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人类单核细胞向巨噬细胞分化与极化的转录谱分析:新分子与基因表达模式

Transcriptional profiling of the human monocyte-to-macrophage differentiation and polarization: new molecules and patterns of gene expression.

作者信息

Martinez Fernando O, Gordon Siamon, Locati Massimo, Mantovani Alberto

机构信息

Istituto Clinico Humanitas, Rozzano, Italy.

出版信息

J Immunol. 2006 Nov 15;177(10):7303-11. doi: 10.4049/jimmunol.177.10.7303.

Abstract

Comprehensive analysis of the gene expression profiles associated with human monocyte-to-macrophage differentiation and polarization toward M1 or M2 phenotypes led to the following main results: 1) M-CSF-driven monocyte-to-macrophage differentiation is associated with activation of cell cycle genes, substantiating the underestimated proliferation potential of monocytes. 2) M-CSF leads to expression of a substantial part of the M2 transcriptome, suggesting that under homeostatic conditions a default shift toward M2 occurs. 3) Modulation of genes involved in metabolic activities is a prominent feature of macrophage differentiation and polarization. 4) Lipid metabolism is a main category of modulated transcripts, with expected up-regulation of cyclo-oxygenase 2 in M1 cells and unexpected cyclo-oxygenase 1 up-regulation in M2 cells. 5) Each step is characterized by a different repertoire of G protein-coupled receptors, with five nucleotide receptors as novel M2-associated genes. 6) The chemokinome of polarized macrophages is profoundly diverse and new differentially expressed chemokines are reported. Thus, transcriptome profiling reveals novel molecules and signatures associated with human monocyte-to-macrophage differentiation and polarized activation which may represent candidate targets in pathophysiology.

摘要

对与人类单核细胞向巨噬细胞分化以及向M1或M2表型极化相关的基因表达谱进行综合分析,得出以下主要结果:1)M-CSF驱动的单核细胞向巨噬细胞分化与细胞周期基因的激活有关,证实了单核细胞被低估的增殖潜力。2)M-CSF导致M2转录组的很大一部分表达,表明在稳态条件下会发生默认的向M2的转变。3)参与代谢活动的基因的调节是巨噬细胞分化和极化的一个突出特征。4)脂质代谢是调节转录本的主要类别,M1细胞中环氧合酶2预期上调,而M2细胞中环氧合酶1意外上调。5)每个步骤的特征是不同的G蛋白偶联受体库,有五个核苷酸受体作为与M2相关的新基因。6)极化巨噬细胞的趋化因子组差异很大,并报道了新的差异表达趋化因子。因此,转录组分析揭示了与人类单核细胞向巨噬细胞分化和极化激活相关的新分子和特征,这些可能代表病理生理学中的候选靶点。

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