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新型白细胞介素 15 受体α剪接变异体在血脑屏障脑内皮细胞中的表达和信号转导。

Expression and signaling of novel IL15Ralpha splicing variants in cerebral endothelial cells of the blood-brain barrier.

机构信息

Blood-Brain Barrier Group, Pennington Biomedical Research Center, Baton Rouge, Louisiana 70808, USA.

出版信息

J Neurochem. 2010 Jul;114(1):122-9. doi: 10.1111/j.1471-4159.2010.06729.x. Epub 2010 Apr 2.

Abstract

Interleukin (IL)-15 and its receptors in cerebral microvascular endothelial cells play an important role in mediating neuroinflammatory signaling across the blood-brain barrier. Although alternative splice variants of IL15Ralpha (the specific receptor) are seen in immune cells, the presence and functions of splice variants have not been studied in the cerebral endothelia that compose the blood-brain barrier. In this study, we identified five splice variants from mouse cerebral capillaries by RT-PCR, cloning, and DNA sequencing, and performed domain analysis. Four of these isoforms have never been described in any tissue. All isoforms were detected by qPCR in enriched mouse cerebral microvessels and their expression was increased by tumor necrosis factor treatment in vivo. To determine their functions, plasmids encoding individual isoforms were transfected into RBE4 cerebral endothelial cells. All of these predicted alkalinic proteins were expressed and most showed post-translational modifications. There were variations in their subcellular distribution. Only the full length IL15Ralpha and to a lesser degree isoform alpha1 were trafficked to the cell surface 24 h after over-expression. As shown by a luciferase reporter for signal transducer and activator of transcription (STAT)-3, over-expression of isoforms alpha2 and alpha4 reduced basal STAT3 activation. In comparison with the control, over-expression of the full length IL15Ralpha had a greater effect in increasing IL15-induced STAT3 transactivation than other isoforms. The results show that IL15 signaling in cerebral endothelia is probably an orchestrated effect of all IL15Ralpha splice variants that determine the eventual outcome by differential regulation.

摘要

白细胞介素 (IL)-15 及其在脑微血管内皮细胞中的受体在介导血脑屏障的神经炎症信号中发挥重要作用。虽然在免疫细胞中可以看到白细胞介素 15 受体 alpha(特定受体)的替代剪接变体,但在构成血脑屏障的脑内皮细胞中,尚未研究这些剪接变体的存在和功能。在这项研究中,我们通过 RT-PCR、克隆和 DNA 测序鉴定了来自小鼠大脑毛细血管的五个剪接变体,并进行了结构域分析。其中四个同种型从未在任何组织中描述过。所有同种型都通过 qPCR 在富集的小鼠脑微血管中检测到,并且它们的表达在体内肿瘤坏死因子处理后增加。为了确定它们的功能,将编码单个同种型的质粒转染到 RBE4 脑内皮细胞中。所有这些预测的碱性蛋白均被表达,并且大多数表现出翻译后修饰。它们的亚细胞分布存在差异。只有全长 IL15Ralpha 以及在较小程度上同种型 alpha1 在过表达 24 小时后被转运到细胞表面。如信号转导和转录激活因子 (STAT)-3 的荧光素酶报告基因所示,同种型 alpha2 和 alpha4 的过表达降低了基础 STAT3 激活。与对照相比,全长 IL15Ralpha 的过表达比其他同种型更能增加 IL15 诱导的 STAT3 反式激活。结果表明,脑内皮细胞中的 IL15 信号可能是所有 IL15Ralpha 剪接变体的协调作用,通过差异调节决定最终结果。

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