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通过一步无模板法形成稳定的有机-无机胶囊对酶进行封装:一种简单高效的固定化酶方法,具有高活性和可循环性。

Encapsulation of enzyme via one-step template-free formation of stable organic-inorganic capsules: A simple and efficient method for immobilizing enzyme with high activity and recyclability.

作者信息

Huang Renliang, Wu Mengyun, Goldman Mark J, Li Zhi

机构信息

Department of Chemical and Biomolecular Engineering, National University of Singapore, 4 Engineering Drive 4, Singapore 117585, Singapore.

出版信息

Biotechnol Bioeng. 2015 Jun;112(6):1092-101. doi: 10.1002/bit.25536. Epub 2015 Apr 17.

DOI:10.1002/bit.25536
PMID:25580912
Abstract

Enzyme encapsulation is a simple, gentle, and general method for immobilizing enzyme, but it often suffers from one or more problems regarding enzyme loading efficiency, enzyme leakage, mechanical stability, and recyclability. Here we report a novel, simple, and efficient method for enzyme encapsulation to overcome these problems by forming stable organic-inorganic hybrid capsules. A new, facile, one-step, and template-free synthesis of organic-inorganic capsules in aqueous phase were developed based on PEI-induced simultaneous interfacial self-assembly of Fmoc-FF and polycondensation of silicate. Addition of an aqueous solution of Fmoc-FF and sodium silicate into an aqueous solution of PEI gave a new class of organic-inorganic hybrid capsules (FPSi) with multi-layered structure in high yield. The capsules are mechanically stable due to the incorporation of inorganic silica. Direct encapsulation of enzyme such as epoxide hydrolase SpEH and BSA along with the formation of the organic-inorganic capsules gave high yield of enzyme-containing capsules (∼1.2 mm in diameter), >90% enzyme loading efficiency, high specific enzyme loading (158 mg protein g(-1) carrier), and low enzyme leakage (<3% after 48 h incubation). FPSi-SpEH capsules catalyzed the hydrolysis of cyclohexene oxide to give (1R, 2R)-cyclohexane-1,2-diol in high yield and concentration, with high specific activity (6.94 U mg(-1) protein) and the same high enantioselectivity as the free enzyme. The immobilized SpEH demonstrated also excellent operational stability and recyclability: retaining 87% productivity after 20 cycles with a total reaction time of 80 h. The new enzyme encapsulation method is efficient, practical, and also better than other reported encapsulation methods.

摘要

酶包封是一种简单、温和且通用的固定化酶方法,但它在酶负载效率、酶泄漏、机械稳定性和可回收性等方面常常存在一个或多个问题。在此,我们报告一种新颖、简单且高效的酶包封方法,通过形成稳定的有机 - 无机杂化胶囊来克服这些问题。基于PEI诱导的Fmoc - FF同时界面自组装和硅酸盐缩聚反应,开发了一种在水相中新型、简便、一步且无模板的有机 - 无机胶囊合成方法。将Fmoc - FF水溶液和硅酸钠加入到PEI水溶液中,可高产率地得到一类具有多层结构的新型有机 - 无机杂化胶囊(FPSi)。由于无机二氧化硅的掺入,这些胶囊具有机械稳定性。将环氧水解酶SpEH和牛血清白蛋白(BSA)等酶直接包封,同时形成有机 - 无机胶囊,可得到高产率的含酶胶囊(直径约1.2毫米),酶负载效率>90%,高比酶负载量(158毫克蛋白质/克载体),且酶泄漏率低(孵育48小时后<3%)。FPSi - SpEH胶囊催化环氧环己烷水解,以高产率和高浓度得到(¹R, ²R)-环己烷 - 1,2 - 二醇,具有高比活性(6.94单位/毫克蛋白质),且对映体选择性与游离酶相同。固定化的SpEH还表现出优异的操作稳定性和可回收性:在20个循环、总反应时间80小时后仍保留87%的生产率。这种新的酶包封方法高效、实用,且优于其他已报道的包封方法。

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