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斑马鱼早期巨噬细胞通过依赖M-CSF受体的侵袭过程定殖于头部间充质以及发育中的脑、视网膜和表皮。

Zebrafish early macrophages colonize cephalic mesenchyme and developing brain, retina, and epidermis through a M-CSF receptor-dependent invasive process.

作者信息

Herbomel P, Thisse B, Thisse C

机构信息

Unité de Génétique des Déficits Sensoriels, URA 1968 du CNRS, Département des Biotechnologies, Institut Pasteur, 25 rue du Dr Roux, Paris Cedex 15, 75724, France.

出版信息

Dev Biol. 2001 Oct 15;238(2):274-88. doi: 10.1006/dbio.2001.0393.

DOI:10.1006/dbio.2001.0393
PMID:11784010
Abstract

The origin of resident (noninflammatory) macrophages in vertebrate tissues is still poorly understood. In the zebrafish embryo, we recently described a specific lineage of early macrophages that differentiate in the yolk sac before the onset of blood circulation. We now show that these early macrophages spread in the whole cephalic mesenchyme, and from there invade epithelial tissues: epidermis, retina, and brain--especially the optic tectum. In the panther mutant, which lacks a functional fms (M-CSF receptor) gene, early macrophages differentiate and behave apparently normally in the yolk sac, but then fail to invade embryonic tissues. Our video recordings then document for the first time the behavior of macrophages in the invaded tissues, revealing the striking propensity of early macrophages in epidermis and brain to wander restlessly among epithelial cells. This unexpected behavior suggests that tissue macrophages may be constantly "patrolling" for immune and possibly also developmental and trophic surveillance. At 60 h post-fertilization, all macrophages in the brain and retina undergo a specific phenotypic transformation, into "early (amoeboid) microglia": they become more highly endocytic, they down-regulate the L-plastin gene, and abruptly start expressing high levels of apolipoprotein E, a well-known neurotrophic lipid carrier.

摘要

脊椎动物组织中驻留(非炎性)巨噬细胞的起源仍知之甚少。在斑马鱼胚胎中,我们最近描述了一种早期巨噬细胞的特定谱系,它们在血液循环开始之前就在卵黄囊中分化。我们现在表明,这些早期巨噬细胞扩散到整个头部间充质,并从那里侵入上皮组织:表皮、视网膜和脑——尤其是视顶盖。在缺乏功能性fms(M-CSF受体)基因的黑豹突变体中,早期巨噬细胞在卵黄囊中分化且行为明显正常,但随后无法侵入胚胎组织。我们的视频记录首次记录了巨噬细胞在被侵入组织中的行为,揭示了早期巨噬细胞在表皮和脑中在上皮细胞间不停地游走的显著倾向。这种意外行为表明组织巨噬细胞可能一直在“巡逻”以进行免疫监测,也可能进行发育和营养监测。在受精后60小时,脑和视网膜中的所有巨噬细胞都会经历一种特定的表型转变,成为“早期(阿米巴样)小胶质细胞”:它们的内吞作用增强,下调L-原肌球蛋白基因,并突然开始高水平表达载脂蛋白E,一种著名的神经营养脂质载体。

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