Affiliation:
1. The Key Laboratory of Synthetic and Biological Colloids, School of Chemical and Material Engineering, Jiangnan University, Ministry
of Education, Wuxi, 214122, P.R. China
2. Research Center for Chemistry, Indonesian Institute of Sciences (LIPI), Kawasan
Puspiptek, Serpong, 15314, Indonesia
Abstract
Abstract:
Immobilized lipase has played an essential role in the chemical and biological sciences
as a viable alternative to standard chemical catalysts. Glutaraldehyde is a low-cost
crosslinking agent at risk of being superseded by developing crosslinking compounds with
biocompatible, biodegradable, and non-toxic characteristics. The multipoint covalent treatment
method using glutaraldehyde has both advantages and disadvantages. Immobilization
techniques can be improved to improve the overall performance of immobilized lipase. The
most recent update on lipase immobilization with multipoint covalent treatment by glutaraldehyde
was summarized in this review. Covalent binding lipase on pre-activated support and
aggregation-crosslinking lipase into crosslinked enzyme aggregates (CLEAs) or adsorptioncrosslinking
lipase on support are the most common immobilization techniques. Based on the
above technologies, the advancement trends in important domains, such as the advancement of supports, additives,
reactors, and cross-linking agents, are summarized. In addition, the application of the improved immobilized lipase
by glutaraldehyde in the production of fatty acids, glycerides, biodiesel, and drug precursors was reviewed. In view
of this, we put forward further studies on multipoint covalent treatment in lipase immobilization with glutaraldehyde.
Various analytical methods are required to provide additional information about the structure of glutaraldehyde
and its crosslinked products for assisting the proper immobilization conditions. Applying the composite strategy
can also bring new opportunities for improving the efficiency of biological catalysts.
Publisher
Bentham Science Publishers Ltd.
Cited by
5 articles.
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