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Crosslinked enzyme aggregates in hierarchically-ordered mesoporous silica: A simple and effective method for enzyme stabilization

✍ Scribed by Moon Il Kim; Jungbae Kim; Jinwoo Lee; Hongfei Jia; Hyon Bin Na; Jong Kyu Youn; Ja Hun Kwak; Alice Dohnalkova; Jay W. Grate; Ping Wang; Taeghwan Hyeon; Hyun Gyu Park; Ho Nam Chang


Publisher
John Wiley and Sons
Year
2007
Tongue
English
Weight
341 KB
Volume
96
Category
Article
ISSN
0006-3592

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✦ Synopsis


Abstract

α‐chymotrypsin (CT) and lipase (LP) were immobilized in hierarchically‐ordered mesocellular mesoporous silica (HMMS) in a simple but effective way for the enzyme stabilization, which was achieved by the enzyme adsorption followed by glutaraldehyde (GA) crosslinking. This resulted in the formation of nanometer scale crosslinked enzyme aggregates (CLEAs) entrapped in the mesocellular pores of HMMS (37 nm), which did not leach out of HMMS through narrow mesoporous channels (13 nm). CLEA of α‐chymotrypsin (CLEA‐CT) in HMMS showed a high enzyme loading capacity and significantly increased enzyme stability. No activity decrease of CLEA‐CT was observed for 2 weeks under even rigorously shaking condition, while adsorbed CT in HMMS and free CT showed a rapid inactivation due to the enzyme leaching and presumably autolysis, respectively. With the CLEA‐CT in HMMS, however, there was no tryptic digestion observed suggesting that the CLEA‐CT is not susceptible to autolysis. Moreover, CLEA of lipase (CLEA‐LP) in HMMS retained 30% specific activity of free lipase with greatly enhanced stability. This work demonstrates that HMMS can be efficiently employed as host materials for enzyme immobilization leading to highly enhanced stability of the immobilized enzymes with high enzyme loading and activity. Biotechnol. Bioeng. 2007;96: 210–218. © 2006 Wiley Periodicals, Inc.


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