Product development issues for PEGylated proteins

被引:38
作者
Payne, Robert W. [1 ]
Murphy, Brian M. [1 ]
Manning, Mark Cornell [1 ]
机构
[1] Legacy BioDesign LLC, Johnstown, CO 80534 USA
来源
PHARMACEUTICAL DEVELOPMENT AND TECHNOLOGY | 2011年 / 16卷 / 05期
基金
美国国家卫生研究院;
关键词
Protein stability; pegylation; development; chemical modification; SITE-SPECIFIC PEGYLATION; COLONY-STIMULATING FACTOR; EPIDERMAL-GROWTH-FACTOR; SODIUM DODECYL-SULFATE; BOVINE SERUM-ALBUMIN; IN-VITRO BIOACTIVITY; POLYACRYLAMIDE-GEL-ELECTROPHORESIS; PERFORMANCE LIQUID-CHROMATOGRAPHY; POLYETHYLENE-GLYCOL CONJUGATION; LIVING RADICAL POLYMERIZATION;
D O I
10.3109/10837450.2010.513990
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Covalent attachment of poly(ethylene) glycol (PEG) groups to proteins, a process commonly called PEGylation, is often used to improve the performance of a protein in vivo. To date, at least eight such PEGylated peptide and protein conjugates have been approved as therapeutic agents and many more have undergone clinical trials. This review examines PEGylation from the perspective of developing a commercially viable drug product. The first section focuses on obtaining a pure and well-characterized drug substance. The latter section discusses formulation and manufacturing issues, with an emphasis on analytical methodology that provides the most detailed description of the purity and stability of PEGylated proteins.
引用
收藏
页码:423 / 440
页数:18
相关论文
共 245 条
[1]  
ABUCHOWSKI A, 1977, J BIOL CHEM, V252, P3582
[2]  
ABUCHOWSKI A, 1977, J BIOL CHEM, V252, P3578
[3]  
ABUCHOWSKI A, 1984, CANCER BIOCHEM BIOPH, V7, P175
[4]   Enhanced molecular volume of conservatively pegylated Hb:: (SP-PEG5K)6-HbA is non-hypertensive [J].
Acharya, SA ;
Friedman, JM ;
Manjula, BN ;
Intaglietta, M ;
Tsai, AG ;
Winslow, RM ;
Malavalli, A ;
Vandegriff, K ;
Smith, PK .
ARTIFICIAL CELLS BLOOD SUBSTITUTES AND BIOTECHNOLOGY, 2005, 33 (03) :239-255
[5]  
[Anonymous], 1992, POLY ETHYLENE GLYCOL
[6]   Polyethylene glycol-conjugated pharmaceutical proteins [J].
Bailon, P ;
Berthold, W .
PHARMACEUTICAL SCIENCE & TECHNOLOGY TODAY, 1998, 1 (08) :352-356
[7]   Rational design of a potent, long-lasting form of interferon:: A 40 kDa branched polyethylene glycol-conjugated interferon α-2a for the treatment of hepatitis C [J].
Bailon, P ;
Palleroni, A ;
Schaffer, CA ;
Spence, CL ;
Fung, WJ ;
Porter, JE ;
Ehrlich, GK ;
Pan, W ;
Xu, ZX ;
Modi, MW ;
Farid, A ;
Berthold, W .
BIOCONJUGATE CHEMISTRY, 2001, 12 (02) :195-202
[8]  
Bailon P, 2009, EXPERT OPIN DRUG DEL, V6, P1, DOI [10.1517/17425240802650568 , 10.1517/17425240802650568]
[9]   N-terminally PEGylated human interferon-β-1a with improved pharmacokinetic properties and in vivo efficacy in a melanoma angiogenesis model [J].
Baker, DP ;
Lin, EY ;
Lin, K ;
Pellegrini, M ;
Petter, RC ;
Chen, LL ;
Arduini, RM ;
Brickelmaier, M ;
Wen, DY ;
Hess, DM ;
Chen, LQ ;
Grant, D ;
Whitty, A ;
Gill, A ;
Lindner, DJ ;
Pepinsky, RB .
BIOCONJUGATE CHEMISTRY, 2006, 17 (01) :179-188
[10]   Site-specific PEGylation of protein disulfide bonds using a three-carbon bridge [J].
Balan, Sibu ;
Choi, Ji-won ;
Godwin, Antony ;
Teo, Ian ;
Laborde, Carlos M. ;
Heidelberger, Sibylle ;
Zloh, Mire ;
Shaunak, Sunil ;
Brocchini, Steve .
BIOCONJUGATE CHEMISTRY, 2007, 18 (01) :61-76
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