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从肽到蛋白质:空肠弯曲杆菌中N-糖基化底物特异性的比较分析

From peptide to protein: comparative analysis of the substrate specificity of N-linked glycosylation in C. jejuni.

作者信息

Chen Mark M, Glover Kerney Jebrell, Imperiali Barbara

机构信息

Department of Chemistry, Massachusetts Institute of Technology 77 Massachusetts Avenue, Cambridge, Massachusetts 02139, USA.

出版信息

Biochemistry. 2007 May 8;46(18):5579-85. doi: 10.1021/bi602633n. Epub 2007 Apr 17.

Abstract

The gram-negative bacterium Campylobacter jejuni was recently discovered to contain a general N-linked protein glycosylation pathway. Central to this pathway is PglB, a homologue of the Stt3p subunit of the eukaryotic oligosaccharyl transferase (OT), which is involved in the transfer of an oligosaccharide from a polyisoprenyl pyrophosphate carrier to the asparagine side chain of proteins within the conserved glycosylation sites D/E-X1-N-X2-S/T, where X1 and X2 can be any amino acids except proline. Using a library of peptide substrates and a quantitative radioactivity-based in vitro assay, we assessed the amino acids at each position of the consensus glycosylation sequence for their impact on glycosylation efficiency, whereby the sequence DQNAT was found to be the optimal acceptor substrate. In the context of a full-length folded protein, the differences between variations of the glycosylation sequences were found to be consistent with the trends observed from their peptidyl counterparts, though less dramatic because of additional influences. In addition to characterizing the acceptor preferences of PglB, we also assessed the selectivity toward the glycan donor. Interestingly, despite recent reports of relaxed selectivity toward the glycan donor, PglB was not found to be capable of utilizing glycosyl donors such as dolichyl-pyrophosphate-chitobiose, which is the minimum substrate for the eukaryotic OT process.

摘要

最近发现革兰氏阴性菌空肠弯曲杆菌含有一条通用的 N - 连接蛋白糖基化途径。该途径的核心是 PglB,它是真核寡糖基转移酶(OT)的 Stt3p 亚基的同源物,参与将寡糖从聚异戊二烯焦磷酸载体转移到保守糖基化位点 D/E - X1 - N - X2 - S/T 内蛋白质的天冬酰胺侧链上,其中 X1 和 X2 可以是除脯氨酸以外的任何氨基酸。我们使用肽底物文库和基于定量放射性的体外测定方法,评估了共有糖基化序列每个位置的氨基酸对糖基化效率的影响,结果发现序列 DQNAT 是最佳受体底物。在全长折叠蛋白的背景下,发现糖基化序列变体之间的差异与从其肽基对应物观察到的趋势一致,不过由于其他影响,差异不太显著。除了表征 PglB 的受体偏好外,我们还评估了其对聚糖供体的选择性。有趣的是,尽管最近有报道称对聚糖供体的选择性有所放宽,但未发现 PglB 能够利用诸如二萜焦磷酸 - 壳二糖等糖基供体,而二萜焦磷酸 - 壳二糖是真核 OT 过程的最小底物。

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