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转谷氨酰胺酶介导的聚乙二醇化酶纳米包被

Transgultaminase-Mediated Nanoarmoring of Enzymes by PEGylation.

作者信息

Grigoletto Antonella, Mero Anna, Maso Katia, Pasut Gianfranco

机构信息

University of Padua, Padua, Italy.

University of Padua, Padua, Italy.

出版信息

Methods Enzymol. 2017;590:317-346. doi: 10.1016/bs.mie.2017.01.002. Epub 2017 Feb 15.

Abstract

PEGylation, the covalent attachment of polyethylene glycol to bioactive molecules, is one of the leading approaches used to prolong pharmacokinetics, to improve the stability, and to reduce the immunogenicity of therapeutic proteins. PEG-conjugated products are associated with better therapy outcomes and improved patient compliance. Widely applied in clinical practice, the technology is mainly used to modify proteins, peptides, and oligonucleotides but also other drug delivery systems such as the liposomal one. Undergoing continuous attempts to optimize therapeutic efficacy and to tune the formation of conjugates, a number of different PEGylation processes are now available to researchers for protein conjugation. Although the possibility of obtaining highly homogeneous conjugate mixtures, preferably formed by a single monoconjugate, from a chemical conjugation reaction continues to be limited, several enzymatic conjugation approaches have recently been investigated to address this need. PEGylation mediated by microbial transglutaminase and its many advantages and modifications are outlined in detail in the current work permitting interested readers to perform site-specific protein derivatization to glutamines or lysines.

摘要

聚乙二醇化,即将聚乙二醇共价连接到生物活性分子上,是用于延长药代动力学、提高稳定性以及降低治疗性蛋白质免疫原性的主要方法之一。聚乙二醇化产物具有更好的治疗效果并能提高患者的依从性。该技术在临床实践中广泛应用,主要用于修饰蛋白质、肽和寡核苷酸,但也用于其他药物递送系统,如脂质体系统。在不断尝试优化治疗效果并调整缀合物形成的过程中,现在研究人员有多种不同的聚乙二醇化方法用于蛋白质缀合。尽管通过化学缀合反应获得高度均一的缀合物混合物(最好由单一单缀合物形成)的可能性仍然有限,但最近已经研究了几种酶促缀合方法来满足这一需求。当前工作详细概述了微生物转谷氨酰胺酶介导的聚乙二醇化及其诸多优点和改进方法,使感兴趣的读者能够对谷氨酰胺或赖氨酸进行位点特异性蛋白质衍生化。

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