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在肾、肺和肝中成像炎症性白细胞募集——对多步骤范式的挑战。

Imaging inflammatory leukocyte recruitment in kidney, lung and liver--challenges to the multi-step paradigm.

机构信息

Department of Medicine, Centre for Inflammatory Diseases, Monash University, Monash Medical Centre, Clayton, Victoria, Australia.

出版信息

Immunol Cell Biol. 2013 Apr;91(4):281-9. doi: 10.1038/icb.2012.83. Epub 2013 Jan 22.

Abstract

Intravital microscopy has been essential in establishing the multi-step paradigm that describes how leukocytes in the bloodstream interact with the blood vessel wall during the process of leukocyte recruitment. Much of this work has been performed in readily-visualized tissues such as the mesentery and the cremaster muscle, where leukocyte-endothelial cell interactions are restricted to postcapillary venules. However, the microvasculatures of the liver, lung and renal glomerulus differ markedly from these conventionally structured microvascular beds. Moreover, the liver, lung and kidney can be the target of life-threatening leukocyte-mediated inflammation. Therefore, a clear understanding of the mechanisms of leukocyte recruitment to these sites is critical. In this review, we examine the advances made in the understanding of leukocyte recruitment in the liver, lung and glomerulus, as determined using intravital microscopy. We describe how leukocyte recruitment to these sites occurs via mechanisms distinct from the conventional rolling/adhesion/transmigration paradigm, and in some cases involves adhesion molecules with minimal roles in conventional postcapillary venules. In addition, we describe how advanced forms of in vivo imaging in combination with novel approaches for labeling immune cell subsets is revealing new complexities in leukocyte function and immune cell interactions in these specialized microvascular beds.

摘要

活体显微镜技术对于建立描述白细胞在血流中如何与血管壁相互作用的多步骤模式至关重要,这个过程是白细胞募集的过程。这项工作主要在肠系膜和提睾肌等易于观察的组织中进行,在这些组织中,白细胞-内皮细胞的相互作用仅限于小静脉后。然而,肝脏、肺部和肾小球的微血管与这些传统结构的微血管床有明显的不同。此外,肝脏、肺部和肾脏可能是危及生命的白细胞介导的炎症的靶器官。因此,清楚地了解白细胞募集到这些部位的机制是至关重要的。在这篇综述中,我们使用活体显微镜检查来研究在理解肝脏、肺部和肾小球中白细胞募集方面取得的进展。我们描述了白细胞如何通过与传统的滚动/黏附/迁移模式不同的机制募集到这些部位,在某些情况下,涉及到在传统的小静脉后黏附分子中作用很小的黏附分子。此外,我们还描述了如何将先进的体内成像形式与新型免疫细胞亚群标记方法相结合,揭示了这些特殊微血管床中白细胞功能和免疫细胞相互作用的新复杂性。

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