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蛋白质糖基化的表观遗传调控的进化和临床意义。

Evolutional and clinical implications of the epigenetic regulation of protein glycosylation.

出版信息

Clin Epigenetics. 2011 Aug;2(2):425-32. doi: 10.1007/s13148-011-0039-1. Epub 2011 Jun 14.

Abstract

Protein N glycosylation is an ancient posttranslational modification that enriches protein structure and function. The addition of one or more complex oligosaccharides (glycans) to the backbones of the majority of eukaryotic proteins makes the glycoproteome several orders of magnitude more complex than the proteome itself. Contrary to polypeptides, which are defined by a sequence of nucleotides in the corresponding genes, glycan parts of glycoproteins are synthesized by the activity of hundreds of factors forming a complex dynamic network. These are defined by both the DNA sequence and the modes of regulating gene expression levels of all the genes involved in N glycosylation. Due to the absence of a direct genetic template, glycans are particularly versatile and apparently a large part of human variation derives from differences in protein glycosylation. However, composition of the individual glycome is temporally very constant, indicating the existence of stable regulatory mechanisms. Studies of epigenetic mechanisms involved in protein glycosylation are still scarce, but the results suggest that they might not only be important for the maintenance of a particular glycophenotype through cell division and potentially across generations but also for the introduction of changes during the adaptive evolution.

摘要

蛋白质 N 糖基化是一种古老的翻译后修饰,它丰富了蛋白质的结构和功能。在大多数真核蛋白质的骨架上添加一个或多个复杂的寡糖(聚糖),使得糖蛋白组比蛋白质组本身复杂几个数量级。与由相应基因中的核苷酸序列定义的多肽不同,糖蛋白的糖部分是由数百种因子的活性合成的,这些因子形成了一个复杂的动态网络。这些因子不仅由 DNA 序列定义,还由参与 N 糖基化的所有基因的表达水平的调节模式定义。由于缺乏直接的遗传模板,聚糖具有特别大的多样性,显然人类变异的很大一部分来自于蛋白质糖基化的差异。然而,个体糖组的组成在时间上非常稳定,表明存在稳定的调节机制。涉及蛋白质糖基化的表观遗传机制的研究仍然很少,但结果表明,它们不仅对通过细胞分裂和潜在跨代维持特定的糖表型很重要,而且对适应进化过程中的变化也很重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d65b/3365393/75b51864e482/13148_2011_39_Fig1_HTML.jpg

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