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Metabolic Glycoengineering with N-Acyl Side Chain Modified Mannosamines

机译:N-酰基侧链修饰甘露糖胺的代谢糖工程

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摘要

In metabolic glycoengineering (MGE), cells or animals are treated with unnatural derivatives of monosaccharides. After entering the cytosol, these sugar analogues are metabolized and subsequently expressed on newly synthesized glycoconjugates. The feasibility of MGE was first discovered for sialylated glycans, by using N-acyl-modified mannosamines as precursor molecules for unnatural sialic acids. Prerequisite is the promiscuity of the enzymes of the Roseman-Warren biosynthetic pathway. These enzymes were shown to tolerate specific modifications of the N-acyl side chain of mannosamine analogues, for example, elongation by one or more methylene groups (aliphatic modifications) or by insertion of reactive groups (bioorthogonal modifications). Unnatural sialic acids are incorporated into glycoconjugates of cells and organs. MGE has intriguing biological consequences for treated cells (aliphatic MGE) and offers the opportunity to visualize the topography and dynamics of sialylated glycans in vitro, ex vivo, and in vivo (bioorthogonal MGE).
机译:在代谢糖工程(MGE)中,用单糖的非天然衍生物治疗细胞或动物。进入胞质溶胶后,这些糖类似物被代谢并随后在新合成的糖缀合物上表达。通过使用N-酰基修饰的甘露糖胺作为非天然唾液酸的前体分子,首次发现了MGE对于唾液酸化聚糖的可行性。前提是Roseman-Warren生物合成途径中酶的混杂。这些酶显示出可耐受甘露糖胺类似物的N-酰基侧链的特定修饰,例如,被一个或多个亚甲基延长(脂族修饰)或被插入反应性基团(生物正交修饰)。非天然唾液酸被掺入细胞和器官的糖缀合物中。 MGE对处理过的细胞(脂族MGE)具有令人感兴趣的生物学影响,并提供了机会在体外,离体和体内可视化唾液酸化聚糖的形貌和动力学(生物正交MGE)。

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