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通过与MHC I类相关受体FcRn可视化IgG回收的位点和动力学。

Visualizing the site and dynamics of IgG salvage by the MHC class I-related receptor, FcRn.

作者信息

Ober Raimund J, Martinez Cruz, Vaccaro Carlos, Zhou Jinchun, Ward E Sally

机构信息

Cancer Immunobiology Center and Center for Immunology, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.

出版信息

J Immunol. 2004 Feb 15;172(4):2021-9. doi: 10.4049/jimmunol.172.4.2021.

Abstract

The MHC class I-related receptor, FcRn, plays a central role in regulating the serum levels of IgG. FcRn is expressed in endothelial cells, suggesting that these cells may be involved in maintaining IgG levels. We have used live cell imaging of FcRn-green fluorescent protein transfected human endothelial cells to analyze the intracellular events that control IgG homeostasis. We show that segregation of FcRn-IgG complexes from unbound IgG occurs in the sorting endosome. FcRn or FcRn-IgG complexes are gradually depleted from sorting endosomes to ultimately generate multivesicular bodies whose contents are destined for lysosomal degradation. In addition, the pathways taken by FcRn and the transferrin receptor overlap, despite distinct mechanisms of ligand uptake. The studies provide a dynamic view of the trafficking of FcRn and its ligand and have relevance to understanding how FcRn functions to maintain IgG homeostasis.

摘要

与MHC I类相关的受体FcRn在调节IgG的血清水平中起核心作用。FcRn在内皮细胞中表达,这表明这些细胞可能参与维持IgG水平。我们利用转染了FcRn-绿色荧光蛋白的人内皮细胞进行活细胞成像,以分析控制IgG稳态的细胞内事件。我们发现,FcRn-IgG复合物与未结合的IgG在分拣内体中发生分离。FcRn或FcRn-IgG复合物从分拣内体中逐渐耗尽,最终产生多囊泡体,其内容物将被溶酶体降解。此外,尽管FcRn和转铁蛋白受体摄取配体的机制不同,但它们所采用的途径存在重叠。这些研究提供了FcRn及其配体运输的动态视图,对于理解FcRn如何维持IgG稳态具有重要意义。

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