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首页> 外文期刊>Biomacromolecules >Carrier-Free Immobilization of Lipase from Candida rugosa with Polyethyleneimines by Carboxyl-Activated Cross-Linking
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Carrier-Free Immobilization of Lipase from Candida rugosa with Polyethyleneimines by Carboxyl-Activated Cross-Linking

机译:通过羧基激活的交联从Candida Rugosa与Candida Rugosa的脂肪酶固定的载体固定化

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摘要

Carrier-free immobilization of Candida rugosa lipase (CRL) and polymers containing primary amino groups were cross-linked using carbodiimide. To accomplish this, the free carboxyl groups of the enzyme were activated with carbodiirnide-succinimide in organic medium, and then the activated proteins were cross-linked with different polyethyle- nimines (PEIs). The effect of the cross-linker chain length, the amount of added bovine serum albumin (BSA), and carbodiimide concentration on the catalytic properties of resulting cross-linked enzyme aggregates (CLEAs) was investigated. The CLEAs' size, shape, specific activity, activity recovery, thermostability and enantioselectivity significantly varied according to the preparation procedure. The highest thermostable CRL-CLEA preparation was obtained with 1.3 kDa polyefhyleneimine as cross-linker, 10 mg of BSA and 28 mM of carbodiimide. This preparation is 1.3-fold more active and thermostable than CLEAs prepared by the traditional method of amino cross-linking with glutaraldehyde, and retains 60% of residual activity after 22 h at 50 °C. Additionally, the CRL-CLEA preparation showed an enantioselectivity of 91% enantiomeric excess (ee). This immobilization procedure provides an alternative strategy for CLEA production, particularly for enzymes where the traditional method of cross-linking via lysine residues leads to enzyme inactivation.
机译:使用碳二酰亚胺交联,无载念珠菌脂肪酶(CRL)和含有伯氨基的聚合物的载体固定化。为了实现这一点,在有机培养基中用Carbodirnide-琥珀酰亚胺激活酶的游离羧基,然后用不同的聚乙烯(PEI)与活化的蛋白质交联。还研究了交联链链长度,添加的牛血清白蛋白(BSA)的量的效果,以及所得交联酶聚集体(CLEA)的催化性质上的碳二亚胺浓度。根据制备程序,CleA'的尺寸,形状,特异性活性,活性回收,热稳定性和对映选择性显着变化。用1.3kDa聚亚胺作为交联剂,10mg BSA和28mM的碳二亚胺,得到最高的热稳定CRL-CLEA制剂。该制剂比通过与戊二醛的传统交联方法制备的甜菜制备的含量更活跃和热稳定,并在50℃下保留22小时后的60%的残余活性。另外,CRL-CLEA制剂显示出91%映体过量(EE)的对映选择性。该固定化程序为CLEA生产提供了一种替代策略,特别是对于通过赖氨酸残基交联的传统方法的酶导致酶灭活。

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  • 来源
    《Biomacromolecules》 |2014年第5期|共8页
  • 作者单位

    Departamento de Biotecnologia Universidad Autonoma Metropolitana Iztapalapa Avenida San Rafael Atlixco #186 Col. Vicentina 09340 Distrito Federal Mexico;

    Biofunctional Nanomaterials unit CIC Biomagune Parque tecnologico de San Sebastian Edificio Empresarial "C" Paseo Miramon 182 20009 Donostia-San Sebastian Guipuzcoa Spain;

    Centro de Nanociencias y Nanotecnologfa UNAM Ensenada Baja California 22780 Mexico;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
  • 关键词

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