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小鼠中树突状细胞的迁移模式。归巢至脾脏中T细胞依赖区,并在边缘区结合。

Migration patterns of dendritic cells in the mouse. Homing to T cell-dependent areas of spleen, and binding within marginal zone.

作者信息

Austyn J M, Kupiec-Weglinski J W, Hankins D F, Morris P J

机构信息

Nuffield Department of Surgery, University of Oxford, United Kingdom.

出版信息

J Exp Med. 1988 Feb 1;167(2):646-51. doi: 10.1084/jem.167.2.646.

Abstract

Using quantitative techniques we have shown elsewhere that dendritic cells (DC) migrate from blood into the spleen, under the control of T cells. Here we traced the localization of DC within the spleen and sought to explain the means by which they entered. DC were labeled with a fluorochrome, Hoescht 33342, and injected intravenously. Spleens were removed 3 or 24 h later and DC were visualized within particular areas that were defined by mAbs and FITC anti-Igs. At 3 h most DC were in the red pulp, whereas by 24 h the majority had homed to T-dependent areas of the white pulp and may have become interdigitating cells. Lymphoid DC, isolated from spleen and perhaps normally present in blood, may thus be a migratory stage distinct from the relatively fixed interdigitating cells. We also developed a frozen section assay to investigate the interaction of DC with various lymphoid elements. When DC were incubated on sections of spleen, at 37 degrees C but not at 4 degrees C they attached specifically within the marginal zone and did not bind to T areas; in contrast, macrophages attached only to red pulp and T cells did not bind specifically. However, DC did not bind to sections of mesenteric lymph node, whereas T cells localized in particular regions at 4 degrees C but not at 37 degrees C, probably the high endothelial venules. DC may thus express "homing receptors," similar to those of T cells, for certain endothelia. We propose that T cells can modify the vascular endothelium in certain areas to allow egress of DC from the bloodstream.

摘要

我们曾在其他地方运用定量技术表明,在T细胞的控制下,树突状细胞(DC)从血液迁移至脾脏。在此,我们追踪了DC在脾脏内的定位,并试图解释它们进入脾脏的方式。用荧光染料Hoescht 33342标记DC,然后静脉注射。3小时或24小时后取出脾脏,通过单克隆抗体(mAbs)和异硫氰酸荧光素(FITC)抗免疫球蛋白来确定特定区域内的DC。3小时时,大多数DC位于红髓,而到24小时时,大多数已归巢至白髓的T细胞依赖区,可能已成为交错突细胞。从脾脏分离出的、可能正常存在于血液中的淋巴样DC,可能是一个与相对固定的交错突细胞不同的迁移阶段。我们还开发了一种冰冻切片检测法来研究DC与各种淋巴样成分的相互作用。当DC在脾脏切片上于37℃而非4℃孵育时,它们特异性地附着在边缘区,而不与T细胞区结合;相反,巨噬细胞仅附着于红髓,T细胞则无特异性结合。然而,DC不与肠系膜淋巴结切片结合,而T细胞在4℃而非37℃时定位于特定区域,可能是高内皮微静脉。因此,DC可能表达与T细胞类似的针对某些内皮细胞的“归巢受体”。我们提出T细胞可在某些区域修饰血管内皮,以使DC从血流中逸出。

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