发挥保护作用。
3. Distinct CpG DNA and Polyinosinic-Polycytidylic Acid Double-Stranded RNA, Respectively, Stimulate CD11c? Type 2 Dendritic Cell Precursors and CD11c+ Dendritic Cells to Produce Type I IFN [J] . Norimitsu Kadowaki, Svetlana Antonenko, Yong-Jun Liu The journal of immunology . 2001,第4期

机译：不同的CpG DNA和多肌苷酸-多聚酸双链RNA分别刺激CD11c？ 2型树突状细胞前体和CD11c +树突状细胞产生I型干扰素
4. A pattern matching algorithm for codon optimization and CpG motif-engineering in DNA expression vectors [C] . Ravi Vijaya Satya, Amar Mukherjee, Udaykumar Ranga . 2003

机译：用于DNA表达载体中密码子优化和CpG基序工程的模式匹配算法
5. New insights into epoxyeicosatrienoic acid-mediated protective effects in cardiac cells. [D] . Alsaleh, Nasser Bader. 2014

机译：环氧二十碳三烯酸介导的心肌细胞保护作用的新见解。
6. The Methyl-CpG-Binding Protein Mbd2 Regulates Susceptibility to Experimental Colitis via Control of CD11c+ Cells and Colonic Epithelium [O] . Gareth-Rhys Jones, Sheila L. Brown, Alexander T. Phythian-Adams, 2020

机译：甲基CpG结合蛋白Mbd2通过控制CD11c +细胞和结肠上皮细胞调节对实验性结肠炎的易感性
7. The effects of DNA containing CpG motif on dendritic cells. [O] . Behboudi, S, Chao, D, Klenerman, P, 2000

机译：含有CpG基序的DNA对树突状细胞的影响。
8. Critical DNA flanking sequences of a CpG Oligodeoxynucleotide, but not the 6 base CpG motif, can be replaced with RNA without quantitative or qualitative changes in Toll-like receptor 9-mediated activity [R] . Sen, G., Flora, M., Chattopadhyay, G., 2004

机译：CpG寡脱氧核苷酸的关键DNa侧翼序列，但不是6碱基CpG基序，可被RNa取代，而Toll样受体9介导的活性无定量或定性变化

T cell-dependent protective effects of CpG motifs of bacterial DNA in experimental colitis are mediated by CD11c+ dendritic cells.

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