首页> 外文OA文献 >Two-photon laser scanning microscopy imaging of intact spinal cord and cerebral cortex reveals requirement for CXCR6 and neuroinflammation in immune cell infiltration of cortical injury sites.
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Two-photon laser scanning microscopy imaging of intact spinal cord and cerebral cortex reveals requirement for CXCR6 and neuroinflammation in immune cell infiltration of cortical injury sites.

机译:完整脊髓和大脑皮层的双光子激光扫描显微镜成像显示皮质损伤部位免疫细胞浸润中需要CXCR6和神经炎症。

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摘要

The mouse spinal cord is an important site for autoimmune and injury models. Skull thinning surgery provides a minimally invasive window for microscopy of the mouse cerebral cortex, but there are no parallel methods for the spinal cord. We introduce a novel, facile and inexpensive method for two-photon laser scanning microscopy of the intact spinal cord in the mouse by taking advantage of the naturally accessible intervertebral space. These are powerful methods when combined with gene-targeted mice in which endogenous immune cells are labeled with green fluorescent protein (GFP). We first demonstrate that generation of the intervertebral window does not elicit a reaction of GFP(+) microglial cells in CX3CR1(gfp/+) mice. We next demonstrate a distinct rostrocaudal migration of GFP(+) immune cells in the spinal cord of CXCR6(gfp/+) mice during active experimental autoimmune encephalomyelitis (EAE). Interestingly, infiltration of the cerebral cortex by GFP(+) cells in these mice required three conditions: EAE induction, cortical injury and expression of CXCR6 on immune cells.
机译:小鼠脊髓是自身免疫和损伤模型的重要部位。颅骨变薄手术为显微镜检查小鼠大脑皮层提供了微创窗口,但是脊髓没有并行的方法。我们介绍一种新颖,方便且便宜的方法,通过利用自然可访问的椎间空间,对小鼠中完整的脊髓进行两光子激光扫描显微镜检查。当与靶向基因的小鼠结合时,这些方法是有效的方法,其中内源性免疫细胞被绿色荧光蛋白(GFP)标记。我们首先证明,椎间窗的生成不会引起CX3CR1(gfp / +)小鼠中的GFP(+)小胶质细胞的反应。接下来,我们展示了在活跃的实验性自身免疫性脑脊髓炎(EAE)期间CXCR6(gfp / +)小鼠脊髓中GFP(+)免疫细胞的独特的尾尾状迁移。有趣的是,这些小鼠中GFP(+)细胞对大脑皮层的浸润需要三个条件:EAE诱导,皮层损伤和免疫细胞上CXCR6的表达。

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