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首页> 外文期刊>Molecular biology of the cell >Neutrophils as sources of dinucleotide polyphosphates and metabolism by epithelial ENPP1 to influence barrier function via adenosine signaling
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Neutrophils as sources of dinucleotide polyphosphates and metabolism by epithelial ENPP1 to influence barrier function via adenosine signaling

机译:中性粒细胞作为二核苷酸多磷酸盐的来源和通过上皮ENPP1来通过腺苷信号传导影响屏障功能

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摘要

Extracellular adenosine signaling is established as a protective component in mucosal inflammatory responses. The sources of extracellular adenosine include enzymatic processing from nucleotides, such as ATP and AMP, that can be liberated from a variety of cell types, including infiltrating leukocytes. Here we demonstrate that activated human neutrophils are a source of diadenosine triphosphate (Ap3A), providing an additional source of nucleotides during inflammation. Profiling murine enteroids and intestinal epithelial cell lines revealed that intestinal epithelia prominently express apical and lateral ectonucleotide pyrophosphatase/phosphodiesterase-1 (ENPP1), a member of the ENPP family of enzymes that metabolize diadenosine phosphates, especially Ap3A. Extensions of these studies demonstrated that intestinal epithelia metabolize Ap3A to ADP and AMP, which are further metabolized to adenosine and made available to activate surface adenosine receptors. Using loss and gain of ENPP1 approaches, we revealed that ENPP1 coordinates epithelial barrier formation and promotes epithelial wound healing responses. These studies demonstrate the cooperative metabolism between Ap3A and ENPP1 function to provide a significant source of adenosine, subserving its role in inflammatory resolution.
机译:细胞外腺苷信号在粘膜炎炎症反应中建立为保护组分。细胞外腺苷的来源包括来自核苷酸的酶促加工,例如ATP和AMP,可从各种细胞类型中释放,包括渗透白细胞。在这里,我们证明活化的人性化学粒细胞是三磷酸三磷酸(AP3A)的源,在炎症期间提供额外的核苷酸源。分析鼠进入毒素和肠上皮细胞系显示肠上皮细胞突出地表达顶端和横向异核苷酸焦磷酸酶/磷酸二酯酶-1(ENPP1),eNPP系列酶的成员代谢磷酸磷酸酯,特别是AP3A。这些研究的扩展证明,肠上皮酶代谢AP3A至ADP和AMP,其进一步代谢为腺苷并可用于活化表面腺苷受体。使用损失和enpp1方法的增益,我们透露enpp1坐标坐标形成上皮屏障形成,促进上皮伤口愈合反应。这些研究证明了AP3A和ENPP1功能之间的合作代谢,以提供腺苷的重要来源,从而为炎症分辨率中的作用。

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  • 来源
    《Molecular biology of the cell》 |2018年第22期|共13页
  • 作者

    Curtis Valerie F.; Cartwright Ian M.; Lee J. Scott; Wang Ruth X.; Kao Daniel J.; Lanis Jordi M.; Burney Krista M.; Welch Nichole; Hall Caroline H. T.; Goldberg Matthew S.; Campbell Eric L.; Colgan Sean P.;

  • 作者单位

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

    Univ Colorado Mucosal Inflammat Program Anschutz Med Campus Aurora CO 80045 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
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