Down-regulation of the forkhead transcription factor Foxp1 is required for monocyte differentiation and macrophage function.

Shi C; Sakuma M; Mooroka T; Liscoe A; Gao H; Croce KJ; Sharma A; Kaplan D; Greaves DR; Wang Y; Simon DI

首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Down-regulation of the forkhead transcription factor Foxp1 is required for monocyte differentiation and macrophage function.

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Down-regulation of the forkhead transcription factor Foxp1 is required for monocyte differentiation and macrophage function.

机译：叉头转录因子Foxp1的下调是单核细胞分化和巨噬细胞功能所必需的。

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Down-regulation of the forkhead transcription factor Foxp1 by integrin engagement controls monocyte differentiation in vitro. To determine whether Foxp1 plays a critical role in monocyte differentiation and macrophage functions in vivo, we generated transgenic mice (macFoxp1tg) overexpressing human FOXP1 in monocyte/macrophage lineage cells using the CD68 promoter. Circulating blood monocytes from macFoxp1tg mice have reduced expression of the receptor for macrophage colony-stimulating factor (c-Fms/M-CSFR), impaired migratory capacity, and diminished accumulation as splenic macrophages. Macrophage functions, including cytokine production, phagocytosis, and respiratory burst were globally impaired in macFoxp1tg compared with wild-type cells. Osteoclastogenesis and bone resorption activity were also attenuated in macFoxp1tg mice. In models of chemical and bacterial peritonitis, macFoxp1tg mice exhibited reduced macrophage accumulation, bacterial clearance, and survival. Enforced overexpression of c-Fms/M-CSFR reversed the cytokine production and phagocytosis defects in macFoxp1tg macrophages, indicating that repression of c-fms/M-CSFR is likely the dominant mechanism responsible for Foxp1 action in monocyte differentiation and macrophage function. Taken together, these observations identify down-regulation of Foxp1 as critical for monocyte differentiation and macrophage functions in vivo.

机译：整联蛋白参与下叉头转录因子Foxp1的下调控制体外单核细胞分化。若要确定Foxp1是否在体内单核细胞分化和巨噬细胞功能中起关键作用，我们使用CD68启动子生成了在单核细胞/巨噬细胞谱系细胞中过表达人FOXP1的转基因小鼠（macFoxp1tg）。来自macFoxp1tg小鼠的循环血单核细胞减少了巨噬细胞集落刺激因子（c-Fms / M-CSFR）受体的表达，迁移能力受损，脾脏巨噬细胞的蓄积减少。与野生型细胞相比，macFoxp1tg中的巨噬细胞功能（包括细胞因子产生，吞噬作用和呼吸爆发）整体受到损害。在macFoxp1tg小鼠中，破骨细胞生成和骨吸收活性也减弱了。在化学和细菌性腹膜炎模型中，macFoxp1tg小鼠表现出减少的巨噬细胞积累，细菌清除率和存活率。强制c-Fms / M-CSFR的过表达逆转了macFoxp1tg巨噬细胞中的细胞因子产生和吞噬缺陷，这表明c-fms / M-CSFR的抑制可能是导致Foxp1在单核细胞分化和巨噬细胞功能中起作用的主要机制。综上所述，这些观察结果确定Foxp1的下调对于体内单核细胞分化和巨噬细胞功能至关重要。

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《Blood: The Journal of the American Society of Hematology》 |2008年第12期|共13页
作者
Shi C; Sakuma M; Mooroka T; Liscoe A; Gao H; Croce KJ; Sharma A; Kaplan D; Greaves DR; Wang Y; Simon DI;
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正文语种 eng
中图分类血液及淋巴系疾病;
关键词
Monocytes; Macrophages; differentiation; Laboratory mice; 单核细胞; 巨噬细胞;

机译：Monocytes;Macrophages;differentiation;Laboratory mice;单核细胞;巨噬细胞;

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专利

1. Down-regulation of the forkhead transcription factor Foxp1 is required for monocyte differentiation and macrophage function. [J] . Shi C, Sakuma M, Mooroka T, Blood: The Journal of the American Society of Hematology . 2008,第12期

机译：叉头转录因子Foxp1的下调是单核细胞分化和巨噬细胞功能所必需的。
2. Differential expression of the TP alpha and TP beta isoforms of the human T Prostanoid receptor during chronic inflammation of the prostate: Role for FOXP1 in the transcriptional regulation of TP beta during monocyte-macrophage differentiation [J] . Mulvaney Eamon P., OSullivan Aine G., Eivers Sarah B., Experimental & Molecular Pathology . 2019,第期

机译：在前列腺慢性炎症期间人T前列腺受体的TPα和TPβ同种型的差异表达：在单核细胞 - 巨噬细胞分化期间对TPβ转录调节的FOXP1的作用
3. Activated T lymphocytes suppress osteoclastogenesis by diverting early monocyte/macrophage progenitor lineage commitment towards dendritic cell differentiation through down-regulation of receptor activator of nuclear factor-kappaB and c-Fos. [J] . Grcevic D, Lukic IK, Kovacic N, Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology . 2006,第1期

机译：活化的T淋巴细胞通过下调核因子-κB和c-Fos受体激活剂的方式使早期单核细胞/巨噬细胞祖细胞谱系转移到树突状细胞分化中，从而抑制破骨细胞生成。
4. Forkhead Transcription Factors: New Targets Of Protein Kinase B (C-Akt) Signalling [C] . Geert J. P. L. Kops and Boudewijn M. Th. Burgering NATO Advanced Study Institute on Molecular Mechanisms of Signal Transduction . 2000

机译：叉头转录因子：蛋白激酶B（C-AKT）信号传导的新靶
5. Macrophage colony stimulating factor-induced differentiation of human cord blood monocytes into IL-10(high)IL-12(absent) dendritic cells with tolerogenic potential and into a rare population of CD16(+) monocytes. [D] . Li, Geling. 2005

机译：巨噬细胞集落刺激因子诱导人脐带血单核细胞分化为具有耐受原性的IL-10（高）IL-12（缺失）树突状细胞和稀有的CD16（+）单核细胞。
6. Phagocytes: Down-regulation of the forkhead transcription factor Foxp1 is required for monocyte differentiation and macrophage function [O] . Can Shi, Masashi Sakuma, Toshifumi Mooroka, -1

机译：吞噬细胞：单核细胞分化和巨噬细胞功能需要前叉转录因子Foxp1的下调
7. Down-regulation of the forkhead transcription factor Foxp1 is required for monocyte differentiation and macrophage function. [O] . Shi, C, Sakuma, M, Mooroka, T, 2008

机译：叉头转录因子Foxp1的下调是单核细胞分化和巨噬细胞功能所必需的。

Down-regulation of the forkhead transcription factor Foxp1 is required for monocyte differentiation and macrophage function.

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