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血管外 CX3CR1+ 细胞将血管内树突状突起延伸到完整的中枢神经系统血管腔中。

Extravascular CX3CR1+ cells extend intravascular dendritic processes into intact central nervous system vessel lumen.

机构信息

Department of Pediatrics, Case Western Reserve University School of Medicine, Cleveland, OH 44106, USA.

出版信息

Microsc Microanal. 2013 Aug;19(4):778-90. doi: 10.1017/S1431927613000482. Epub 2013 May 3.

Abstract

Within the central nervous system (CNS), antigen-presenting cells (APCs) play a critical role in orchestrating inflammatory responses where they present CNS-derived antigens to immune cells that are recruited from the circulation to the cerebrospinal fluid, parenchyma, and perivascular space. Available data indicate that APCs do so indirectly from outside of CNS vessels without direct access to luminal contents. Here, we applied high-resolution, dynamic intravital two-photon laser scanning microscopy to directly visualize extravascular CX3CR1+ APC behavior deep within undisrupted CNS tissues in two distinct anatomical sites under three different inflammatory stimuli. Surprisingly, we observed that CNS-resident APCs dynamically extend their cellular processes across an intact vessel wall into the vascular lumen with preservation of vessel integrity. While only a small number of APCs displayed intravascular extensions in intact, noninflamed vessels in the brain and the spinal cord, the frequency of projections increased over days in an experimental autoimmune encephalomyelitis model, whereas the number of projections remained stable compared to baseline days after tissue injury such as CNS tumor infiltration and aseptic spinal cord trauma. Our observation of this unique behavior by parenchyma CX3CR1+ cells in the CNS argues for further exploration into their functional role in antigen sampling and immune cell recruitment.

摘要

在中枢神经系统 (CNS) 中,抗原呈递细胞 (APCs) 在调节炎症反应中起着至关重要的作用,它们将 CNS 来源的抗原呈递给从循环系统募集到脑脊液、实质和血管周围空间的免疫细胞。现有数据表明,APCs 是在没有直接进入管腔内容物的情况下,从 CNS 血管外部间接进行的。在这里,我们应用高分辨率、动态活体双光子激光扫描显微镜,直接观察两种不同解剖部位的两个不同炎症刺激下,未受干扰的 CNS 组织深处血管外 CX3CR1+APC 的行为。令人惊讶的是,我们观察到 CNS 驻留的 APC 可动态地将其细胞突起穿过完整的血管壁延伸到血管腔中,同时保持血管完整性。虽然在大脑和脊髓的未受炎症影响的完整血管中,只有少数 APC 显示出血管内延伸,但在实验性自身免疫性脑脊髓炎模型中,突起的频率在数天内增加,而与组织损伤(如 CNS 肿瘤浸润和无菌性脊髓损伤)后的基线天数相比,突起的数量保持稳定。我们观察到 CNS 实质 CX3CR1+细胞的这种独特行为,这表明需要进一步探索它们在抗原取样和免疫细胞募集中的功能作用。

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