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大鼠脑周血管细胞的更新

Turnover of rat brain perivascular cells.

作者信息

Bechmann I, Kwidzinski E, Kovac A D, Simbürger E, Horvath T, Gimsa U, Dirnagl U, Priller J, Nitsch R

机构信息

Institute of Anatomy, Humboldt-University Hospital Charité, Berlin, Germany.

出版信息

Exp Neurol. 2001 Apr;168(2):242-9. doi: 10.1006/exnr.2000.7618.

Abstract

Brain perivascular spaces harbor a population of cells which exhibit high phagocytic capacity. Therefore, these cells can be labeled by intraventricular injection of tracers. Such perivascular cells at the interface between blood and brain are believed to belong to the monocyte/macrophage lineage and to be involved in antigen presentation. Currently, it is unclear whether these cells undergo a continuous turnover by entering and leaving the bloodstream. Using bone-marrow-chimeric animals, migration of donor macrophages into brain perivascular spaces has been reported. On the other hand, following intracerebral injection of india ink into nontransplanted animals, ink-labeled perivascular cells were still found 2 years after injection, suggesting a high stability of this cell pool. Thus, the turnover of perivascular cells observed in chimeras might be a result of bone marrow transplantation rather than a physiological occurrence. To address this issue, we monitored de novo invasion of macrophages into perivascular spaces of apparently healthy adult rats by applying techniques other than bone marrow transplantation, (i) consecutive injections of different tracers and (ii) ex vivo isolation of macrophages from the blood, cell labeling, and reinjection into the same animal to avoid MHC mismatch. Both approaches revealed vivid de novo invasion of macrophages into perivascular spaces, but not into brain parenchyma, rendering untenable the concept of perivascular cells forming a stable population of macrophages in the brain. Thus, brain perivascular spaces are under permanent immune surveillance of blood borne macrophages in normal adult rats.

摘要

脑周血管间隙中存在一群具有高吞噬能力的细胞。因此,这些细胞可通过脑室内注射示踪剂进行标记。人们认为,血液与脑之间界面处的此类周血管细胞属于单核细胞/巨噬细胞谱系,并参与抗原呈递。目前尚不清楚这些细胞是否通过进出血流进行持续更新。据报道,利用骨髓嵌合动物,供体巨噬细胞可迁移至脑周血管间隙。另一方面,在未移植动物脑内注射印度墨汁后,注射2年后仍可发现被墨汁标记的周血管细胞,这表明该细胞池具有高度稳定性。因此,在嵌合体中观察到的周血管细胞更新可能是骨髓移植的结果,而非生理现象。为解决这一问题,我们通过应用骨髓移植以外的技术,监测了巨噬细胞向明显健康的成年大鼠周血管间隙的从头侵袭,(i)连续注射不同的示踪剂,(ii)从血液中离体分离巨噬细胞、进行细胞标记并重新注射到同一动物体内以避免MHC不匹配。两种方法均显示巨噬细胞可生动地从头侵袭至周血管间隙,但不会侵袭至脑实质,这使得周血管细胞在脑中形成稳定巨噬细胞群体的概念站不住脚。因此,在正常成年大鼠中,脑周血管间隙受到血源巨噬细胞的永久免疫监视。

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