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首页> 外文期刊>Chemistry: A European journal >Systematic Synthesis of Bisubstrate-Type Inhibitors of N-Acetylglucosaminyltransferases
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Systematic Synthesis of Bisubstrate-Type Inhibitors of N-Acetylglucosaminyltransferases

机译:N-乙酰氨基葡萄糖氨基转移酶双底物型抑制剂的系统合成

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Bisubstrate-type inhibitors for N-acetylglucosaminyltransferase (GnT)-V and -IX were designed and synthesized. These compounds carry both an acceptor trisaccaride and an UDP-GlcNAc component tethered by a linker of variable length. The acceptor trisaccharide unit was constructed using a combination of a polymer support and a resin capture-release strategy. Namely, starting with a beta-manno-side bound to low molecular weight monomethyl PEG (MPEG), successive glycosylations with donors having chloroacetyl group produced the trisaccharide, which was subjected to the capture-release purification using cys-teine loaded resin. UDP-GlcNAc units carrying phosphate moieties were separately synthesized from the bromoace-tamide-containing glucosamine derivative. Ligation between the acceptor thiol and each alkyl bromide on the donor unit readily proceeded, and produced the coupling product. The introduction of the UMP component gave target compounds. All of the synthesized compounds had significant activities to GnT-V and -IX. Their potencies were dependent upon the linkers length. GnT-IX was more sensitive to these inhibitors and optimum linker length was clearly different between these GnTs. The most potent inhibitor of GnT-V had K_i = 18.3 muM, while that of GnT-IX had K_i = 4.7 muM.
机译:设计并合成了双底物型的N-乙酰氨基葡萄糖氨基转移酶(GnT)-V和-IX抑制剂。这些化合物既带有受体三糖苷,又带有由可变长度的连接子束缚的UDP-GlcNAc组分。受体三糖单元使用聚合物载体和树脂捕获-释放策略的组合构建。即,从与低分子量单甲基PEG(MPEG)结合的β-甘露糖苷侧开始,与具有氯乙酰基的供体相继糖基化产生了三糖,将其用载有半胱氨酸的树脂进行捕获-释放纯化。由含溴代酰胺的葡糖胺衍生物分别合成带有磷酸基团的UDP-GlcNAc单元。受体硫醇与供体单元上的每个烷基溴之间的连接容易进行,并产生偶联产物。引入UMP组分得到目标化合物。所有合成的化合物均对GnT-V和-IX具有显着的活性。它们的效力取决于接头的长度。 GnT-IX对这些抑制剂更敏感,并且最佳连接子长度在这些GnT之间明显不同。最有效的GnT-V抑制剂的K_i = 18.3μM,而GnT-IX的抑制剂的K_i = 4.7μM。

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