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R-Ras调节小鼠T细胞迁移和细胞间黏附分子-1结合。

R-Ras Regulates Murine T Cell Migration and Intercellular Adhesion Molecule-1 Binding.

作者信息

Yan Xiaocai, Yan Mingfei, Guo Yihe, Singh Gobind, Chen Yuhong, Yu Mei, Wang Demin, Hillery Cheryl A, Chan Andrew M

机构信息

Department of Pediatrics, The Medical College of Wisconsin, Milwaukee, Wisconsin, United States of America.

School of Biomedical Sciences, The Chinese University of Hong Kong, Shatin, Hong Kong SAR.

出版信息

PLoS One. 2015 Dec 28;10(12):e0145218. doi: 10.1371/journal.pone.0145218. eCollection 2015.

DOI:10.1371/journal.pone.0145218
PMID:26710069
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4692399/
Abstract

The trafficking of T-lymphocytes to peripheral draining lymph nodes is crucial for mounting an adaptive immune response. The role of chemokines in the activation of integrins via Ras-related small GTPases has been well established. R-Ras is a member of the Ras-subfamily of small guanosine-5'-triphosphate-binding proteins and its role in T cell trafficking has been investigated in R-Ras null mice (Rras-/-). An examination of the lymphoid organs of Rras-/- mice revealed a 40% reduction in the cellularity of the peripheral lymph nodes. Morphologically, the high endothelial venules of Rras-/- mice were more disorganized and less mature than those of wild-type mice. Furthermore, CD4+ and CD8+ T cells from Rras-/- mice had approximately 42% lower surface expression of L-selectin/CD62L. These aberrant peripheral lymph node phenotypes were associated with proliferative and trafficking defects in Rras-/- T cells. Furthermore, R-Ras could be activated by the chemokine, CCL21. Indeed, Rras-/- T cells had approximately 14.5% attenuation in binding to intercellular adhesion molecule 1 upon CCL21 stimulation. Finally, in a graft-versus host disease model, recipient mice that were transfused with Rras-/- T cells showed a significant reduction in disease severity when compared with mice transplanted with wild-type T cells. These findings implicate a role for R-Ras in T cell trafficking in the high endothelial venules during an effective immune response.

摘要

T淋巴细胞向外周引流淋巴结的迁移对于启动适应性免疫反应至关重要。趋化因子通过Ras相关小GTP酶激活整合素的作用已得到充分证实。R-Ras是小GTP结合蛋白Ras亚家族的成员,其在T细胞迁移中的作用已在R-Ras基因敲除小鼠(Rras-/-)中进行了研究。对Rras-/-小鼠的淋巴器官检查发现,外周淋巴结的细胞数量减少了40%。形态学上,Rras-/-小鼠的高内皮微静脉比野生型小鼠的更紊乱且成熟度更低。此外,来自Rras-/-小鼠的CD4+和CD8+ T细胞表面L-选择素/CD62L的表达降低了约42%。这些外周淋巴结异常表型与Rras-/- T细胞的增殖和迁移缺陷有关。此外,趋化因子CCL21可激活R-Ras。事实上,CCL21刺激后,Rras-/- T细胞与细胞间黏附分子1的结合减弱了约14.5%。最后,在移植物抗宿主病模型中,与移植野生型T细胞的小鼠相比,输注Rras-/- T细胞的受体小鼠疾病严重程度显著降低。这些发现表明,在有效的免疫反应过程中,R-Ras在高内皮微静脉中的T细胞迁移中发挥作用。

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