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O-聚糖酶促合成对T细胞转运的调控

Regulation of T Cell Trafficking by Enzymatic Synthesis of O-Glycans.

作者信息

Hobbs Samuel J, Nolz Jeffrey C

机构信息

Department of Molecular Microbiology and Immunology, Oregon Health and Science University, Portland, OR, United States.

Department of Cell, Developmental and Cancer Biology, Oregon Health and Science University, Portland, OR, United States.

出版信息

Front Immunol. 2017 May 24;8:600. doi: 10.3389/fimmu.2017.00600. eCollection 2017.

Abstract

Selectins constitute a family of oligosaccharide binding proteins that play critical roles in regulating the trafficking of leukocytes. In T cells, L-selectin (CD62L) controls the capacity for naive and memory T cells to actively survey peripheral lymph nodes, whereas P- and E-selectin capture activated T cells on inflamed vascular endothelium to initiate extravasation into non-lymphoid tissues. The capacity for T cells to interact with all of these selectins is dependent on the enzymatic synthesis of complex O-glycans, and thus, this protein modification plays an indispensable role in regulating the distribution and homing of both naive and previously activated T cells . In contrast to neutrophils, O-glycan synthesis is highly dynamic in T cell populations and is largely controlled by extracellular stimuli such as antigen recognition or signaling though cytokine receptors. Herein, we review the basic principles of enzymatic synthesis of complex O-glycans, discuss tools and reagents for studying this type of protein modification and highlight our current understanding of how O-glycan synthesis is regulated and subsequently impacts the trafficking potential of diverse T cell populations.

摘要

选择素构成了一类寡糖结合蛋白家族,在调节白细胞运输中发挥关键作用。在T细胞中,L-选择素(CD62L)控制着幼稚和记忆T细胞积极巡视外周淋巴结的能力,而P-选择素和E-选择素则在炎症血管内皮上捕获活化的T细胞,以启动向非淋巴组织的外渗。T细胞与所有这些选择素相互作用的能力取决于复杂O-聚糖的酶促合成因此,这种蛋白质修饰在调节幼稚和先前活化T细胞的分布和归巢中起着不可或缺的作用。与中性粒细胞不同,O-聚糖合成在T细胞群体中高度动态,并且在很大程度上受细胞外刺激(如抗原识别或通过细胞因子受体的信号传导)控制。在此,我们综述复杂O-聚糖酶促合成的基本原理,讨论用于研究此类蛋白质修饰的工具和试剂,并强调我们目前对O-聚糖合成如何被调节以及随后如何影响不同T细胞群体运输潜力的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3898/5442166/599ebc570f99/fimmu-08-00600-g001.jpg

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