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Engineering the Acceptor Specificity of Trehalose Phosphorylase for the Production of Trehalose Analogs

机译:设计用于生产海藻糖类似物的海藻糖磷酸化酶的受体特异性

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Trehalose (α-D-glucopyranosyl-(1,1 )-α-D-glucopyranoside) is widely used in the food industry, thanks to its protective effect against freezing and dehydration. Analogs of trehalose have the additional benefit that they are not digested and thus do not contribute to our caloric intake. Such trehalose analogs can be produced with the enzyme trehalose phosphorylase, when it is applied in the reverse, synthetic mode. Despite the enzyme's broad acceptor specificity, its catalytic efficiency for alternative monosaccharides is much lower than for glucose. For galactose, this difference is shown here to be caused by a lower K_m whereas the k_(cat) for both substrates is equal. Consequently, increasing the affinity was attempted by enzyme engineering of the trehalose phosphorylase from Thermoanaerobacter brockii, using both semirational and random mutagenesis. While a semirational approach proved unsuccessful, high-throughput screening of an error-prone PCR library resulted in the discovery of three beneficial mutations that lowered K_m two- to three-fold. In addition, it was found that mutation of these positions also leads to an improved catalytic efficiency for mannose and fructose, suggesting their involvement in acceptor promiscuity. Combining the beneficial mutations did not further improve the affinity, and even resulted in a decreased catalytic activity and thermostability. Therefore, enzyme variant R448S is proposed as new biocatalyst for the industrial production of lactotrehalose (α-D-glucopyranosyl-(1 ,1 )-α-D-gal-actopyranoside).
机译:海藻糖(α-D-吡喃葡糖基-(1,1)-α-D-吡喃葡糖苷)具有防冻和防脱水作用,因此在食品工业中得到了广泛的应用。海藻糖类似物的另一个好处是不会被消化,因此不会增加我们的热量摄入。当将海藻糖磷酸化酶以相反的合成方式应用时,可以用海藻糖磷酸化酶产生这种海藻糖类似物。尽管该酶具有广泛的受体特异性,但其对替代单糖的催化效率远低于对葡萄糖的催化效率。对于半乳糖,此处的差异是由较低的K_m引起的,而两种底物的k_(cat)相等。因此,使用半理性诱变和随机诱变通过来自布氏嗜热厌氧杆菌的海藻糖磷酸化酶的酶工程化,试图增加亲和力。尽管半定量方法证明是不成功的,但对容易出错的PCR文库的高通量筛选导致发现了三个有益的突变,这些突变将K_m降低了2至3倍。另外,发现这些位置的突变还导致对甘露糖和果糖的催化效率提高,表明它们参与了受体的混杂。组合有益突变并不能进一步改善亲和力,甚至导致催化活性和热稳定性降低。因此,提出了酶变体R448S作为乳果糖(α-D-吡喃葡萄糖基-(1,1)-α-D-gal-乙酰基吡喃糖苷)的工业生产的新生物催化剂。

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