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人类细胞表面糖蛋白动力学的定量研究。

Quantitative investigation of human cell surface -glycoprotein dynamics.

作者信息

Xiao Haopeng, Wu Ronghu

机构信息

School of Chemistry and Biochemistry , The Petit Institute for Bioengineering and Bioscience , Georgia Institute of Technology , Atlanta , Georgia 30332 , USA . Email:

出版信息

Chem Sci. 2017 Jan 1;8(1):268-277. doi: 10.1039/c6sc01814a. Epub 2016 Aug 15.

Abstract

Surface glycoproteins regulate nearly every extracellular event and they are dynamic for cells to adapt to the ever-changing extracellular environment. These glycoproteins contain a wealth of information on cellular development and disease states, and have significant biomedical implications. Systematic investigation of surface glycoproteins will result in a better understanding of surface protein functions, cellular activities and the molecular mechanisms of disease. However, it is extraordinarily challenging to specifically and globally analyze surface glycoproteins. Here we designed the first method to systematically analyze surface glycoprotein dynamics and measure their half-lives by integrating pulse-chase labeling, selective enrichment of surface glycoproteins, and multiplexed proteomics. The current results clearly demonstrated that surface glycoproteins with catalytic activities were more stable than those with binding and receptor activities. Glycosylation sites located outside of any domain had a notably longer median half-life than those within domains, which strongly suggests that glycans within domains regulate protein interactions with other molecules while those outside of domains mainly play a role in protecting the protein from degradation. This method can be extensively applied to biological and biomedical research.

摘要

表面糖蛋白几乎调控着每一个细胞外事件,并且它们对于细胞适应不断变化的细胞外环境而言是动态变化的。这些糖蛋白包含了大量有关细胞发育和疾病状态的信息,并且具有重要的生物医学意义。对表面糖蛋白进行系统研究将有助于更好地理解表面蛋白功能、细胞活动以及疾病的分子机制。然而,特异性和全面性地分析表面糖蛋白极具挑战性。在此,我们设计了第一种方法,通过整合脉冲追踪标记、表面糖蛋白的选择性富集和多重蛋白质组学来系统地分析表面糖蛋白动力学并测量它们的半衰期。目前的结果清楚地表明,具有催化活性的表面糖蛋白比具有结合和受体活性的表面糖蛋白更稳定。位于任何结构域之外的糖基化位点的中位半衰期明显长于结构域内的糖基化位点,这强烈表明结构域内的聚糖调节蛋白质与其他分子的相互作用,而结构域外的聚糖主要在保护蛋白质不被降解方面发挥作用。该方法可广泛应用于生物学和生物医学研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d4f2/5458730/988a6e75b2d4/c6sc01814a-f1.jpg

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