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IL-15 在类风湿关节炎滑膜成纤维细胞上的表达促进了 B 细胞的存活。

IL-15 expression on RA synovial fibroblasts promotes B cell survival.

机构信息

Department of Rheumatology, Hospital Universitario La Paz, Madrid, Spain.

出版信息

PLoS One. 2012;7(7):e40620. doi: 10.1371/journal.pone.0040620. Epub 2012 Jul 9.

Abstract

INTRODUCTION

The purpose of this study was to examine the role of RA Synovial Fibroblast (RASFib) IL-15 expression on B cell survival.

METHODS

Magnetically sorted peripheral blood memory B cells from 15 healthy subjects were cocultured with RASFib.

RESULTS

RASFib constitutively expressed membrane IL-15. Survival of isolated B cells cultured for 6 days, below 5%, was extended in coculture with RASFib to 52+/-8% (p<0.001). IL-15 neutralizing agents but not isotype controls, reduced this rate to 31+/-6% (p<0.05). Interestingly, rhIL-15 had no effect on isolated B cells but significantly increased their survival in coculture with RASFib. In parallel, B cell IL-15R chains were upregulated in cocultures. BAFF and VCAM-1, that are expressed on RASFib, were tested as potential candidates involved in upregulating B cell IL-15R. Culture of B cells in the presence of rhBAFF or rhVCAM-1 resulted in significantly increased survival, together with upregulation of all three IL-15R chains; in parallel, rhIL-15 potentiated the anti-apoptotic effect of BAFF and VCAM-1. Both BAFF and VCAM-1 neutralizing agents downmodulated the effect of RASFib on B cell survival and IL-15R expression. In parallel, rhIL-15 had a lower effect on the survival of B cells cocultured with RASFib in the presence of BAFF or VCAM-1 neutralizing agents. Peripheral blood B cells from 15 early RA patients demonstrated an upregulated IL-15R and increased survival in cocultures.

CONCLUSION

IL-15 expression on RASFib significantly contributes to the anti-apoptotic effect of RASFib on B cells. IL-15 action is facilitated by BAFF and VCAM-1 expressed on RASFib, through an upregulation of IL-15R chains.

摘要

简介

本研究旨在探讨 RA 滑膜成纤维细胞(RASFib)IL-15 表达对 B 细胞存活的作用。

方法

从 15 名健康受试者中分离外周血记忆 B 细胞,用磁珠分选后与 RASFib 共培养。

结果

RASFib 持续表达膜结合型 IL-15。在与 RASFib 共培养 6 天的情况下,分离的 B 细胞的存活率从低于 5%延长至 52+/-8%(p<0.001)。IL-15 中和剂而非同型对照可将该比率降低至 31+/-6%(p<0.05)。有趣的是,rhIL-15 对分离的 B 细胞没有影响,但显著增加了其在与 RASFib 共培养时的存活率。同时,B 细胞 IL-15R 链在共培养中上调。BAFF 和 VCAM-1 表达于 RASFib 上,作为参与上调 B 细胞 IL-15R 的潜在候选物进行了测试。在 rhBAFF 或 rhVCAM-1 的存在下培养 B 细胞可显著提高存活率,并同时上调所有三种 IL-15R 链;同时,rhIL-15 增强了 BAFF 和 VCAM-1 的抗凋亡作用。BAFF 和 VCAM-1 中和剂均下调了 RASFib 对 B 细胞存活和 IL-15R 表达的影响。同时,rhIL-15 对在 BAFF 或 VCAM-1 中和剂存在下与 RASFib 共培养的 B 细胞的存活的影响较低。15 例早期 RA 患者的外周血 B 细胞显示 IL-15R 上调,并在共培养中存活率增加。

结论

RASFib 上的 IL-15 表达显著促进了 RASFib 对 B 细胞的抗凋亡作用。IL-15 作用通过 RASFib 上表达的 BAFF 和 VCAM-1 促进 IL-15R 链的上调而得到促进。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6ba4/3392224/69ede49baf8f/pone.0040620.g002.jpg

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