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Immobilization of Neutral Protease from Bacillus subtilis for Regioselective Hydrolysis of Acetylated Nucleosides: Application to Capecitabine Synthesis

机译:固定化枯草芽孢杆菌中性蛋白酶的乙酰化核苷的区域选择性水解:在卡培他滨合成中的应用

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This paper describes the immobilization of the neutral protease from Bacillus subtilis and its application in the regioselective hydrolysis of acetylated nucleosides, including building blocks useful for the preparation of anticancer products. Regarding the immobilization study, different results have been obtained depending on the immobilization procedure. Epoxy hydrophobic carriers gave a poorly stable derivative that released almost 50% of the immobilized protein under the required reaction conditions. On the contrary, covalent immobilization on a differently activated hydrophilic carrier (agarose) resulted in very stable enzyme derivatives. In an attempt to explain the obtained enzyme immobilization results, the hypothetical localization of lysines on the enzyme surface was predicted in a 3D structure model of B. subtilis protease N built in silico by using the structure of Staphylococcus aureus metalloproteinase as the template. The immobilized enzyme shown a high regioselectivity in the hydrolysis of different peracetylated nucleosides. A stable enzyme derivative was obtained and successfully used in the development of efficient preparative bioprocesses for the hydrolysis of acetylated nucleosides, giving new intermediates for the synthesis of capecitabine in high yield. View Full-Text
机译:本文描述了枯草芽孢杆菌中性蛋白酶的固定化及其在乙酰化核苷区域选择性水解中的应用,包括可用于制备抗癌产品的结构单元。关于固定化研究,已根据固定程序获得了不同的结果。环氧疏水性载体产生的稳定性差,在所需的反应条件下释放了近50%的固定蛋白。相反,共价固定在不同活化的亲水性载体(琼脂糖)上会产生非常稳定的酶衍生物。为了解释获得的酶固定化结果,在金黄色葡萄球菌金属蛋白酶结构的计算机模拟的枯草芽孢杆菌蛋白酶N的3D结构模型中,预测了赖氨酸在酶表面的定位。固定的酶在不同的过乙酰化核苷的水解中显示出很高的区域选择性。获得了稳定的酶衍生物,并将其成功用于开发用于乙酰化核苷水解的高效制备生物过程,从而为高产率合成卡培他滨提供了新的中间体。查看全文

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