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Dynamic Buffering of Extracellular Chemokine by a Dedicated Scavenger Pathway Enables Robust Adaptation during Directed Tissue Migration

机译:专用清除途径的细胞外趋化因子的动态缓冲使得在定向组织迁移期间能够鲁棒适应

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摘要

How tissues migrate robustly through changing guidance landscapes is poorly understood. Here, quantitative imaging is combined with inducible perturbation experiments to investigate the mechanisms that ensure robust tissue migration in vivo. We show that tissues exposed to acute "chemokine floods'' halt transiently before they perfectly adapt, i.e., return to the baseline migration behavior in the continued presence of elevated chemokine levels. A chemokine-triggered phosphorylation of the atypical chemokine receptor Cxcr7b reroutes it from constitutive ubiquitination-regulated degradation to plasma membrane recycling, thus coupling scavenging capacity to extracellular chemokine levels. Finally, tissues expressing phosphorylation-deficient Cxcr7b migrate normally in the presence of physiological chemokine levels but show delayed recovery when challenged with elevated chemokine concentrations. This work establishes that adaptation to chemokine fluctuations can be "outsourced'' from canonical GPCR signaling to an autonomously acting scavenger receptor that both senses and dynamically buffers chemokine levels to increase the robustness of tissue migration.
机译:如何通过更改的指导景观来恢复组织是如何理解的。这里,定量成像与诱导型扰动实验结合,以研究确保体内稳健的组织迁移的机制。我们表明,在完全适应的情况下,瞬时暴露于急性“趋化因子洪水”的组织,即,恢复到升高的趋化因子水平持续存在下的基线迁移行为。非典型趋化因子受体CXCR7B的趋化因子触发磷酸化重新排除组成型泛素泛素循环降解到血浆膜再循环,从而偶联清除容量对细胞外趋化因子水平。最后,在生理趋化因子水平的存在下,表达磷酸化缺陷型CXCR7B的组织通常在挑战趋化因子浓度时显示出延迟恢复。这项工作建立了对趋化因子波动的适应可以是从规范GPCR信号传导到自主作用的清除剂受体中的“外包”,即感化和动态缓冲趋化水平以增加组织迁移的鲁棒性。

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  • 来源
    《Developmental cell》 |2020年第4期|共27页
  • 作者单位

    Univ Zurich Dept Mol Life Sci Winterthurerstr 190 CH-8057 Zurich Switzerland;

    European Mol Biol Lab Cell Biol &

    Biophys Unit Meyerhofstr 1 D-69117 Heidelberg Germany;

    European Mol Biol Lab Cell Biol &

    Biophys Unit Meyerhofstr 1 D-69117 Heidelberg Germany;

    European Mol Biol Lab Struct &

    Computat Biol Unit Meyerhofstr 1 D-69117 Heidelberg Germany;

    Luxendo GmbH Kurfursten Anlage 58 D-69115 Heidelberg Germany;

    European Mol Biol Lab Electron Microscopy Core Facil Meyerhofstr 1 D-69117 Heidelberg Germany;

    European Mol Biol Lab Cell Biol &

    Biophys Unit Meyerhofstr 1 D-69117 Heidelberg Germany;

    European Mol Biol Lab Cell Biol &

    Biophys Unit Meyerhofstr 1 D-69117 Heidelberg Germany;

    European Mol Biol Lab Struct &

    Computat Biol Unit Meyerhofstr 1 D-69117 Heidelberg Germany;

    Univ Zurich Dept Mol Life Sci Winterthurerstr 190 CH-8057 Zurich Switzerland;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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