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在小鼠伤口愈合过程中,中性粒细胞衍生的Ym1蛋白的摄取在缺乏白细胞介素-4信号传导的情况下区分伤口巨噬细胞。

Uptake of neutrophil-derived Ym1 protein distinguishes wound macrophages in the absence of interleukin-4 signaling in murine wound healing.

作者信息

Goren Itamar, Pfeilschifter Josef, Frank Stefan

机构信息

pharmazentrum frankfurt/ZAFES, Klinikum der Johann Wolfgang Goethe-Universität, Frankfurt am Main, Germany.

pharmazentrum frankfurt/ZAFES, Klinikum der Johann Wolfgang Goethe-Universität, Frankfurt am Main, Germany.

出版信息

Am J Pathol. 2014 Dec;184(12):3249-61. doi: 10.1016/j.ajpath.2014.08.011. Epub 2014 Oct 7.

DOI:10.1016/j.ajpath.2014.08.011
PMID:25307347
Abstract

The determination of regenerative wound-healing macrophages as alternatively activated macrophages is currently questioned by the absence of IL-4 in wound tissue. Yet, murine wound tissue expressed high levels of Ym1 (chitinase 3-like 3), an established marker of the IL-4-induced alternatively activated macrophage phenotype. Ym1 was expressed in wound neutrophils but not in macrophages. Initially, Ym1-free wound-healing macrophages, invading from the wound margins, became gradually positive for the protein in the absence of IL-4 signaling and Stat6 activation, as they entered the neutrophil-populated wound regions. IL-4 failed to induce Ym1 protein in ex vivo-cultured wound tissue explants containing wound-healing macrophages. Recombinant Ym1 protein was selectively taken up by macrophages but not by keratinocytes and endothelial cells. Cultured macrophages lost the ability to take up the recombinant protein when four highly conserved residues and the 70-amino acid small α+β domain essential for Ym1 function were removed. The data suggest that the IL-4/Stat6-independent presence of Ym1 protein in wound-healing macrophages is of exogenous origin, with Ym1 taken up from wound neutrophils as the cellular source. The data suggest that in situ determination of wound-healing macrophages, often defined by Ym1, might not essentially describe an IL-4-dependent macrophage phenotype. Consequently, wound-healing macrophages should not be classified by the established categories of the well-accepted but simplified paradigm of M1/M2 macrophage activation.

摘要

由于伤口组织中缺乏白细胞介素-4(IL-4),目前关于再生性伤口愈合巨噬细胞是否为替代性激活巨噬细胞的判定受到质疑。然而,小鼠伤口组织表达了高水平的Ym1(几丁质酶3样3),这是一种已确定的IL-4诱导的替代性激活巨噬细胞表型的标志物。Ym1在伤口中性粒细胞中表达,但在巨噬细胞中不表达。最初,从伤口边缘侵入的无Ym1的伤口愈合巨噬细胞,在进入中性粒细胞聚集的伤口区域时,在没有IL-4信号传导和信号转导及转录激活因子6(Stat6)激活的情况下,逐渐对该蛋白呈阳性。IL-4未能在含有伤口愈合巨噬细胞的体外培养伤口组织外植体中诱导Ym1蛋白表达。重组Ym1蛋白被巨噬细胞选择性摄取,但不被角质形成细胞和内皮细胞摄取。当去除Ym1功能所必需的四个高度保守的残基和70个氨基酸的小α+β结构域时,培养巨噬细胞失去摄取重组蛋白的能力。数据表明,伤口愈合巨噬细胞中Ym1蛋白的存在不依赖于IL-4/Stat6,其来源是外源性的,Ym1是从伤口中性粒细胞摄取作为细胞来源。数据表明,通常由Ym1定义的伤口愈合巨噬细胞的原位判定可能并不能本质上描述一种依赖IL-4的巨噬细胞表型。因此,伤口愈合巨噬细胞不应按照广为接受但简化的M1/M2巨噬细胞激活范式的既定类别进行分类。

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