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本文引用的文献

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Chemoenzymatic synthesis of C8-modified sialic acids and related α2-3- and α2-6-linked sialosides.C8 修饰的唾液酸及其相关的 α2-3-和 α2-6-连接的唾液糖的酶促化学合成。
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Human xeno-autoantibodies against a non-human sialic acid serve as novel serum biomarkers and immunotherapeutics in cancer.人抗非人类唾液酸自身抗体可作为癌症的新型血清生物标志物和免疫疗法。
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Shotgun glycomics: a microarray strategy for functional glycomics. shotgun 糖组学:一种功能糖组学的微阵列策略。
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Novel anti-carbohydrate antibodies reveal the cooperative function of sulfated N- and O-glycans in lymphocyte homing.新型抗碳水化合物抗体揭示了硫酸化 N- 和 O-聚糖在淋巴细胞归巢中的协同功能。
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Use of glycan microarrays to explore specificity of glycan-binding proteins.使用聚糖微阵列来探索聚糖结合蛋白的特异性。
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Innate immune lectins kill bacteria expressing blood group antigen.天然免疫凝集素可杀死表达血型抗原的细菌。
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Comparative distribution of human and avian type sialic acid influenza receptors in the pig.猪中人类和禽源唾液酸流感受体的比较分布。
BMC Vet Res. 2010 Jan 27;6:4. doi: 10.1186/1746-6148-6-4.
8
Sialidase substrate specificity studies using chemoenzymatically synthesized sialosides containing C5-modified sialic acids.使用化学酶合成的含有 C5 修饰的唾液酸的唾液酸苷研究唾液酸酶的底物特异性。
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Advances in the biology and chemistry of sialic acids.唾液酸的生物学和化学研究进展。
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How bacterial carbohydrates influence the adaptive immune system.细菌碳水化合物如何影响适应性免疫系统。
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唾液酸化聚糖微阵列揭示了修饰的唾液酸与蛋白质和病毒的新型相互作用。

A sialylated glycan microarray reveals novel interactions of modified sialic acids with proteins and viruses.

机构信息

Department of Biochemistry and the Glycomics Center, Emory University School of Medicine, Atlanta, Georgia 30322, USA.

出版信息

J Biol Chem. 2011 Sep 9;286(36):31610-22. doi: 10.1074/jbc.M111.274217. Epub 2011 Jul 12.

DOI:10.1074/jbc.M111.274217
PMID:21757734
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3173124/
Abstract

Many glycan-binding proteins in animals and pathogens recognize sialic acid or its modified forms, but their molecular recognition is poorly understood. Here we describe studies on sialic acid recognition using a novel sialylated glycan microarray containing modified sialic acids presented on different glycan backbones. Glycans terminating in β-linked galactose at the non-reducing end and with an alkylamine-containing fluorophore at the reducing end were sialylated by a one-pot three-enzyme system to generate α2-3- and α2-6-linked sialyl glycans with 16 modified sialic acids. The resulting 77 sialyl glycans were purified and quantified, characterized by mass spectrometry, covalently printed on activated slides, and interrogated with a number of key sialic acid-binding proteins and viruses. Sialic acid recognition by the sialic acid-binding lectins Sambucus nigra agglutinin and Maackia amurensis lectin-I, which are routinely used for detecting α2-6- and α2-3-linked sialic acids, are affected by sialic acid modifications, and both lectins bind glycans terminating with 2-keto-3-deoxy-D-glycero-D-galactonononic acid (Kdn) and Kdn derivatives stronger than the derivatives of more common N-acetylneuraminic acid (Neu5Ac) and N-glycolylneuraminic acid (Neu5Gc). Three human parainfluenza viruses bind to glycans terminating with Neu5Ac or Neu5Gc and some of their derivatives but not to Kdn and its derivatives. Influenza A virus also does not bind glycans terminating in Kdn or Kdn derivatives. An especially novel aspect of human influenza A virus binding is its ability to equivalently recognize glycans terminated with either α2-6-linked Neu5Ac9Lt or α2-6-linked Neu5Ac. Our results demonstrate the utility of this sialylated glycan microarray to investigate the biological importance of modified sialic acids in protein-glycan interactions.

摘要

许多动物和病原体中的糖结合蛋白识别唾液酸或其修饰形式,但它们的分子识别机制仍不清楚。在这里,我们使用一种新型的含有不同糖链骨架上呈现的修饰型唾液酸的唾液酸化聚糖微阵列,描述了对唾液酸识别的研究。在非还原端具有β-连接的半乳糖且在还原端具有含烷基胺荧光团的糖,通过一锅三步酶系统被唾液酸化,生成具有 16 种修饰型唾液酸的α2-3-和α2-6-连接的唾液酰化聚糖。所得的 77 种唾液酰化聚糖被纯化和定量,通过质谱法进行表征,共价打印在活化的载玻片上,并与多种关键的唾液酸结合蛋白和病毒进行检测。唾液酸结合凝集素 Sambucus nigra agglutinin 和 Maackia amurensis lectin-I 对α2-6-和α2-3-连接的唾液酸的常规检测受到唾液酸修饰的影响,这两种凝集素都与以 2-酮-3-脱氧-D-甘油-D-半乳糖酸(Kdn)和 Kdn 衍生物结尾的聚糖结合,其结合强度强于更常见的 N-乙酰神经氨酸(Neu5Ac)和 N-羟乙酰神经氨酸(Neu5Gc)的衍生物。三种人类副流感病毒与以 Neu5Ac 或 Neu5Gc 及其某些衍生物结尾的聚糖结合,但不与 Kdn 及其衍生物结合。流感 A 病毒也不与以 Kdn 或 Kdn 衍生物结尾的聚糖结合。人类流感 A 病毒结合的一个特别新颖的方面是其能够等效地识别以α2-6-连接的 Neu5Ac9Lt 或α2-6-连接的 Neu5Ac 结尾的聚糖。我们的结果表明,这种唾液酸化聚糖微阵列可用于研究修饰型唾液酸在蛋白-聚糖相互作用中的生物学重要性。