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效应T细胞与新生自身免疫性中枢神经系统病变中脑膜血管结构的相互作用。

Effector T cell interactions with meningeal vascular structures in nascent autoimmune CNS lesions.

作者信息

Bartholomäus Ingo, Kawakami Naoto, Odoardi Francesca, Schläger Christian, Miljkovic Djordje, Ellwart Joachim W, Klinkert Wolfgang E F, Flügel-Koch Cassandra, Issekutz Thomas B, Wekerle Hartmut, Flügel Alexander

机构信息

Max Planck Institute for Neurobiology, 82152 Martinsried, Germany.

出版信息

Nature. 2009 Nov 5;462(7269):94-8. doi: 10.1038/nature08478. Epub 2009 Oct 14.

Abstract

The tissues of the central nervous system are effectively shielded from the blood circulation by specialized vessels that are impermeable not only to cells, but also to most macromolecules circulating in the blood. Despite this seemingly absolute seclusion, central nervous system tissues are subject to immune surveillance and are vulnerable to autoimmune attacks. Using intravital two-photon imaging in a Lewis rat model of experimental autoimmune encephalomyelitis, here we present in real-time the interactive processes between effector T cells and cerebral structures from their first arrival to manifest autoimmune disease. We observed that incoming effector T cells successively scanned three planes. The T cells got arrested to leptomeningeal vessels and immediately monitored the luminal surface, crawling preferentially against the blood flow. After diapedesis, the cells continued their scan on the abluminal vascular surface and the underlying leptomeningeal (pial) membrane. There, the T cells encountered phagocytes that effectively present antigens, foreign as well as myelin proteins. These contacts stimulated the effector T cells to produce pro-inflammatory mediators, and provided a trigger to tissue invasion and the formation of inflammatory infiltrations.

摘要

中枢神经系统的组织通过特殊的血管与血液循环有效隔离开来,这些血管不仅对细胞不可渗透,而且对血液中循环的大多数大分子也不可渗透。尽管有这种看似绝对的隔离,但中枢神经系统组织仍受到免疫监视,并且易受自身免疫攻击。在实验性自身免疫性脑脊髓炎的Lewis大鼠模型中使用活体双光子成像技术,我们在此实时呈现效应T细胞与脑结构从首次到达直至出现自身免疫疾病的相互作用过程。我们观察到,进入的效应T细胞依次扫描三个平面。T细胞停滞于软脑膜血管并立即监测管腔表面,优先逆着血流爬行。穿出血管后,细胞继续在血管外表面和下方的软脑膜(蛛网膜)膜上进行扫描。在那里,T细胞遇到能有效呈递抗原(包括外来抗原和髓磷脂蛋白)的吞噬细胞。这些接触刺激效应T细胞产生促炎介质,并为组织侵袭和炎性浸润的形成提供了触发因素。

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