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Effect of protein immunogenicity and PEG size and branching on the anti-PEG immune response to PEGylated proteins

文献类型:期刊论文

作者Wan, Xue1,2; Zhang, Juankun1; Yu, Weili2; Shen, Lijuan2; Ji, Shaoyang2; Hu, Tao2
刊名PROCESS BIOCHEMISTRY
出版日期2017
卷号52页码:183-191
关键词Immunogenicity Pegylation Anti-peg Antibody Conjugation
ISSN号1359-5113
DOI10.1016/j.procbio.2016.09.029
文献子类Article
英文摘要

PEGylation has successfully improved the pharmacological properties of therapeutic proteins. However, polyethylene glycol (PEG) has been burdened by immunogenicity that renders a negative clinical effect on therapeutic proteins. The anti-PEG immune response to PEGylated proteins possibly depends on the nature of proteins and the conjugated methoxy PEG (mPEG). Thus, it is necessary to investigate the effects of protein immunogenicity, the extent of PEGylation, the molecular weight (Mw), and the branching of mPEG on the anti-PEG immune response. Ovalbumin, tetanus toxoid cm, TT-TT conjugate, and TT-bovine serum albumin conjugate were used as target proteins. PEGylated proteins with different extents of PEGylation were obtained by fractionation of the PEGylated IT with size exclusion chromatography. The PEGylated proteins with different Mw and branching of mPEG were obtained by modification of TT with linear mPEG (5 kDa and 20 kDa) and branched mPEG (20 kDa). The PEGylated proteins elicited high levels of anti-PEG antibodies (predominantly IgM and IgG1). The anti-PEG immune response depended on the immunogenicity of proteins, the extent of PEGylation, and the Mw of mPEG. In contrast, branching of mPEG had an insignificant effect on the anti-PEG immune response to the PEGylated proteins. (C) 2016 Elsevier Ltd. All rights reserved.

WOS关键词Glycol-modified Proteins ; Polyethylene-glycol ; Accelerated Clearance ; Conjugate Vaccine ; Igm ; Antibodies ; Liposomes ; Linker ; Hypersensitivity ; Pharmacokinetics
WOS研究方向Biochemistry & Molecular Biology ; Biotechnology & Applied Microbiology ; Engineering
语种英语
WOS记录号WOS:000392774600021
资助机构Beijing Natural Science Foundation(7142104) ; National Natural Science Foundation of China(20906095 ; STS Project of Chinese Academy of Sciences(KFJ-EW-STS-027 ; 81402861) ; KFJ-EW-STS-098)
源URL[http://ir.ipe.ac.cn/handle/122111/21892]  
专题过程工程研究所_生化工程国家重点实验室
作者单位1.Tianjin Univ Sci & Technol, Coll Biotechnol, Tianjin 300457, Peoples R China
2.Chinese Acad Sci, Inst Proc Engn, State Key Lab Biochem Engn, Beijing 100190, Peoples R China
推荐引用方式
GB/T 7714
Wan, Xue,Zhang, Juankun,Yu, Weili,et al. Effect of protein immunogenicity and PEG size and branching on the anti-PEG immune response to PEGylated proteins[J]. PROCESS BIOCHEMISTRY,2017,52:183-191.
APA Wan, Xue,Zhang, Juankun,Yu, Weili,Shen, Lijuan,Ji, Shaoyang,&Hu, Tao.(2017).Effect of protein immunogenicity and PEG size and branching on the anti-PEG immune response to PEGylated proteins.PROCESS BIOCHEMISTRY,52,183-191.
MLA Wan, Xue,et al."Effect of protein immunogenicity and PEG size and branching on the anti-PEG immune response to PEGylated proteins".PROCESS BIOCHEMISTRY 52(2017):183-191.

入库方式: OAI收割

来源:过程工程研究所

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