首页> 美国卫生研究院文献>International Immunology >Rapid immunosurveillance by recirculating lymphocytes in the rat intestine: critical role of unsulfated sialyl-Lewis X on high endothelial venules of the Peyer’s patches
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Rapid immunosurveillance by recirculating lymphocytes in the rat intestine: critical role of unsulfated sialyl-Lewis X on high endothelial venules of the Peyer’s patches

机译:通过大鼠肠中淋巴细胞的循环进行快速免疫监测:未硫酸化的唾液酸化的刘易斯X在Peyer斑块的高内皮小静脉上的关键作用

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摘要

Naive lymphocytes systemically recirculate for immunosurveillance inspecting foreign antigens and pathogens in the body. Trafficking behavior such as the migration pathway and transit time within the gastrointestinal tract, however, remains to be elucidated. Rat thoracic duct lymphocytes (TDLs) were transferred to a congeneic host that had undergone mesenteric lymphadenectomy. The migration pathway was investigated using newly developed four-color immunohistochemistry and immunofluorescence. Donor TDLs showed rapid transition in gut tissues from which they emerged in mesenteric lymph around 4 h after intravenous injection. Immunohistochemistry showed that donor TDLs predominantly transmigrated across high endothelial venules (HEVs) at the interfollicular area of the Peyer’s patches (PPs), then exited into the LYVE-1+ efferent lymphatics, that were close to the venules. The rapid recirculation depended largely on the local expression of unsulfated sialyl-Lewis X on these venules where putative dendritic cells (DCs) were associated underneath. Recruited naive T cells briefly made contact with resident DCs before exiting to the lymphatics in the steady state. In some transplant settings, however, the T cells retained contact with DCs and were sensitized and differentiated into activated T cells. In conclusion, we directly demonstrated that lymphocyte recirculation within the gut is a very rapid process. The interfollicular area of PPs functions as a strategically central site for rapid immunosurveillance where HEVs, efferent lymphatics and resident DCs converge. PPs can, however, generate alloreactive T cells, leading to exacerbation of graft-versus-host disease or gut allograft rejection.
机译:幼稚的淋巴细胞会全身循环以进行免疫监视,以检查体内的外来抗原和病原体。然而,诸如胃肠道内的迁移途径和传播时间之类的贩运行为仍有待阐明。将大鼠胸导管淋巴细胞(TDL)转移到接受了肠系膜淋巴结清扫术的同类宿主中。使用新开发的四色免疫组织化学和免疫荧光技术研究了迁移途径。静脉注射后约4小时,供体TDLs在肠道组织中迅速转变,并从肠组织淋巴结中出现。免疫组织化学显示,供体TDL主要在派伊尔斑(PPs)的小泡间区域跨高内皮小静脉(HEV)迁移,然后进入靠近小静脉的LYVE-1 + 淋巴管内。 。快速再循环在很大程度上取决于这些小静脉上未硫酸化的唾液酸化的刘易斯X的局部表达,这些小静脉下方与假定的树突状细胞(DC)相关。招募的幼稚T细胞短暂地与驻留DC接触,然后以稳定状态离开淋巴管。然而,在某些移植环境中,T细胞保持与DC的接触,并被敏化并分化为活化的T细胞。总之,我们直接证明了肠道内淋巴细胞的再循环是一个非常快速的过程。 PPs的小孔间区域是HEV,传出的淋巴管和驻留DC汇合的快速免疫监视的战略中心位置。 PPs可产生同种异体反应性T细胞,导致移植物抗宿主病加重或肠道异体移植物排斥。

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