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首页> 外文期刊>New biotechnology >Substrate specificity and transfucosylation activity of GH29 alpha-L-fucosidases for enzymatic production of human milk oligosaccharides
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Substrate specificity and transfucosylation activity of GH29 alpha-L-fucosidases for enzymatic production of human milk oligosaccharides

机译:GH29α-L-岩藻糖苷酶的底物特异性和转乳溶胶化活性,用于酶促生产人乳寡糖

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Human milk oligosaccharides (HMOs) constitute a unique family of bioactive lactose-based molecules present in human breast milk. HMOs are of major importance for infant health and development but also virtually absent from bovine milk used for infant formula. Among the HMOs, the fucosylated species are the most abundant. Transfucosylation catalysed by retaining alpha-L-fucosidases is a new route for manufacturing biomimetic HMOs. Seven alpha-L-fucosidases from glycosyl hydrolase family 29 were expressed, characterized in terms of substrate specificity and thermal stability, and shown to be able to catalyse transfucosylation. The alpha-L-1,3/4-fucosidase CpAfc2 from Clostridium perfringens efficiently catalysed the formation of the more complex human milk oligosaccharide structure lacto-N-fucopentaose II (LNFP II) using 3-fucosyllactose as fucosyl donor and lacto-Ntetraose as acceptor with a 39% yield. alpha-L-Fucosidases FgFCO1 from Fusarium graminearum and Mfuc5 from a soil metagenome were able to catalyse transfucosylation of lactose using citrus xyloglucan as fucosyl donor. FgFCO1 catalysed formation of 2'-fucosyllactose, whereas Mfuc5 catalysis mainly produced an unidentified, non- HMO fucosyllactose, reaching molar yields based on the donor substrate of 14% and 18%, respectively.
机译:人乳寡糖(HMOS)构成了在人母乳中存在的独特的生物活性乳糖基分子。 HMOS对婴儿健康和发展具有重要意义,但实际上缺乏用于婴儿配方奶粉的牛奶。在HMOS中,岩氧化物种是最丰富的物种。通过保留α-L-岩藻糖苷酶催化的转乳囊化是制造仿生HMOS的新途径。表达来自糖基水解酶29的七种α-L-氰化酶,其特征在于底物特异性和热稳定性,并且显示能够催化转乳菌化。来自梭菌的α-1,3 / 4-岩糖苷酶CPAFC2通过3-FUCOSYLLACTONE作为岩藻糖基供体和乳清蛋白酶和乳清蛋白酶和乳清蛋白酶和乳酰基 - Ntetroose,高效地催化了更复杂的人牛奶寡糖结构乳酸-N-粘葡萄球菌II(LNFP II)的形成。受体率为39%。来自Fusarium Gramearum的FGFCO1和来自土壤偏葡聚糖的MFUC5的FGFCO1能够使用柑橘木葡聚糖作为岩氧基供体催化乳糖的转霉区。 FGFCO1催化形成2'-岩氧树脂,而MFuc5催碱主要产生未识别的非HMO岩氧蛋白酶糖糖糖,分别达到14%和18%的供体基材达到摩尔产率。

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