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纤连蛋白的CS1黏附基序在T细胞黏附于滑膜和外周淋巴结内皮中的作用。

Role of the CS1 adhesion motif of fibronectin in T cell adhesion to synovial membrane and peripheral lymph node endothelium.

作者信息

van Dinther-Janssen A C, Pals S T, Scheper R J, Meijer C J

机构信息

Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.

出版信息

Ann Rheum Dis. 1993 Sep;52(9):672-6. doi: 10.1136/ard.52.9.672.

Abstract

OBJECTIVES

It has previously been shown that the very late antigen-4/vascular cell adhesion molecule-1 (VLA-4/VCAM-1) pathway functions as a receptor/ligand interaction system mediating the recruitment of activated lymphocytes to inflamed synovium of patients with rheumatoid arthritis. This study was performed to determine whether VLA-4 also affects lymphocyte adhesion to inflamed synovium through interaction with the alternatively spliced CS1 domain of fibronectin.

METHODS

The effect of the synthetic peptide CS1 on lymphocyte binding to human synovial and peripheral lymph node high endothelial venules (HEVs) was measured in an in vitro frozen section assay.

RESULTS

In the presence of the CS1 peptide or antibody to fibronectin, significant inhibition of binding was observed (54 and 51% respectively). Blocking with antibody to VCAM-1 yielded inhibition of binding to 46% of the control value. Maximum inhibition of binding was obtained with a combination of antibody to VCAM-1 and CS1 (65%) and with antibody to VLA-4 alpha (68%). Blocking the classical fibronectin receptor with antibody to VLA-5 alpha gave a slightly lower inhibition at 42%. In normal peripheral lymph nodes, the synthetic peptide CS1 and antibodies to fibronectin and VLA-5 also partially inhibited T cell binding to HEVs (45, 47, and 52% respectively).

CONCLUSION

These results show that fibronectin mediates lymphocyte-HEV interactions not only through its classical VLA-5 receptor, but also through its CS1 adhesion motif in inflamed synovium and peripheral lymph nodes.

摘要

目的

先前的研究表明,极晚期抗原-4/血管细胞黏附分子-1(VLA-4/VCAM-1)通路作为一种受体/配体相互作用系统,介导活化淋巴细胞募集至类风湿关节炎患者的炎症滑膜。本研究旨在确定VLA-4是否也通过与纤连蛋白可变剪接的CS1结构域相互作用影响淋巴细胞与炎症滑膜的黏附。

方法

在体外冰冻切片试验中检测合成肽CS1对淋巴细胞与人滑膜及外周淋巴结高内皮微静脉(HEV)结合的影响。

结果

在存在CS1肽或抗纤连蛋白抗体的情况下,观察到结合显著抑制(分别为54%和51%)。用抗VCAM-1抗体阻断导致结合抑制至对照值的46%。抗VCAM-1抗体与CS1联合使用(65%)以及抗VLA-4α抗体(68%)时获得最大结合抑制。用抗VLA-5α抗体阻断经典纤连蛋白受体时抑制作用稍低,为42%。在正常外周淋巴结中,合成肽CS1以及抗纤连蛋白和VLA-5抗体也部分抑制T细胞与HEV的结合(分别为45%、4i7%和52%)。

结论

这些结果表明,纤连蛋白不仅通过其经典的VLA-5受体介导淋巴细胞与HEV的相互作用,还通过其在炎症滑膜和外周淋巴结中的CS1黏附基序发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9d1b/1005145/62e5d4ead340/annrheumd00484-0055-a.jpg

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